Professional Documents
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This book is served as an overview to General Paediatrics and specially tailored to UM`s teachings.
It integrates comprehensive information from various reliable sources (either lecturers` teachings,
seminar slides, standard textbooks or protocols). However, it would not be able to replace all
textbooks and students should still opt to refer standard textbooks for detailed understandings
and concepts. To those who have prior knowledge in Paediatrics, it will serve as a QuickReview for
revision purpose before final exam. Our team had tried our best to maintain the accuracy and
latest information within our capability. If there is any mistake or suggestion, please email us at
umpaedsfeedback@gmail.com.
Acknowledgement
We would like to acknowledge UPM for their old yet useful senior notes as our major inspiration
and references. Besides, this book follows essential concept and management listed in Paediatrics
Protocol as well. The compilation of this book is not possible without all references enlisted below
and we would express our gratitude and sincerely give a token of appreciation to each of them:
- Nelson Textbook of Pediatrics 20th Edition - WHO Pocketbook of Hospital Care for Children
- Nelson Essentials of Pediatrics 7th Edition - Netter`s Paediatrics
- Illustrated Textbook of Paediatrics 4th Edition - Netter`s Illustrated Human Pathology Updated Ed
- Easy Paediatrics - Handbook of Hospital Paediatrics 2005
- Examination Paediatrics 4th Edition - UM Paediatrics Lecturers
Jun Min, Em
Editorial Board:
Chief Editor : Em Jun Min
Co-Editors : Adrian Lim Jia Hwa Khoo Wan Thien Ooi Ying Shi
Audrey Lee Ying Shin Koay Zhong Lin Oon Chun Huat
Aun Yi Yang Koh Ee Yin (Audrey) Quek Ven Chin
Bryan Lee Yen Pei Kong Chen Xi Sherwin Johan Ng
Celia Low Fang Ying Kow Yun Shi Sia Jo Ee
Chan Pei Qi Lai Weng Wai Tan Bee Cher
Chan Xiao Min Leong Hui Ling Tan Hui Ting
Cheah Tian Phern Liew Hun Nee Tan Siang Lyn
Chen Chin Chern Lim Eng Seng Tay Tun Khong
Chew Ai Wie Low Qiong Cong Tee Wei Jie
Chian Xue Han New Ru Peng Teoh Yi Ming
Chuah Chun Wooi Ng Kar Aik Tung Yu Feng
Goh Saw Huan Ng Yun Hui Wong Hong Nang
Heng Kai Voon Ngio Yi Chen Yan Hui Xin
Hoh Wee Liam Ong Jin Xu See Toh Yiling (Yaslyn)
Jaclyn Tay Yi Ling Ooi Chieh Yin Yaw Mei Sim
Jasmine Low Chay Lee Ooi Sze Ting Yong Pei Yee
References
1. Ismail, Hussain Imam Hj Muhammad, Hoong Phak Ng, and Terrence Thomas. Paediatric
Protocols for Malaysian Hospitals. Ministry of Health, 2012.
2. Kliegman, Robert M. Nelson textbook of pediatrics. Saunders Elsevier, 2012.
3. Marcdante, K. J., & Kliegman, R. (2015). Nelson essentials of pediatrics (7th edition.).
Philadelphia: Elsevier/Saunders.
4. Lissauer, Tom, and Graham Clayden, eds. Illustrated textbook of paediatrics. Elsevier Health
Sciences, 2011.
5. Sidwell, Rachel U., and Mike A. Thomson, eds. Easy paediatrics. CRC Press, 2011.
6. Procopis, Peter G. Examination Paediatrics; A Guide to Paediatric Training. Journal of
Paediatrics and Child Health 43.4 (2007): 322-322.
7. World Health Organization. Pocket book of hospital care for children: guidelines for the
management of common illnesses with limited resources. 2013 Revised Edition. Available at:
http://whqlibdoc. who. int/publications/2005/9241546700. pdf. (2015).
8. Maconochie, I., Bingham, R., Eich, C., López-Herce, J., Rodríguez-Núnez, A., Rajka, T., &
Biarent, D. (2015). European resuscitation council guidelines for resuscitation 2015 section 6
Paediatric Life Support. Resuscitation, 95, 222-247
9. Florin, Todd, et al. Netter's Pediatrics. Elsevier Health Sciences, 2011.
10. Buja, M. L., & Krueger, G. R. F. (2013). Netter's Illustrated Human Pathology Updated Edition
(2nd ed.). London: Elsevier Health Sciences.
11. Lee W. S., Thong M. K., Wong C.P. Handbook of Hospital Paediatrics. 289 pages. 2005,
UniPress Publishing.
12. CPG for the Management of Childhood Asthma (p.20). (2014).
13. CPG for the Management of Transfusion-Dependent Thalassaemia (p.99). (2009)
14. CPG for the Management of Neonatal Jaundice (p.62). (2014)
Disclaimer
According to the Malaysia Copyright Act 1987 section 13(2) and TRIPS agreement, this book is
intended for non-profit, educational purpose in view of the use of illustrations, diagrams or
tables from acknowledged reference sources. The amount of copyrighted materials used in this
book is minimal and appropriate to achieve a non-profit transformative purpose in favour of fair
use. However, to avoid any deprivation of authors` rights for all the original sources being used
by this book, its use should only be confined for each individual without any other commercial
purpose. Therefore, students are advised to refer and purchase these original books enlisted in
the `References` section for a more detailed explanation or for browsing of the related contents.
All editors would not held responsibility for any unauthorised distribution of this book in which
fair use would no longer applicable with regards to the use of materials from original sources.
Table of Content
PART IV : CARDIOLOGY
- CONGENITAL HEART DISEASE 130
- RHEUMATIC FEVER 149
- INFECTIVE ENDOCARDITIS 155
- KAWASAKI`S DISEASE 160
PART V : RESPIRATORY
- COMMON RESPIRATORY INFECTIONS 163
- UPPER RESPIRATORY TRACT INFECTIONS (URTI) 165
- VIRAL CROUP 170
- ACUTE EPIGLOTTITIS 173
- ACUTE BRONCHIOLITIS 175
- BRONCHIAL ASTHMA 179
- PNEUMONIA 187
- PERTUSSIS (WHOOPING COUGH) 194
- CYSTIC FIBROSIS 196
- BRONCHOPULMONARY DYSPLASIA (BPD) 204
PART VI : GASTROENTEROLOGY
- ACUTE GASTROENTERITIS (AGE) 205
- DEHYDRATION & ELECTROLYTE IMBALANCES 212
- GASTROESOPHAGEAL REFLUX DISEASE (GERD) 217
- INFLAMMATORY BOWEL DISEASE (IBD) 219
- HIRSPRUNG DISEASE 228
- INTUSSUSCEPTION 230
- PYLORIC STENOSIS 232
- MALROTATION & VOLVULUS 233
- MECKEL`S DIVERTICULUM & MESENTERIC ADENITIS 234
PART XI : NEONATOLOGY
- CONGENITAL HYPOTHYROIDISM 344
- NEONATAL HEPATITIS SYNDROME 349
- NEONATAL JAUNDICE 353
- RESPIRATORY DISTRESS SYNDROME (RDS) 375
INDEX 402
PART I
CLINICAL PAEDIATRICS
Reference Ranges
Age Groups:
Neonates (≤ 28 days)
Infants (0-1 year old)
Toddlers (1-3 years old)
Pre-schooler (3-5 years old)
Grade-schooler (5-12 years old)
Adolescent (12-19 years old)
Young Adults (20-24 years old) * No longer considered Paediatric patient after 18 years old
Weight:
- First 7-10 days loses 10-15% body weight
- Regain birth weight by 7-10th day To calculate:
- First 3 months weight gain by 20-25 gm/day 1 - 9 years old : Wt (kg) = (Age + 4) x 2
- Double birth weight by 5 months 7 - 12 years old : Wt (kg) = Age x 3
- Triple birth weight by 1 year of age.
1
Tanner Pubertal Staging:
Male
1) Genitalia Development (G)
Stage I The testes, scrotal sac, and penis have a size and
proportion similar to those seen in early childhood.
Stage II There is enlargement of the scrotum and testes
and a change in the texture of the scrotal skin. The
scrotal skin may also be reddened, a finding not
obvious when viewed on a black and white
photograph.
Stage III Further growth of the penis has occurred, initially
in length, although with some increase in
circumference. There also is increased growth of
the testes and scrotum.
Stage IV The penis is significantly enlarged in length and
circumference, with further development of the
glans penis. The testes and scrotum continue to
enlarge, and there is distinct darkening of the
scrotal skin. This is difficult to evaluate on a black-
and-white photograph.
Stage V The genitalia are adult with regard to size and
shape.
2
Female
1) Breast Development (B)
3
Reporting Tanner Staging:
Male`s stage G(1-5), P(1-5), A(1-3) + Testicular volume (2-25 ml)
Female`s stage B(1-5), P(1-5), A(1-3) + Menarche
Puberty
Male
- Testicular enlargement (> 3mls Prader Orchidometer or > 2.5cm in longest diameter)
- Penile growth and pubic hair
- Growth spurt at P4 (testes at 10-12mls) at average 14 years [Late event]
- Growth completed when bone age is 16 years.
Female
- Breast development
- Growth spurt, B and P 2-3 (average 12 years) [Early event]
- Pubic hair and axillary hair
- Menarche: 13 years (10-14), Bone age 13 years, Tanner B & P3-4.
- After menarche little growth left (2-5cm)
- Growth completed when bone age is 14 years.
Guthrie`s Test
- Neonatal heel-prick screening for selective diseases.
- Mnenomics (Children Can Present More Seriously)
- Congenital hypothyroidism (TSH)
- Cystic fibrosis (Immunoreactive trypsinogen using dried blood)
- Phenylketonuria
- Maple Syrup Urine Disese (MSUD)
- Medium-Chain Acyl-CO-A Dehydrogenase Deficiency (MCADD)
- Sickle-cell anaemia
Fluid Requirement
Neonate
Day 1 : 60 mls/kg/day
Day 2 : 90 mls/kg/day
Day 3 : 120 mls/kg/day
Day 4 : 150 mls/kg/day (Same until 6th months)
6 months - 1 year : 120 mls/kg/day
After 1 year,
1st 10 kg : 100 mls/kg
2nd 10 kg : 50 mls/kg
Subsequent kgs : 20 mls/kg
4
History-Taking
Dr Revathi MD (USM), MPaeds (UM), Fellowship (Oncology)
Prof Surendran MD (UK), MB BCh BAO (UK), MRCPCH (UK), Fellowship (Respiratory)
Clean Hands
Introduce yourself
Informed consent & rapport
Biodata:
- Name, Gender, Age
- Date of Birth (DOB), Date of Admission (DOA)
- Informant like parents, caretakers, guardians (Reliability)
Presenting/Chief Complaint:
- Max 3 complaints, preferably only one complaint eg. Fever for 5 days prior to admission
5
Systemic Review: (To rule out)
- CVS - VSD/ASD, heart failure
- GIT – LOA/LOW, Jaundice
- CNS – Altered behaviour, seizure
- GUS (Genitourinary) – Increased frequency, Dysuria
Past-Medical History:
- Disease & Presentation
- Time of diagnosis, who diagnosed and where?
- Reason on previous admission
- Investigation done (What was done?)
- Treatment (compliance, control, complications) & Follow up
- Current status (well/poor controlled)
- Any planning surgery/procedure
6
- Not to be missed:
- Cyanotic heart disease & VSD/ASD
- Cystic fibrosis
- eg. Underlying history of VSD (heart failure) currently admitted for AGE
- PC focusing about AGE vomiting history (post-tussive), frequency
- eg. History of VSD (heat failure) admitted for respiratory distress
- PC: Difficulty in breathing HPOI: VSD history
- eg. Cerebral palsy child admitted with aspiration pneumonia, seizure, bed sore, electrolyte
imbalance prior to poor oral intake
- PC: Aspiration pneumonia & seizure HPOI: Cerebral palsy
Past-Surgical History:
- Important for VSD, cerebral palsy
- VP Shunt (hydrocephalus)
- Laparotomy (GI problems)
Paediatrics History:
- Antenatal
- Maternal medical conditions
- DM, HPT, Heart failure, Hyperthyroidism, Anemia-any supplement taken
- Infective screening (VRDL, HepB, HIV, CMV)
- Intrauterine growth restriction
- Symmetrical ht,wt, HC <3rd centile -> Occurs at 1st trimester (Microcephaly)
- Asymmetrical ht,wt <3rd centile; HC>3rd centile -> Occurs at 2nd/3rd trimester (PIH, GDM)
- Ultrasound findings, Blood group
- Intra-partum
- Delivery
- EMLSCS/ELSCS
- SVD (Any induction/ assisted delivery)
- When born? POG? Term or Preterm
- Baby weight LBW (1.5-2.5kg), VLBW (1-1.5kg), ELBW (<1kg)
- Apgar score (Ask whether baby cry/activity when born/ appear blue when born)
- Complications (Require resuscitation, Meconium-stained liquor)
- Post-partum
- Meconium Aspiration Syndrome (MAS)
- Ventilator, Duration, Oxygen supply, Complications like jaundice
- Neonatal Jaundice (NNJ) -> Kernicterus -> Cerebral palsy
- Pathological (<24hrs of life, >2 weeks of life - Persisted)
- Physiological (D2 to 2 weeks of life)
- Onset, Phototherapy, Exchange transfusion
- Baby blood group
- G6PD (From cord blood) – Cannot discharge until 5-10 days dt peak onset on 4-5 days
- Thyroid function (From cord blood) - Starts thyroxine treatment for hypothyroidism
within 2 weeks, if persists more than 1 month without treatment -> Mental retardation
7
Immunisation History:
- Details (Age, Dose, Duration, Follow immunisation chart, Complications)
- Completed immunisation (Up-to-date)
- eg. Baby at 4 months
- Baby has completed immunisation (up-to-date) by receiving BCG, HepB on birth, 2nd dose of
HepB on 1st month, 2nd dose of Hib, DPT, IPV on 2nd month, 3rd dose of Hib, DPT, IPV on 3rd
Month without any complications
- Possible complications (Local reaction, fever, rash, allergy, cellulitis/hematoma)
Family History:
- Draw Family tree
- Take note for any siblings presented with same problems
- Ask about consanguinity
Social History:
- Father/Mother occupation
- Income (any financial problem?)
- Housing area/environment/electric & water supply
- Smoking/alcohol history (parent & patient)
- Academic performance (Special school/Normal school)
- Exam result (Good/excellent/average/poor) eg. ranking, interested subjects
- Extracurricular activities (important for chronic diseases eg. asthma)
- Sibling rivalry (Sick attention, relationship/coping, low self-esteem/emotional status)
- Social (Interaction with friends, Hobbies, Acitivity limitation, Mobility support, Support group,
Caretaker - who spends most time with child?)
8
Diet History:
- Breastfeeding history (Exclusive for 6 months)
- Weaning diet (Semi-solid food >6 months)
- Current diet
- If on milk, how many Oz/scoop each time?
- Normal/balanced adult diet
- Malnutrition (Adjusted diet)
- Cystic fibrosis (No fatty foods)
- Failure to thrive (how often)
Drug History:
- Drug, frequency, compliance, complications/side effects (eg. Lipodystrophy, local infection)
- Who observes/supervises patient when taking medicine
Summary:
- Age, Gender, Chief complaint
- Associated significant aspects of history
eg. Assoc with global developmental delay or Incomplete immunisations
- Give provisional and differential diagnosis
9
Physical Examination (General)
Dr Revathi MD (USM), MPaeds (UM), Fellowship (Oncology)
1) Approach
2) Patient Consent
- Opportunistic (Depending on child coorperation)
3) Anthropometry chart/parameters
- Based on serial parameters on centile chart
- 3rd, 5th, 25th, 50th, 75th, 95th, 97th Centile (CDC)
- Below 3rd centile (CDC) = 2 SD below mean (WHO)
- 1 centile = 2/3 of an SD
- Height, Weight -> Plot up to 18 yrs old
- Head Circumference (HC) -> Plot up to 3 yrs old
- Female (Pink/Green), Male (Blue)
- Separate own charts for Down syndrome,Turner`s
syndrome, Achondroplasia, VLBW (<1.5kg)
- Reason for dropping in centile? Refer pg. 44
- Nutrition deficiency, family conflicts/neglect,
serious infections (eg. pneumonia, meningitis)
- Reason of dropping & crossing ≥2 centile?
- Failure to thrive FTT, malabsorption syndrome
* Malaysia doesn`t have own growth chart but using WHO ones
4) Vital Signs
- Blood Pressure, Pulse Rate, Respiratory Rate (Refer Reference Ranges)
- Temperature (same as adult) : 36.5 - 37.5`C
- Normal BP in neonates 60/40 – 50/30 mmHg (If 90/60 is hypertensive in neonates)
- Lowest acceptable normal SBP for 5th centile = (Age x 2) + 70 = ___ mmHg
- Appropriate cuff size (2/3 of arm) for adult, children, infant, neonate
- Smaller arm -> Hypertension (overestimate)
- Bigger arm -> Hypotension (underestimate)
- Change in BP is indicated in loss of fluid (kidney disease), septic shock, hypovolemic shock
- Plot on BP centile charts
Hypertension is defined as average SBP and/or DBP that is >95th percentile for gender, age & height on
at least 3 separate occasions. (Normal SBP & DBP is <90th percentile) -Handbook of Hospital Paediatrics
10
General Inspection:
- Appearance
- Color (poycythaemia/pallor/pink/cyanosis)
- Dysmorphic features
- Head (flat occiput/low set ears: >1/3 of ear is above line parallel to inner canthus/
skin tags/deformed pinna/hypertelorism: nasal bridge is more than single-eye diameter)
- Eye (cataract/squint/blue sclera/coloboma: hole in eye structures eg iris, retina, choroid,
optic disc/aniridia: no iris)
- Neck (web neck: excessive skin folds in Down/Turner`s syndrome)
- Skeletal deformity: syndactyly/polydactyly (webbed toes)/ bifid thumb/ absence thumb/
absence toe/Arachnodactyly/Ectrodactyly/Brachydactyly (clubbed thumb)/Acheiropodia/
Ectromelia (Phocomelia, Amelia, Hemimelia)/Arthrogryposis/ varus (club foot)/ Pigeon toe/
valgus (flat feet)/ Pes cavus/ Rocker bottom foot/ Hammer toe
- Skin changes: hypopigmentation/hyperpigmentation (café au lait spot): dt neurocutaneous
stigmata, inherited CNS disease eg. Sturge-weber syndrome (AD, Portwine stain),
Neurofibromatosis, Tuberous sclerosis
- Spine: Spina bifida
11
- Hand
- Finger clubbing, peripheral cyanosis, capillary refill time, koilonychia, leukonychia,
- Splinter haemorrhage, Osler`s node, Janeway lesions
- Dystrophic nails in Rheumatic heart disease
- Pulse (Rate, rhythm, volume, character)
- Forearm/Arm
- Birth marks, scratch marks, bruises
- Epitrochlear lymph nodes
- Eyes
- Scleral jaundice, conjunctival pink/pallor
- Oral cavity
- Dental hygience
- Hydration level (AGE, vomiting, diarrhoea)
- Glossitis (nutrition deficiency)
- Angular stomatitis (iron deficiency)
- Mouth ulcer
- Central cyanosis (respiratory & cardiac disease)
- Neck
- JVP/thyroid mass/lymph nodes (submental, submandibular, pre/post auricular, occipital,
anterior/posterior cervical, supraclavicular lymph nodes)
- Limbs
- Clubbing, dystrophic nails, oedema, deformity
- eg. CTEV (Congenital talipus quinovarus/club foot)
- Back
- Spina bifida, sacral oedema
12
Physical Examination (Cardiovascular System)
Dr Revathi MD (USM), MPaeds (UM), Fellowship (Oncology)
1) Approach
2) Patient Consent
- Opportunistic (Depending on child coorperation)
3) Positioning patient at 45’
4) Growth
- If Small for Age `I would like to confirm by plotting on the growth chart appropriate for the
age and gender`
Peripheral Examination
General Inspection:
- Activity
- Conscious level - Assess using modified Glasglow Coma Scale (GCS)
- Appearance
- Dysmorphic features
- Hand
- Finger clubbing, peripheral cyanosis, capillary refill time, koilonychia (if needed)
- Splinter haemorrhage, Osler`s node, Janeway lesions
- Dystrophic nails in Rheumatic heart disease, Palmar erythema
- Pulse (Rate, rhythm, volume, character)
- Forearm/Arm
- Birth marks, scratch marks, bruises
- Collapsing pulse (Aortic regurgitation, Patent Ductus Arteriosus, Hyperdynamic circulation)
- Radio-radial delay (Subclavian artery stenosis, Pre-ductal coarctation of aorta - Left UL delay)
- Radio-femoral delay (Post-ductal coarctation of aorta - Lower Limbs delay)
- Pulse volume (normal flow with reduced volume, not always delayed)
- Femoral pulse no delay but with coarctation? Aortic stenosis (pulse weaker)
- Blood pressure (hypotension/hypertension)
- 4 limbs BP (UL, LL): difference in blood pressure in UL, LL*
- Eyes
- Scleral jaundice, conjunctiva pallor
- Conjunctival polycythaemia (Hct very high)
- Congenital cyanotic heart disease - chronic hypoxia eg. Tetralogy of Fallot (ToF),
transposition of great arteries (TGA), trunchus arteriosus (problem with heart anatomy,
mixing of oxygenated and deoxygenated blood > body compensate by producing more RBC
- Acyanotic heart disease - L>R shunt in interventricular septum
- Eisenmenger syndrome : VSD (heart failure) > Pulmonary hypertension (R>L shunt)
- can be cyanotic and acyanotic heart disease
13
- Oral cavity
- Dental hygience, dental caries (Infective endocarditis), high-arch palate (Marfan`s syndrome),
angular stomatitis (iron deficiency), central cyanosis (respiratory & cardiac disease), hydration
- Neck
- JVP (examine only if more than 5 to 6 years)
- Lymph nodes (submental, submandibular, pre/post auricular, occipital, anterior/posterior
cervical, supraclavicular lymph nodes)
- Limbs
- Clubbing, dystrophic nails, oedema, deformity
- Right lateral thoracotomy
- Back - Modified BT shunt,
- Spina bifida, sacral oedema - Lung (lobectomy)
- Tracheosphageal fistula repair
CVS Examination - Left lateral thoracotomy
- Modified BT shunt
Precordium
- Coarctation repair
- Scar (Refer table beside)
- PDA ligation
- Chest asymmetry (Precordial buldge) - Pulmonary artery (PA) banding
- Chest deformity (Pectus excavatum, Pectus carinatum) - Lung (lobectomy)
- Whether patient is tachypnic (subcostal, intercostal, - Median sternotomy
suprasternal recession) - Any bypass surgery
- Calculate Respiratory Rate (RR) - Look for previous chest drain
- Any visible pulse (Apex beat pulsation) sites, mediastinal drain sites,
- Dilated veins pacemakers
- Pacemaker box (Bulging)
- Mechanical prosthetic heart valve (Audible clicking sounds)
Palpation
- Warm hands (normal apex beat for paeds at 4th intercostal space, midclavicular line)
- Both hands palpate for apex beat (Not miss out dextrocardia)
- Thrill (4 areas)
- Parasternal heave at left sternal edge (Right ventricular hypertrophy)
- Palpable P2 at pulmonary area (Pulmonary hypertension)
- Suprasternal notch thrill (AS - carotid radiation)
Ascultation
- Mitral, Tricuspid, Aortic, Pulmonary areas
- Murmurs (grade, systolic/diastolic, radiation, best heard, maneuvers-inspi/expiration) 6 grades
- Grade 3 Murmur heard, without thrill
- Grade 4 Murmur heard, with thrill
- Mitral regurgitation (not common in paediatrics, often older dt cardiomyopathy,incompetence,
infections, radiate to axilla)
- Ventricular septal defect (common in children, pansystolic murmurs, not radiate to axilla)
14
- Usually VSD will close by itself at age at 10 y/o, surgival intervention when too large > Heart
failure, pulmonary hypertension
- Mitral area (MR, VSD) common in paediatrics
- Tricuspid area (TR) rarely happen in children, mainly adult and IVDU (Infective endocarditis)
- Pulmonary areas (loud 2nd heart sound, any fixed 2nd heart sound – not alter by respiration or
posture)
- Listen murmur at the back
PS murmur – Ejection systolic murmur (mild), if severe might have no murmur
PDA murmur – Continuous murmur
Coarctation of aorta murmur
4 Cardinal Signs of Heart Failure:
Pulmonary atresia - No valve, no murmur
- Tachycardia
- Listen to lungs for bibasal crepitations
- Tachypnea
- Feel for pulsatile liver and hepatomegaly
- Cardiomegaly
- Back for deformity, scar and radiation
- Hepatomegaly
Describe heart sounds:
- First and second heart sounds dual rhythm, normal intensity (no loud 2nd heart sound or no
added sound), no murmurs
Arteriovenous shunt
- Right pulse weaker than left pulse (unlike coarctation whereby right stronger than left)
- Look for any scar (shunt) behind axillary region
- Shunt connecting subclavian artery to pulmonary artery to bypass pulmonary stenosis/atresia
- Volume is smaller in right pulse as it splits into half
- Shunt murmur can be heard during ascultation at the area, if absent indicate shunt blockage.
Tetralogy of Fallot:
- *Pulmonary stenosis (most severe) -> no blood flow to lung
- Overriding of aorta
- Right ventricular hypertrophy
- Ventricular septal defect
15
Physical Examination (Respiratory System)
Dr Revathi MD (USM), MPaeds (UM), Fellowship (Oncology)
1) Approach
Signs of Respiratory Distress:
2) Patient Consent
- Grunting
- Opportunistic (Depending on child coorperation) - Nasal flaring
3) Positioning (45` or Sitting position) - Tracheal tug
- Intercoastal/subcoastal/
Peripheral Examination supraclavicular recession
General Inspection - Head bobbing
- Alert, conscious - Tachypnoea
- Active to surrounding - Tachycardia
- Appearance (Cyanosis/pink) - Use of acessory muscle
- Lethargic
- On any oxygen or IV drip (not important in CVS, mainly for hydration, unless poor oral intake or
patient has polycythaemia, sluggish blood flow > stroke, dilute the blood by volume-volume
transfusion)
- Dysmorphic features
- Any audible sounds (stridor/ wheezing)
- Nasal flaring (in respiratory distress)
- Calculate Respiratory Rate (RR) tachynoea?
- Hand
- Finger clubbing (suppurative lung disease, chronic lung abscess, pneumonia)
- Palmar crease pallor
- Pulse (Rate, rhythm, volume, character)
- Bounding pulse in CO2 retention
- Forearm/Arm
- Blood pressure taking
- Visible scars
- Eyes
- Scleral jaundice, conjunctiva pallor
- Oral cavity
- Dental hydration, central cyanosis (respiratory & cardiac disease)
- Neck
- JVP (indicated only when more than 5 to 6 years)
- Lymph nodes (submental, submandibular, pre/post auricular, occipital, anterior/posterior
cervical, supraclavicular lymph nodes)
- Nasal polyps (end of examination)
- Limbs
- Clubbing (unlikely in lower limb)
- Skin infections (2` immunodeficiency eg. Kartagener syndrome, Cystic fibrosis, Gluten ds)
16
Chest Examination
Inspection
- Scar (Medial sternotomy, lateral thoracostomy, Chest drain for chest tubes)
- Chest asymmetry (Precordial buldge)
- Chest deformity (Pectus excavatum, Pectus carinatum)
- Whether patient is tachypnic (subcoastal, intercoastal, suprasternal recession)
Palpation
- Apex beat (needed if suspect for mediastinal shift)
- Tracheal deviation (5- 6 y/o)
- Chest expansion (above, upper and lower chest wall)
- Tactile fremitus
Percussion
- Supraclavicular, Intercostal spaces (comparing both sides)
- Hyperinflation of lungs when loss of:
- Liver dullness on percussion (Liver ptosis)
- Cardiac dullness on percussion
Ascultation
- Bell for supraclavicular, Diaphragm for all areas
- If very subtile then only request for deep inspiration
- Breath through the mouth
- `99` vocal fremitus
Back
- Hug pillow to avoid scapula occulding ascultation
- Ascultate for all lung areas (compare bilaterally)
- Breath through the mouth
- `99` vocal fremitus
End of examination,
- Observe any nebuliser attached to patient
- Sputum pot
- Aerochamber (chamber with mouthpiece, take 10 breaths), Inhaler (salbutamol) indicates
asthmatic patient)
- Creon (small tablets) - exogenous enzymes for pancreatic deficiency, indicates cystic fibrosis
17
Physical Examination (Gastrointestinal System)
Dr Revathi MD (USM), MPaeds (UM), Fellowship (Oncology)
1) Approach
2) Patient Consent
- Opportunistic (Depending on child coorperation)
3) Positioning patient lying flat with single pillow
4) Growth
`I would like to confirm by plotting on the growth chart appropriate for the age and gende`r
Peripheral Examination
General Inspection:
- Activity indicates severity
- Conscious level
- Appearance
- Dysmorphic features
- Nasogastric tube feeding (cannot swallow, have reflux, GI problem)
- Hand
- Finger clubbing (liver cirrhosis, IBD - UC, CD)
- Leuconychia, Muehrcke`s lines (chronic liver disease, hypoalbuminaemia)
- Koilonychia (iron deficiency)
- Palmar erythema (chronic liver disease, polycythaemia, thyrotoxicosis)
- Pallor (GI blood loss, malabsorption, chronic liver disease)
- Forearm/Arm
- Birth marks
- Bruises (clotting abnormalities)
- Petechiae (hypersplenism)
- Scratch marks (pruritus in cholestatic/obstructive jaundice -> conjugated bile pigments
deposition to skin; uraemia)
- Spider naevi
- Pulse (rate, rhythm, volume, character) -> anemia, tachycardia
- Blood pressure (hypotension/hypertension)
- Eyes
- Scleral jaundice, conjunctiva pallor
- Kayser-Fleischer rings (Wilson disease)
- Xanthelasma (cholestasis, hypercholesterolaemia, liver disease)
- Cataract (TORCHES, Intrauterine infections -> conjugated jaundice + cataract + microcephaly)
- Oral cavity
- Oral hygience & hydration
- Glossitis (Vitamin B12 deficiency)
- Aphthous ulcer (Crohn`s disease)
18
- Angular stomatitis (iron deficiency anaemia)
- Palatal petechiae
- Blisters (small hematoma)
- Neck
- Skin colours (Pale - haematological malignancy; Fair, shallow complexion - chronic renal
failure hyperpigmented - chronic renal failure, thalassaemia; Jaundice - liver problem
- Lymph nodes (submental, submandibular, pre/post auricular, occipital, anterior/posterior
cervical, supraclavicular, Virchow lymph nodes) *End of Examination unless suspect lymphoma
- Chest:
- Spider naevi (bigger children)
- Gynaecomastia (bigger children)
- Any loss of axillary hair
- Limbs
- Ankle edema (Protein malnutrition, protein-losing enteropathy, 3rd space water accumulation)
- Scratch marks
- Bruises
Abdominal Examination GIT problem might be in either:
Abdomen - Hepatobiliary
- Abdominal distention - Genitourinary
- Scars - Haematological
- Umbilicus inverted/everted - Endocrine (Cushing`s syndrome,
- Dilated veins adrenal gland)
Palpation
- 9 quadrants eg. local tenderness over which quadrant
- `Do you feel pain any where?` - Last quadrant to be palpated (inform examiner patient is pain)
- Superficial Palpation: Tenderness, soft/guarding/rebound tenderness
- `Look at patient whether crying/pain`
- Deep Palpation: (organs-hepatosplenomegaly, any masses)
- Describe mass (site, size, shape, mobility, consistency, surface/margin, tenderness,
discharge, any skin changes) eg. pancreatic mass, bowel mass, lipoma, ill-defined mass
- Palpate for liver (fix hand, deep expiration moves, inspiration palpate)
- Percuss upper border, midclavicular line from angle of Louis
- Liver measurement (Liver is enlarged, _ cm below subcoastal margin at midclavicular line)
- >2 cm palpable liver is significant in >2 years old child
- Differentiate hyperinflation of lung (liver ptosis) or hepatomegaly
- Avoid using fingerbreadth, unless state how many cm
Describe:
There is a mass palpable below the right subcoastal margin at the right hypochondriac region
which moves with respiration inferiorly, smooth surface, sharp margin, extending to epigastric
region, nodular(cirrhosis)/smooth surface, hard/firm in consistency, non-tender, dull on
percussion, upper border is at ___th intercoastal space, __cm enlarged below right subcoastal
margin, cannot get above it.
Normal liver span: Newborn (~4.5-5 cm), 12 years of age (6-6.5 cm for females and 7-8 cm for males).
In between these times there should be appropriate linear growth with the child.
Adult (8-12 cm; female is 8-10 cm while male is 10-12 cm)
19
Describe:
There is a mass palpable over right hypochondrium region which is round in shape, upper border
is palpable, measuring __ cm, tender/non-tender, firm in consistency, mobile/non-mobile (any
attached overlying structure)
Precocious puberty
Girls - Secondary sexual characteristics (breast & menses) developing < 8 years
- Menarche <10 years
- Mostly familial causes
Boys - Secondary sexual characteristics developing < 9 years
- Mostly pathological cause (congenital adrenal hyperplasia, intracranial
tumours, dysgerminomas
Pathologically,
If girls have menarche first before hair/breast development, must suspect for Ovarian CA.
Physiologically, boys will have adrenarche, usually have testicular enlargement first, then only
have pubic hair, axillary hair development and hoarseness of voice
Pathologically, if boys have moustache, axillary and pubic hair without testicular enlargement
- Testosterone is not produced by testis, but produced externally eg. malignancy, pituitary
changes
21
Physical Examination (Neurological System)
Dr Revathi MD (USM), MPaeds (UM), Fellowship (Oncology)
Dr Ang Hak Lee MD (UKM), MPaeds (UM), Fellowship (Cardiology)
1) Approach
2) Patient Consent
- Opportunistic (Depending on child`s coorperation)
3) Inspection (Mostly)
Peripheral Examination
General Inspection:
- Activity movement, floopy/active
- Conscious level
- Assess using modified Glasglow Coma Scale (GCS)
- Motor (6), Verbal (5) & Eye (4) Max 15/15 Min 3/15
- Appearance
- Color (poycythaemia/pallor/pink/cyanosis)
- Facial asymmetry, one-eye ptosis, drooling of saliva
- Dysmorphic features
- Microcephalic
- Macrocephalic (increase CSF, increased brain parenchyma or congenital malformation)
- Hydrocephalus (dilated ventricles, not necessary macrocephalic, can be microcephalic in
congenital toxoplasmosis associated with cerebellar atrophy + hydrocephalus)
- Environment
- External Ventricular Drainage (EVD) - hydrocephalus, draining of CSF
- Wheelchair/Clutches/Walking frame
Listen to instructions
1) Examine the lower limbs
- Stand, expose properly to upper thigh
- Start with gait examination (ask patient to walk to-and-fro)
- Scissoring gait (cerebral palsy)
- Waddling gait (proximal myopathy)
- High-stepping gait (footdrop,peroneal nerve palsy),
- Hemiplegic gait (stroke, ask patient to walk on lateral sides of feet (Fog`s test) if there is
subtle hemiplegic gait)
- Broad-base gait (cerebellar ataxia)
- Parkinsonian gait
22
- Stamping gait (proprioceptive disorders)
- Apraxic gait (hydrocephalus)
- Antalgic gait (pain with weight-bearing)
- Psychogenic gait
- Ask patient to run, if cannot see any gait
- Tandem gait (balance in one line, dorsal column problem)
- Romberg`s sign (dorsal column, if ataxia, fall when close the eyes; cerebellar will fall
with/without closing eyes)
- Gower`s sign (Ask patient to squat and stand, in proximal myopathy like Duchenne Muscular
Dystrophy (DMD), patient will use shin to climb)
- Look at patient`s back for any swelling over spinal region, tuft of hair or observable scars
- If patient cannot walk, ask patient to stand and slowly sit down (assess mobility)
- Lie down
- Inspection
- Leg posture (Hip)
- Normal posture: internally rotated & abducted
- Cerebral palsy,scissoring gait: externally rotated & adducted
- Knee (flexed/no)
- Any muscle wasting (most commonly affect vastus medialis)
- Any scars (eg. muscle biopsy scar, archilles tendon scar for
contracture)
- Any deformity (fracture, nail changes, shortening of leg)
- Any skin lesions (hypopigmentation/hyperpigmentation)
- Look for muscle fasciculations (tapping)
- LMN lesion
- Look for muscle tone (start from proximal, relax and test for range of motion)
- hypertonia/hypotonia
- Test for clonus (involuntary movement of ankle, >5 is significant)
- perform sudden flexion at the ankle
- Test for power
0 No movement
1 Flickering of toes
2 Move sideway, cannot move against gravity
3 Move against gravity
4 Move against gravity with resistance (less strong)
5 Can resist fully (strong)
- `Can u touch my hand with your toes?`
- Proximal muscle weakness (proximal power is about _/5)
- Distal muscle weakness (distal power is about _/5)
- Test for reflexes (knee, ankle, plantar reflexes - upgoing is UMN, downgoing is normal)
- Do Jendrassic maneuver if little movement
- Barbinski`s sign only elicit up to 1 month infant (unless persistent primitive reflex)
- Test for sensory dermatomes, ask patient to close eyes
23
- Head T2, Nipple T4, Umbilical T10.
- If lesion near T1-T2, patient will not be alive,
might be brain death
- Test for proprioception in dorsal column
- big toe up or down
- Examine the spine (if patient lying initially)
- spina bifida (LL paralysis, unable to walk)
- Palpate abdomen for
- Constipation (due to lower lumbar patho)
- Urinary incontenence (distended bladder)
- Look for any scars
- DDx for Hydrocephalus + Spina bifida:
- Arnold-chiari malformation
- Dandy-Walker syndrome
24
- Test for coordination (cerebellar sign)
- For both UL & LL
- Ask patient to walk (broad-base gait,
ataxia)
- Past-pointing (dysmetria)
- Dysdiadochokinesia
- Holmes Rebound phenomenon
- Pendulum knee jerk
- Heel-shin test
CN V (Trigeminal nerve)
- Motor
- Clench teeth, palpate masseter & temporal
25
- Close opened mouth, palpate medial pterygoid
- Sensory
- corneal reflex (both eyes blinking)
- facial sensation (3 divisions)
CN XI (Acessory nerve)
- Shrug shoulder to feel for trapezius
- Turn head against resistance for sternocleidomastoid
26
Localising signs (more significant in adolescent and adults):
Limbic Signs
- Loss or confusion of long-term memory prior to focal neuropathy (Retrograde amnesia)
- Inability to form new memories (Anterograde amnesia)
- Loss/reduced emotions (Apathy)
- Loss of olfactory functions, decision making ability
Cerebellar signs
- Unsteady and clumsy motion of the limbs or torso (Ataxia)
- Inability to coordinate fine motor activities (Intention tremor & Dysmethria)
- Inability to perform rapid alternating movements (Dysdiadochokinesia)
- Involuntary left-right eye movements (Nystagmus)
- Hypotonia, Dysarthria, Heel-shin test, Scanning/staccato speech
27
PART II
FUNDAMENTALS OF
PAEDIATRICS
Immunisation
Definition:
Vaccine Any suspension of antigen which is intended to produce protective immunity
in the host after administration.
Toxoid Modified biological toxin which is rendered non-toxic but maintains its ability
to provoke an immune response.
Adjuvant/Conjugate Compount linked to a vaccine to enhance the immune response in the host.
Most common eg aluminium salts
Live attenuated Live suspension of microorganisms which have been rendered non-virulent but
vaccine retain their infectivity (multiply) and immunogenicity (antigenic) in the hos.
They generally confer long-lasting immunity.
Attenuated strains that are almost or completely devoid of pathogenicity. They
multiply in host cells and induce antigenic stimulation
- Cellular immunity -> T-lymphocytes
- Adaptive immunity (humoral) -> B-lymphocytes -> Plasma cell -> Abs ->
Memory B & T cells -> Active immunisation -> Lifelong immunity
Killed vaccine Purified extracts from live organism which are incapable of replcation and
therefore non-infectious. They induced relatively short period of protective
immunity.
MOH Schedule
Age (Months) School years
0 1 2 3 5 6 9 10 12 18 4yrs 7yrs 13yrs 15yrs
BCG 1 *
Hep B 1 2 3
DTaP 1 2 3 B
IPV 1 2 3 B
Hib 1 2 3 B
Measles(Sabah)
MMR 1 2
JE(Sarawak) 1 2 3 4
HPV 3X*
DT B
TT
* For BCG, injection given at age of 7 if no scar.
3X* For HPV, 3 doses within 6 months (0,1, 6) at age of 13.
In UM, Pentaxim vaccine is given (DTPa-IPV + Hib) together
Mode of Administration:
- BCG (Intradermal), Others (IM/SC). All are killed vaccines except MMR, BCG, OPV (Polio).
- Many vaccines (inactivated or live) can be given together simultaneously (does not impair
antibody response or increase adverse effect). But they need to be given at different sites unless
given in combined preparation which avoid multiple injections to child. (eg. DTaP, IPV, Hib)
- Site of administration:
- Oral : (Rotavirus, Live typhoid vaccines)
- Intradermal (ID) : BCG, Left deltoid area (Proximal to insertion of deltoid muscle)
- Deep SC, IM injections : ALL vaccines except the above
- Anterolateral aspect of thigh : Preferred site in children
- Upper arm : Preferred site in adults
- Upper outer quadrant of buttock : Associated with lower antibody level production
28
Contraindications:
29
F) Special Contraindications
Footnotes:
1. For infants < 6 wks age, use Recommended Immunisation Schedule for Infants & Children.
2. Measles vaccine should be given only after 9 mths. (exception - given at 6 months in Sabah)
3. For special groups of children with no regular contact with Health Services and with no immunisation
records, BCG, HBV, DTaP- Hib-IPV and MMR can be given simultaneously at different sites at first
contact.
4. It is not necessary to restart a primary course of immunisation regardless of the period that has elapsed
since the last dose was given. Only the subsequent course that has been missed need be given. (eg. An
infant who has been given IPV1 and then 9 months later comes for follow-up, the IPV1 need not be
repeated. Go on to IPV2.). Only exception is Hepatitis A vaccine.
5. Vaccination programme changed in Oct 2008 from OPV (lived) to IPV (killed) as polio wild type
no longer endemic in Malaysia, preventing OPV S/E of paralytic disease.
6. Transplacental transfer of maternal Ig lasted in body around 6 months, avoid giving lived vaccine
except in Sabah for measles. For testing vertical transmission of infection, measure IgG only after 6
months.
7. At birth the immune system of baby is immature, pre-term baby is more prone to infection. At 36th
POG, maternal Ig will pass to fetus via placenta, level will be reduced by 4-6 weeks postnatally.
30
Possible Side Effects from Vaccination:
BCG - Local reaction: Papule at site of vaccination occurs within 2-6 weeks. This
grows and flattens with scaling and crusting. Occasionally a discharging ulcer
may occur. This heals leaving a BCG scar of ≥4 mm in successful vaccination.
- BCG adenitis may occur.
Hep B - Local reaction. Fever and flu-like symptoms in 1st 48 hours. Rarely erythema
multiforme or urticaria.
DPT - Local swelling and redness within 24-72 hours lasting 1-2 weeks.
- Acute encephalopathy (0-10.5/million)
- Shock and unusual shock-like state (3.5-250/100,000)
- Anaphylaxis (2/100,000 cases)
- Protracted crying (0.1-6%)
DT & T - Swelling, redness, pain.
- A small painless nodule at injection site (harmless).
- Transient fever, headache, malaise, rarely anaphylactic reaction.
- Neurological reactions rare.
OPV - Vaccine associated paralytic polio (VAPP)
IPV - No serious side effects have been documented, except local reaction.
- Indicated for children with severe immunocompromised conditions (eg. 1`
and 2` eg HIV, malignancy, organ transplant)
Measles - Transient rash in 5% cases.
- Fever between D5-D12 post vaccination lasting 1-3 days.
- URTI symptoms.
- Febrile convulsions (D6-D14)
- Encephalopathy within 30 days (1/100,000 cases)
- SSPE (1/1,000,000 cases) incidence of acquired infection is 6-22/1,000,000)
Mumps - Rarely transient rash, pruritus, purpura.
- Parotitis in 1% of vaccines, ≥3 weeks after vaccination.
- Orchitis and retrobulbar neuritis very rare.
- Meningoencephalitis is mild and rarely occur (1/800,000) natural infection is
1/400)
Rubella - May have rash, fever, lymphadenopathy, thrombocytopenia, transient
peripheral neuritis.
- Arthritis and arthalgia occurs in up to 3% children and 20% adults who
receive the vaccine.
- Rarely polyneuropathy (like GBS)
Hib - Local swelling, redness and pain soon after vaccination and last up to 24
hours in 10% of vaccines.
- Malaise, headache, fever, irritability, inconsolable crying. Very rarely seizure.
Special Circumstances:
31
B) Patient with past history or family history of febrile seizures, neurological or developmental
abnormalities that would predispose to febrile seizure:
- Febrile seizure may occur 5 to 10 days after measles (or MMR) vaccination or within the first 72
hours following pertussis immunisation.
- Give PCM (120mg or ¼ tablet) prophylaxis after immunisation (esp DPT) 4-6 hourly for 48 hours
regardless of whether the child is febrile.
- This reduces the incidence of high fever, fredfulness, crying, anorexia and local inflammation.
- Rectal diazepam may need to stand by for patient with previous febrile convulsions.
E) Children with Asplenia (elective or emergency splenectomy, asplenic syndrome, sickle cell
anaemia) are susceptible to encapsulated bacteria and malaria.
- Pneumococcal, Meningococcal A, C, Y & W-135, Haemophilus influenza B vaccine.
- For elective splenectomy/chemotherapy/radiotherapy: Give vaccine preferably ≥ 2 weeks
before procedure. However, they can be given even after the procedure.
- Penicillin prophylaxis should continue ideally for life. If not until 16 years old for children or 5
years post-splenectomy in adults.
F) Babies born to mothers who are HbsAg OR HbsAg positive should be given Hepatitis B Ig (200
IU) and vaccinated with the Hepatitis B vaccine within 12 - 48 hours. Given in different syringes
and at different sites.
G) Premature infants may be immunised at the same chronological age as term infants.
32
Developmental Assessment (DA)
Definition:
- Development is the progressive, orderly, acquisition of skills and abilities as a child grows. It is
influenced by genetic, neurological, physical, environmental and emotional factors.
- Main objectives:
- Assess the differing of child development potential by age
- Early detection of delay or abnormal development
- Provide therapy promptly
- Constitutes of 4 aspects (Gross motor, Fine motor, Speech/language, Social) + Primitive reflexes
Warning Signs:
- Discrepant head size or crossing centile lines (too large or too small)
- Persistence of primitive reflexes > 6 months.
- No response to environment or parent by 12 months
- Not walking by 18 months.
- No clear spoken words by 18 months.
- No 2 word sentences by 2 years.
- Problems with social interaction at 3 years.
- Congenital anomalies, odd facies.
- Any delay or failure to reach normal milestones.
* Parental concerns must always be taken seriously.
History
- Consanguinity
- Family history of developmental delay
33
- Maternal drugs, alcohol, illness and infection in pregnancy
- Prematurity, perinatal asphyxia
- Severe neonatal jaundice, hypoglycaemia or seizures
- Serious childhood infections, hospital admissions or trauma
- Home environment conditions (environmental deprivation)
Physical examination
- Head circumference, dysmorphic features
- Neurocutaneous markers
- Neurological abnormalities
- Full developmental assessment
Investigations
Consider:
(individualised according to history, physical
- Hypothyroidism
findings)
- Chromosomal anomaly
- Visual and auditory testing
- Cerebral palsy
- T4, TSH
- Congenital intrauterine infection
- Chromosomal Analysis
- Congenital brain malformations
- Consider
- IEM (Inborn errors of metabolism)
- Creatine kinase in boys
- Autistic spectrum disorder
- MRI Brain
- Attention deficit hyperactivity
- Metabolic screen
disorder (ADHD)
- Specific genetic studies
- Prior brain injury, brain infections
(Fragile X, Prader Willi or Angelman syndrome)
- Neurocutaneous disorders
- Refer to a geneticist
- Duchenne`s muscular dystrophy
- EEG if history of seizures
Management
- Formal hearing assessment
- Speech-language assessment and interventions
34
HearingTests at different ages
Age Test Comments
Newborn Automated Otoacoustic Determines cochlear function. Negative
screening Emission (OAE) test test in conductive hearing loss, middle ear
infections, or in moderate to severe
sensorineural hearing loss.
Any age Brainstem Auditory Evoked Measures brainstem responses to
Responses (BAER) sound. Negative test in sensorineural
hearing loss
7-9 months Distraction Test (DT) Determines response to sound whilst
presented during a visual distraction.
Infants Behavioural Observation Audiologist identifies bod- ily reactions to
Assessment (BOA) test sound, i.e. cessation of activity, body
movement, eye widening and opening
suckling rate.
> 2.5 years Conditioned Play Audiometry Earphones placed on child and various
games are done when test tone is heard.
Older Children Pure Tone Audiometry Patient presses a response button or
(~4 yrs old) raises a hand when the test tone is heard
35
- General : more commonly seen in children with some degree of intellectual impairment or from
an extremely understimulated environment
- Strength of the child perceived by parents and teachers
- Who is the main caregiver at home?
- Social background of the family
Review School concerns with the patient, parents & teachers (always ask for teachers report)
- Common symptoms
- Apathy towards school
- Avoidance or poor performance in specific subject areas
- Disruptive or negative behaviour in certain classes
Physical Examination
- Anthropometric measurement
- General alertness and response to surrounding (Children with dyslexia will be very alert and
usually very enterprising)
- Dysmorphism
- Look for neurocutaneous stigmata
- Complete CNS examination including hand eye coordination as children may have a associated
motor difficulties like dyspraxia
- Complete developmental assessment.
- Ask child to draw something he or she likes (this can help to get a clearer picture about intellect
of the child)
Block and Pencil test (From Parry TS: Modern Medicine, 1998)
Age Block Test Pencil Test
3 - 3.5 yrs Build a bridge Draw a circle O
3.5 - 4 yrs Draw a cross +
3 - 4.5 yrs Build a gate Draw a square
5 - 6 yrs Build steps Draw a triangle Δ
This test screens cognitive and perceptual development for age.
Block test: build the structure without child observing then ask the child to copy the structure.
Pencil test: Draw the object without child observing then ask the child to copy it.
36
Differential Diagnosis
Common Causes - Autism
- ADHD or combination of both
- Specific learning difficulty like dyslexia
- Limited environmental stimulation
Genetic/ chromosomal - Fragile X
disorder - Hypothyroidism
- Intellectual impairment
- Tourette
- Neurofibromatosis
Neurological - Seizures
- Neurodegenerative conditions
Miscellaneous - Anaemia
- Auditory or visual impairment
- Toxins (Fetal alcohol syndrome, prenatal cocaine
exposure, lead poisoning)
Investigations
Clinical impressions guides choice. Consider:
- DNA analysis for Fragile X syndrome for males with Intellectual impairment
- Genetic tests, e.g. Prader Willi, Angelman, DiGeorge, Williams syndromes
- Inborn errors of metabolism
- TSH if clinically indicated
- Creatine Kinase if clinically indicated
- MRI brain study abnormal neurological examination
- EEG only if clinically indicated
Global Developmental Delay (GDD)
- When a child has not reached two or more milestones in 4 domains of development
37
E) Primitive Reflexes
- Appear from birth and then lost as development progresses.
- High motor center will inhibit the reflexes in later life.
- Persistence beyond these age indicates failure of CNS maturation.
Asymmetrical Tonic It is activated as a result of turning the head to one side. As the head is
Neck Reflex (ATNR) turned, the ipsilateral arm and leg will extend while contralateral limbs
or Tonic labyrinthine will flex and bend, mimics a fencer. This reflex is inhibited by 6 months
reflex of agein the waking state. Its persistence beyond 8 to 9 months will
disable the baby to support the weight by straightening arms and
bringing knees beneath the body. Signs of retention include problem
with eye-hand coordination, crossing vertical midline, visual tracking.
Symmetrical Tonic It occurs with either the extension or flexion of the infant`s head.
Neck Reflex Extension of the head results in extension of arms and flexion of legs,
while flextion of head results in flextion of arms and extension of legs.
This reflex is inhibited by 6 months to enable crawling. Signs of retention
include tendency to slump while sitting, poor muscle tone, inability to sit
still and concentrate.
38
Barbinski or Plantar It is triggerd by stroking one side of the infant`s foot upwards from the
reflex heel and across the top of the foot. Infant responds by hyperextending
the toes, great toe flexes towards the top of the foot and the other toes
fan outwards. It generally inhibited 6-9 months postnatally.
Pupillary reflex It occurs with darkening the room and shining a pen-torch directly into
the neonate`s eyes for several seconds. The pupil should both constrict
equally. This reflex should not disappear.
Spinal Galant reflex It is stimulated by placing the infant on the stomach or lightly
supporting him or her under the abdomen with a hand and using a
fingernail, gently stroking one side of the neonate`s spinal column from
the head to the buttocks. The response is positive when neonate`s trunk
curving towards the stimulated side. This reflex can become inhibited
anytime between 3-9 months. Signs of retention include fidgeting,
bedwetting, poor concentration or short term memory, unilateral or
bilateral posture issues.
Doll`s eye reflex It is noted with infant in supine position, slowly turning the head to
either side. The infant`s eye will remain stationary. This reflex should
disappear between 3-4 months.
Prone-crawl reflex It can be stimulated by placing the neonate in prone (face down) on a
flat surface. The neonate will attempt to crawl forward using the arms
and legs. This reflex will be inhibtied by 3-4 months.
Swimming reflex It is stimulated when placing neonate face down in water, the neonate
will make corrdinated swimming movements. This reflex should
disappear at 6-7 months.
Landau reflex It is seen in horizontal suspension with the head, leg and spine
extended. If the head is flexed, hip, knees and elbows will also flex. It
appears about 4 to 5 months, disappear at 1 year old. Absence of this
reflex can occur in hypotonia, hypertonia or mental abnormality.
Parachute reflex It appears around 6-9 months and persist to adulthood. It is elicited by
holding the child in ventral suspension and suddenly lowering to the
couch, infant will react by extension of arms as defensive reaction. It will
be absent or abnormal in CP, asymmetrical in spastic hemiplegia.
Blinking reflex It is stimulated by momentarily shining a bright light directly into the
neonate`s eyes causing him or her to blink. It should not be inhibited.
Cough, Gag, Sneeze, These reflexes should not be inhibited but persisted into adulthood.
Yawn reflexes
39
Gross Motor Fine Motor
Age Descriptions Age Descriptions
6 weeks - Head lag, rounded back, head same plane as 6 weeks - Fix, focus and follow object to 90’
body (Pull to sit) - Follow object to 180` (Past midline)
- Raised chin, high pelvic, knees below abdomen 3 months - Hand grasp object loosely, not
(Ventral suspension) reaching out
3 months - Slight head lag, head above body - Reach for toy
5 months
- Good head control, head lift 45-90’ - No squint
- Pull self up - Palmar grasp (ulnar) of cube
6 months
4 months - Roll from Prone to Supine - Move head, eyes in all direction
5 months - Roll from Supine to Prone 7 months - Transfer object
- No head lag, sit straight back 9 months - Inferior pincer grasp (scissor grasp)
6 months - Sit with support, bear weight on legs, - Neat pincer grasp
support with hands 1 year old - Bang 2 cubes
7 - 8 months - Commander crawl (Creeping) - Tower of 2
9 months - Pull self to sit, sit steadily - Tripod grip
- Stand with support/holding - Flip page one by one
- Lean forward without pivot 1.5 year old - Scribbles spontaneously
- Visual test (Pie chart)
10 months - Pull self to stand - Tower of 3
11 months - Walk with both hand held - Imitates train cube without chimney
1 year old - LSCS (Lie, Sit, Crawl, Stand) 2 years old - Copies straight line
- Walk like a bear (one hand held) - Tower of 6
- Stand alone well - Hold pencil well
1.5 year old - Up & down stairs with one hand held - Imitates train cube with chimney
- Throw ball without falling 2.5 years old
- Copies straight lines - |
- Sit on chair - Tower of 8
2 years old - Up & down stairs (2 feet/step) - Imitates bridge cube of 3
- Walk backwards 3 years old - Copies circle
- Kick ball without falling - Tower of 9
2.5 years old - Jump on both feet - Copies square and plus
4 years old
- Walk on tip toes - Goodenough test 4
3 years old - Pedal tricycle - Copies cross and triangle
5 years old
- Up (1/step) & down (2/step) stairs - Goodenough test 8
- Stand on one foot for seconds - Copies diamond and complex square
4 years old - Up & down stairs (1 foot/step) 6 years old - Goodenough test 12
- Skip/hop on one foot - Tower of 10
5 years old - Skip on both feet
- Run on toes Speech/ Language
6 years old - Heel to toe walk
- Kick, run, climb Age Descriptions
6 weeks - Quiet & startle to sound
Social 8 weeks - Vocalising
Age Descriptions
- Squel with delight
6 weeks - Smile responsively 3 months
- Turn head around (ear level)
3 months - Social smile (Smile spontaneously)
- Babbling with single syllable
- Resist toy pull, smile at itself in mirror 6 months
5 months - Distraction test
- Mouthing
8 months - Babbling with combined syllable
9 months - Stranger anxiety
9 months - Localising sound above,below ear 1m
- Play `peek-a-boo’
- Understand phases
- Feed with spoon occasionally
1 year old - 2-3 words with meaning-papa,mama
- Understand `NO’
- Localising sound above head
1 year old - Casting & follow object
- Recognize >5 words, Picture card -1
- Drink, feed with cup, spoon but spills 1.5 year old
- Point 2-3 body parts
- Play ball with examiner
- Join 2-3 words into sentence
- Clap hands
2 years old - Point 4 body parts, Picture card - 3
- Toilet-trained
- Obey 4 simple commands
1.5 year old - Imitate housework
- Know full name & sex
- Drink & feed with cup and spoon 2.5 years old
- Name one colour
- Dry by day (put on shoes,socks,pant)
2 years old - Count to 10, form sentences
- Play near children 3 years old
- Name two colours, Nursery rhymes
- Unbutton, dress, undress with help
- Fluent conversation, ask questions
- Dry by night 4 years old
3 years old - Name three colours, A-Z
- Play with other children
- Know AGE, Fluent speech
- Parallel/interactive play
- Name four colours
- Buttons clothes fully 5 years old
4 years old - Triple order preposition
- Attend own toilet needs
- Tell time
- Dress/undress alone
5 years old
- Tie shoelaces
40
DENVER DEVELOPMENTAL SCREENING TOOL II (Malaysia Modified version)
Generally, Malaysian and Denver children appear to be similar in their development during first six years of life except for some minor differences in the
personal-social, language and gross motor sectors. Malaysians appear to be slower in self-care but more advanced in "helping around the house", "playing
interactive games" and in "separating from mother". They were slightly slower in gross motor function during first year of life but more advanced during the
second year of life. They were also slightly more advanced in language development. Differences can partly be explained by differences in socio-economic or
cultural differences or genetic factors between these two groups of children.
41
Denver`s Guide on Performing Developmental Assessment
42
Information needed during history taking of a child with suspected developmental disabilities:
43
Physical findings of a child with suspected developmental disabilities:
44
Failure to Thrive (FTT)
Definition:
- Reduction by ≥2 centiles on the weight and height plotted on growth chart.
- Growth parameters are persistently below 3rd centile.
- For WHO chart: <2 standard deviation (SD) below the mean for age
- It is a sign that describes underlying problem but NOT a diagnosis
- Rate of growth is significantly lower than that of other children of similar age and gender.
- Suboptimal weight gain or growth in infants or toddlers
Growth Chart:
- Ideally should be recorded from birth till 18 years old (weight, height) or 3 years old (HC)
- 3rd centile is the lower limit of normality (3% of normal children fall within this limit)
- Single plot is insufficient to interpret as FTT (can comment underweight) unless
- Markedly below 3rd centile
- Markedly discrepant from HC/ length
- Repeated observations are important to identify problems where change in weight is
compared with change in HD/ length
- Special chart needed for Down synrome, Turner syndrome
- Weight over 85th centile is considered overweight while over 97th centile is considered obese.
- Premature infants are plotted as `Corrected` age using the formula:
Corrected age = Gestational age - Number of weeks of prematurity (40 weeks POG as baseline)
- For example, 4 months baby (gestational age) born at 32th weeks POG (8 weeks from 40th
weeks) will have corrected age of 2 months (8 weeks).
- Corrected age is not required when
- Infant born at 36th weeks of POG onwards (not considered premature)
- Baby reaches 2 years old and should be plotted normally like any other child.
Specific Growth Patterns Requiring Further Evaluation:
Pattern Representative Diagnoses to Further Evaluation
Consider
Weight, length, HC all - Familiai short stature - Midparental heights
<5th percentile - Constitutional short stature - Evaluation of pubertal
- Intrauterine insult development
- Genetic abnormality - Examination of prenatal records
- Chromosomal analysis
45
Aetiology:
Organic Non-organic
- Inadequate food intake - Inadequate food intake
- Inability to feed - Feeding problems
- Mechanical problem (eg. cleft palate) - Insufficient breast milk
- Lack of coordination (eg. cerebral palsy) - Poor breastfeeding technique
- Vomiting - Incorrect infant formula preparation
- GERD, pyloric stenosis - Insufficient food offered
- Chronic diseases causing anorexia - Lack of regular feeding time
- Respi (cystic fibrosis, asthma) - Infant hard to feed (resist
- CVS (congenital heard disease) feeding/disinterested)
- GIT (malabsorption, D, V, Crohn`s disease)
- Renal (UTI, CRF, Renal tubular acidosis) - Environmental deprivation
- Malignancy - Socioeconomic
- Low income
- Diminished food absorption - Poor education
- Protracted diarrhoea - Poor social support
- Short bowel synrome (post-operation) - Family dysfunction
- Small intestinal disease (Celiac disease) - Marital discord/ single parent
- Pancreatic disease (cystic fibrosis) - Maternal mental illness
- Post-necrotising enterocolitis - Alcohol/ drug abuse
- Child abuse/ neglect
- Protein-losing enteropathy
- Intestinal lymphangiectasia
- Milk protein intolerance (prolonged AGE)
- Inflammatory bowel disease (IBD)
- Metabolic
- Hypothyroidism
- Congenital adrenal hyperplasia (CAH)
- Amino acid & organic acid disorders
- Miscellaneous
- Chromosomal disorders (Down, Noonan,
Turner syndrome)
- Congenital infections
46
Clinical features:
Symptoms Signs
- Global developmental delay - Malabsorption
- Gross & fine motor skills - Respiratory
- Mental & social skills - CVS
- Delayed secondary sexual maturation - Neurological
(adolescent stage) - GIT (abdominal distention)
- Constipation (Poor feeding) - Renal (UTI, RTA, CRF - anaemia, sallow)
- Excessive sleepiness (Lethargy) - Physical abuse (eg. Bruises)
- Irritability - Dysmorphic features (underlying syndrome)
- Enlarged tonsils (OSA can lead to FTT)
History:
Birth History Intrauterine insults (IUGR), Prematurity, Birth weight, Infective
screening, Exposure toharmful agents (smoking, alcohol)
Past-Medical History Frequency of acute/chronic illness, Past-hospitalisations,
Previous medical conditions
Feeding History Quantity of milk consumed, Feed preparation, Weaning (when,
what & quantity), Dietary recall and diary
Family History Maternal & paternal height, Growth of other family members &
any illness in family (familial short stature)
Detailed Social History Parental( depression, marital disharmony, substance abuse,
unemployment, poverty) Food insecurity/shortage, Living
condition, Psychosocial problem, Abuse, Neglect
Physical Examination:
- Anthropometric (weight, height, HC - small for age; mid-arm circumference for skeletal muscle
mass; triceps skin-fold thickness for subcutaneous fat storage)
- Evidence of neglected hygiene (eg. diaper rash, unwashed skin, overgrown and dirty nails or
dirty clothing) or signs of non-accidental injury (NAI) or abuse (scars, bruises, ecchymoses)
- Dymorphic features, poor eye contact, lack of facial expression, absence of cuddling response
- Vital signs: hypotension(adrenal/thyroid insufficiency), hypertension(renal disease),
tachycardia/tachypnoea(increased metabolic demand)
- HEENT: Chronic otitis media(structural oro-facial defect), Cataracts(congenital rubella
syndrome, galactosemia), aphthous stomatitis(Crohn`s disease), Thyroid enlargement(hypoT)
- GI: Finger clubbing (Crohn`s disease), Leukonychia (hypoalbuminaemia), Rectum(empty
ampulla for Hirschsprung`s disease)
- Respi: wheezing (CF, asthma)
- CVS: murmur (congenital heart disease)
- Neuro: abnormal deep tendon reflex(CP), dysphagia(CN palsy)
- Uro: diaper rash (diarrhoea, neglect)
- Skin: Pallor(anaemia), Candidiasis(immunodeficiency), Eczema(allergy), Erythema nodosum
(ulcerative colitis, vasculitis)
- Behavioral: Uncooperative (difficult to feed)
47
Investigations:
Blood - FBC
- Anaemia (chronic disease, iron-deficiency, vitamin B12)
- Infections
- Inflammation & immune deficiency
- BUSE + creatinine (renal failure, RTA, metabolic disorders)
- VBG (for RTA - normal anion gap metabolic acidosis)
- LFT (liver disease, malabsorption, metabolic disorders) *ALP↑ osteoclastic activity
- TFT (hypothyroidism)
- Immunoglobulins (immunodeficiency)
- Anti-endomysial, anti-gliadin antibodies (celiac disease)
Urine - U-FEME + C&S (UTI, renal disease)
*Congo red stain for fat gobules under microscopy
Stool - Ova + cysts (worms/ parasitic infections)
- Faecal elastase (pancreatic insufficiency)
Karyotyping - Turner syndrome (short stature)
Management:
- Correction of underlying aetiology (if possible)
- Enteral or Parenteral feeding, follow up patient and monitor growth chart
- For patient with severe malnutrition, resuscitation protocol is indicated.
48
E) If child deteriorates (RR +5/min or PR +25bpm or fails to improve with IV/IO fluid)
- Stop infusion as this can worsen child`s condition
- Discuss case with Paediatrician immediately and referral
C) Monitoring
- Avoid causing heart failure
- Suspect if: sustained increase (>2 hrs) of respiratory rate (increases by 5/min), and/or
heart rate by 25/min from baseline.
- If present: reduce feed to 100ml/kg/day for 24 hr then slowly increase as follows:
-15ml/kg/day for next 24 hrs; then 130ml/kg/day for next 48 hrs.
- Then increase each day by 10 mls.
- Ensure adequate weight gain
- Weigh child every morning before feeds; ideal weight gain is > 10g/kg/day
- If poor weight gain < 5g/kg/day do a full reassessment
- If moderate weight gain (5-10g/kg/day) check intake or check for infection
- Watch for secondary infection
E) Discharge criteria
- Not oedematous.
- Gaining weight well.
- Afebrile.
- Has completed antibiotics.
- Aged ≥ 12 mths (*<12 mths: A Specialist opinion is required before discharge).
49
Infant Feeding
A) Breast-Feeding
Dr Koe Swee Lee MD(NUS), MMed(NUS), MRCP(Edinburgh), IBCLC(Queensland)
Prof. Dr. Lucy Lum Chai See, MBBS(UM), MRCP(UK)
Advantages:
Baby Mother
- Provide ideal nutrition for infants during 4-6 - Free of charge (saves medical expenses)
months of life - Promotes close attachment btw mother-child
- Easily digest, optimal temperature, less allergy - Natural contraception (lactational amenorrhoea)
- Reduce GI infections (developing country), - Not fully reliable but effectiveness increase with
Necrotising enterocolitis (preterm infants) time interval between children
- Improve cognitive development (dt presence of - Important in reducing birth rate in developing
polyunsaturated long chain fatty acids, takes part countries (family planning)
in myelination) - Reduce post-partum haemorrhage (PPH) during
- Foster maternal-infant bonding rooming-in, stimulates oxytocin production
- Reduce indicence of IDDM, obesity, IBD, STD, - Reduce risks of pre-menopausal breast cancer,
pneumonia, otitis media, meningitis osteoporosis
- Enhance visual acuity, IQ, speech development
50
Disadvantages:
Intake Unknown volume of milk intake (under or over-concentration)
Infections Transmission of CMV, hepatitis & HIV from infected mother
Breastmilk Jaundice Unconjugated hyperbilirubinaemia due to:
- Increased enterohepatic circulation (increased brush border B-
glucuronidase deconjugation activity and reabsorption)
- Pregnanediol in breastmilk inhibit glucuronyl transferase reducing
conjugation and reduce excretion of conjugated bilirubin.
- Mild, self-limiting (NOT an indication to stop breastfeeding)
Drug transmission Transmission of drugs from maternal blood (eg. anti-thyroid, cathartics,
anti-metabolites)
Nutrient Prolonged exclusively breastfeeding > 6 months of age, leading to poot
weight gain, nutritional deficiency (eg. rickets)
Vitamin K deficiency (insufficient vit K to prevent haemorrhagic disease
of newborn)
Contamination Environmental contaminants (eg. nicotine, alcohol, caffeine etc)
Less flexibility Other family members unable to take part unless expressed breastmilk
Emotion Emotional upset if unsuccessful
Guidelines on Breastfeeding:
- WHO recommends exclusive breastfeeding for 6 months then continue breastfeeding to 2
years and beyond with addition of complementary food (weaning).
- First step: Facilitate breastfeeding in first hour (latest by fourth hours)
- Baby takes 40-50 minutes to latch naturally on nipple
- Rooming-in provides skin-skin contact, keeps baby warm
- Receive colostrm (produced for first few days, low volume, more concentrated, higher protein
and immunoglobulin content as compared to mature mlik) -> Baby is rotected from flora
acquired from mother
- Second step: Feed frequently (1-2 hourly during day, 3 hourly during night)
- Third step: Feed properly
- Position (chest-to-chest contact with baby lies on side, direct mouth-to-nipple not opposite)
- Cradle position, Cross-cradle position
- Latching (infant latches on mother`s nipple and much of the areola, stimulate upper lip,
mouth wide opens)
- Practice
- Chin against breast makes deep suckling movement and swallowing to be heard
- Do not pull baby off breast while still feeding, feed till baby sleeps and let go
- Offer the breast again till baby is satisfied, feed 1 feed on 1 breast
- No limit in duration and frequency of breastfeeding, must satisfy baby`s suckling needs
- Colostrum
- Thick, yellowish milk secreted for first 5-7 days (small amount during first few days due to high
progestrogen which inhibits prolactin from stimulating milk production)
- Ideal nutrient and immunological substances Constituent Colostrum Mature
- Volume of colostrum: Remarks: /100ml Milk
Day 1: 50ml/day Lactose prevents Energy [K cal] 58.0 70.0
Day 2: 100ml/day hypoglycaemia, facilitates Lactose [g] 5.3 7.0
passage of meconium and Protein [g] 2.3 0.9
Day 3: 135ml/day
excretion of bilirubin Fat [g] 2.9 4.2
51
- Mother produces less breastmilk because of poor breastfeeding practice:
- Lack of information and family support
- Limited breastfeeds in frequency and duration
- Switch breastfeeding, Given bottle feeds and water with breastfeeding
- Baby given pacifiers or not given night breastfeeds
- Symptoms when baby has enough breast milk:
- Passing pale urine 5-6 times/day
- Passing yellow stools 3-8 times/day
- Baby is contented about 1 hour after a feed
- Baby puts on at least 20g/day
- Differences between:
Breastfeeding Jaundice Breastmilk Jaundice
- Suboptimal breastfeeding - Prolonged jaundice for 6-8 weeks
- Baby does not get enough breast milk and - increased brush border B-glucuronidase
calories deconjugation activity and reabsorption)
- Jaundice of starvation - Pregnanediol in breastmilk inhibit
- Reabsorption of unconjugates bilirubin glucuronyl transferase reducing
- Management: Correct breastfeed practice, conjugation and reduce excretion of
increase feeding frquency and duration conjugated bilirubin.
- Normal development
- Management: Continue breastfeeding
- Contraindications to breastfeeding:
- Mother is HIV positive
- Mother is being treated for cancer soon after delivery
- Mother is on radioactive drugs for any treatment or investigation
- Maternal conditions (acute infections, septicaemia, ecampsia, nephritis, profuse haemorrhage,
active TB, leprosy, typhoid fever, breast cancer, malaria, chronic poor nutrition, cardiac failure,
substance abuse, inverted nipples, fissuring or cracking of nipples, lactational mastitis)
- Infantile conditions (metabolic disease like galactossaemia, phenylketonuria)
- Non-contraindications to breastfeeding:
- Children is ill with respiratory infections or diarrhoea and is on medications
- Mother is ill with infections and other illnesses
- On other medications (most drugs are compatible with breastfeeding)
B) Formula Feeding
- WHO & MOH recommend formula feeding if the conditions are AFASS (Affordable, Feasible,
Acceptable, Sustainable, Safe)
- Unmodified formula milk (unsuitable for infancy feeding as it contains too much protein and
electrolyte but inadequate iron and vitamins)
- Modified formula milk (Casein: Whey ratio = 40: 60, similar to breastmilk which forms smaller
curd and provides similar amino acid profile)
- Raw milk (unsuitable for infants before 6 months, easily contaminated, form large milk curd,
difficult to digest)
- Pasteurised milk (may contain high bacterial count, should be boiled before consumption)
- Condensed milk (added with cane sugar, 60% carbohydrate, unsuitable for infants)
- Dried skim milk (high mineral and protein content, may cause severe dehydration, unsuitable
for infants)
52
C) Pasturised Cow`s Milk (eg. Dumex)
- Higher casein (Casein: Whey ratio = 63: 37), which is more difficult to digest
- Higher in Ca, Na, PO4 (increased renal solute load)
- Deficient in Vitamin A, C, D and iron
D) Goat`s milk
- Used in cow`s milk allergy, low in vitamin D, iron and folic acid
- Susceptible to megaloblastic anaemia, brucellosis (boiled before use)
Weaning
- Introduction of solid food which is ideally done between the age of 4 to 6 months.
- After 6 months of age, breast milk becomes nutritionally inadequate as a sole feed, leading to
deficiencies in energy(increased calorie demand), vitamins and iron
- Breastmilk still essential during weaning, encourage as long as possible.
- New food should be offered once a day in a small amount: 1-2 tablespoon(s)
- Use small spoon that fits infant`s mouth, anticipate `spitting out`
- Use same food for 1-2 week until infant is used to the food before introducing new food
- Avoid overzealous, infantile obesity
- Suitable foods: cereals, fruits, vegetabl, eggs, home-prepared food.
- Feeding difficulties during first year of life:
- Underfeeding: restless, hungry, failure to gain weight
- Overfeeding: regurgitation, vomiting, infantile and adult obesity
- Regurgitation and vomiting (common in first few months, usually self-limiting)
- Loose or diarrhoeal stools, Constipation(rare in breastfed infants)
53
Malnutrition
- Categorised into short-term response of wasting (weight for height ratios) and long-term
response of stunting (height for age, sex ratio) [weight for age ratio cannot differentiate short or long term]
Nutritional Assessment:
- Dietary history
- Food intake as recalled by parents or recorded ina diary over several days
- Food quantity, preparation, frequency, budget limitation
- Physical Examination
- Anthropometry
- Height (stunted growth in chronic malnutrition)
- Weight (reduced weight with normal height(wasting) indicates acute malnutrition)
- Mid-arm circumference (indication of skeletal muscle mass, <115mm: severe malnutrition)
- Triceps skin-fold thickness (measurement of subcutaneous fat stores)
- Physical signs (Refer pg.52)
- Investigations:
- Serum albumin (nutritional status, reduced in severe malnutrition)
- FBC (low Hb, lymphocyte count)
- Blood glucose
- Serum calcium, phosphate, vitamin D, potassium, magnesium
- Serum B12, folate, iron, ferritin; Schilling test - to differentiate causes of vit B12 deficiency
- Radiology (wrist X-ray)
54
Physical Signs of Nutritional Deficiency Disorders:
Protein-energy Malnutrition:
Marasmus Kwashiorkor
- Deficiency of both protein and calories, results in - Disproportionately low protein intake compared
non-oedematous malnutrition with calorie intake, oedematous malnutrition
- Decreased weight for age & sex ratio (<60% mean) - Near-normal weight for age & sex ratio (<80%)
- Appears loose, wrinkled skin, `old man` wizened, - Appears oedematous, hypoalbuminaemic, overall
decreased skin turgor `fatness`, moon face, lethargic, miserable, LOA
- Muscle atrophy and little subcutaneous fat - Marked muscle atrophy but spared subcutanous fat
(reduced mid-arm circumference, skinfold thickness)
- Thin, sparse, easily pull out hair, hair colour unusual - Thin, red hair and darkened skin (hyperpigmented
changes hyperkeratosis), erythematous macular rash
(pellagroid),`Flaky-paint` rash, angular cheilosis,
monilial stomatitis, fissures, ulcers), parotid gland
enlargement, hepatomegaly
- Hypothermia, bradycardia, hypotension (reduced - Precipitated by infections, secondary
metabolic rate) immunodeficiency
55
Mixed Maramus-Kwashiorkor
- Concurrent wasting and oedema with stunting
- Weight for age & sex ratio (<60%) + Oedema
- Features: dermatitis, neurological abnomalities, fatty liver
Management
- Nutritional rehabilitation should be initiated and advanced slowly to minimize complications:
- Enteral nutrition (Preferred whenever possible, via GI tract, nasogastic or gastostomy tube)
- Parenteral nutrition (Directly into circulation)
- Antibiotics or antiparasites if indicated
- Oral rehydration over IV fluid is recommended to avoid excessive fluid, solute load and
resultant heart/ renal failure.
- Calorie intake is increased till appropriate regrowth or catch-up growth is initiated.
- Refers to gaining weight > 50th percentile for age and may require ≥150% calories than well-
nourished child
- General rule of thumb for infants and children ≤3 years age: Provide 100-120 kcal/kg based on
ideal weight for height
- Complication: Refeeding Syndrome
- Characterized by fluid retention, hypophosphatemia, hypomagnesemia, hypokalemia.
56
Micronutrients Deficiency
Overview:
Vitamin Clinical Condition in Deficiency Source
Vitamin A - Night blindness Liver, mlik, eggs, green
(Retinol) - Xerophthalmia and yellow vegetables,
- Bitot spots fruits
- Follicular hyperkeratosis, immune defects
Vitamin B1 - Beri-beri (polyneuropathy, calf tenderness, Liver, meat, milk, cereals,
(Thiamine) heart failure, oedema, opthalmoplegia) nuts, legumes
Vitamin B2 - Anorexia, mucositis Milk, cheese, liver, meat,
(Riboflavin) - Anaemia, cheilosis eggs, whole grains, green
- Nasolabial seborrhoea leafy vegetables
Vitamin B3 - Pellagra (photosensitivity, dermatitis, Meat, fish, liver, whole
(Niacin) dementia, diarrhoea, death) grains, green leafy
vegetables
Vitamin B9 - Megaloblastic anaemia Meat, fish, cheese, eggs
(Folate) - Neural tube defects
Vitamin B12 - Megaloblastic anaemia Meat, fish, cheese, eggs
(Cobolamin) - Peripheral neuropathy
- Subacute combined degeneration of spinal
cord (posterolateral dorsal column disease)
- Vitiligo
Ascorbic acid - Scurvy (irritability, purpura, bleeding gums, Citrus fruits, green
periosteal haemorrhage, aching bones) vegetables, cooking
destroys
Vitamin D - Rickets (reduced bone mineralisation) Fortified milk, cheese,
liver, sunlight
Vitamin E - Haemolysis in preterm infants Seeds, vegetables, germ
- Areflexia, ataxia, opthalmoplegia oils, grains
Vitamin K - Haemorrhagic disease of newborn Liver, green, vegetables,
- Elevated protein-induced vitamin K absence made by intestinal flora
(PIVKA)
Vitamin A Deficiency:
- Vitamin A is necessary for membrane stability and plays a role in vision, keratinisation,
cornification and placental development.
- Functions:
- Retinol is metabolised to form rhodopsin, first step in visual process
- Growth and differentiation of epithelium
- Complications:
- Xerophthalmia (Xerosis of conjunctiva and cornea, untreated leads to ulceration, necrosis,
keratomalacia, corneal scarring)
- Night blindness (impaired dark adaptation)
- Immunodeficiency (increased risk of infection esp measles, increased mortality risk in
developing nations)
*Hypervitaminosis A (headaches, pseudotumour cerebri, hepatotoxicity, teratogenity)
57
Vitamin D Deficiency:
- Most common form of vitamin deficiency, appears as Ricket in children and Osteomalacia in
post-pubertal adolescents.
- Functions:
- Enhanced intestinal absorption of calcium and phosphate via 1,25-(OH)2-D
- Direct anabolic effect on bone
- Inhibit PTH secretion via negative feedback of raised 1,25-(OH)2-D
- Causes of deficiency:
- Failure to achieve minimum daily nutritional requirement of vitamin D of 400IU especially in
infants who are breastfed for a protracted period (most common)
- Decreased sun exposure especially in infants with dark skin pigmentation, urban living
conditions and winter
- Inherited abnormalities of vitamin D metabolism or vitamin D receptor
- Mineral deficiency eg. X-linked hypophosphataemia
- Decreased activity of 1α-hydroxylase in chronic renal disease (renal osteodystrophy)
- Liver disease (impaired metabolism of vitamin D)
- Anticonvulsants eg. phenytoin (metabolises vitamin D)
- Prematurity
- Metabolic bone disease in the premature infant occurs if the milk used contains inadequate
calcium and phosphorus (1,25-(OH)2-D raised due to hypophosphataemia stimulus, but there
is osteopenia and inadequate minieralisation of growing bone)
- Increased phosphate excretion (familial hypophosphataemic rickets, vitD-dependent rickets -
type I or II (receptor defect), Fanconi syndrome)
Rickets
- Inadequate mineralisation of bone matrix (osteoid) of the growing bones due to vitamin D
deficiency.
- Demineralised bone is less rigid, bends and twists in an abnormal way
- Clinical features:
General - Misery, hypotonia, developmental delay, growth failure
- Dwarfism, pot belly, kyphosis, small pelvis, coxa vara
Head - Large anterior fontanelle with delayed closure (> 2 years)
- Craniotabes (ping-pong ball sensation on touching skull, thinning of
outer table of skull)
- Frontal bossing
- Late dentition with enamel defects
Chest - Rachitic rosary (enlargement of costochondral junctions)
- Harrison sulcus (horizontal depression/groove along the lower border of
the thorax corresponding to costal insertion of diaphragm)
- Pigeon chest
Skeletal - Thickened wrists and ankles (enlarged metaphyses)
- Bow legs (caused by weight bearing)
- Knock knees
- Greenstick fractures (long bones)
Metabolic - Hypocalcaemia (seizures, neuromuscular instability (tetany occurs when
serum Ca <7.5 mg/dl), apnoea, stridor
58
- Diagnosis:
History - Poor vitamin D intake
- Little exposure to direct UV sunlight
Blood - Serum calcium (low/normalise by 2` hyperPTH)
- Serum phosphate (low)
- Serum ALP (elevated)
- Serum PTH (elevated)
- Serum 1,25-(OH)2-D low/normal
- Serum 24,25-(OH)2-D undetectable
Radiology - Distal ulna and radius changes
- Distal widening, increased joint space
- Concave cupping and fraying
- Poorly dermacated ends
- Increased space between distal ends of radius and ulna
- Enlarged metacarpal bones
- Non-ossified metaphysis
- Cysts, subperiosteal erosions, fractures, Looser`s zones
- Management:
- Prevention by health education, exposure to sunlight, diet supplementation with minerals
and vitamin D
- Treatment of nutritional rickets with vitamin D3 (1,25-(OH)2-D) 5,000-10,000IU/day initially for
several weeks followed by provision of 400IU/day in the diet
- Biochemical and radiological monitoring may be required
- Monitor for excess chronic vitamin D symptoms (hypercalcaemia, muscle weakness, polyuria,
nephrocalcinosis)
Rachitic rosary
59
Prematurity
Definition:
Premature infant < 37 weeks Period of Gestation (POG)
Low Birth Weight (LBW) < 2.5 kg at birth
Very Low Birth Weight (VLBW) < 1.5 kg at birth
Extremely Low Birth Weight (ELBW) < 1.0 kg at birth
Small for Gestational Age (SGA) < 10th centile of birth weight for age
Large for Gestational Age (LGA) > 90th centile of birth weight for age
60
Management:
- Adequate Resuscitation
- Admission Routine
- Ensure thermoneutral temperature for infant. Incubator/ radiant warmer is necessary for more
premature and ill infants.
- Ventilation in NICU is often necessary if ventilated during transfer. However, some infants take
longer to adapt to extrauterine life and may not require ventilation especially those with no
risk factors and given a full course of antenatal steroids. For the larger preterm infants above
1250 grams, review the required ventilation to maintain a satisfactory blood gas and consider
extubation if the ventilator requirements are low, patient has good tone and good
spontaneous respiration.
- Maintain SaO2 between 89-92% for ELBW; 90-94% for the larger preterm
- Head circumference (OFC), length measurements, bathing can be omitted.
- Quickly and accurately examine and weigh the infant.
- Assess the gestational age with Dubowitz or Ballard score when stable
- Monitor temp, HR, RR, BP and SaO2.
61
- General Measures for Premature infants
- Monitor vitals signs (colour, temperature, apex beat, respiratory rate). Look for signs of
respiratory distress (cyanosis, grunting, tachypnoea, nasal flaring, chest recessions, apnoea). In
VLBL and ill infants pulse oximetry and blood pressure monitoring are necessary.
- Check Blood Sugar
- Keep warm in incubator at thermoneutral temperature for age and birth weight. ELBW should
preferably have humidified environment at least for the first 3 days.
- Ensure adequate nutrition.
- Provide parental counselling and allow free parental access.
- Infection control: observe strict hand washing practices.
- Immunisation:
- Hep B vaccine at birth if infant stable and BW is >1.8 kg. Otherwise give before discharge.
- Ensure BCG vaccine is given on discharge.
- For long stayers other immunisation should generally follow the schedule according to
chronological rather than corrected age.
- Defer immunisation in the presence of acute illnesses.
- Supplements:
- At birth: IM Vitamin K (0.5 mg for BW<2.5 kg; 1 mg for BW ≥ 2.5 kg)
- Once on full feeding, give Infant Multivitamin drops 1 mls OD (continue till fully established
weaning diet).
- For preterm infants, use a formulation with Vit D 400 IU, and Folic acid 1 mg OD.
- Starting at ~4 weeks of life: Elemental Iron 2-3 mg/kg/day - to be continued for 3-4 months.
- Discharge
- Cranial Ultrasound for premature infants ≤32 weeks is recommended at:
- Within first week of life to look for intraventricular haemorrhage (IVH).
- Around day 28 to look for periventricular leucomalacia (PVL).
- As clinically indicated.
- Screening for Retinopathy of Prematurity (ROP) at 4-6 weeks of age is recommended for:
- All infants ≤32 weeks gestation at birth or birth weight <1.5 kg
- All preterms <36 weeks who received oxygen therapy depending on individual risk
- Infants are discharged once they are well, showing good weight gain, established oral
feeding and gestational age of at least 35 weeks.
NEONATOLOGY
62
Paediatrics Basic & Advanced Life Support (PBLS & PALS) [Source: Resus.org.uk]
SECTION A : PAEDIATRICS BASIC LIFE SUPPORT (PBLS)
Introduction:
Cardiorespiratory arrest occurs less frequently in children than in adults; thus, both healthcare
professionals and lay people are less likely to be involved in paediatric resuscitation. It is
therefore important to be familiar with the knowledge and skills required for paediatric BLS so
that the best care possible can be delivered in what is often a stressful situation.
Cardiopulmonary resuscitation (CPR) should start ASAP for optimum outcome. This should start
with the first person on scene, who is often a bystander (eg. a lay rescuer).
Majority of paediatric cardiorespiratory arrests are not caused by primary cardiac problems but
are secondary to other causes, mostly respiratory insufficiency, hence the order of delivering the
resuscitation sequence: Airway (A), Breathing (B) and Circulation (C).
Guideline Notes:
i) Recognition of cardiorespiratory arrest
- If a layperson or healthcare provider considers that there are no `signs of life`, CPR should be
started immediately.
- Pulse is neither reliable to imply effective/inadequate circulation, nor as CPR sole determinant
The presence or absence of `signs of life`, such as response to stimuli, normal breathing (rather
than abnormal gasps) or spontaneous movement must be looked for as part of the child`s
circulatory assessment.
- If healthcare provider does feel for a pulse in an unresponsive child, they must be certain that
one is present for them NOT to start CPR. In this situation, there are often other signs of life
present (Lay rescuers should not be taught to feel for a pulse as part of the assessment of need
for CPR). Decision to start CPR should take <10 seconds from starting the initial assessment of
the child`s circulatory status and if there is still doubt after that time, start CPR.
ii) Compression : Ventilation Ratios
- Rescuers who are unable or unwilling to provide breaths should be encouraged to perform at
least compression-only CPR. Child is far more likely to be harmed if the bystander does nothing.
- All providers should be encouraged to initiate CPR in children even if they haven't been taught
specific paediatric techniques. CPR should be started with the C:V ratio that is familiar and for
most, this will be 30:2.
- Paediatric modifications to adult CPR should be taught to those who care for children but are
unlikely to have to resuscitate them. Specific paediatric sequence incorporating the 15:2 ratio is
primarily intended for those who have the potential to resuscitate children as part of their role.
iii) Chest compression quality
- Uninterrupted, high quality chest compression is vital, with attention being paid to all
components of each chest compression including the rate, depth and allowing adequate time
for chest recoil to occur (approx 50% of the whole cycle should be the relaxation phase).
- In order to facilitate this for children, approximate dimensions of one-third compression depths
in infants & children are about 4 cm and 5 cm respectively.
- To maintain consistency with adult BLS guidelines, compression rate remains at 100-120 min
- Ideally chest compressions should be delivered on a firm surface otherwise depth of
compression may be difficult to achieve.
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Paediatric basic life support algorithm (Healthcare professionals with a duty to respond):
Unresponsive → Shout for help → Open airway (to assess breathing)
Not breathing normally → 5 rescue breaths (then check for signs of life)
No signs of life → 15 chest compression → 2 rescue breaths, 15 chest compressions (if still fail)
Call resuscitation team (1 min CPR first, if alone)
PBLS Sequence:
For Healthcare professional teams,
1. Ensure the safety of rescuer and child
2. Check the child`s responsiveness:
- Gently stimulate the child and ask loudly, `Are you all right?`
3A. If the child responds by answering or moving:
- Leave the child in the position in which you find him (provided he is not in further danger)
- Check his condition and get help if needed
- Reassess him regularly
3B. If the child does not respond:
- Shout for help
- Turn the child onto his back and open the airway using head tilt and chin lift:
- Place your hand on his forehead and gently tilt his head back.
- With your fingertip(s) under the point of the child`s chin, lift the chin.
- Do not push on the soft tissues under the chin as this may block the airway.
- If you still have difficulty in opening the airway, try the jaw thrust method: place first two
fingers of each hand behind each side of child`s mandible (jaw bone) & push jaw forward.
- Have a low threshold for suspecting injury to the neck. If you suspect this, try to open the
airway using jaw thrust alone. If this is unsuccessful, add head tilt gradually until the airway is
open. Establishing an open airway takes priority over concerns about the cervical spine.
4. Keeping the airway open, look, listen, and feel for normal breathing by putting your face close
to the child`s face and looking along the chest:
- Look for chest movements
- Listen at the child`s nose and mouth for breath sounds
- Feel for air movement on your cheek
- In the first few minutes after cardiac arrest a child may be taking infrequent, noisy gasps. Do
not confuse this with normal breathing. Look, listen, and feel for no more than 10 seconds
before deciding - if you have any doubts whether breathing is normal, act as if it is not normal.
5A. If the child IS breathing normally:
- Turn the child onto his side into the recovery position (see below).
- Send or go for help : call the relevant emergency number. Only leave the child if no other way
of obtaining help is possible.
- Check for continued normal breathing.
5B. If the breathing is NOT normal or absent:
- Carefully remove any obvious airway obstruction.
- Give 5 initial rescue breaths.
- Although rescue breaths are described here, it is common in healthcare environments to have
access to bag- mask devices. Providers trained in their use should use them as soon as they
are available.
- While performing the rescue breaths note any gag or cough response to your action. These
responses, or absence, will form part of your assessment of `signs of life`, described below.
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Rescue breaths for an infant:
- Ensure a neutral position of the head (as an infant`s head is usually flexed when supine, this
may require some extension) and apply chin lift.
- Take a breath and cover the mouth and nasal apertures of the infant with your mouth,
making sure you have a good seal. If the nose and mouth cannot both be covered in the
older infant, the rescuer may attempt to seal only the infant`s nose or mouth with his mouth
(if the nose is used, close the lips to prevent air escape).
- Blow steadily into the infant`s mouth and nose over 1 second sufficient to make the chest rise
visibly. This is the same time period as in adult practice.
- Maintain head position and chin lift, take your mouth away, and watch for his chest to fall as
air comes out.
- Take another breath and repeat this sequence four more times.
Rescue breaths for a child over 1 year:
- Ensure head tilt and chin lift.
- Pinch the soft part of his nose closed with the index finger and thumb of your hand on his
forehead.
- Open his mouth a little, but maintain the chin lift.
- Take a breath and place your lips around his mouth, making sure that you have a good seal.
- Blow steadily into his mouth over 1 second sufficient to make the chest rise visibly.
- Maintaining head tilt & chin lift, take your mouth away & watch for his chest to fall as air
comes out.
- Take another breath and repeat this sequence four more times. Identify effectiveness by
seeing that the child`s chest has risen and fallen in a similar fashion to the movement
produced by a normal breath.
For both infants and children, if you have difficulty achieving an effective breath, the airway may
be obstructed:
- Open child`s mouth & remove any visible obstruction. Do not perform a blind finger sweep.
- Ensure there is adequate head tilt and chin lift but also that the neck is not over extended.
- If head tilt and chin lift has not opened the airway, try the jaw thrust method.
- Make up to 5 attempts to achieve effective breaths. If unsuccessful, move to chest compression
6. Assess the circulation (signs of life):
Take no more than 10 seconds to:
- Look for signs of life. These include any movement, coughing, or normal breathing (not
abnormal gasps or infrequent, irregular breaths).
- If you check the pulse take no more than 10 seconds:
- In a child aged over 1 year : feel for the carotid pulse in the neck
- In an infant : feel for the brachial pulse on the inner aspect of the upper arm
- For both infants and children the femoral pulse in the groin (mid-way between the anterior
superior iliac spine and the symphysis pubis) can also be used.
7A. If confident that you can detect signs of a circulation within 10 seconds:
- Continue rescue breathing, if necessary, until the child starts breathing effectively on his own.
- Turn the child onto his side (into the recovery position) if he starts breathing effectively but
remains unconscious.
- Re-assess the child frequently.
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7B. If there are no signs of life, unless you are CERTAIN that you can feel a definite pulse of >60
min-1 within 10 seconds:
- Start chest compressions.
- Combine rescue breathing and chest compressions.
For rescuers who have been taught adult BLS, and have no specific knowledge of paediatric
resuscitation, should use the adult sequence. The following modifications to the adult
sequence will make it more suitable for use in children:
- Give 5 initial rescue breaths before starting chest compression.
- If you are on your own, perform CPR for 1 min before going for help.
- Compress the chest by at least one-third of its depth, approximately 4 cm for an infant and
approximately 5 cm for an older child. Use two fingers for an infant under 1 year; use one or
two hands for a child over 1 year to achieve an adequate depth of compression.
- Compression rate should be 100-120 min-1.
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When to call for help:
- It is vital for rescuers to get help as quickly as possible when a child collapses:
- When >1 rescuer is available, ≥1 starts resuscitation while another goes for assistance
- If only one rescuer is present, undertake resuscitation for about 1 min before going for
assistance. To minimise interruptions in CPR, it may be possible to carry an infant or small child
whilst summoning help.
- Only exception to performing 1 min of CPR before going for help is in the unlikely event of a
child with a witnessed, sudden collapse when the rescuer is alone and primary cardiac arrest is
suspected. In this situation, a shockable rhythm is likely and the child may need defibrillation.
Seek help immediately if there is no one to go for you.
Recovery position
An unconscious child whose airway is clear and who is breathing normally should be turned
onto his side into the recovery position. There are several recovery positions; each has its
advocates. The important principles to be followed are:
- Place child in as near a true lateral position as possible to enable drainage of fluid from mouth
- Ensure the position is stable. In an infant, this may require the support of a small pillow or a
rolled-up blanket placed behind his back to maintain the position
- There should be no pressure on the chest that impairs breathing.
- It should be possible to turn the child onto his side and to return him back easily and safely,
taking into consideration the possibility of cervical spine injury.
- Ensure the airway is accessible and easily observed.
- Adult recovery position is suitable for use in children.
Explanatory Notes:
- Differences between adult and paediatric resuscitation are largely based on differing aetiology,
primary cardiac arrest more common in adults while secondary cardiac arrest more in children
- Onset of puberty, which is the physiological end of childhood, is the most logical landmark for
the upper age limit for use of paediatric guidelines
- Automated external defibrillators (AEDs)
- Capable of identifying arrhythmias accurately in children & extremely unlikely to advise a
shock inappropriately.
- Nevertheless, if there is any possibility that an AED may need to be used in children, the
purchaser should check that the performance of the particular model has been tested in
paediatric arrhythmias.
- Purpose-made paediatric pads (attenuate machine output : 50-75 J) are recommended for
children between 1- 8 years.
- Unmodified adult AED may be used if no such system or manually adjustable machine is
available
- For an infant in a shockable rhythm, risk: benefit ratio favours the use of an AED (preferably
with an attenuator) if a manually adjustable model is not available.
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SECTION B : PAEDIATRICS ADVANCED LIFE SUPPORT (PBLS)
Introduction:
Most paediatric arrests arise from decompensated respiratory/circulatory failure (predominantly
secondary cardiorespiratory arrests). Although in adulthood, primary arrests resulting from
arrhythmias are more common, many young adults have similar causes to children (eg. trauma,
drowning & poisoning), thus respiratory failure is also common in this population.
Cardiorespiratory arrest generally has a poor outcome in children hence the identification of the
seriously ill or injured child is an absolute priority. Directed interventions at the compensated or
decompensated stages of illness/injury can be life-saving and prevent progression to
cardiorespiratory arrest. Any unwell child or infant should be assessed in a systematic manner to
identify extent of any physiological disruption & interventions started to correct the situation.
Order of assessment & intervention for any seriously ill/injured child follows ABCDE principles:
Airway (for airway and cervical spine stabilisation for the injured child)
Breathing
Circulation (with haemorrhage control in the injured child)
Disability (level of consciousness and neurological status)
Exposure (full examination, respecting child`s dignity & ensuring body temp conservation)
Interventions are made at each step to identify abnormalities. Next step of the assessment is not
started until preceding abnormality has been treated & corrected if possible (exception if child
presenting with life-threatening haemorrhage after serious injury - circulatory interventions will
be made simultaneously with assessment, management of airway & breathing).
Paediatric rapid response team (RRT) or medical emergency team (MET) may reduce risk of
respiratory and/or cardiac arrest in hospitalised children. It should include at least one clinician
with paediatric expertise & one specialist nurse.
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4. Assess rhythm and check for signs of life:
- Look for signs of life, which include responsiveness, coughing, spontaneous movements and
normal breathing.
- Assess the rhythm on the monitor:
- Non-shockable : asystole or pulseless electrical activity (PEA)
- Shockable : ventricular fibrillation (VT) or pulseless ventricular tachycardia (pVT)
5A. Non-shockable (asystole or PEA):
This is the more common finding in children.
Perform continuous CPR:
- Continue to ventilate with high-concentration oxygen.
- If ventilating with bag-mask give 15 chest compressions to 2 ventilations.
- Use a compression rate of 100-120 min-1.
- If the patient is intubated, chest compressions can be continuous as long as this does not interfere
with satisfactory ventilation.
- Once the child's trachea has been intubated and compressions are uninterrupted use a ventilation
rate of approximately 10-12 min-1. Note: Once there is return of spontaneous circulation (ROSC), the
ventilation rate should be 12-20 min-1. Measure end-tidal CO2 to monitor ventilation and ensure
correct tracheal tube placement.
Give adrenaline:
- If vascular access is established, give adrenaline 10 mcg kg-1 (0.1 mL kg-1 of 1/10,000 solution).
- If there is no circulatory access, obtain intraosseous (IO) access.
Continue CPR, only pausing briefly every 2 min to check for rhythm change.
- Give adrenaline 10 mcg kg-1 every 3-5 min (eg. every other loop), while continuing to maintain
effective chest compression and ventilation without interruption.
Consider and correct reversible causes (4Hs and 4Ts):
- Hypoxia
- Hypovolaemia
- Hyper/hypokalaemia, metabolic
- Hypothermia
- Thromboembolism (coronary or pulmonary)
- Tension pneumothorax
- Tamponade (cardiac)
- Toxic/therapeutic disturbance
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Resume CPR:
- Without reassessing rhythm or pulse, resume CPR immediately, starting with chest compression.
- Consider and correct reversible causes (4Hs and 4Ts).
Continue CPR for 2 min, then pause briefly to check the monitor:
- If still VF/pVT, give a second shock (with same energy level & strategy for delivery as first shock)
Resume CPR:
- Without reassessing rhythm or feeling for a pulse, resume CPR immediately, starting with chest
compression.
Continue CPR for 2 min, then pause briefly to check the monitor:
- If still VF/pVT, give a third shock (with same energy level and strategy for delivery as previous shock).
Resume CPR:
- Without reassessing the rhythm or feeling for a pulse, resume CPR immediately, starting with
chest compression.
- Give adrenaline 10 mcg kg-1 and amiodarone 5 mg kg-1 after the third shock, once chest compressions
have resumed.
- Repeat adrenaline every alternate cycle (eg. every 3-5 min) until ROSC.
- Repeat amiodarone 5 mg kg-1 one further time, after fifth shock if still in a shockable rhythm.
Continue giving shocks every 2 min
- Continuing compressions during charging of defibrillator & minimising breaks in chest compression
as much as possible.
- After each 2 min of uninterrupted CPR, pause briefly to assess the rhythm:
- If still VF/pVT: Continue CPR with the shockable (VF/pVT) sequence.
- If asystole: Continue CPR & switch to the non-shockable (asystole or PEA) sequence as above.
- If organised electrical activity is seen, check for signs of life and a pulse:
- If there is ROSC, continue post-resuscitation care.
- If there is no pulse (or a pulse rate of <60 min-1), and there are no other signs of life, continue CPR
and continue as for the non-shockable sequence above.
- If defibrillation was successful but VF/pVT recurs, resume the CPR sequence and defibrillate. Give an
amiodarone bolus (unless two doses have already been given) & start a continuous drug infusion.
Important note:
Uninterrupted, high quality CPR is vital. Chest compression and ventilation should be interrupted only
for defibrillation. Chest compression is tiring for providers and the team leader should repeatedly
assess and feedback on the quality of the compressions. To prevent fatigue, change providers should
every two minutes. This will mean that the team can deliver effective high quality CPR so improving
the chances of survival.
Explanatory Notes:
Tracheal tubes - Studies show no greater risk of complications for children <8 years when cuffed,
rather than uncuffed, tracheal tubes are used in OT & ICU.
- Cuffed tracheal tubes are as safe as uncuffed tubes for infants (except neonates) &
children if rescuers use the correct tube size, cuff inflation pressure & verify tube
position. The use of cuffed tubes increases the chance of selecting the correct size at
first attempt. Under certain circumstances (eg. poor lung compliance, high airway
resistance, and facial burns) cuffed tracheal tubes may be preferable.
Alternative - Bag-mask ventilation remains first line method for achieving airway control &
airways ventilation in children
- Laryngeal mask airway (LMA) is an acceptable airway device for providers trained in
its use. It is particularly helpful in airway obstruction caused by supraglottic airway
70
abnormalities or if bag-mask ventilation is not possible.
- Other supraglottic airways (SGA) (eg. i-gel) which have been successful in children`s
anaesthesia may also be useful, but there are few data on the use of these devices in
paediatric emergencies. Supraglottic airways do not totally protect the airway from
aspiration of secretions, blood or stomach contents, and therefore close observation
is required as their use is associated with a higher incidence of complications in
small children compared with older children or adults.
Capnography - Monitoring end-tidal CO2 with waveform capnography reliably confirms tracheal
tube placement in a child weighing more than 2 kg with a perfusing rhythm and
must be used after intubation and during transport of an intubated child. The
presence of a capnographic waveform for >4 ventilated breaths indicates that tube
is in tracheobronchial tree, both in presence of a perfusing rhythm and during CPR.
- It does not rule out intubation of a bronchus. The absence of exhaled CO2 during
CPR does not guarantee tube misplacement because a low or absent end-tidal CO2
may reflect low or absent pulmonary blood flow.
- Povides information on the efficiency of chest compressions and a sudden rise in the
end-tidal CO2 can be an early indication of ROSC. Try to improve chest compression
quality if the end-tidal CO2 remains below 2 kPa as this may indicate low cardiac
output and low pulmonary blood flow
- Be careful when interpreting end- tidal CO2 values after giving adrenaline or other
vasoconstrictor drugs when there may be a transient decrease in end-tidal CO2, or
after the use of sodium bicarbonate when there may be a transient increase in the
end-tidal values. Current evidence does not support the use of a threshold end-tidal
CO2 value as an indicator for stopping the resuscitation attempt.
Post-Resuscitation Care:
Oxygen - Room air is recommended for initial resuscitation of newborn
- 100% oxygen should be used for initial resuscitation for older child
- After ROSC, titrate the inspired oxygen, using pulse oximetry, to achieve an oxygen
saturation of 94-98%.
- In situations where dissolved oxygen important in oxygen transport eg. smoke
inhalation (CO poisoning) & severe anaemia, maintain a high inspired oxygen (FiO2).
Carbon - Controlled ventilation for those not recover immediately from ROSC (may help
dioxide prevent further secondary brain injury)
- Usual target range for PaCO2 in this setting is 4.5-5.0 kPa, but target value should be
towards anticipated value for the individual patient as `normal value` for a child with
a chronic respiratory disorder may exceed the quoted ranges based on children
without adaptive physiology.
IV fluids and - Following ROSC, use of fluids or inotropes to avoid hypotension is recommended to
inotropes ensure dequate tissue perfusion.
Extracorporeal - For rescue and post-ROSC, may benefit to those with cardiac origins of arrest &
membrane where it can be instituted rapidly.
oxygenation
(ECMO)
Prognostic - No single factor is sufficiently reliable, factors should consider include circumstances
factors for of the arrest, initial rhythm, duration of resuscitation and other features such as
resuscitation presence of hypothermia and severe metabolic derangement
outcomes - Comatose children with ROSC receiving mechanical ventilation who fulfill
72
neurological criteria for death, or in whom withdrawal of life-sustaining treatments is
planned should be considered as potential organ donors
Therapeutic - Child who has ROSC, but remains comatose after cardiorespiratory arrest, may
hypothermia benefit either from being cooled to a core temperature of 32-34`C (TH) or having
their core temperature actively maintained at 36.8`C for at least 24 h post arrest.
- Do not actively rewarm a successfully resuscitated child with hypothermia unless the
core temperature is below 32`C. Following a period of mild hypothermia, rewarm the
child slowly at 0.25-0.5`C h-1
Blood glucose - Both hyperglycaemia and hypoglycaemia are associated with poor outcome after
control cardiorespiratory arrest
- Closely monitor plasma glucose concentrations, do not give glucose-containing
fluids during CPR except for treatment of hypoglycaemia.
Parental Presence:
- Reports show that being at the side of the child is comforting to parents or carers and helps
them to gain a realistic view of attempted resuscitation and death.
- Bereaved families who have been present in the resuscitation room show less anxiety and
depression several months after the death.
- Encourage healthcare providers` professional behaviour & facilitate their understanding of the
child in the context of his/her family.
- A dedicated staff member should be present with the parents at all times to explain process in
an empathetic and sympathetic manner. They can also ensure that the parents do not interfere
with the resuscitation process or distract the resuscitation team. If the presence of the parents
is impeding the progress of the resuscitation, they should be gently asked to leave. When
appropriate, physical contact with the child should be allowed.
- Resuscitation team leader should decide when to stop the resuscitation; this should be
expressed with sensitivity and understanding. After the event, debriefing of the team should be
conducted, to express any concerns and to allow the team to reflect on their clinical practice in
a supportive environment.
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Algorithm for Paediatrics Advanced Life Support (PALS):
74
PART III
NEUROLOGY
Down`s Syndrome (Trisomy 21)
Introduction:
- Most common autosomal trisomy, most common genetic cause of severe learning difficulties
and the development of complication.
Incidence of Down syndrome
Epidemiology: Maternal Age-Specific Risk for Trisomy
- Incidence is about 1:650 live births 21 at Livebirth (Overall Incidence: 1 in
- BUT individual incidence dependent on maternal 800 -1000 newborns)
age Age (years) Incidence
20 1 : 1500
30 1 : 900
35 1 : 350
40 1 : 100
41 1 : 70
42 1 : 55
43 1 : 40
44 1 : 30
45 1 : 25
TRISOMY 21
50 1 : 10
- However, most of DS babies are born to younger mothers because proportionately they have
more babies
- > 85% will survive to 1 year old; at least 50% affected individual live longer than 50 years old
- Risk factors : Increased maternal age and Family history (recurrence)
Cytogenetics (Inheritance):
Non-disjunction - Karyotype: 47, XY + 21
(95%) - Mostly from error during meiosis
- Paired chromosomes 21 failed to separate à 1 gamete with 2
chormosomes 21 and 1 gamate has none
- Fertilization of gamete with 2 chr 21 à trisomy 21
- Parental chromosome do not need to be examined
- Incidence rises with increased maternal age BUT not paternal
- Only 5 % are paternally derived
- Risk of recurrence of DS when have one child with trisomy 21
- 1 in 200 (<35 years old)
- 1 in 100 (>35 years old)
Translocation (4%) - Karyotype: 46, XY, -14, +t (14q21q)
- Results from an unbalanced Robertsonian translocation
- Usually extra chr21 translocated onto chr14, more rarely 15, 22 & 21.
- Affected child has 46 chromosomes, BUT 3 copies of chr21 material
- Parental chromosome analysis is essential due to parent translocation
carrier
- Risk of recurrence with one DS baby
- 10-15% recurrence risk if mother is carrier and 2.5% if father is carrier
- 100% if parent has the 21:21 translocation (very rare)
- <1% if neither parent has a translocation
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Mosaicism (1%) - Karyotype: 47, XY + 21/46, XY
- Result from non-disjuction during mitosis after fertilisation
- Some cells are normal and some with trisomy 21
- Milder phenotype of DS
Clinical Features:
Newborn
Facial appearance - Round face & short neck
- Flat occiput (brachycephaly & third fontanelle)
- Hypertelorism (abnormal ratio btw interpupillary distance and distance btw
lateral canthus
Brushfield spots
- Bilateral upward slanting of eyes Small, white, grayish
- Brushfield spots in iris or brown spots on the
- Congenital cataract, squint & glaucoma periphery of the iris in
the human eye due to
- Epicanthic folds aggregation of
- Flat nasal bridge connective tissue, a
- Protruding tongue normal iris element.
- Low set ears (ear lobe less than 1/3 below imaginary intercanthal line)
Upper and lower - Single palmar crease (simian crease)
limbs - Clinodactyly (incurved 5th finger)
- Short, stubby fingers
- Hypotonia
- Sandal gap between big toe and second toe
CVS Congenital heart defects
- AVSD(most common), VSD, PDA, ASD primum & Fallot`s tetralogy
GIT - Feeding problem
- Duodenal atresia
- Pyloric stenosis
- Tracheoesophageal fistula
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- Hirschsprung disease
- Anorectal malformation
CNS - Congenital cataracts
- Glaucoma
Endocrine - Hypothyroidism
- Hypogonadism
Musculoskeletal - Congenital dislocation of the hips
* Walking, language & self-care are usually attained BUT independence is rare.
Adolescent and Adulthood
Puberty - Girls menarche only slightly delayed (fertility presumed)
- Boys are usually infertile due to low testosterone level
Others - Increased risk of Dementia/Alzheimer disease in adult life
- Shorter life expectancy
Diagnosis:
Antenatal Ultrasound - Nuchal fold thickness >3mm
(At 10-14th week)
- Double bubble sign (dilatation of
proximal duodenum & stomach)
Amniocentesis - Karyotyping: Trisomy 21
- At early 2nd trimester (16-18 weeks) - FISH
Chorionic villous sampling - Triple assessment
- After 18th week - ↓ AFP
- ↓ Oestradiol
- ↑ HCG
Newborn Blood sampling - Karyotyping & FISH
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Routine blood test:
The blood should be screened for the following:
- Full blood count (FBC)
- C-reactive protein or viscosity
- Urea and electrolytes (Kidney function)
- Liver function Tests
- Thyroid function tests
- Random glucose and glycosylated haemoglobin (HgbA1c)
- Lithium and anti-epilepsy drug (AED) levels: check level before morning dose (`trough level`)
- Calcium and vitamin D levels if on AED, poor sun exposure or from a black or ethnic minority
- FSH in women who have not had a period for 6 months
- Consider prostate specific antigen (PSA) in men over 50 years
Management:
The following information and explanation should be conveyed before discharge from hospital:
- Information on Down Syndrome
- Short and long term implications
- Counseling (to deal with feeling of disappointments, anger and guilt)
- Contact with local parent support group
- Every child with down syndrome should have access to an Early Intervention Programme as
soon as possible
- Advice on potential recurrence risk and contraception until chromosomal diagnosis is available
Follow-up:
At 6 weeks old 1. Review chromosomal results and provide nondirective counseling for
next pregnancy
2. Review T4/TSH results
3. Cardiac assessment
4. Confirm involvement in parent support group and EIP
5. Discuss parents` concerns
First year 1. Developmental assessment
(Every 3 months 2. Growth
for 12 months) 3. Hearing assessment at 6 to 10 months
4. Visual assessment for squint
5. Fill in forms for registration with welfare department
1-6 years old 1. Regular development assessment
(Once yearly) 2. Annual hearing and visual assessment
3. Annual thyroid function test
4. Begin Dental checks at 2 years old and continue 6 monthly thereafter
5. Check on EIP. Encourage entry into normal kindergarden
6. Plan school by age of 5
7-12 years old 1. Check on school performance and placement
(Once to twice 2. Dental checks 6 monthly
yearly) 3. Annual Hearing, Visual, Thyroid function test
Adolescent 1. Discuss sexuality and employment
79
Recommendations for Medical Surveillance for children with Down Syndrome
Birth-6 weeks 6-10 12 months 18 mths-2.5 yrs 3-3.5 yrs 4-4.5 yrs
months
Thyroid tests T4, TSH T4, TSH, T4, TSH,
antibodies antibodies
Growth Length, weight & head circumference checked Length, weight & head circumference checked at least
monitoring regularly & plotted on Down`s syndrome annually & plotted on Down`s syndrome growth charts
growth charts
Eye Visual behaviour. Check for congenital cataract Orthoptic, Visual acuity,
examination refraction,opthalmic refraction, opthalmic
examination examination
Hearing Neonatal Full audiological review (hearing, impedence, otoscopy) by 6-10 months and then
check screening annually.
Cardiology, Echocardiogram Dental assessment
other advice 0-6 weeks
Age 5 to 19 years Footnote:
Paediatric review Annually 1, Asymptomatic patients with mildly raised TSH (<10mu/l)
Hearing 2 yearly audiological review but normal T4 does not need treatment but test more
Vision/ Orthoptic check 2 yearly frequently for uncompensated hypothyroidism.
Thyroid blood test At age 5 years, then 2 yearly 2, Down syndrome centile charts at www.growthcharts.
School performance Check performance & placement Consider weight for length charts of typically developing
Sexuality & employment Discuss when appropriate, in children for weight assessment. If BMI > 98th centile or
adolescence underweigh, refer for nutritional assessment and guidance.
Note: The above table are suggested ages. Check at any other Re-check thyroid function if accelerated weight gain.
time if parental or other concerns. Perform DV during each 3, Performed by optometrist/ophthalmologist.
visit.
Adapted from Down Syndrome Medical Interest Group (DSMIG) guidelines.
80
- Past-Medical & Surgical History
Past-medical - Indications for, and number of, previous hospital admissions
condition - Pattern and timing of change in condition
- CVS aspects: when cyanosis or heart failure developed, when and how it was
controlled
- GIT aspects: when operative procedures were undertaken, duration of
hospitalisation, how long until feeding was established). Episodes of
infection.
- Other disease complications
- Development of hypothyroidism, coeliac disease, obstructive sleep apnoea
(OSA), seizures, leukaemia
Past-medical or - CVS: Past surgery, complications, plans for further operative procedures. Past
surgical interventional catheter procedures. Medications, past & present, side effects of
intervention these, monitoring levels, treatment plans for the future. Antibiotic prophylaxis
for dental procedures, maintenance of dental hygiene. Compliance with
treatment. Any identification bracelet. Instructions for air travel and high
altitude. Any recent investigations monitoring treatment. Any recent changes
in treatment regimen, and indications for these.
- GIT: Past surgery, complications thereof, plans for further operative
procedures. Compliance with treatment (eg. following diet for coeliac disease).
Any recent investigations monitoring treatment. Any recent changes in
treatment regimen, and indications for these.
- Hearing and vision: past ear, nose and throat surgical intervention, hearing aid
placement, ophthalmological intervention, glasses.
- OSA: Past adenotonsillectomy, nasal mask continuous positive airway pressure
(CPAP).
- Treatments for other conditions: hypothyroidism, atlantoaxial subluxation,
seizures, leukaemia, arthritis, diabetes mellitus.
81
orofacial movements with teeth grinding), intervention for malocclusion, non-
compliance with dental recommendations).
- Respiratory problems (recurrent pneumonia due to silent aspiration)
- Orthopaedic issues
- Limping can be due to atlantoaxial subluxation, acetabular dysplasia with
subluxing hips [not more common in DS, but may appear later], slipped femoral
epiphysis, arthritis or leukaemia
- Foot problems (hallux valgus, hammer toe deformities, plantar fasciitis, pedal
arthritis)
- Joint problems (polyarticular onset juvenile arthritis-like arthropathy)
- Diabetes mellitus (increased drinking or eating, weight loss, lethargy)
- Hypothyroidism (dry skin, cold intolerance, lethargy)
- Haematological neoplasia
Acute lymphoblastic leukaemia (ALL) or acute non-lymphoblastic leukaemia
(ANLL) occur 10-15x more frequently in DS, with usual symptoms of pallor,
bruising, fever, hepatosplenomegaly and lymphadenopathy
- Reproductive issues in adolescents
Difficulties with menstrual hygiene, use of oral contraceptives, Depo-provera,
presentation of premenstrual syndrome (PMS) with temper tantrums, autistic
behaviour episodes, seizures, sex education, desire to reproduce
- Neurological issues
Seizures (more frequent than general population, but less than other causes of
intellectual impairment), strokes (due to cyanotic CHD, or moyamoya disease)
Current state Ask about possible co-morbid psychiatric/behavioural issues:
of behaviour - Symptoms of ADHD (inattention, hyperactivity, impulsivity); any treatment for
these.
- Symptoms of ASD (impaired social interaction, impaired communication,
behaviour patterns including preferring own company, tendency to be loner, `in
their own world`), most problematic behaviours at present (eg. rituals, anxiety,
aggression, self-injury); any treatment for these.
- Other behavioural concerns: depression, conduct disorder, oppositional defiant
disorder, aggressive behaviour; any treatment for these.
- Impact of these co-morbid issues (on family, educational facility [eg. special
school], therapists, carers)
- Paediatrics history
Birth history Relevant antenatal, intrapartum & post-natal history, cord blood screening
Immunisation Any delays, local doctor`s attitudes, parents` understanding of importance of
immunisation.
Developmental Any developmental delay
Dietary Breastfeeding, weaning, feeding difficulty, food history
- Social history
Impact on Level of functioning in activities of daily living (ADLs), schooling (type of school,
child level of support from education department, therapists, academic performance,
teachers` attitudes, peer attitudes, teasing, amount of school missed and whether
schooling is appropriate
Impact on Effect of family`s financial burden, whether siblings feel comfortable to bring
siblings friends home, whether siblings miss out on parental time, plans for siblings to act
as guardians in future.
82
Impact on Financial situation, financial burden of disease so far, government allowances
parent being received, marriage/partnership stability, restrictions on social life, plans for
further children,genetic counselling, availability of prenatal diagnosis,contingency
plans for child`s future, guardianship and power of attorney issues
Social support Social worker, contact with DS parent support groups, any available respite.
Parents` degree of understanding regarding health supervision issues in DS.
Access to Access to local doctor, paediatrician, neurodevelopmental clinic, various
health subspecialty clinics attended (where, how often), other clinics attended,alternative
practitioner (e.g. homeopathy) involvement.
2) Physical Examination
A. Measurement
Height, Weight, Head circumference, Plot & assess growth chart, Calculate height velocity, Request/
plot birth parameters, parent`s percentiles and ages at puberty
B. Systematic
HEENT, Upper limbs - Diagnostic facies
(General inspection) - Tanner stagging
- Nutritional status (obese/thin)
- Skeletal anomalities (pectus excavatum/scoliosis)
- Skin (cutis marmorata, atopic eczema, hyperkeratotic dry skin, fungal
infections, pustular folliculitis, vitiligo, seborrhoeic dermatitis)
- UL (manoeuvres: palm up (detect simial crease,clinodactlyl), check for
hyperextensibility (hypotonia)
- Fingers (brachydactyly-short fingers), 5th finger (hypoplasic mid-phalanx)
- Nails (clubbing in cyanotic heart disease)
- Palms (Simian creases)
- Blood pressure (elevated in occult renal disease)
- Joints (hyperflexibility, restricted movement: arthropathy)
- Head (microcephaly, brachycephaly, flat occiput, facial profile: fat, late
fontanelle closure)
- Eye (examine glasses for myopia, check vision with wearing glasses,
epicanthal folds, upward slant of palpebral fissures, prominent eyes:
coexistent hyperthyroidism, blocked-tear duct: infant, ptosis, squint,
nystagmus)
- Conjunctival pallor (iron deficiency, TAM, AML, ALL)
- Scleral jaundice (coexistent liver disease)
- Iris (Brushfield`s spots: white speckling of peripheral iris)
- Cornea (buphthalmos: large, cloudy, glaucoma, keratoconus)
- Visual fields (defect, CVA from cyanotic heart disease)
- Eye movement (nystagmus)
- Ophthalmoscopy (cataracts)
- Nose (small, flat nasal bridge)
- Mouth, chin (central cyanosis: various CHD, tendency to open mouth)
- Palate (short hard palate)
- Teeth (hypodontia,irregular placement,periodontal disease,dental caries)
- Tongue (protruding, fissured)
- Tonsils (enlarged causing OSA, absence: previous adenotonsillectomy)
- Ears (wear hearing aid, assess hearing loss (conductive/sensorineural,
small, overfolded upper helix, small/absent earlobes, low-set, eardrum:
83
chronic serous otitis media, atelectatic eardrum, tympanic membrane
scarring, permanent perforation, middle-ear cholesteatoma)
- Neck (short, pterygiumcolli, scoliosis, excess skin back of neck, low
posterior hairline, goitre(thyroid disease), torcollis (spinal cord
compression from atlanto-axial instability)
Chest - Inspection
- Scars (repair of CHD:, repair of tracheo-oesophageal fistula, insertion of
access port for chemotherapy for ALL, AML)
- Tanner staging in girls
- Sternal deformity: pectus excavatum or carinatum
- Palpate & auscultate praecordium
- Various forms of CHD, loud S2 with OSA, development of mitral valve or
tricuspid valve prolapse or AR)
Abdomen - Inspection
- Scars (repairs of GIT anomalies eg. duodenal atresia, pyloric stenosis,
Hirchsprung disease, omphalocele, imperforate anus; repairs of urinary
tract anomalities eg. vesicoureteric reflux, posterior urethral valve; renal
transplantation eg. dysplastic kidneys, glomerulosclerosis; others
operative condition eg. Crohn`s disease)
- Palpation
- Hepatomegaly (CCF)
- Splenomegaly (SBE)
- Hepatosplenomegaly (ALL, AML)
- Enlarged kidneys (hydronephrosis)
Genitalia - Tanner staging: measure penis length & testicular volume
- Penile abnomalies: hypospadias (infant), corrected hypospadias
- Testicular anomalies: cryptochidism, enlarged(seminoma), leukaemic
deposits
Lower limbs, Gait, Back - Lower limbs
- Inspection (Clubbing of toes (CHD), saddle gap, single plantar crease,
hallux valgus, hammer toes, fungal infection of nails (adolescents), pes
planovalgus)
- Palpation (ankle oedema- CCF with CHD)
- Back (short neck/neck webbing, bend over and touch toes for scoliosis)
- Neurological (Hypotonia, normal power, Long tract signs)-quadriparesis/
quadriplegia, Hyperreflexia (Spinal cord compression from atlanto-axial
instability, CVA/cerebral abscess complicating cyanotic CHD)
- Joint (hyperflexibility, restriction of movement)
A.Developmental assessment
Refer pg. 40. Most children with Down syndrome have developmental quotient (DQ) and later
intelligence quotient (IQ) in the range 50-70.
84
Meningitis
Definition:
- Inflammation of the meninges covering the brain, following infection of subarachnoid space.
Aetiology:
Infectious
B) Bacterial infection
- >80% bacterial meningitis are in children <16 years old in UK (5 -10% mortality), >10% of
survivors have long term neurological impairment
- Pathophysiology
- Usually follow bacteraemia
- Damage to meninges result from host response to infection (not from bacterial itself)
body release inflammatory mediators and activate leucocytes à endothelial damage à
increase permeability à cerebral edema, ↑ICP, ↓cerebral blood flow
- Severe consequences
Duration/Condition Causative organism
Neonatal - 3 months - Escherichia coli (E. coli)
- Group B Streptococcus (S. agalactiae)
- Klebsiella sp.
- Listeria monocytogene
1 month - 6 years - Haemophilus influenza (H. influenza)
- Streptococcus pneumoniae
- Neisseria meningitidis
> 6 years - Streptpcoccus pneumoniae
- Neisseria meningitidis
Fistulae/Shunt - Coagulase negative staphylococcus
(S. epidermidis, S. saprophyticus)
Immunocompromised - Fungal infection
- Low virulence organism
- Opportunistic organism
- Well known association between pneumococcal infections & H. influenza with sickle-cell
disease, asplenism or removal of spleen.
C) Fungal infection
Non-Infectious
85
Autoimmune disease - RA, SLE, Sjogren, Vasculitis (Kawasaki`s disease)
- Sarcoidosis
Drugs & contrast media - NSAIDS, amoxicillin, IV Ig, Methotraxate, Isoniazid, TMP/SMX
(Stimulates Type III, IV hypersensitivity reaction)
.
Risk Factors:
Environment - Overcrowded closed communities, schools, day cares
- Low socio-economic status dt malnutrition and low birth weight
Host - Male are commonly affected
- Too young (preterm) or too old
- Complement or antibody deficiency
- Immunosuppresion: Carcinoma, AIDS, no effective spleen, sickle cell
disease (autosplenectomy), hypo-gammaglobulinemia, DM
Head - Head injury (especially basal skull, cranial or spinal surgery)
- Encephalocele or leaking myelomeningocele
Septic site - Blood route (eg. pneumonia, UTI)
- Local route (eg. sinusitis, mastoiditis, otitis media)
Foreign body - CSF shunt
Clinical Features
- Early stage, there if non-specific and makes early diagnosis difficult.
Symptoms Signs
Non-specific Meningism
- Fever, Irritability, lethargy, drowsiness - Neck stiffness
- Vomiting, poor feeding - Lying with an arched back (opisthotones)
- Seizure - Kernig`s sign +ve (stretch of meninges)
- Child lying supine & with hip, knee flexed à
Meningism back pain on extension of knee
Classical triad: - Brudzinski`s sign +ve
- Headache, Photophobia, Stiff neck - Child lying supine & neck flexed à flexion of
the knee and hip
86
↑ICP ↑ICP
- Irritability, drowsiness, vomiting, fits - Bulging anterior fontanelle
- Reduced consciousness, coma - Papilloedema
- Bradycardia, hypertension
- Irregular respiration
- Sunset eyes (squint CN6 palsy)
Septicaemia Septicaemia (signs of shock)
- Fever, malaise, arthritis, rash - Tachycardia
- Odd behavior, DIC (bleeding) - Hypotension
- Purpuric skin lesion - Tachypnea
- Oligouria
- Prolonged capillary refill time (>2s)
Complications:
Brain Local cerebral infarction
- May result in focal or multifocal seizures (increase risk of epilepsy)
Subdural effusion
- Accumulation of high protein & xanthochromic fluid in the subdural region
- Usually sterile, over temporoparietal region
- Associated with H. influenza or pneumonoccal meningitis
- Usually resolve spontaneously
Cerebral abscess
- CF usually suddenly deteriorates with emergency of SOL
- Confirmed by CT scan drainage of the abcess is required
Hydrocephalus
- Impaired resorption of CSF (communicating)
Neurological lesion
- Cranial nerve palsy: commonly 3,4,6 monoplegia/hemiplegia
87
Early complications Late complications
- Cerebral infarction - Cerebral palsy
- Seizure - Blindness
- Cerebral edema - Deafness
- Cerebral abcess - Mental retardation
- Local vasculitis - Behavior problem
- Meningococcaemia - Epilepsy
- DIC, Coagulopathy - Hydrocephalus
- Shock - Developmental delay
- SIADH
Investigation:
Lumbar puncture - Obtain CSF to confirm diagnosis
- Send for biochemistry test (cell count, protein, sugar)
- Gram stain, culture and sensitivity, AFB, antigen test
- Contraindicated in:
- Cardiorespiratory arrest
- Haematological unstablity
- Focal neurological signs
- Signs of raised ICP:
- Coma, hypertension, bradycardia, pappiloedema, pintpoint pupil
- Local infections
Blood test - FBC (Hb, MCH, MCV for anaemia, WCC for infection)
- ESR/CRP (signs of inflammation)
- RP (hydration status, electrolyte imbalance)
- LFT/CP (nutritional status, liver impairment, coagulopathy)
- RBS (hypoglycaemia)
- Blood gas (metabolic acidosis)
Culture & Sensitivity - Blood, CSF, urine samples
Rapid antigen screen/ PCR - Virology screening (a serology diagnosis can be made on
convalescent serum 4-6 weeks after the presenting illness.
CXR, Mantoux test - If suspected for TB
88
CSF findings in various CNS infections
Condition Appearance Pressure White cell Protein (g/L) Glucose
(cm H2O) (/mm3) (% of blood sugar)
Normal neonate Maybe 5 -10 up to 30 0.5 -2.0 > 60%
xanthochormic
Normal Infant Clear 5 - 10 up to 10 0.2 -1.0 >50 %
Normal child >1 y/o Clear 5 - 10 <10 0.15 - 4.0 > 50%
Acute Bacterial Turbid Usually 100 - 60,000 PMN 0.18 - 4.0 < 40 %
meningitis elevated predominate
Partially treated Usually clear Normal or 1- 10,000 PMN predominate 0.8 -2.0 Normal or low
bacterial meningitis elevated unless treated for extended
period
TB meningitis Hazy, may be Usually 10-500 PMN predominate 0.6 - 6.0, Higher in Very low especially if
viscous elevated initially, followed by obstruction treatment delayed
lymphocyte
Fungal Hazy, may be Usually 25- 500 PMN predominate 0.4 - 4.0 <50 %, lower if
viscous elevated initially, mononuclear cell treatment delayed
predominate later
Viral meningitis/ Usually clear, Normal, PMN early, mononuclear cell 0.4 -1.5 Generally normal.
meningoencephalitis may be slightly predominate later. Rarely May be low in some
hemorrhagic elevated >1000 except in eastern viral (15-20% in
equine mumps)
Abscess Turbid Elevated Usually normal unless Usually normal or Low
epidural or rupture into mildly elevated
ventricle
Brainstem encephalitis Usually clear Usually ~240/mm3, lymphocytes Mildly elevated in Only mildly reduced
normal predominate in 58% of 85% of cases, in 20 % of cases
cases normal in others
89
Management:
1. Supportive treatment
- Monitor vital signs and input/output 4 hourly
- Nil by mouth
- Careful fluid balance required. Usually a maintenance IV fluid is sufficient. Only if SIADH
occurs, reduce to 2/3 maintenance for the initial 24 hrs. Patient may need more fluid if
dehydrated. If fontanel hasn`t close, note daily head circumference. Ultrasound ± CT scan (if
effusion or hydrocephalus is suspected)
- Fit chart
- Daily CNS assessment is essential
- Patient must be observed for 24 hrs after stopping therapy, discharged if no complication
90
2. Medical Management
i) Antibiotic
- Remember to use the correct dosage af antibiotic that will penetrate the CSF
- Start antibiotics ASAP (normally after LP)
Recommended antibiotic therapy according to likely pathogen
Age Group Initial Antibiotic Likely Organism Duration (if uncomplicated)
< 1 month C Penicillin + Cefotaxime Grp B Streptococcus 21 days
E. coli
1 - 3 months C Penicillin + Cefotaxime Group B Streptococcus 10 - 21 days
E. coli
H. influenza
Strep. pneumoniae
> 3 months C Penicillin + Cefotaxime, H. influenzae 7 - 10 days
OR Ceftriaxone Strep. pneumoniae 10 - 14 days
N. meningitides 7 days
Note:
・ Review antibiotic choice when infective organism has been identified.
・ Ceftriaxone gives more rapid CSF sterilisation as compared to Cefotaxime or Cefuroxime.
・ If Streptococcal meningitis, request for MIC values of antibiotics. *MIC = minimal
MIC level Drug of choice: inhibitory
- MIC < 0.1 mg/L (sensitive strain) C Penicillin concentration
- MIC 0.1-< 2 mg/L (relatively resistant) Ceftriaxone or Cefotaxime
- MIC > 2 mg/L (resistant strain) Vancomycin + Ceftriaxone or Cefotaxime
・Extend duration of treatment if complications eg. subdural empyema, brain abscess.
91
v) Partially treated bacterial meningitis
- Children are frequently give oral antibiotics for a non-specific febrile illness
- If they have early meningitis, this partial treatment with antibiotics can cause diagnostic
problem
- CSF examination shows highly elevated WCC but culture will be negative
- Rapid antigen tests & PCR are helpful
Meningococcal Menigitis
- Neisseria meningitides
- Reduce incidence dt introduction of conjugate vaccine agst grp A & C (but still no effective vaccine agst grp B)
- Emergency, can kill previously healthy child within hours
- Associate with speticaemia & purpuric rash (lesions are non-blanching on palpation, irregular shape & size,
necrotic centre)
- Lower risk of long term neurological sequel and recover fully
- Common in middle east, ask about travel history
Haemophilus Meningitis
- Immunization has been highly effective (Hib B vaccine)
- Now it is a rare cause
Pneumonoccal Meningitis
- Increased incidence
- >30% develop neurological impairment
- Associated with sickle cell disease, asplenism or removal of spleen
Tuberculous Meningitis
- History: Insidious onset, 2-3 weeks, minimal meningism, TB contact, chronic cough/illness, ESR>100
- Suspected by +ve Mantoux test (>10mm in 48-72 hours)
- Abnormal CXR
- Confirm diagnosis by LP with Ziehl-Nielson stain
- Start muti-antimicrobial regime ASAP due to increased morbidity & mortality
92
Lumbar Puncture (Spinal tap/ CSF fluid tap)
Definition:
A procedure to collect CSF. It involves inserting a needle between the 3rd and 4th lumbar
vertebrae in the back and extracting a sample of fluid.
Indications:
1. Diagnostic method - Meningitis/encephalitis
- GBS
- Multiple sclerosis (chronic, demyelinating disease caused by
inflammation, destruction & scarring of sheath covering nerve
fibers in brain & spinal cord)
- CNS syphilis
- Certain forms of hydrocephalus
- Lymphoma, leukemia or other cancers involving brain or CNS
- Bleeding in the brain or spinal cord
- Any disorder affecting the nervous system
2. Others - Drain spinal fluid to lower ICP
- Administer dye for imaging studies
- Administer medications (eg. chemotherapy/epidural anesthesia)
Contraindications:
- Increase ICP (S&S , raised BP, fundoscopic sign)
- Bleeding tendency : Platelet count <50,000/mm3 or Prolonged PT and APTT
- Cardiorespiratory instability
- Focal neurological signs
- Local infections at site of LP
Complications:
- Pain or abnormal burning sensations in the legs OR post-spinal tap headache
- Bleeding into CSF (Spinal, epidural, subdural or subarachnoid hematomas)
- A local infection at the site
- CNS infections
- Brain herniation associated with increase ICP
- Inflammation of the arachnoid mater
- Temporary paralysis of a cranial nerve
- Rupture of the soft, central portion of the intervetebral disk (nucleus pulposus)
93
Preparation:
- Sterile set
- Sterile bottles for CSF , bottle for RBS
- Spinal needle 20-22G, lenth 1.5 inch with stylet (length 3.5 inches for children >12 y/o
Procedure:
- Give sedation (midazolam) apply local anaesthetic
- Place child in lateral recumbent position with neck, body, hips and knees flexed.
- Monitor oxygen saturation continuously.
- Visualise vertical line between highest point of both iliac crest and its transaction with the
midline of the spine (at level L3-4)
- Clean area with standard aseptic technique using povidone iodine and 70% alcohol.
- Gently puncture skin with spinal needle at the identified mark and pointing towards the
umbilicus. The entry is distal to the palpated spinous process of L4.
- Gently advance a few millimeters at a time until there is a blackflow of CSF (there may be a
`give` on entering the dura mater before the CSF bckflow). Collect CSF in designated bottles.
- Gently withdraw needle, spray with op-site, cover with gauze and bandage.
- Take RBS
- Ensure child lies supine for next 4-6 hours, continue monitoring till s/he recovers from sedation.
Laboratory Findings:
CSF - Appearance
- Pressure
- Microbiology
- Gram stain
-C&S
- India ink test : detection of meningitis caused by Cyptococcus
neoformans antibody mediated test (latex agglutination, treponemal
titres, cocciciodes antibody)
Latex agglutination test - Determines the presence of
- H. Influenza, Staphylococcus aureus, E. coli, Group B strep, Listeria sp.
- PCR has been a great advance in diagnosis of some types of meningitis. It
has high sensitivity and specificity for many infections of the CNS, is fast
and can be done with small volumes of CSF. Even though testing is
expensive, it saves cost of hospitalization.
Cytology - Identify the presence of maglinant cells
94
Syndrome of Inappropriate Antidiuretics Hormone (SIADH)
Introduction:
- Occurs when excessive levels of antidiuretics hormone (ADH) are produced
- Causes the fluid retention in the body and hyponatraemia
Aetiology:
Tumours - Small cell lung CA
- Prostate tumor
- Thymus tumor
- Pancreas tumor
- Lymphomas
Pulmonary lesion - Pneumonia
- Tuberculosis (TB)
- Lung abscess
Metabolic - Alcohol withdrawal
- Prophyria
CNS - Meningitis
- CNS tumours
- Head injury
- Subdural haematoma
- Cerebral abscess
- SLE vasculitis
Drugs - Chloropropamide
- Carbamezapine
- Cyclophospahmide
- Phenothiazines
Diagnosis:
- Plasma dilutional hyponatraemia (<130 mmol/L)
- Low plasma osmolality (<270 mmol/kg) [Normal range: 285-295 mmol/kg)
- Inappropriate urine osmolality(>150 mmol/kg)
- Continued urine sodium excretion
Treatment:
- Treat underlying cause
- Symptomatic Tx
- Restrict fluid intake to 500-
1000mL/day.
- If not adequate give
demeclocycline( as an
inhibitor of arginine
vasopressin)
- Plasma osmolality,
sodium & body weight
should be measured
frequently
- If very severe give
frusemide with extra
caution 95
Encephalitis/Encephalopathy
Definition:
- Inflammation of the brain parenchyma ± meninges
Aetiology:
- Unknown
- Possible viral or bacterial infections
- Direct invasion of the cerebrum by neurotoxic virus
- Delayed brain swelling following a disordered neuroimmunological respose to an antigen,
usually a virus (post-infectious encephalopathy)
- Slow virus infection; HIV, Subacute sclerosing panencephalitis(SSPE) following measles
Viral Bacterial
1. Enterovirus 1. Mycoplasma
- Poliovirus 2. Borrelia burgdorferi (Lyme disease)
- Coxsackie virus 3. Bartonella nenselae (cat scratch disease)
2. Respiratory virus 4. Rickettsial infection
- RSV
- Parainfluenza virus
3. Arbovirus (arthropod-borne virus)
- Dengue virus (epidermic outbreak)
4. Herpes virus
- Herpes Simplex virus (HSV)
- rare but devastating
5. EBV, CMV
6. HIV
7. Measles (SSPE)
8. Mumps, Rubella
Pathology:
- Frequently non-specific
- Compromise brain swelling, vascular congestion, cellular infiltration, cerebral edema
96
Clinical Features:
- Usually acute onset
- Full recovery within a few days or weeks
- Most devastating illness à death or recovery with permanent neurological sequel
* It is not possible to clinically differentiate viral meningitis vs encephalitis vs myelitis
Symptoms Sign
- Fever, headache, malaise, dizziness - Various neurological sx
- Altered consciousness - Depend on the site & extent of the
- Behavioral change inflammation
- Neck stiffness - Such as paraplegia, sensory disturbance,
- Often seizure, mental confusion, stupor, speech difficulty, involuntary movement,
delirium ataxia, neurologic bladder
- Associate with skin rash (measles, varicella)
Diagnosis:
- Dx by exclusion except for the epidemic encephalitis or following of exanthematous fever
- Confirmatory by CSF virology
- EEG & MRI may show the focal change in the frontal/temporal lobe
Management:
- Mainly is supportive (monitor hydration status, careful nursing)
- Antiviral: All children with encephalitis should cover by acyclovir (HSV - devastated Cx)
Lennox-Gastaut syndrome
- Childhood epileptic encephalopathy
- Onset 2-6 years old
- Associated with status epilepticus (seizure >30 minutes)
- Brain distressed by frequent seizure and multiple different seizure type
- Causing mental retardation & behavioral problem, slow global development
- Associated Seizure: 1. Tonic (90%)
2. Myoclonic
3. Atonic
4. Absence
5. Complex partial
6. Tonic clonic
- Aetiology: Unknown, tuberous sclerosis, hereditary metabolic ds, encephalitis, meningitis,
Hypoxic ischemic encephalopathy (HIE), birth injury
- Diagnosis:
- EEG (abnormal EEG: paroxysmal fast activity, generalized slow spike & wave discharge (1.5 HZ)
- MRI
- CT Scan
- Treatment
- Sodium valproate
- Benzodiazepine
97
Fever/ Headache
Meningitis Encephalitis
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Cerebral Palsy
Definition:
- Disorder of movement & posture due to a non-progressive lesion of motor pathway in the
developing brain (<2 years old)
Epidemiology:
- Most common cause of motor impairment in children
- Incidence: 2 per 1000 livebirths
Pathology:
- Cerebral atrophy, often with cavity formation in the subcorticla white matter
- Porencephaly (an abnormal communication between the lateral ventricles and the surface of
the brain)
- Degeneration of basal ganglia
Aetiology:
Antenatal (80%) Intrapartum (10 %) Pospartum (10%)
1. Cerebral dysgenesis 1. Birth asphyxia (HIE) 1. Preterm infant
2. Failure of migration of - APGAR score - Periventricular leucomalacia
grey matter - Respiratory distress (PVL): ischaemic necrosis of
3. Cerebral malformation - Chord prolapsed periventricular white matter
- Congenital cyst - Chord strangulation
- Fusion defect - Meconium aspiration 2. Intraventricular/
4. Congenital infections subependymal haemorrhage
- TORCHES 2. Trauma
5. Vascular occlusion - Instrumental delivery 3. Cerebral anoxia/ischaemia
- Abruption placenta
- Placenta praevia 4. Meningitis/encephalitis/
6. GDM, PIH encephalopathy
5. Head trauma/non-accidental
injury (shaken baby
syndrome)
6. Symptomatic hypoglycemia
7. Hydrocephalus
8. Hyperbilirubinaemia
(Kernicterus)
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Clinical features:
Symptoms Signs
- Feeding difficulties - Delayed motor milestones
- Oromotor discoordination - Abnormal limb tone & posturing
- Slow feeding - Abnormal gait (hemiplegic gait)
- Gagging & vomiting - Once walking is achieved
- Developmental delay in language & social - Hand preference (<12 months old)
skills - Signifies hemiparesis
- Persistence of primitive reflex (> 6 months)
- Becomes obligatory
* Symptoms and signs are not static & a changing pattern of physical symptooms is observed
with increasing age for a considerable period of time
Associated Problems:
General - Learning difficulties/ intellectual impairment (60%)
- Speech and language disorders (from combination of)
- Hearing loss
- Muscle discoordination
- Learning impairment
- Behavioral disorders
- Hyperactivity
- Poor concentration
- Temper outburst
Head - Epilepsy (40%)
- Visual impairment (20%): refractive errors & cortical damage
- Strabismus, squint, mylopia, nystagmus
- Hearing loss (20%)
Respiratory - Aspiration pneumonia
- Hypostatic pneumonia
- Chest infections
GIT - Sucking & swallowing difficulty
- FTT
- GERD
Others - Urinary incontinence
- Constipation
- Menstruation problem
- Pressure sores
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(1) Classification based on motor function
Spastic (70 %) Ataxic (10%) Dyskinetic (10%) Mixed (10%)
- Damage to the upper motor neuron - Affects coordinated movements, - Pathophysiology - Any combination of
pathway: pyramidal & corticospinal balance and posture - Perinatal injury by kernicterus the different types
pathway (common)à damage to basal ganglia
- Pathophysiology: or extrapyramidal pathway - Commonest is a
- Clinical features: - Genetic cause commonest - Hypoxic ischaemic encephalopathy (HIE) mixture of Spastic &
- Persistent primitive reflex - Cerebellar dysfunction or its pathways at term Athetoid
- Initial hypotonia (esp at head & neck)
- Hypertonia (spasicity): tight fisting of the - Clinical features (usually symmetrical) - Clinical features
hand, clasp knife spasticity Early - Constant involuntary movements
- Up-going plantar reflex (Babinski`s - Hypotonia - Athetosis
positive) after 2 years old - Poor balance - Dystonia
- Scissoring of legs when the infant is grown - Delayed motor development - Chorea
up (spasicity of extensor/adductor muscle Late - Choreoathetoid
of LL) - Uncoordinated & involuntary - Poor postural control (flopiness)
- Equinovarus deformity of foot (dorsiflex & movement - Delayed motor development
inversion) - Rigidity - Intellect relatively unimpaired, no seizure
- Windswept hip deformity (ipsilateral - Ataxic gait (broad base)
internal rotation & adduction of hip joint - Obligatory tonic neck reflex Athetosis
with external rotation & abduction of - Control of eye movement & depth - Repetitive involuntary, slow, sinous,
contralateral hip joint) perception can be impaired writhing movements @ arms, legs,
- Fine motor skills requiring hands
- Forms of spastic cerebral palsy coordination of eyes and hands eg. Dystonia
- Hemiplegia writing are difficult - Impairment of muscular tonus
- Diplegia (truncal >limbs)
- Quadriplegia Chorea
* Refer Classification II (topographical - Irregular movement, non-repetitive,
distribution) more jerky and shaky
Choreoathetoid
- Combination of chorea + athetosis
- irregular movement but twisting and
curving
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(2) Classification based on topographical distribution
Hemiplegia - Aetiology:
- 2/3, congenital: Perinatal stroke, Cerebral malformation
- 1/3, Acute postpartum event
- Destruction of brain at level of the cortex or internal capsule
- Clinical features (usually appears at 4 -12 months of age):
- Unilateral involvement of arm & leg (prefer use only one side of the body)
- Arm usually affected more than leg, face spared
General Limb signs (affected side)
- Initially flaccid & hypotonic Hand
- Then, hypertonia develops - Fisting of affected hand
- Intellectual level is low than - Asymmetric reaching
normal - Flexed arm
- Pronated flexed forearm
- Flexed wrist
Leg
- Limping when walk + circumduction
of affected leg
- Tiptoe walk (toe-heel gait)
-
Diplegia - Aetiology: Preterm infant
- Involvement of all for limbs but legs are affected more then arms
- Hand function appears relatively normal in later life
- Clinical features:
- Floppy in the first few month of life
- Gradually increase the extensor posture
- Clumsiness in grasping
- Walking is abnormal
Quadriplegia - Aetiology: HIE & Congenital event
- Involvement of all four limbs with fairly similar degree (arms > legs)
- Clinical features:
- Poor head control
- Low central tone
- Extensor posturing (trunk involvement)
- Disused atrophy
- Associated problems
- Seizures
- Microcephaly
- Moderate to severe intellectual impairment
Monoplegia - Affect only 1 limb
Paraplegia - Lower half of both including both legs
Triplegia - Involve 3 limbs
Double hemiplegia - One side of body more affected than the other
Pentaplegia - All 4 limbs + neck & head paralysis
- Often accompanied by eating and breathing complications
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(3) Classification based on severity level
Mild - Child can move without resistance
- Daily activities not limited
Moderate - Child will need braces, medications, adaptive technology to accomplish
daily activities
Severe - Require wheelchair.
- Have significant challenges in accomplishing daily activities
No CP - Has CP sign but impairment happens after completion of brain development
- Classified under incident eg. traumatic brain injury/encephalopathy
(4) Classification based on Gross Motor Function Classification System (GMFCS)
Level I Walk w/o limitations
Level II Walks with limitations:
- Cannot walk for long distance
- Difficulties in balancing , thus cannot run and jump
- May need mobility device
Level III - Walks with adaptive assistance
- Require hand held mobility device assistance (indoor)
- Use wheelchair outdoors
- Can sit by own
Level IV - Use of powered mobility assistance
- Sit supported
- Transported in wheelchair
Level V - Severe head and trunk control limitations
- Extensive use of assisted technology device
- Self-mobility by powered wheechair
Diagnosis
- Not easy to detect in early of life
- Suspected when:
- Risk/etiology affected the brain
- Delay in reaching normal development milestone
- Persistent remain of primitive reflex
(moro reflex, grasping reflex, stepping reflex à cycling movement)
- Less facial expression
- Abnormal gait & posture
Investigation
- Imaging studies (neonatal brain sonography: brain MRI)
- can help to evaluate brain damage and to determine those at risk for cerebral palsy BUT
support a definitive diagnosis of cerebral palsy are lacking
- EEG is useful in evaluating seizure condition
- Hearing and vision screening
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Management
There is no curative treatment. An early diagnosis can be useful to help get necessary support
(and funding) in place. Once the child has been diagnosed, then their care is taken care of by a
type of MDT known as the CDS (Child development services). This essentially comprises of the
paediatricians, social workers, physiotherapists, occupational therapists, psychologists,
dieticians etc.
Prognosis
- Cure is not possible
- Based on patern of evolving signs & child`s developmental progress
- HOPI
- SOCRATES about presenting complaint(s), TRO other differential diagnosis
- Paediatrics History
Birth history - Relevant antenatal, intrapartum & post-natal history
(look for possible - Maternal past history of miscarriages or infertility.
causes) - Pregnancy: hyperemesis, hypertensive disease of pregnancy,
teratogenic medications, placental problems, clinical evidence of, or
exposure to, infection (eg. TORCH), quality of fetal movements,
gestational age.
- Delivery: presentation (eg. breech, face), instrumental delivery, Apgar
score,resuscitation required, birth weight, oxygen supply, nursery care.
- Neonatal period: respiratory distress, feeding difculties, seizures,
hyperbilirubinaemia (phototherapy or exchange transfusion),
intraventricular haemorrhage (IVH), periventricular leukomalacia (PVL),
hydrocephalus, retinopathy of prematurity (ROP).
Immunisation Any delays, local doctor`s attitudes, parents` understanding of
importance of immunisation.
Developmental - Any developmental delay
- Assess gross motor, social, language
- Ascertain quality of attainment!
eg. bottom shuffling, development of early hand preference, splaying
of fingers when attempting grasp
Dietary Breastfeeding, weaning, feeding difficulty, food history
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- Current management
- Recent management in hospital
- Usual treatment at home
- Usual doctors seen
- Compliant with follow up?
- Frequency of therapy (physiotherapy, occupation therapy, speech therapy)
- Social History
- Impact on parents and siblings
- Disruption to family routine
- Family financial considerations (e.g. private health insurance, visits to multiple specialists,
cost of hospitalisations, surgical procedures, aids, home modifcations, drugs, benefts
received, such as Child Disability Allowance),
- Social supports (social worker, extended family, respite care, involvement of Spastic Centre,
self-help groups)
- Legal proceedings surrounding perinatal care
- Understanding of problems and prognosis: Parents` and siblings` understanding; degree of
education regarding CP
- Special school/sheltered workshop, self-help group
2) Physical Examination
A. General Observations
- Dysmorphic features (eg. chromosomal anomalies).
- Parameters: head circumference (often obvious microcephaly), weight (often failing to thrive), height
(usually decreased), progressive percentile charts.
- Posture (eg. fisting, increased extensor tone, asymmetric tonic neck reflex [ATNR], hemiplegic,
quadriplegic).
- Movement:
(a) involuntary (eg. choreoathetoid movements, dystonic spasms, seizures)
(b) voluntary (eg. immature gait pattern with wide base, up on toes, arms out for balance; hemiplegic,
diplegic gaits; note posturing of arms when walking)
- Asymmetry (eg. hemiatrophy: look at the size of the thumbnails and the great toenails for subtle clues
to asymmetry)
- Behaviour (eg. lack of interaction with environment, crying)
- Eye signs (eg. squint, nystagmus)
- Bulbar signs (eg. dysarthria, drooling)
- Interventions (eg. nasogastric tube, gastrostomy tube, scars of orthopaedic procedures)
- Clothing (eg. nappies in child over 4 years old)
- Peripheral aids (eg. wheelchair, splints, orthoses)
* Look for bed sores
B. Demonstration of signs of CP
- If possible, perform a standard gait examination.
- If the child cannot walk, but can crawl, look for abnormal crawling:
(a) those with spastic diplegia or quadriplegia—buttock crawling and `bunny-hopping` (jumping
while on knees)
(b) those with hemiplegia - asymmetrical crawl
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- Gross motor `180°manoeuvre`, incorporating primitive reflexes:
(a) lying supine (assess position adopted, e.g. ATNR)
(b) pull to sit by hands (to assess head lag and grasp)
(c) sitting (assess sitting ability, then lateral propping)
(d) hold up vertically, under axillae (to detect increased extensor tone, scissoring, automatic walking)
(e) tilt sideways (to assess head righting)
(f) ventral suspension (to detect excessive extensor tone)
(g) parachute reflex (to detect asymmetry)
(h) place prone (to detect back arching)
- Inspect carefully for tendon release scars
- Palpate muscle bulk in each muscle group
- Tone: as above, plus assessment of upper and lower limbs, and evaluation of contractures (eg. tight
hip adductors, and tendon achilles)
- Power: voluntary movement, functional power (grasp of toys, cloth cover test)
- Reflexes: the head should be held in the midline (eg. by an examiner) so that an ATNR does not give a
false impression of unilateral hypertonia; note whether there is any crossed adductor reflex, spread of
reflexes, clonus or upgoing plantar responses.
C. Complications of CP
- Measure the head (for microcephaly, or macrocephaly due to hydrocephalus)
- Check the vision, visual felds and extraocular movements (for myopia, squint)
- Check the hearing (for sensorineural deafness)
- Check the ears (for chronic serous otitis media)
- Ask to check the gag refex (bulbar dysfunction)
- Look at the teeth (for dental caries)
- Look at the back (for kyphoscoliosis)
- Inspect and auscultate the chest (for chest infection)
- Palpate the abdomen (for constipation)
- Examine the hips (for dislocation)
- Screen nutritional status (demonstrate fat and protein stores)
- Perform a functional assessment for activities of daily living (eg. ofer cup, spoon, fork, knife, comb,
toothbrush; ask the child to put on a piece of clothing)
- Assess other areas of development (social & language)
- Summary
1) Classify type of CP based on :
- Motor function
- Topographical distribution
- Severity level
- GMFCS
2) List associated problems
- Poor swallowing, chest infection, urinary incontinence, behaviour problems, contractures etc.
- Functional status: ADL, Mobility
- Current management
3) Postulate underlying causes (if confident)
à Antenatal/perinatal/Postnatal
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3) Discussion
- Differential diagnosis for Global Developmental Delay:
1. Hypothyroidism
2. Chromosomal anomaly
3. Structural brain disorder
4. Cerebral Palsy
5. Congenital infections - TORCHES
6. Neurocutaneous syndrome
7. Inborn error of metabolism
8. Postnatal injury eg. Head injury, intracranial bleed, HIE
9. Muscular dystrophy
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Febrile Convulsion/ Seizure
Definition:
Seizure - Clinical event in which there is a sudden disturbance of neurological
function in association with abnormal or excessive neuronal discharge
Epilepsy - Continuing tendency to have seizures (recurrent seizure) without
provoking factors
Febrile - Seizure associated with fever
convulsion - Absence of other causes (eg. metabolic disturbance, trauma) and no
intracranial infections (eg. meningitis, encephalitis)
- Diagnosis of exclusion
Epidemiology:
- Occurs in about 3% of children: 6 months to 6 years of age
- Earlier the age of occurence, the higher risk of recurrence
- Genetic predisposition (10-20% have positive family history including relatives)
Focal seizures:
Clinical features: - Parietal: numbness/tingling
- Have recent infection hx such as URTI, Otitis media, UTI, AGE sensation
- Raised in temperature rapidly - Temporal: deja vu
- Frontal: wave-like sensation in
- Fitsà generalized tonic-clonic seizure
head
- Occipital: visual disturbance/
hallucination
Classification:
Simple (75%) Complex(25%)
- Last for <5 minutes - Last >5 minutes
- NO focal seizures - Focal seizures present
- NO recurrence in 24 hrs - Multiple seizures in 24 hrs (>1 episode)
- NO brain damage - Risk of subsequent epilepsy (30%)
- Generelised tonic-clonic - Intellectual performance may be affected
- Normal development - Residual neurological deficit post ictally eg.
- No encephalopathy Todd`s paralysis*
- No intracranial pathology - Abnormal development
- Usually during 1st day of fever - No encephalopathy
- Usually aged between 6 months - 6 y/o - No intracranial pathology
- Positive family history of febrile convulsion- Usually occurs other than 1st day of fever
- Normally in those aged <6 months or >6
years old
- Family history of epilepsy or epilepsy
syndrome eg. GEFS+**
* Todd`s paralysis: paralysis of the involved limbs after seizure
** GEFS+ (Generalized Epilepsy with Febrile Seizure Plus)
- An unusual epilepsy syndrome. It describes families who have several members from
different generations with epileptic seizures. The epileptic seizures nearly always start after a
family member has had febrile convulsions.
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Complications:
Epilepsy - Occurs in ~1% of patients
- Risk factors:
- Neurodevelopmental abnormality eg. cerebral palsy
- Complex febrile convulsion
- Family history of epilepsy
- Brief duration between onset of fever and initial convulsion
Recurrence - Recur in ~15% in the same illness
- Risk of recurrence:
- Family history of febrile convulsion
- Age <18 months (early onset)
- Low degree of fever (<40⁰C) during 1st febrile convulsion
- Brief duration (<1 hour) between onset of fever and convulsion
Differential Diagnosis:
Infection - Meningitis/encephalitis
- UTI
Trauma - Brain lesion (in head trauma, intracranial bleed)
Metabolic - Hypoglycemia
- Hypocalcaemia
- Hypomagnesemia
- Hypo/hypernatraemia
- Inborn error of metabolism (IEM)
Others - Poisons/toxins/drugs
- Hypoxic ischaemic insult
- GEFS+
- A group of AD disorder with variable phenotypes
- Disorders are divided into 4 main groups (1,2,3, and SCN2A), each
associated with defect in either α, β, γ subunit. Several genetic defects
are implicated.
- GEFS+ may mimic febrile seizure in the early stage
- Seizure usually extend beyond 6 years old, there may be intercurrent
afebrile seizures & there may be other seizure in addition to the typical
generalized tonic-clonic seizure of febrile seizure.
- Consequently psychomotoe retardation may accompany GEFS+
Investigations:
Blood - FBC (evidence of infection)
- BUSE (hypo/ hypernatraemia)
- Serum calcium & magnesium
- Dextrostix or RBS (hypoglycemia)
- Blood C & S (for evidence of septicaemia)
Urine - U-FEME + C & S (exclude UTI)
LP - Indicated in patients <18 months (subtle S & S)
- TRO meningitis & encephalitis
EEG - Not indicated even for those with multiple recurrence or with complex
febrile convulsions
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Lumbar Puncture
- Must be done (unless contraindicated)
- Any signs suspicious of intracranial infection
- Prior antibiotic therapy
- Persistent lethargy and not fully interactive 6-8 hrs after the seizure
- Strongly recommended:
- <12 months old
- First complex febrile convulsion
- In district hospital without peadiatrician
- If parents have a problem with bringing the child again to hospital in event of deterioration
at home
Management:
Not all children need to be admitted. The main reasons for admission are:
- TRO intracranial pathology especially infections
- Fear of recurrent fits
- To investigate and treat the cause of fever besides meningitis/encephalitis
- To ally parental anxiety, especially if they are staying far from hospital
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Management at ward
13. Put on fit chart
14. Reassess patient and risk of recurrence
15. PCM
16. teach home management
17. Educate parents on monitoring body
temperature and prognosis of febrile seizure
18. Prophylatic anticonvulsant
- Phenobarbitone/sodium valproate
- Indications ( not absolute):
- Severe seizures or high risk of recurrence
- Patient <1 year old
- Patient with risk factors for AFS
- Excessively anxious parents
Status Epilepticus:
Immediate 1. Assess cardiorepiratory function (ABC)
management 2. Oral airway & administer oxygen
3. Establish IV lines, draw blood for glucose, BUSE & anticonvulsant
levels (in treated patients)
4. IV infusion of glucose (50% glucose bolus)
5. IV diazepam ( 0.25-0.5mg/kg) at rate no faster than 2 mg/min
- Rectal diazepam (0.5-0.75 mg/kg) if IV line not established
6. Monitor vital functions
- Correct any metabolic disturbances (eg. glucose, electrolytes)
- Lower body temperature
- Tracheal intubation & assisted ventilation may be necessary
2nd Step IV Phenytoin (20mg/kg) over 20 mins
Management - Investigate possible causes of SE that may require emergency Rx
If seizures NOT IV Phenobarbitone (10-20 mg/kg)
controlled - Monitor BP & RR (esp if pts received diazepam during initial Mx)
Resistant Seizures 1. Further dose of IV Phenobarbital (if patient still fitting)
- May be necessary to exceed usual recommended upper therapeutic
level of 50 mg/mL
- Monitor for respiratory distress
2. Close monitoring
- EEG monitoring
- Closed supervision (specialized nursing & medical personnel)
3. Consider other anticonvulsant
- eg. Paraldehyde, Lignocaine, Sodium valproate
4. IV barbiturate or halothane + neuromascular blockade
- Induce barbiturate coma if the above drugs fail to terminate seizure
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Epilepsy
Pathophysiology:
- Instability of neuronal cell membrane (imbalance excitatory & inhibitory neurotransmission) →
Paroxysmal neuronal discharge which produces the clinical seizure (neurological disturbances)
Aetiology:
- Genetic
- Congenital malformation of the brain
- Perinatal complications (brith asphyxia, trauma, intracranial haemorrhage)
- Neurocutaneous syndrome
- CNS infections (meningitis, encephalitis, brain abscess)
- Trauma
- Cerebrovascular accident
- Neoplasm
- Metabolic (hypoglycaemia)
- Any prolonged seizure
* About 50% of epileptic cases, no cause can be found
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1) Partial - Simple partial (consciousness retained) may involve motor, sensory,
Seizure autonomic, psychic
- involve one - Complex partial (consciousness impaired)
region of - Partial seizure with secondary generation
cortex - `Dyscognitive seizure` is used when difficult to distinguish simple & complex
*According to ILAE 2015 (UpToDate), the terms simple partial, complex partial & secondarily
generalized have been eliminated, since they were difficult to define pragmatically & were often
used incorrectly. Instead, the proposal uses various descriptors of focal seizures to describe an event
more precisely. Examples of preferred descriptors include:
- Without impairment of consciousness or awareness
- Involving subjective sensory or psychic phenomena
- With impairment of consciousness or awareness, or dyscognitive
- Evolving to a bilateral convulsive seizure
.
2) Generalised - Absence
Seizure - Tonic-clonic
- involve both - Myoclonic
hemispheres - Tonic
- Clonic
- Atonic
3) Unclassified - Epileptic/Infantile spasms
Unclassified epilepsies
Infantile spasms - Usually occurs in infancy (4-6 months)
- Triads of attacks:
- Lightning attack (sudden, severe myoclonic movement of mody, legs bend
(flexor involved more severe than extensor)
- Nodding attack (seizure of throat & neck flexor muscle, during which chin
is fitfully jerked towards breast or head is drawn inwards)
- Salaam or jack-knife attack (flexor spasm with rapid bending of head &
torso forward, simultaneous raising & bending of arms while partially
drawing hands together in front of chest/flailing, similar to ceremonial
greeting)
- Last for several secondas & often occur in multiple burst spasms
- West syndrome (triads of infantile spasms, pathognomonic hypsarrhythmia
EEG pattern & developmental regression)
- Prognosis is poor & intellectual handicap frequently follows
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Investigations:
- Baseline blood & urine test (TRO hypoglycaemia, hypocalcaemia, systemic illness)
- ECG (suspect cardiac dysrhythmia)
- EEG
- Indicated to support the clinical diagnosis of epileptic seizures, classify the epileptic
syndrome, selection of anti-epileptic drug and prognosis
- Helps in localization of seizure foci in intractable epilepsy
- Normal EEG does not rule out epilepsy, epileptiform EEG does not indicate pts had clinical
seizure
- Neuroimaging (preferably MRI) indications:
- Epilepsy occurring in the first year of life, except febrile seizures
- Focal epilepsy except benign rolandic epilepsy
- Developmental delay or regression
- Intractable epilepsy
- Progressive neurological symptoms & signs of raised ICP
Diagnosis:
- Primarily based on a detailed history of characteristics of fits from eyewitnesses
- Any factor which suggest patient is prone to fits
- Neurological examination is essential First Aid Measures during a Seizure (Advise for Parents/
Teachers)
- Differential diagnosis: - Do not panic, remain calm. Note time of onset of the seizure
- Loosen the child`s clothing especially around the neck
- Breath holding attack - Place the child in a left lateral position with head lower than
- Refelx anoxic seizure the body
- Vasovagal syncope - Wipe any vomitus or secretion from the mouth
- Cardiac arrhythmias - Do not insert any object into the mouth even if the teeth are
- Migraine clenched
- Do not give any fluids or drugs orally
- Benign paroxysmal vertigo - Stay near the child until the seizure is over and comfort the
child as he/she is recovering
Management:
A) Principle of anti-epileptic drug therapy for Epilepsy):
- Treatment recommended if ≥ 2 episodes (recurrence risk up to 80%)
- Attempt to classify the seizure type(s) and epileptic syndrome. Monotherapy as far as possible.
- Choose most appropriate drug, increase dose gradually until epilepsy controlled or maximum
dose reached or side effects occur.
- Add on the second drug if first drug failed. Optimise second drug, then try to withdraw first
drug. (alternative monotherapy)
- Rational combination therapy (usually 2 or maximum 3 drugs) eg. combines drugs with
different mechanism of action and consider their spectrum of efficacy, drug interactions &
adverse effects.
- Drug level monitoring is not routinely done (except phenytoin), unless non-compliance,
toxicity or drug interaction is suspected.
- When withdrawal of medication is planned (generally after being seizure free for 2 years),
consideration should be given to epilepsy syndrome, likely prognosis and individual
circumstances before attempting slow withdrawal of medication over 3-6 months (maybe
longer if clonazepam or phenobarbitone). If seizures recur, the last dose reduction is reversed
and medical advice sought.
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B) Selecting antiepileptic drugs according to seizure types:
Seizure type First line Second line
Focal Seizures
Carbamazepine Valproate Lamotrigine,Topiramate, Levetiracetam, Clobazam,
Phenytoin, Phenobarbitone
Generalized Seizures
Tonic-clonic / clonic Valproate Lamotrigine,Topiramate, Clonazepam,
Carbamazepine1, Phenytoin1, Phenobarbitone
Absence Valproate Lamotrigine, Levetiracetam
Atypical absences, Valproate Lamotrigine,Topiramate, Clonazepam, Phenytoin
Atonic, tonic
Myoclonic Valproate Clonazepam Topiramate, Levetiracetam Clobazam, Lamotrigine2,
Phenobarbitone
Infantile Spasm ACTH, Prednisolone, Vigabatrin3 Nitrazepam, Clonazepam, Valproate,Topiramate
Footnote:
1, May aggravate myoclonus/absence seizure in Idiopathic Generalised Epilepsy.
2, May cause seizure aggravation in Dravet syndrome and JME.
3, Especially for patients with Tuberous Sclerosis.
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E) In patients with `Intractable Epilepsy`, re-evaluate:
- Is it a seizure or a non-epileptic event?
- Antiepileptic drug dose not optimised
- Poor compliance to antiepileptic drug.
- Wrong classification of epilepsy syndrome, thus wrong choice of antiepileptic drug
- Antiepileptic drug aggravating seizures
- Lesional epilepsy, hence a potential epilepsy surgery candidate
- Progressive epilepsy or neurodegenerative disorder
F) When to refer to a Paediatric Neurologist?
- Refer immediately (to contact paediatric neurologist)
- Behavioural or developmental regression
- Infantile spasms.
- Refer
- Poor seizure control despite monotherapy with 2 different antiepileptic medications
- Difficult to control epilepsies beginning in the first two years of life
- Structural lesion on neuroimaging
G) Advice for Parents
- Educate and counsel on epilepsy
- Emphasize compliance if on an antiepileptic drug
- Don`t stop the medication by themselves. This may precipitate breakthrough seizures
- In photosensitive seizures: watch TV in brightly lit room. Avoid sleep deprivation
- Use a shower with bathroom door unlocked
- No cycling in traffic, climbing sports or swimming alone
- Know emergency treatment for seizure
- Inform teachers and school about the condition
Definition:
Failure of normal fusion of the neural plate to form neural tube during the first 28 days following
conception.
Epidemiology:
- Based on Malaysian National Neonatal Registry 2013, prevalence of NTD was 0.42 per 1000
livebirths, highest among indigenous people of Sarawak, lowest among Chinese descent
- Most common type of NTDs: Anencephaly (0.19/1000), Spina bifida (0.11/1000), Encephalocele
(0.07/1000)
- Associate with high mortlity, long-term monitoring of NTD with folic fortification is
recommended.
Overview:
Brain
Spinal Cord
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Spinal Meningocele - Protrusion of meningeal sac without any neural element via a
spinal defect
- Neurological symptoms & signs are absent
- Often present as a swollen fluctuant mass covered with a full
thickness of skin with positive transilluminatoin test
- Can be repaired surgically & have good prognosis
Spinal Myelomeningocele - Failure of posterior neural tube closure causing protrusion of
meninges with neural tissue & CSF
- Can be presented with wide range of problems (refer below)
- Closure of spinal defects should be done within 1st week of life
- Severely affected children may develop handicap after active Tx
- Subsequent care is best managed by multidisciplinary teams with
the aim of improving their quality of life
Spinal bifida occulta - Failure of closure of vertebral arch occurs in ≥5% population
- Mostly asymptomatic (incidental finding on X-ray)
- Commonly in lumbosacral region with overlying skin changes
(tuft of hair, lipoma, birth mark or dermal sinus)
- Whenever associated with neurologic involvement, it is termed
occult/closed spinal dysraphism
Occult/closed spinal dysraphism - Spina bifida occulta with distortion of spinal cord or spinal roots
by fibrous bands and adhesions, intraspinal lipoma, dermoid or
epidermoid cyst, fibrolipoma, tethered cord/ diastematomyelia
(most common)
- With growth, it may cause neurological deficits of bladder, bowel
function & lower limbs
- Neurosurgical relief of tethering is usually indicated
Problem in Myelomeningocele:
Problem Management
Paralysis of legs (variable) - Physiotherapy (prevent joint contracture &
- Depends on level of lesion (muscle innervated by strengthen paralysed muscles)
nerve below lesion will be paralysed) - Walking aids & wheelchair (permit mobility)
Dislocation of hip & talipes equinovarus (Imbalance)
- Due to partial denervation of LL
Sensory loss (anaesthesia) - Skin care
- Dermtomes below level of lesion - Prevent development of skin lesion & ulcer
- May lead to pressure sores
Neuropathic bladder (bladder denervation) - Indwelling catheter or intermittent
- Can lead to hydronephrosis & UTI, renal failure, catheterisation
reflux nephropathy - Medication (Oxybutinin & Ephedrine)
- May improve bladder function & dribbling
- Regular urine check for UTI
- Prophylactic antibiotics can be given
- Monitor hydronephrosis & renal failure (USS)
Neuropathic bowel (bowel denervation) - Regular toileting & suppositories
- Laxatives
Scoliosis - Surgical repair
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Spina bifida Short Case (Template)
- General planning for this case:
- Demonstrate the level of lesion
- Functional assessment (ability to walk)
- Look for associated abnormalities or complications (hydronephrosis, hydrocephalus)
Q: `This boy has spina bifida. Would you please assess his/her function above the level of lesion?`
Physical Examination
Introduce self - Interact with child, gain impression of development
General Inspection - Alertness
- Cry (high-pitched with ACM)
- Nasogastric tube (severe ACM)
- Respiratory distress
- Hoarseness of voice (severe ACM)
- Posture (deformity eg. TEV, dislocated hips)
- Muscle bulk (LL vs UL)
- Movement (LL vs UL, Ataxia - ACM)
- Head (Size, Shunts, Eye signs)
- Skin
Back - Lesion
- Site (closure scar if have, describe)
- Spinal deformity (scoliosis, kyphosis)
- Scars (eg. fixation rod)
Lower limbs (LL) - Inspect, Palpate, Tone, Power, Reflexes, Joint movement, Sensation
Abdominal & pressure - Inspect (scars eg. VP shunt; distention-lax muscles, ileal conduit,
areas patulous
anus, dribbling of urine, Tanner staging-precocity, Pressure sores
- Palpate (kidney: hydronephrosis)
- Percuss (bladder: urinary retention)
- Check (Abdominal reflexes, Anal wnk, Anal tone)
- Urinalysis (detect CRF, shunt nephritis, UTI)
Head - Inspect (Size, Shape eg. frontal prominence, Signs of hydrocephalus:
scalp vein prominence, shiny skin, sun-setting eyes, shunt scars)
- Measure head circumference & request progressive percentiles
- Palpate (sitting up): Fontanelles, Sutures, Shunt (trace tubing)
Eyes - Inspect (Nystagmus: severe ACM, Squint eg. with ACM)
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- Visual acuity
- External ocular movement (CN6 palsy, Impaired upward gaze: Parinaud`s
syndrome with hydrocephalus)
- Fundi (Papilloedema: raised ICP, Optic atrophy: long-standing raised ICP)
Hearing & bulbar function - Assess hearing
- Check lower CN 9,10,11,12
- Suck & swallow reflexes
- Gag reflex (if cannot swallow)
- Tongue atrophy
Upper limbs (UL) Full examination for signs of syringomyelia
Blood pressure Hypertension (CRF)
Chest Full examination of praecordium & lung fields for signs of heart failure dt:
- Hypertension (CRF)
- Cor pulmonale (kyphoscoliosis)
Functional/developmental - Assess ADL in older children
assessment - Perform developmental assessment in infants
Details of possible findings on Spina Bifida examination
Respiratory signs - Stridor (severe ACM)
- Apnoea (severe ACM)
- Tachypnoea (aspiration pneumonia, heart failure)
Skin - Pressure sores
- Scars (eg. VP shunts, tendon releases)
Growth parameters - Head circumference (increased in hydrocephalus)
- Height (usually decreased)
- Arm span (use instead of height, may be normal for age)
- Weight (obese for height, not for arm span)
Lower Limbs - Inspection
- Muscle bulk wasting
- Joint deformity (eg. dsislocated hips, talipes)
- Contractures
- Scars (eg. tendon release, transfers or osteotomies)
- Spontaneous movement
- Palpation (muscle bulk, each muscle compartment)
- Check tone, power, reflexes (including with reinforcement)
- Joint movement
- Hip (eg. fixed flexion deformity, check for dislocation last)
- Knee (eg. fixed hyperextension)
- Ankle (eg. fixed dorsiflexion)
- Check hip for dislocation
- Sensation: demonstrate sensory level (may use a new pin in infants, full
examination in older children)
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Hydrocephalus
Definition:
Obstruction to the flow of CSF → leading to dilatation of the ventricular system proximal to the
site of obstruction.
Aetiology:
- Can be either due to;
- Non-communicating (Obstructive hydrocephalus)
- Obstruction within the ventricular system or aqueduct → Interrupt with CSF flow
- Communicating
- Obstruction at the arachnoid villi → Failure of CSF reabsorption
* Rarely due to overproduction of CSF (choroid plexus papilloma)
Non-communicating Communicating
- Congenital malformation - Subarachnoid haemorrhage (SAH)
- Aqueduct malformation/stenosis - Decreased CSF reabsorption
- Danky-Walker Syndrome - Meningitis: Pneumococcal, Tuberculous
- Atresia of the outflow foramina of the 4th (follow by adhesion & obstruction to the flow
ventricle of CSF)
- Arnold-Chiari malformation - Intrauterine infection (Toxoplasmosis, CMV)
(medulla oblongate & cerebellum protrude - Choroid plexus papilloma (rare)
into the spinal canal) - Increased CSF production
- Posterior fossa neoplasm
- Medulloblastoma
- Cystic cerebellar astrocytomas
- Vascular malformation
- Intraventricular haemorrhage (preterm)
(Blood in the CSF may give rise to adhesion
which obstruct the flow of CSF)
*Some can cause both non-communicating and communicating hydrocephalus
Clinical features:
- Depend on 3 factors:
- Whether the fontanelle & sutures have fused
- Whether the obstruction is acute vs chronic
- Underlying pathology cause
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- S & S of increased ICP (usually in older chidren > 2 years old:
Symptoms Signs
- Headache (worse on lying down, cough) - Bradycardia *Cushing`s reflex
- Irritable, non-stop crying - Hypertension
- Morning vomiting - Papilledema (if present for long time)
- Changes in personality or mood & school - Diplopia (CN 6 paresis)
performance
Complications:
- Seizure
- Failure to thrive (FTT)
- Mental retardation - Cerebral atrophy
- Neurological deficit
- Cranial nerve palsy
- Cerebellar ataxia
- Affected limb
Investigation:
- Radiology
- Cranial USS (Look for evidence of ventricular dilatation)
- CT/MRI
- Ophthalmoscopy - Look for evidence of papilledema
- Centile charts - Head circumference should be monitored over time
Diagnosis:
- Usually can be diagnosed by history & clinical examination
- Can be diagnose antenatally by USS screening or routine cranial USS in preterm
Management:
- Head circumference should be monitoring over time on centile charts
- Aims of intervention are:
- Treat to the cause of hydrocephalus
- Symptomatic relief
- Minimise neurological damage
- Mainstay of management is ventricular shunt
(either ventriculo-atrial or ventriculo-peritoneal)
- Endoscopy & ventriculostomy can now be performed alternatively
- Complications:
- Shunt malfunction
- Infection (particularly with coagulase-negative Staphylococcus)
- Overdrainage of fluid
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Neurocutaneous Disorders
Introduction:
- Syndromes involving abnormalities of skins and nervous systems (which have common
ectodermal origin)
- Include Neurofibromatosis Type 1, Tuberous sclerosis & Sturge-Weber syndrome
A) NEUROFIBROMATOSIS
Neurofibromatosis 2 (NF-2):
- Central neurofibromatosis
- Due to mutation on different gene on chromosome 22
- Much rarer form (affecting1 in 40000 live births)
- Characteristic presentation:
- Bilateral acoustic neuromata (may cause deafness)
- Other presentations: Cerebellopontine angle syndrome with a facial (VII) nerve
paresis & cerebellar ataxia
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B) TUBEROUS SCLEROSIS
Introduction:
- Autosomal dominant inherited disorders
- 70% cases represent new mutation
- Affecting 1 in 7000 live births
Cutaneous features:
- Depigmented ash leaf shaped patches: Fluoresce under Wood`s light
- Roughened patches (shagreen patches): usually over lumbar spine
- Adenoma sebaceum (angiofibromata): In butterfly distribution before 3 years old
* Most people carry no features other than the cutaneous stigmata
Neurological features:
- Infantile spasm
- Developmental delay
- Epilepsy (often focal)
- Intellectual impairment (learning difficulties with autistic features)
126
Other features:
- Subungual fibromata(fibromata beneath the nails)
- Phakomata (dense white area on the retina)
- Rhabdomyomata of the heart
- Polycystic kidneys
- Gliomatous change in CNS
C) STURGE-WEBER SYNDROME
- Sporadic disorder characteristics by;
- Unilateral facial naevus lesion (Port-wine stain) in trigeminal nerve distribution
- Leptomeningeal angiomatosis
- There are abnormal blood vessels over the brain surface: may be associate with seizures,
hemiplegia and learning difficulties
- CT brain
- Unilateral intracranial calcification with a double contour `rail-road ` subcortical calcification
- Associated parenchymal volume loss due to cortical atrophy
- Evident enlargement of calvarial and regional sinus
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Muscular Dystrophy
Epidemiology:
- Commonest cause of muscular dystrophy
- Incidence is about 1 in 4000 male infants (UK)
Cytogenetic:
- Inherited as an X-linked recessive disorder (thus only in males)
- Deletion of chromosomal material on the short arm of X-chromosome (Xp21 site)
- Known to code a protein called dystrophin to maintain the integrity of muscle cell wall
- Deficiency of dystrophin causes
- Influx of Ca2+
- Breakdown of calcium-calmodulin complex
- Excess free radicals being released
- One-third are new mutations
Clinical Features:
- Average age of diagnosis is 5.5 years
Symptoms Signs
Early childhood - Gower`s sign
- Delayed walking - Difficulty in getting up from sitting position
- Difficulty in getting up from sitting position due to weak proximal muscles
- Difficulty in climbing - Waddling gait
- Tendency to falling - Tendency to walk on toes
- Weak anterior tibial muscle
Early School Years - Marked lumbar lordosis
- Slower & clumsy than their peers - Scoliosis
(Learning difficulties) - Pseudo-hypertrophy (calf muscle)
- Non-ambulant by the age of 10-14 years - Selective atrophy
(Atrophy & muscle weakness) - Brachioradialis
- Sternal head of pectoralis major
- Depressed reflexes (except ankle jerk)
Investigation:
128
Complication:
- Scoliosis (common complication)
- Inability to walk (Paralysis)
- Deaths (usually in the late teens or early 20s)
- Respiratory failure (Nocturnal hypoxia due to weak intercostal muscles)
- Cardiomyopathy
Management:
Conservative Operative
- Prevention of contracture - Lengthening of Achilles tendon
- Passive stretching - Facilitate ambulation
- Provision of night splints - Management of scoliosis
- Maintenance of muscle power by - Insertion of metal rod into the spine
appropriate muscle exercise
- Prolonged mobility
- Delays the onset of scoliosis
- Orthoses
- Prolongation of walking
- Management of scoliosis
- Maintaining good sitting posture
- Trunchal brace, moulded seat
- Respiratory aids
- Indicated when weakness of intercostal
- Muscles develop
- Provision of special schooling
- Emotional support
Clinical features:
- Similar to DMD but clinically the disease progresses more slowly
- Average age of onset = 11 years old
- Inability to walk in late 20s
- Deaths in early 40s
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PART IV
CARDIOLOGY
Congenital Heart Disease
Introduction:
- Commonest congenital malformation seen in children, prevalence of 8-10/1000 live birth.
- Most common type of heart defect is VSD.
- About 95% of babies born with a non-critical CHD are expected to survive to 18 years of age.
- About 69% of babies born with critical CHDs are expected to survive to 18 years of age. [CDC 2012]
- In 2006, a study on under five deaths in Malaysia had showed that 10% mortality was directly
related to CHD. [MyCDHR]
- Most structural defects are now diagnosed non-invasively via echocardiography.
- About 10-15% have complex lesions with more than one cardiac abnormality.
- About 10-15% also have a non-cardiac abnormality.
Aetiology:
Cardiac abnormalities Frequency
Maternal disorders
- Rubella infection - PDA, Peripheral PS 30-35 %
- SLE - Complete heart block 35 %
- GDM/ DM - Increased in overall incidence 2%
Maternal drugs
- Warfarin therapy - PS, PDA 5%
- Fetal alcohol syndrome - ASD, VSD, TOF 25 %
Chromosomal abnormalities
- Down syndrome (Trisomy 21) - AVSD, VSD, PDA, ASD, TOF 30 %
- Turner`s syndrome (45 XO) - AS, COA 15 %
- Chromosome 22q11, 2 deletion - Aortic arch abnormalities, TOF
- William`s syndrome - Supravalvular AS, Peripheral PS
(chromosome 7 microdeletion)
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Congenital heart defect may be presented as/via:
- Antenatal & postnatal diagnosis
- Heart murmur
- Cyanosis
- Heart failure
1) Antenatal diagnosis - Detailed ultrasound scan done at the end of first trimester
Postnatal diagnosis - Routine echocardiogram done on high-risk children:
- With Down syndrome
- Siblings with congenital heart disease
- Mother with congenital heart disease
2) Heart murmur - Murmurs from cardiac defect have to be differentiated from
innocent murmurs
- 2 main types:
- Ejection murmurs (from the outflow tracts)
- Venous hum (from head & neck veins)
- Characteristics of an innocent murmurs:
- Soft, left Sternal edge, Small area, Systolic, normal heart Sound,
aSymptomatic patient (6S)
3) Cyanosis - Peripheral cyanosis (blueness of hands & feet due to poor perfusion)
- Central cyanosis (concentration of reduced Hb >5g/dl in capillary blood
or >3g/dl in arterial blood, less pronounced if the child is anemic)
- Congenital heart disease which cause neonatal cyanosis:
Reduced pulmonary Tetralogy of Fallot
blood flow Tricuspid atresia
(Obtructed) Pulmonary atresia
Abnormal mixing Transposition of great artery (TGA)
(Discordant arterial Hypoplastic left heart syndrome
connection) AVSD (complete)
Total anomalous pulmonary venous drainage
- Diagnosis can be confirmed by HYPEROXIA (nitrogen wash) test
- Hypoxaemia caused by cardiac defects not corrected by increasing
inspired fraction of inspired oxygen (FiO2)
- Child with FiO2 100%, right radial arterial PaO2 <150mmHg suggests
cyanotic CHDs.
- Most infants with cyanotic heart disease in first few days of life are duct-
dependant. Thus, maintenance of ductal patency with IV Prostaglandin
(Prostin) is the key to early survival of these children.
131
- Causes of heart failure in:
Neonates Infants
- Usually due to obstruction to - Usually due to left to right
the left ventricle (duct- shunts
dependant) - Large VSD, AVSD, large PDA
- Hypoplastic left heart, critical
aortic stenosis, severe
coarctation
Investigation:
- Chest X Ray
A normal CXR and ECG does not exclude CHD
- ECG
- Echocardiography ( look at heart structure ) + Doppler ( look at the flow )
- Cardiac catheterisation mainly used for hemodynamic measurements and intervention
- Pulmonary vasculature
- Plethoric: TGA, TAPVC, Truncus arteriosus
- Oligaemic: TOF, Tricuspid atresia
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Acyanotic Congenital Heart Disease
Clinical features:
Symptoms Signs
- Small VSD (Asymptomatic) - Small VSD
- Large VSD - Loud PSM at left sternal edge
- Heart failure - Thrill at Left sternal edge
- FTT especially in 2nd to 3rd month of life - Large VSD
- Recurrent chest infections - Soft PSM at left sternal edge/ No murmur
- Poor feeding - Loud P2 with pulmonary hypertension
- Diaphoresis - Cardinal signs of heart failure:
- Dyspnea - Tachycardia
- Tachypnoea
- Hepatomegaly
- Cardiomegaly
Investigations:
Chest X Ray - Small VSD (Normal)
- Large VSD
- Cardiomegaly
- Enlarged pulmonary arteries
- Plethoric lung fields
- Pulmonary oedema (may present)
133
ECG - Small VSD (Normal)
- Large VSD
- LV Hypertrophy/ biventricular hypertrophy
- Signs of pulmonary hypertension (upright T wave)
Echocardiography - Demonstrates anatomy of defect in
heart
- Assess its haemodynamic effects
using Doppler
- Pulmonary hypertension in large
defects
Management:
Small VSD Large VSD
- Advise subacute bacterial endocarditis - Medical
(SBE) prophylaxis - Control heart failure
- Surgery (indicated if) - Oxygen therapy
- The child has an episode of infective - Fluid restriction, nasogastric feeding if
endocarditis (IE) acutely unwell
- There is any sign of progression to - Drugs ( furosemide, spironolactone, thiazide,
pulmonary hypertension ACE inhibitor )
- Prolapsed aortic valve - Subacute bacterial endocarditis prophylaxis
- Surgical
- Indications: severe symptoms with failure to
thrive; pulmonary hypertension with possibly
progression to pulmonary vascular disease;
VSD with PS/AR
- Approaches:
- Transcatheter closure (Amplatzer occluder)
- Dacron or PTFE (Gore-Tex or Impra) patch
- Pulmonary artery banding(↓pulmonary HPT)
Complications:
- Aortic regurgitation
- Infective endocarditis
- Eisenmenger`s syndrome (R>L shunt)
- Infundibular stenosis
- Pulmonary Hypertension
Eisenmenger syndrome
- Occurs when there is cyanosis due to R > L shunting as a result of increased pulmonary blood flow,
pulmonary hypertension, right ventricular hypertrophy and pulmonary vascular disease.
- Complications:
- Hyperviscosity secondary to polycythaemia (headache, dizziness, visual disuturbance)
- Haemoptysis due to pulmonary infarct/ rupture of pulmonary arterioles
- Cerebral infarct due to embolism/ venous thrombosis
- Congestive cardiac failure (CCF)
134
2) Atrial Septal Defect (ASD)
- 4 types: (2 major)
Ostium Secundum (80%, most common)
- Deficiency of the foramen ovale and
surrounding
Ostium Primum
- Deficiency of the atrioventricular septum and
is associated with abnormal atrioventricular
valves
- Inter-atrial communication between atrial
septum and AV valves
Sinus venosus
- Occurs at SVC and RA junction, drainage of
pulmonary vein into RA instead of LA
Coronary sinus (Rarest)
- Located within coronary sinus, passes behind
LA.
Clinical features:
Symptoms Signs
- Mostly asymptomatic - Fixed split S2 (stroke volume equal in both
- Recurrent chest infections inspiration & expiration)
- Heart failure - Ejection Systolic Murmur at upper left sternal
- Arrhythmias in adult (4th decades onwards) edge (↑flow via pulmonary valve)
- Paradoxical embolus (when straining, it can - Apical pansystolic murmur from AV valves
cause clot to go from right to left causing regurgitation (ASD primum)
stroke ) - Loud P2
Investigation:
CXR Echocardiography Echocardiography
- Cardiomegaly ± pulmonary - Right axis deviation - For haemodynamic
plethora - Partial/complete RBBB measurements and assess ASD
- RV hypertrophy size
(sometimes)
135
Management:
- Nearly all ASDs require closure
- Surgical
- Transcatheter
- Usually done at 4th or 5th year of life, earlier if symptomatic
Complications:
- Eisenmenger`s syndrome
- Paradoxical embolism (rare)
136
3) Patent Ductus Arteriosus (PDA)
- Ductus arteriosus connects pulmonary
artery to the descending aorta. it usually
closes shortly after birth with decrease
in prostaglandin in blood
Clinical features:
Symptoms Signs
- Asymptomatic in small PDA - Collapsing pulse (wide pulse pressure)
- Symptoms of heart failure in large PDA - Continuous murmur, beneath the left clavicle
- In preterm infants, the murmur may be soft and
systolic - usually presents with a collapsing pulse
and failure to wean off the ventilator (wet lung)
Investigations:
CXR & ECG Echocardiography Cardiac catheterisation
- Depends on the size of PDA - Evaluates heart structure & - For haemodynamic
If large, CXR & ECG may show function, assess blood flow measurements and closure
findings similar to large VSD pattern, PDA opening size of PDA (therapeutic)
Management:
Conservative Operative
- Fluid restriction - Surgical ligation
- Pharmacological - Transvenous occlusions with a coil device
- Indomethacin (PG synthase inhibitor) * Depending on symptom severity, PDA size &
- Diuretics (if heart failure) body weight
* In asymptomatic PDA, closure is recommended to eliminate risk of endocarditis.
137
B) Without left to right shunt
Symptoms: Symptoms:
- Usually asymptomatic - Depends on severity:
- A small number of neonates with critical PS - Mild à asymptomatic
have a duct-dependant pulmonary - Critical à severe heart failure/duct-
circulation in the first few days of life. dependant circulation in neonatal period,
reduced exercise tolerance, chest pain on
exertion & syncope
Signs: Signs:
- Ejection systolic murmur at pulmonary area - Small volume plateau pulse
(upper left sternal edge) radiating to the back - Ejection systolic murmur at aortic area
- Thrill at upper left sternal edge (upper right sternal edge) radiating to the
- Ejection click neck
- Loud P2 - Suprasternal/ carotid thrill
Investigation: Investigation:
- CXR à Post stenotic dilatation of pulmonary - CXR à Post stenotic dilatation of
artery ascending aorta
- ECG à RV hypertrophy (upright T wave) - ECG à LV hypertrophy
- Echocardiogram (Tall R in V5,V6; Deep S in V1,V2)
- Echocardiogram
Management: Management:
- Transcatheter pulmonary valvuloplasty - Surgical or balloon valvotomy
(balloon dilatation) - Aortic valve replacement
* Symptomatic children with high resting pressure gradient (>64mmHg) across the pulmonary and
aortic valve are indicated for intervention
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2) Coarctation of Aorta
Pre-ductal Post-ductal
Clinical features:
Symptoms Signs
- Depends on severity: - Weak of absent peripheral pulses
a) Mild: - Radiofemoral delay (bypass via collateral vessels)
- Heart failure (usually presented early) - BP in the upper limb is higher than BP in the
- Systemic hypertension(older children & adults) lower limb
b) Severe - ± Systolic murmur over the upper left sternal
- Duct-dependent circulation & circulatory edge or back
collapse in neonate
Investigations:
CXR ECG Echocardiography
- Rib notching (development of - Signs of LVH (Dominant R at - Evaluates heart structure &
large collateral intercoastal V5,V6; Deep S in V1,V2, total >7 function, assess blood flow
arteries running posteriorly to big squares) pattern, coarctation size
bypass obstruction
V1
V6
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Management:
Neonatal severe CoA:
- Frequently associated with large malaligned VSD, intractable heart failure
- Sick infants require temporary stabilisation:
- Mechanical ventilation
- Correction of metabolic acidosis, hypoglycaemia, electrolyte disorders
- IV Prostaglandin E (Prostin) infusion
- Early surgical repair (single-stage CoA repair) + VSD closure or 2-stage CoA followed by VSD
closure at later date)
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Cyanotic Congenital Heart Disease
1) Tetralogy of Fallot
Introduction:
- Most common
congenital heart disease
- Most are diagnosed
antenatally
- 4 cardinal features:
- Ventricular septal defect
- Pulmonary stenosis
- Right ventricular
hypertrophy
- Overriding aorta
Clinical features:
Symptoms Signs
- Most present with a murmur in the first 2 - Cyanosis, Clubbing (earliest clubbing: 6 months)
months of life - Loud & harsh ejection systolic murmur (ESM) at
- Cyanosis develops later (after a few months) left sternal edge (pulmonary area) from D1 of life
- Life threatening hypercyanotic spells (rapid - Single second heart sound (A2)
increase in cyanosis, usually associated with
irritability or inconsolable crying due to severe * With increasing right ventricular outflow tract
hypoxia, breathlessness & pallor) obstruction, the murmur duration will shorten
- May lead to MI, CVA, & death if untreated while the cyanosis will be worsened (infundibular
- Squatting following exertion in older child spasm).
Investigations:
CXR ECG Echo & Cardiac Catheterisation
- Boot-shaped heart (uplifting - Right axis deviation - Show detailed anatomy of
apex due to RVH), oligaemic - Right ventricular hypertrophy pulmonary arteries
lung fields, PA bay - Tall P wave (P pulmonale for
right atrial enlargement)
141
Management:
Conservative Surgical
- Hypercyanotic spells - Temporary surgery
- Usually self-limiting & followed by a period of - To increase pulmonary blood flow
sleep - eg. Modified Blalock-Taussig shunt for very
- Prompt treatment if prolonged >15 minutes cyanosed infants
- Morphine ( sedative )
- Oxygen, knees to chest position - Corrective surgery
- Propanolol (relieve infundibular spasm + - Usually done at 6 months of age
peripheral vasoconstriction)
- Bicarbonate (corrects acidosis)
- Muscle paralysis and artificial ventilation
(decrease metabolic oxygen demand)
- More potent vasoconstrictors (eg. phenylephrine
and noradrenaline)
Hypercyanotic spells
- Sudden severe episodes of intense cyanosis caused
Complications: by reduction of pulmonary flow
- This is due to spasm of the right ventricular outflow
- Infarction tract or reduction in systemic vascular resistance
- Polycythaemia (hyperviscosity syndrome) (eg. hypovolaemia) with resulting increased in right
- Cerebral abscess (R>L shunt, paradoxical embolism) to left shunt across the VSD, releasing lactate, leads
- SBE/IE to metabolic acidosis
- Clinical feature:
- Failure to thrive
- Peak incidence: 3-6 months
- Often in morning, precipitated by crying, feeding,
If TOF patient without murmur, consider: defaecation
- Severe cyanosis, hyperpnoea, metabolic acidosis
- Concurrent pulmonary atresia (silent heart)
- Severe: syncope, stroke or death
- Develops polycythaemia - Reduced intensity of systolic murmur during spell
- Management:
- Treat as medical emergency, knee-chest/squatting
position (place baby on mother`s shoulder with
knees tucked up underneath (calming effect,
reduce systemic venous return, increase TPR)
- Give 100% O2, IV/IM/SC morphine 0.1-0.2mg/kg to
reduce distress & hyperpnoea.
- If fails, give IV propanolol slow bolus/IV Esmolol
with volume expander. IV sodium carbonate.
- In resistant case, consider IV Pneylephrine/
noradrenaline increase TPR, reduce R>L shunt.
142
2) Transposition of Great Artery (TGA)
Introduction:
- Aorta is connected to RV, pulmonary
artery is connected to LV (discordant
ventriculo-arterial connection)
- Deoxygenated blood is therefore
returned to the body while
oxygenated blood returns to lungs
- Two parallel circulations are
incompatible to life unless there is
mixing of blood between them (eg.
VSD, ASD, PDA)
Clinical features:
Symptoms Signs
- Cyanosis, may be profound & life threatening, - Cyanosis +/- finger clubbing (rare)
usually in the first few days (eg. day 2) of life, - ± Systolic murmur (due to increased flow within
leads to marked reduction in mixing of oxyge- LV (pulmonary outflow tract)
nated and deoxygenated blood - Acidosis
- Cyanosis will be less severe and delayed if there - Single second heart sound
is more mixing of blood from associated
anomalies eg. VSD, ASD, PDA
Investigations:
CXR ECG Echo & Cardiac Catheterisation
- Egg-on-side appearance, - Rarely helpful - Show detailed anatomy of heart
often increased pulmonary with transposition of aorta and
vascular markings pulmonary artery
Egg-on-side appearance:
- Due to anteroposterior
relationship of great vessels
- Narrow vascular pedicle &
hypertrophied RV.
Management:
Simple TGA (intact - IV Prostaglandin E infusion promotes intercirculatory mixing at PDA
ventricular septum) - Temporary surgery: Early Balloon Atrial Septostomy (BAS) if restrictive
interatrial communication
- Definitive surgery: Arterial switch operation at 2-4 weeks age
- LV regression may occur if repair not performed within 4 weeks of life
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TGA with VSD - Does not usually require intervention during early neonatal period
- May develop heart failure at 1-2 months age
- Elective 1-stage arterial switch operation + VSD closure <3 months age
TGA with VSD & PS - Blalock-Taussig shunt during infancy followed by Rastelli repair at 4-6
years of age
Arterial Switch:
Introduction:
- Special form of VSD
- Ranges from ASD primum to
a large defect within a
common AV valve
- Most commonly seen in
children with Down syndrome
- Defect in middle of heart with a
single 5-leaflet valve between AV
junction & tends to leak
- Large defects lead to pulmonary
hypertension
Presentation:
- Present at antenatal ultrasound screening
- Detected through routine ultrasound screening for baby with Down`s syndrome
- Cyanosis at birth or heart failure at 2-3 weeks of life with no murmur
Treatment:
- Treat heart failure medically
- Surgical repair at 3-6 months
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4) Tricuspid Atresia
Introduction:
- Only left ventricle is effective
- Right ventricle is small and non-
functioning (underdeveloped)
- There is common mixing of
systemic & pulmonary venous
return in LA
Clinical features:
- Cyanosis in the newborn which is duct-dependant
- Well at birth and become cyanosed and breathless
- ECG (left axis deviation) is diagnostic
Management:
Temporary surgery Corrective surgery
- Blalock Taussig shunt (for cyanosed infants) - Semi Fontan/ Glenn operation at 6 months of age
- Pulmonary artery banding (for breathless - Fontan operation at 3-5 years of age
infants)
Fontan procedure:
First stage: Bi-directional Glenn (graft reroutes from SVC to PA and to lung for oxygenation, bypass RA)
Second stage: Fontan (graft & internal baffle re-route rom IVC to PA)
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5) Hypoplastic Left Heart Syndrome
Introduction:
- Underdevelopment of entire left side of the heart
- Left ventricle is diminutive
- Mitral and aortic valve are usually atretic
- Ascending aorta is usually very small
- ASD
Clinical features:
- Sickest of all neonates with duct-dependant
circulation
- Profound acidosis & rapid cardiovascular collapse
(due to absence of blood flow in the left heart
and ductal constriction )
- Weakness or absence of all peripheral pulses
- Failed hyperoxia (nitrogen washout) test
Management:
- Maintain ABC and immediate initiation of prostaglandin infusion
- Complex surgical correction (Norwood procedure)
Norwood procedure:
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6) Total Anomalous Pulmonary Venous Connection (TAPVC)
Introduction:
- Connection of all pulmonary veins to
somewhere other than LA (1-3% of
congenital heart lesions)
- Pulmonary veins connect to:
- Supradiaphragm (70%)
- Vein (commonest innominate vein)
- Heart (coronary sinus or RA)
- Infradiaphragm (25%) - obstructive
- Portal vein or its branches
- Ductus venosus
- Mixed (5%)
Clinical features:
A) Obstructive
- Marked cyanosis (from decreased
pulmonary blood flow accentuated
by pulmonary oedema & pulmonary
arterial hypertension)
- Tachypnoea, Respiratory distress
B) Non-obstructive
- Minimal cyanosis
- CCF (pulmonary overcirculation)
Management:
- Surgical with anastomosis of
pulmonary vein confluence to LA
(extracardiac anomalous connection)
- Unroofing coronary sinus (sinus type)
- Repositioning of atrial septum (RA type)
Surgery for TAPVR to Left SVC: Surgery for TAPVR to Coronary Sinus:
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7) Truncus Arteriosus
Introduction:
- Denotes a single
arterial trunk
serves ascommon
origin of aorta,
pulmonary artery
& coronary arteries
- 2-2.8% of
congenital heard
lesions
- Almost always
associated with
a VSD
- Associated heart
defect include
right aortic arch
(33%)
Clinical features:
- Minimal cyanosis (hihgh pulmonary blood flow)
- Tachypnoea, Respiratory distress
- CCF exaggerated by poor coronary perfusion 2` to low diastolic pressure from runoff into PA
Management:
- Surgical separation of aorta & pulmonary artery, placement of extracardiac RV to PA conduit,
closing VSD by baffling LV to aorta (refer diagram above)
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Rheumatic Fever
Introduction:
- Inflammatory disease that involves heart, joints, CNS, skin & subcutaneous tissues
Epidemiology:
- Most common cause of acquired heart disease in children & adult
- Mainly in under developed countries
- First infection is usually between 5-15 years of age (F>M)
- Extremely rare in infancy and <4 years old children
- Associated with adverse social economic factors, medical care & overcrowding
Aetiology:
- Group A β-haemolytic Streptococcus untreated pharyngitis in susceptible individual
- It has been confirmed this genetic susceptibility is inherited as autosomal recessive (AR) gene
Pathogenesis:
- Streptococci trigger autoimmune reaction à inflammation
- NOT direct infection from the bacteria to the heart
- Antibody produced by the infection showed to cross react with host tissue in the valvular
tissue, myocardium, joint, subthalamic & caudate nuclei
- The inflammatory lesion is in many systems à valvular damage in mitral & aortic, less in
tricuspid & pulmonary
- Characteristic Aschoff bodies in atrial myocardium (inflammatory lesion + swelling +
fragmented collagen fibres)
Clinical features:
- History of pharyngeal infection or URTI for previous 2-6 weeks
Definite Diagnosis:
- 2 major criteria OR 1 major + 2 minor infection
- With supporting evidence of preceding streptococcal infection
- History of scarlet fever
- Positive throat swab (for group A streptococcus)
- Raised anti-streptolysin O titre (ASOT) >200U/ml or anti-DNAse B
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Clinical features Description
Sydenham`s - Usually occurs 2-6 weeks after Streptococal infection
chorea - Characterised by: (3-6 months)
(St Vitus dance) - Involuntary, purposeless movements
- Followed by motor weakness & hypotonia
- Preceded by emotional lability
- Physical signs:
- Pronator sign à extension of the arms above the head produces
pronation of the 1 or both hand
- Milking sign à ask the patients to squeeze the examiner finger,
irregular contraction of the muscle of the hand will be evident
- Spoon/Dishing sign à extension of the hand forward will lead to
hyperextension of the finger
Subcutaneous - Usually found on the extensor surface of joint & occasionally on the scalp
nodule or spine
- Clinical features:
- Painless & free mobile
- Pea-sized & hard
Migratory - Usually involve larger joints (eg wrists, knees & ankles)
polyarthritis
Symptoms Signs
- Arthralgia which is fleeting - Joints involved
- Lasting <1 week - Redness
- Asymmetrically & migrating to other - Swelling
- Joints over 1-2 months - Tender
- Limitation of movement & non- - Very responsive to salicylates
damaging
Complications:
- Causes scarring & fibrosis of valve tissue
- Mitral valve ( 85% ) à Mitral stenosis
- Aortic valve ( 55% )
- Tricuspid valve & pulmonary valves ( <5% )
Management:
Acute Phase Secondary Prophylaxis
- Evaluate FBC, ESR, CRP, CXR, ECG, Echo, & ASOT - Duration of prophylaxis is controversial
- Encourage bed rest & limitation of exercise - Lifelong for patients with carditis & valvular
- Eradication of Grp A β-haemolytic Streptococci involvement
- Penicillin V 250mg 6 hourly x 10 days (children), - Until age 21 years or 5 years after last attack of
500mg 6 hourly (adolescents) ARF whichever was longer
- For patients with allergy to penicillin, - Penicillin
erythromycin or cephalosporin is used - Monthly IM benzathine Penicillin(most effective)
- Anti-inflammatory agents (suppress - Oral penicillin V BD is an alternative
inflammatory response in joints or heart) - Oral erythromycin (if allergic to penicillin)
- High dose aspirin
- Corticosteroids (if fever & inflammation do not
resolve rapidly)
- Treat associated problems
Cardiac failure Diuretics & ACE inhibitor
Pericardial effusion Pericardiocentesis
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Mitral Stenosis
Introduction:
- In children it is mostly congenital, commonest RHD in adults
Pathology:
- Fibrosis of the leaflets, fusion of rings with calcification & immobility
- Left atrium, right side heart enlarged and hypertrophied
- Followed by pulmonary venous hypertension, pulmonary oedema & right heart failure
Clinical features:
- Asymptomatic or symptomatic on exertion, rarely related to AF & IE.
- Dyspnoea, orthopnea, paroxysmal nocturnal dyspnea
- Palpitation, hemoptysis
Physical findings:
- Left parasternal heave (RV hypertrophy), weak peripheral pulse, Normal Pulse Pressure
- Right heart failure: Distended neck veins, raised JVP, hepatomegaly, ascites & oedema
- Functional Tricuspid regurgitation, pansystolic murmur
- Loud S1 (tapping apex beat)
- Narrow split of S2, maybe loud
- Opening snap soon after S2
- Mid-diastolic rumbling at apex with presystolic accentuation
- Graham Steell (pulmonary regurgitation at upper left sternal border, early diastolic, inspiration,
due to pulmonary hypertension)
- Ejection click
Investigations:
ECG - RA dilatation, LA hypertrophy, RV hypertrophy due to pulmonary hypertension
- AF rare in children
CXR - LA, RV enlargement, pulmonary venous congestion with interstitial oedema
(Kerley B lines), calcifications
Echocardiography - Most accurate
Management:
Medical Surgical
- Good oral hygiene & prophylaxis vs acute - Indicated in
rheumatic fever & IE - Symptomatic patient
- Varying degree of activity restriction - Recurrent AF
- Digoxin for AF, anticoagulation to all MS - Thromboembolism
patients - Hemoptysis
- Balloon valvuloplasty, M-commissurotomy or
replacement if calcification presents
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Mitral Regurgitation
Introduction:
- The most common Rheumatic involvement in children
Pathology:
- Loss of valve tissue, shortening & fibrosis of leaftlets
- Left ventricle enlarges, left atrium dilates with increased pressure à followed by pulmonary
edema & CHF
Clincial features:
- Asymptomatic mild & moderate disease, rarely get fatigue & palpitation with atrial fibrillation
- Stable for long duration, but MS may supervene
- Can develop LVF & pulmonary hypertension in adult life
Physical findings:
- JVP is normal in the absence of CHF
- Heaving cardiac impulse if severe
- S1 is normal or decreased
- S2 widely split, may be loud
- S3 present & loud
- Pansystolic murmur, grade 2-4/6, at the apex with radiation to the axilla, best on left lateral
decubitus position
- Short diastolic rumble maybe present at apex due to increased flow through the valve
Investigation:
ECG - LV dominance, LVH, AF develops in adults
CXR - LV/LA enlargement, CHF with PVC
Echo - Severity related to degree of dilatation of LV/LA
Catheterization - Left ventriculography
Management:
- Prophylaxis against acute rheumatic fever recurrence & IE
- CHF: Digoxin (also for AF), diuretics
- Indications for surgery :
- Intractable CHF
- Progressive cardiomegaly with symptoms
- Pulmonary hypertension
- It is either valvuloplasty or valve replacement if thick and scarred
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Aortic Regurgitation
Introduction:
- Usually combined with Mitral Regurgitation
- Remains asymptomatic for long duration but symptomatic if started they deteriorate rapidly
- Rare in IE patients
Pathology:
- Semilunar cusps deformed, ring dilated so they fail to oppose tightly
Clinical features:
- If severe AR or in CHF they will have exercise intolerance
- Angina, CHF & multiple pulmonary venous congestions are unfavourable signs
Investigation:
ECG LV hypertrophy in severe AR, chronic LA hypertrophy
CXR Cardiomegaly of LV, prominent aortic knuckle, pulmonary venous
congestion if in LV failure
Echo Detects severity of AR
Management:
Medical Surgical
- ARF & IE prophylaxis - Indication for surgery
- CHF (Digoxin & diuretics) - Angina or dyspnoea on exertion
- Cardiomegaly even if asymptomatic à valve
replacement or pulmonary root autograft
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Infective Endocarditis (IE)
Definition:
- Microbacteria infection à Exudative & proliferative inflammatory alterations of the
endocardium or vascular endothelium
Introduction:
- IE is a rare but very serious complication of patient with structural heart disease
- Typically affect older children with structural heart disease
- 2 factors in its pathogenesis:
- Structural abnormality of heart or great artery by turbulent flow à platelet-fibrin deposition
à Non-bacterial thrombotic endocarditis à Adherence
- Bacteremia resulting in endothelial damage & platelet à Adherence à Colonisation à Fibrin
thrombus (vegetation) formation
Aetiology:
Bacteria Fungus Others
- Streptococcus viridans - Candida albicans - SLE
(Bacterial flora of pharynx & - Aspergillus (Libman-Sacks endocarditis)
upper respiratory tract, - Histoplasma
dental procedures) - Cryptococcus neoformans
- Staphylococcus aureus
- Enterococcus fecalis
- Staphylococcus epidermidis
- Gram -ve organisms (rare)
- HACEK group
- Haemophilus spp
- Actinobacillus
actinomycetemcomitans
- Cardiobacterium hominis
- Eikenella corrodens
- Kingella kingae
- Coxiella burnetii (Q fever)
- Chlamydia
Risk groups:
- IV drug abuser
- Patients with congenital heart disease or rheumatic heart disease
- After cardiac surgery (prosthetic valves)
- Chronic IV catheterization
- Immunosuppressants
Clinical features:
- Fever + new murmur is endocarditis until proven otherwise
(Common symptoms: Unexplained, remitting fever >1 week, LOW, LOA, myalgia)
155
Symptoms Signs
- Fever Hands & limbs
- Malaise - Peripheral stigmata of infective endocarditis
- Anorexia - Clubbing (late)
- Weight loss - Splinter haemorrhage
- Arthralgia - Osler nodes
- History of predisposing factors, procedures (eg - Janeway lesion
dental, surgical), central venous catheter - Necrotic skin lesion
insertion - Pallor (due to anemia)
Head
- Roth`s spot on fundoscopy (retinal infarcts)
CNS
- Neurological signs from cerebral infarction
CVS
- New/ changing cardiac murmur
GIT
- Splenomegaly
Genitourinary
- Microscopic hematuria
Musculoskeletal
- Arthritis (arthralgia)
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**Congenital heart disease
- Highest risk if there is a turbulent jet of blood:
- VSD
- Coarctation of Aorta (COA)
- Patent ductus arteriosus (PDA)
- Exception for AS
*** Vascular phenomena (major arterial emboli, septic pulmonary infarcts, mycotic aneurysm,
intracranial hemorrhage, conjunctival hemorrhages, Janeway lesions),
Immunological phenomena (GN, Osler nodes, Roth spots, rheumatoid factor)
Investigations:
Blood - FBC
- Normochromic normocytic anemia (unexplained)
- Polymorphonuclear leucocytosis (evidence of bacterial infection)
- Thrombocytopenia (occasionally)
- Acute phase reactant
- Increased ESR & CRP (indicate inflammation)
- Blood C&S
- For evidence of bacteremia of typical organism
- Serum immunoglobulin & complement (Raised)
- Low total complement & C3 complement
- LFT (mildly disturbed)
- Raised alkaline phosphatase (ALP)
- Serology (chlamydia, candida, coxiella, brucella) if culture negative
Urine - UFEME
- Microscopic hematuria To look for glomerulonephritis
- Urine dipstick (proteinuria)
Imaging - Echocardiogram (visualise endocardial & valvular vegetations measuring
≥2mm. Transesophageal more sensitive than transthoracic in adolescent
or adult with prosthetic valve but often unnecessary for children
Other test includes:
Prognosis: RP for glomerulonephritis
Baseline ecg
- Prognosis is variable Transthoracic echocardiogram
- Mortality is high ( 20-30% of patients particularly ) Chest x ray for septic pulmonary infarct
Ct scan to look for abscess
- Acute staphylococcal infection Consider rheumatoid factor?
- Fungal infection
- Infected prosthetic material
- Survivors at risk of recurrence
Management:
- Can be divided into conservative and surgery
- Ensure 3 blood cultures taken before antibiotic therapy, do not wait for echocardiography
- Use empirical antibiotics, until culture results available
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Conservative Surgery
- Intravenous antibiotic (bactericidal agents) - Adjunct to medical therapy in certain
for 4-8 weeks à for bacterial endocarditis circumstances
- Monitor clinical response (+ acute phase - Less chance of complete eradication
reactant) - Indications:
- Commonly used is high-dose penicillin in - Infected prosthetic materials
combination with aminoglycosides - Prosthetic valves
- VSD patches or shunts
- Embolization & large vegetations
- Progressive cardiac failure
- Worsening renal failure
Prophylaxis
1) Procedures requiring prophylaxis
Oral, dental Dental surgery(eg. tooth extraction, placement of orthodontic bands)
Respiratory system Tonsillectomy, adenoidectomy
Rigid bronchoscopy, Flexible bronchoscopy with biopsy
GIT Sclerotherapy (oesophageal varices), Oesophageal stricture dilatation
ERCP, Appendicectomy
Genitourinary Cystoscopy, Urethral dilatation
158
2) Prophylactic Regimen
Oral, Dental - Ampicillin before procedure
Respiratory Tract - Clindamycin if allergic to Ampicillin
Esophagus
159
Kawasaki Disease (Mucocutaneous Lymph Node Syndrome)
Introduction:
- Systemic febrile condition, infantile polyarteritis of unknown case
- It is one of the most common vasculitides of childhood (70-80% together with HSP)
- First describe in Japan in 1967
- Results from immune hyperactivity to a variety of triggers in a genetically susceptible people
Epidemiology:
- 80% of patients are <5 years old (6 months-4 years old)
- Peak incidence at the end of first year
- More severe in young infants compared with older child
- All races affected but highest incidence in Asian
population
- Commoner in boys (M : F = 1.5 : 1)
Red, cracked lip & conjunctival inflammation.
Aetiology: Peeling of fingers, developed on 15th of illness
- Unknown
- Probable association with microbial agents (staphylococcal & streptococcal)
- Bacterial toxin acts as superantigen
Pathology:
- Vasculitis of small and medium-sized vessels (eg. coronary arteries)
- Inflammatory process involves the entire vascular wall à aneurysm +/- thrombus
- Eventually results in intimal proliferation, scarring, calcification, stenosis & recanalization
Clinical features: (diagnostic criteria)
- Acute fever for at least 5 days + 4/5 of the following features:
- Other diagnosis need to be excluded (diagnosis of exclusion)
Eye - Bilateral conjunctival injection without exudate
Mucosal changes in mouth - Injected pharynx
- Strawberry tongue
- Cracked and erythematous lips
Neck - Cervical lymphadenopathy (>2 LN & >1.5 cm) At least one LN >1.5cm
Body - Polymorphous exanthema, maculopapular rash or perianal rash
/generalised rash
Changes in extremities - Redness & swelling of the hands and feet
- Desquamation, peeling of the finger (convalescent phase)
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Disease Progression:
Most important complication is coronary vasculitis, usually within 2 weeks of illness, affecting up
to 25% of untreated children. Usually asymptomatic, it may manifest as myocardial ischaemia,
infarction, pericarditis, myocarditis, endocarditis, heart failure or arrhythmia.
Investigations:
Blood - FBC
- Anemia (low Hb) Often present with normochromic normocytic anaemia
- Neutrophilia (low WBC) Leukocytosis according to UpToDate
- Thrombocytosis (high PLT - in convalescent phase) Esr typically raised after IVIG so
- Acute phase reactant not suitable to monitor
progression
- Increased ESR & CRP (indicate active inflammation) Crp on the other hand drop with
- ANA & RA factor (negative) ivig
161
Management:
Medical General Measures
- IV immunoglobulin (within first 10 days of illness) - Serial echocardiogram
- Lower risk of coronary artery aneurysm - Long-term cardiology follow-up for those with
- Fever and systemic complaints resolve within coronary artery abnormalities
24-48 hours
Prognosis:
- Mortality 1-2% usually from cardiac complications within 1-2 months of onset
- Recovery is complete in children who do not have coronary artery involvement, 80% of
aneurysm 3-5mm in diameter resolve, 30% of 5-8mm aneurysms resolve
- Prognosis worst for aneurysms >8mm in diameter
Incomplete Kawasaki Disease
- Patients who do not fulfill the classic diagnostic criteria (outlined in previous page)
- Tends to occur in infants and the youngest patients
- High index of suspicion should be maintained for diagnosis of incomplete KD
- Higher risk of coronary artery dilatation or aneurysm occurring
- Echocardiography is indicated in patients who have prolonged fever with:
- Two other criteria
- Subsequent unexplained periungual desquamation
- Two criteria + thrombocytosis
- Rash without any other explanation
Atypical Kawasaki Disease
- For patients who have atypical presentation, eg. renal impairment, that generally is not seen in
Kawasaki Disease
- Treatment:
Primary treatment
- IV Immunoglobulins 2 Gm/kg infusion over 10 - 12 hours. Therapy < 10 days of onset effective in
preventing coronary vascular damage.
- Oral Aspirin 30 mg/kg/day for 2 wks or until patient is afebrile for 2-3 days.
Maintainence:
- Oral Aspirin 3-5 mg/kg daily (anti-platelet dose) for 6 - 8 weeks or until ESR & platelet count
normalise
- If coronary aneurysm present, then continue aspirin until resolves
- Alternative: Oral Dipyridamole 3 - 5 mg/kg daily.
Kawasaki Disease not responding to Primary Treatment
- Defined as persistent/ recrudescent fever ≥ 36hrs after completion of initial dose of IVIg
Treatment
- Repeat IV Immunoglobulins 2 Gm/kg infusion over 10-12 hours
- Vaccinations
- Use of Immunoglobulins may impair efficacy of live-attenuated virus vaccines
- Delay these vaccinations for at least 11 months
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PART V
RESPIRATORY
Common Respiratory Infections
Introduction:
- Most common cause of death in children worldwide.
- Preschool child has, on average, 6-8 respiratory infections a year.
- Cystic fibrosis is the most common inherited life-limiting disorder in Caucasians.
- Children are prone to respiratory infection especially <2 years old due to smaller airways (easily
blocked), lower resistance and immunity.
- Pathogens (viral-caused: 80-90% of childhood respiratory infections):
RSV Parainfluenza Influenza AdenoV EnteroV RhinoV Mycoplasma
Colds + + + ++ ++ ++++ +
Tonsillitis/ ++ ++ +
Pharyngitis
Otitis media + + + +
Laryngotracheitis + ++++ + +
Bronchitis + + + +
Bronchiolitis ++++ ++ + + +
Pneumonia ++ + + ++
* Viruses & Mycoplasma commonly associated with acute respiratory infection, diagnosis is from nasopharyngeal
aspirate
Wheezing
- High-pitched musical sound produced by air flowing through narrowed airways.
- Heard mostly during the expiratory phase (normal tendency of the intrathoracic airways to narrow when
intrapleural pressure exceeds intraluminal pressure during expiration)
- Sign of increased airway resistance resulting from obstruction in intrathoracic airways.
- Heterophonous or polyphonic when there is diffuse narrowing of the airways. Most common causes of this
wheezing are viral bronchiolitis & asthma.
- Homophonous is when single set of pitches originates in larger airways but can be transmitted widely. Common
causes include tracheomalacia, bronchomalacia, foreign body aspiration & anatomic compression of airways.
Stridor
- Distinct harsh inspiratory noise due to obstruction occurs in the extrathoracic airways.
164
Upper Respiratory Tract Infection (URTI)
Introduction:
- Infection involving the nose, throat, ears & sinuses
- Approximately 80% of all respiratory infection
- Common URTI:
- Common cold (Coryza)
- Sore throat (Pharyngitis including tonsillitis)
- Acute otitis media
- Sinusitis (Relatively uncommon)
- Commonest presentation:
- Nasal discharge and blockage
- Fever
- Sore throat
- Ear pain
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3) Acute Otitis Media
- Acute infection of the middle ear
- Most children have at least 1 episode of acute otitis media (AOM)
- Most common at 6-12 months of age, up to 20% will have ≥3 episodes (Recurrent OM)
- Infant & young children prone to acute OM as their Eustachian tubes are short, horizontal &
function poorly.
- Common pathogens: RSV, Rhinoviruses, Adenoviruses (viral origin)
Streptococcus pneumoniae
Haemophilus influenza
Moraxella catarrhalis
- Presentation: Pain, irritable ear, fever
- Examination: Findings on tympanic
- Otoscopy/ tympanometry (tympanic membrane) - diagnostic membrane:
- Complication: - Bright red
- Mastoiditis - Bulging
- Meningitis - Loss of light reflection
- Pus visible in external canal
- Recurrent ear infection may lead to chronic serous otitis
(in acute perforation)
media (result in conductive hearing
loss)
- Management:
- 80% resolve spontaneously by 24 hours
- Symptomatic treatment for pain and fever (Paracetamol)
- Antibiotics: Amoxicillin/ Augmentin (Co-amoxiclav) - shorten duration of pain but not shown
to reduce hearing loss
- Neither decongestants nor antihistamines help in Eustachian Tube drainage
Chronic Serous Otitis Media (CSOM)/ Otitis media with effusion (OME/ Glue ear)
Introduction:
- Usually asymptomatic/ mild earache and resolves spontaneously
- Very common between ages of 2 & 7 years old, peak incidence 2.5-5 years old
- Most common cause of conductive hearing loss in children
- May interfere with normal speech development & result in learning difficulties in school
Investigations:
- Tympanometry (flat trace is diagnostic)
- Dull and retracted tympanic membrane
- Fluid level and air bubbles
- Pure tone audiometry (conductive loss, possible if >4 years old)
- Distraction test (reduced hearing, younger children)
Management:
- Grommets (Ventilation tubes) insertion
- Adenoidectomy +/- Tonsillectomy (which causes recurrent OM)
- Adenoids harbour organisms within biofilms contribute to infection spreading up to tubes
- Gross hypertrophied adenoids may obstruct & affect function of Eustachian tubes.
- Speech therapy
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Normal Acute otitis media Otitis media with effusion Grommet
4) Sinusitis
- Infection of paranasal sinuses
- Common pathogens : viral origin, occasionally with secondary bacterial infection
- Presentation: pain, swelling and tenderness over cheek (infection from maxillary sinus)
* Frontal sinusitis is uncommon since frontal sinuses do not develop until late childhood
- Management:
- Antibiotics and analgesics are used in addition to topical decongestants
- Concurrent use of intranasal corticosteriods/ antihistamines with antibiotics (hasten recovery)
5) Choanal stenosis/atresia
- Congenital, presenting during neonatal period (cyanose when normal, pink when crying)
- Bilateral or unilateral and is relatively rare
- Neonates are generally obligate nose breathers, so obstruction of nasal passages can cause
significant respiratory distress, especially when feeding
- Crying bypasses the obstruction as crying infants breathe through their mouths
- Inability to easily pass a small catheter through the nostrils should raise the suspicion
- Diagnosis is confirmed by CT scan & inspecting area directly with a flexible nasopharyngoscope
- Oral airway may be useful in the short term, but definitive treatment is surgery
6) Apnoea
- Defined as the cessation of airflow due to
- Lack of respiratory effort (central apnea)
- Upper airway obstruction (obstructive apnea)
- Central apnea lasting <10 seconds is common in healthy infants & can be present in normal
children during sleep, especially after a sigh breath. Central pauses lasting >15-20 seconds are
considered abnormal. More common in infants
- Obstructive apnea, especially during sleep, is more common in older children.
167
- Premature infants can have apnea of prematurity, which consists of recurrent apneic episodes
that are often of central origin, though they can be mixed. It should resolve by 44 weeks
postconceptional age.
Categories of Apnoea:
Diseases Examples Mechanism Signs Treatment
Apnea of Premature Central control, upper Apnea, bradycardia Caffeine, HFNC,
prematurity (<36 weeks) airway obstruction CPAP, intubation
Central apnea/ CCHS, Arnold-Chiari Abnormal central Apnea Mechanical
hypoventilation malformation control ventilation
Obstructive sleep Obesity, Airway obstruction Snoring, restless Adenotonsillectom
apnea adenotonsillar due to excess tissue, sleep, enuresis, poor y, CPAP/BiPAP,
hypertrophy, Pierre loss of pharyngeal school performance, uvuloveloplasty,
Robin sequence, tone or crowded behavior problems, tracheostomy
Down syndrome, anatomy mouth breathing
cerebral palsy
Breath-holding <3 yr old who turns Prolonged expiratory Cyanosis, syncope, Reassurance;
spells blue after crying, apnea; reflex anoxic brief tonic-clonic condition is self-
may have syncope seizures movements after limiting. Must
cyanosis exclude seizure
disorder
168
169
Viral Croup (Laryngotracheobronchitis)
Definition:
- Progressive spread of viral inflammatory process down the respiratory tract involving larynx,
trachea & bronchi (till subglottic area around cricoid)
- Clinical syndrome characterised:
- Barking cough
- Inspiratory stridor
- Hoarseness of voice (due to inflammation of vocal cord)
- Respiratory distress of varying severity
Epidemiology:
- Occurs from 6 months to 6 years of age (peak incidence in 2nd year of life)
- Most severe in children <3 years of age
- Accounts for >95% of laryngotracheal infections
Pathophysiology:
- Infection causes mucosal inflamation & increased secretions affecting larynx, tracheal &
bronchi
- Oedema of subglottic area causes critical narrowing of tracheal (potentially dangerous)
Clinical Features:
Symptoms Signs
Early (12 – 72 hours) Inspection
- Low grade fever - Signs of respiratory distress
- Coryzal symptoms (Runny nose, sore throat) - Tachypnea & Tachycardia
- Nasal flaring, expiratory grunting & head
Late bobbing
- Inspiratory, harsh stridor - Suprasternal, intercostal & subcostal recessions
- Barking cough (like sea lion) - Central cyanosis (severe hypoxaemia)
- Hoarseness of voice - Use of accessory muscles
- Respiratory distress (varying degree)
Auscultation
- Poor air entry (reduced breath sound)
- Expiratory rhonchi
Diagnosis:
- Croup is a clinical diagnosis. Studies show it is safe to visualise pharynx TRO acute epiglotitis,
retropharyngeal abscess etc.
- In severe croup, it is advisable to examine the pharynx under controlled conditions (eg. in the
ICU or Operation Theatre)
- Neck Radiograph is not necessary, unless the diagnosis is in doubt, eg. TRO foreign body.
170
Assessment of severity:
- Severity from Clinical Assessment of Croup (Wagener)
- Mild : Stridor with excitement or at rest, with no respiratory distress
- Moderate : Stridor at rest with intercostal, subcostal or sternal recession
- Severe : Stridor at rest with marked recession, decreased air entry & altered consciousness
- Pulse oximetry is helpful but not essential
- Arterial blood gas is not helpful as blood parameters may remain normal to the late stage. The
process of blood taking may distress the child.
Investigation:
Blood - FBC (WBC: lymphocytosis)
- ESR (inflammation)
Pulse oximetry - To measure the oxygen saturation (< 93% considered severe)
Neck radiography - Steeple sign (Laryngeal air column narrowing below vocal cord)
Laryngoscopy - Only perform TRO peritonsillar abscess (quinsy)
Management:
- Children with viral croup can be managed at home/ hospital
- Factors to be considered for home management:
- Mild cases (mother should observe closely for signs of increased
severity)
- Time of the day
- Ease of access to hospital
- Age of the child (Low threshold for child <12 months of age)
- Parental understanding & confidence about the disease
- Indications for hospital admission:
Anteroposterior radiograph of
- Moderate and severe viral croup upper airway with croup. The
- Age less than 6 months subglottic tracheal narrowing
produces an inverted V-shape
- Poor oral intake known as Steeple sign.
- Toxic, sick appearance.
- Family lives a long distance from hospital; lacks reliable transport
- Decision to intubate under controlled conditions (in OT/ICU, with standby for tracheostomy) is
based on clinical criteria, often from increasing respiratory distress
- Indications for oxygen therapy include:
- Severe viral croup
- Percutaneous SaO2 <93%
* With oxygen therapy, SaO2 may be normal despite progressive respiratory failure and high PaCO2,
hence clicnical assessment is most important
- Antibiotics are not recommended unless bacterial super-infection is strongly suspected or
patient is very ill. IV fluids are not usually necessary except for those unable to drink.
171
Treatment:
- Algorithm for the Management of Viral Croup
- Sustained action of steroids combined with the quick action of adrenaline may reduce the rate of
intubation from 3% to nil.
- Antibiotics are not recommended unless bacterial super-infection is strongly suspected or patient is
very ill.
- IV fluids are not usually necessary except for those unable to drink
172
Acute Epiglottitis
Introduction:
- Acute inflammation of the epiglottis & surrounding structures (aryepiglottic fold & arytenoid
soft tissue)
- Life threatening emergency case (high risk of respiratory obstruction)
- 99% decreased in incidence since the introduction of HiB immunization
- Affects all age group but most common in children 1-6 years of age
Aetiology:
- Haemophilus influenza type b Epiglottitis triads:
- Group A, B and C Streptococci - Severe sore throat with
- Streptococcus pneumoniae dysphagia/drooling
- Klebsiella pneumoniae - Hoarse voice
- Staphylococcus aureus - Pyrexia, generally unwell,
- Haemophilus parainfluenza dehydrated
Pathophysiology:
- Infective agents invade the epiglottis causing inflammation
- Bacteria invade directly into the loosely attached submucosa membrane and might followed
by bacteremia
- Result in oedema of epiglottis and surrounding tissues, leading to airway obstruction
Clinical features:
- Important to differentiate from viral croup as it requires quite different management
Symptoms Signs
Onset is very acute General
- High grade fever - Ill and toxic looking child
- Difficult to speak and swallow - Child sit immobile, upright & open mouth to
- Drooling of saliva optimize the airway
- Noisy breathing (soft inspiratory & expiratory - Stridor is a late sign
stridor)
- Followed by SOB over hours Examination
- No throat examination with spatula until
Uncommon presentation resuscitation equipment is ready
- Cough (minimal/ absence)
Diagnosis:
- Established on the basis of the clinical history & sign of toxicemia & upper airway obstruction
- Mortality is high if the diagnosis is delayed
Investigations:
- Notify senior anesthetist, pediatrician & ENT surgeon
- Perform laryngoscopy to diagnose in ICU/ OT
- Clinical features: Cherry red, intense swelling of epiglottis & surrounding tissues
- Intubate the child before obstruction occurs
173
- Blood investigation
- Blood C & S (only after the airway has been secured)
- Neck X-ray is not recommended, may precipitate total airway obstruction and death
Management:
- Admit child to the hospital urgently
- Child should be transferred to ICU or anesthetist room + senior medical stuff in case respiratory
obstruction occurs
- Require either tracheostomy / endotracheal intubation in general anesthetic
- Administered high flow humidified oxygen saturation to achieve maximal alveoli O2 saturation
- Monitor any respiratory and cardiac problem
- The patient should be supervised all time by the medical staff
Medical Treatment:
- IV antibiotic started right after the diagnosis and patent airway
- Second/ third generation cephalosporin (Ceftriaxone, Cefotaxime)
- Given for 2-5 days
- Add Flucloxacillin if the cause is Staphylococcal LTB
- Tracheal tube is usually removed after 24 hours
- Longer if the causative agent is Staphylococcus LTB
Prognosis:
- Usually resolve after 2-3 days of treatment
Prevention:
- Prophylactic rifampicin for close household contacts
Introduction:
- Commonest serious lower respiratory tract infection of infant (<2 years old)
Epidemiology:
- 2-3 % of all infants are admitted to the ward each year (annual winter epidemics)
- 90% aged 1-18 months (rare after 1 year old)
- Aged affected 1-2 years, Peak incidence is 1-6 months
Aetiology:
Virus Bacteria
- Respiratory syncytial virus (RSV) - Chlamydia trachomatis
- Adenovirus
- Rhinovirus
- Myxovirus
- Human Metapneumovirus
Risk Factors:
- Preterm Infants (who develop bronchopulmonary dysplasia)
- Congenital heart disease
Protective factors:
- Breastfeeding
- Parental avoidance of smoking
Clinical Features:
Symptoms Signs
Early General
- Coryzal symptoms (nasal congestion & - Sharp & dry cough
discharges, mild cough) - Tachycardia
- Low grade fever (<38. 5 ˚C) - Cyanosis or pallor
Inspection
Late
- Tachypnoea
- Persistent cough (chesty cough as children
- Subcostal & Intercostals recession
like to swallow sputum, may last for ≥14 days)
- Nasal flaring (when the nostrils enlarge
- SOB/ rapid breathing
during breathing) and grunting
- Noisy breathing (wheezing) - about 7 days
- Difficulty feeding related to nasal congestion Percussion
& rapid breathing which can results in - Hyperinflated chest
dehydration - Displaced liver (up to 2 cm or >6th
- Apnea intercostal space in midclavicular line)
(A pause in breathing for >15/ 20 seconds) -↓Cardiac & liver dullness
can be the first sign of bronchiolitis in an - Prominent sternum
infant. (More commonly premature baby & Auscultation
infants <2 months) - ↓air entry
- Fine end-inspiratory crepitation
- High-pitched wheezes/ rhonchi
(expiratory > inspiratory)
- Prolonged expiration
175
Complications
- Recurrent apnoea
- Asthma (20-30% of patients)
- RSV specific IgE is produced in the nasopharynx
- Magnitude related to number of wheezing episodes
- Bronchiolitis obliterans (rare)
- Permanent damage to the airways
- Mostly associated with adenovirus infection rather than RSV
Differential diagnosis:
- Bronchopneumonia
- Asthma
- Cardiac Failure
Investigations:
Blood - FBC (evidence of bacteria infection)
- Pulse Oximetry (SaO2)
- ABG (only in severe cases)
-↓PaO2 &↑PaCO2
Imaging CXR
- Evidence of hyperinflation
- Anterior > 6 ribs or posterior >7 ribs in the midclavicular line
- Flattening of diaphragm
- Horizontal ribs
- Increased hilar bronchial markings
- Occasional scattered area of consolidation/segmental collapse due to atelectasis
Others - Nasopharyngeal secretion
- Demonstrating binding of immunofluorescent antibody
* The diagnosis of bronchiolitis is based upon a history and physical examination. Blood tests and CXR are
not usually necessary
Management:
Supportive (Non-Pharmacological) Pharmacological
- Humidified O2 (concentration is determined - Nebulized bronchodilators (eg. salbutamol or
by pulse oximetry which maintained >93%) ipratropium bromide)
- By nasal prong or headbox - Often used even though not shown to reduce
- Mechanical ventilation (2% of infants) severity & duration of illness
176
- Monitor patient with pulse oximetry - Antiviral Rx (eg. Ribavirin)
(look for signs of worsening condition) - Indications:
- Tachycardia - Pre- existing cardiorespiratory distress
- Tachypnoea - Immunodeficiency
- Increased O2 requirement - Only maginally shortens the viral excretion &
clinical symptoms
- Encourage fluids
- Cough medicines, decongestants and sedatives, are not recommended. Cough medicines and
decongestants have not been proven to be helpful, and sedatives can mask symptoms of low blood
oxygen and difficulty breathing.
- Coughing is one way for the body to clear the lungs, and normally does not need to be treated. As
the lungs heal, coughing caused by the virus resolves. Smoking in the home or around the child
should be avoided because it can worsen a child's cough. The child should be kept out of
daycare or school until the fever and runny nose have resolved (eg. the time during which they are
most contagious).
Prognosis:
- Overall is good (90% will discharge well); most infants improve within 2-5 days, recover from
acute infection within 2 weeks
- Wheezing may last for 3-4 weeks
- 50% will have recurrent episodes of cough & wheeze over the next 3-5 years
Prevention:
- Monoclonal antibody of RSV
- IM injection monthly
- reduces the number of hospital admissions in high-risk infants (mainly preterm)
- Very expensive thus limited its usage in hospital
177
Differences between acute bronchiolitis, asthma & pneumonia:
Features Bronchiolitis Asthma Pneumonia
Age - Mostly infants <2 yrs old - Older children - Any age
Aetiology Virus Allergens Bacteria
Risk Factors - Pre-term infants - Family history of asthma - Immunodeficiency
- Congenital heart disease - URTI triggers (eg. Down`s syndrome)
- Atopy - Sick contact
- Weather
- Exercise-induced
Pathophysiology Inflammation of small Affects mainly airway. Lung infection.
airway. Particularly from Particularly from Mostly affect alveoli.
bronchioles onwards as bronchioles onwards as Some of the alveoli can
cartilages are replaced by cartilages are replaced by function, some can`t.
plaques. When part of the plaques. When part of the Hence there is a rapid
airway is partially or airway is collapsed, air breathing to enhance
completely blocked, trapping remains in the gaseous exchange at
wheezing occurs and air alveoli. those functional alveoli.
trapping remains in the
alveoli.
History - Happy wheezer - Shortness of breath - Appeared sicker, more
- Coryzal symptoms - Wheezing irritable.
- Low grade fever - Unable to speak in - Coryzal symptoms
- Shortness of breath complete sentence/ - High grade fever
- Wheezing words(normally no fever) - Loss of appetite
- Wheezing
Physical - Active expiration (due to - Active expiration - Shallow and rapid
Findings indrawing of stomach breathing
wall muscles to expel the
air out)
Chest - Labored breathing - Hyperinflated chest - Reduced on affected
Movements - Hyperinflated chest (air trapping) side
- Chest wall recession - Chest wall retraction
- Use of accessory muscle
178
Bronchial Asthma
Prof. Dr. Lucy Lum Chai See, MBBS(UM), MRCP(UK)
Definition:
- Chronic airway inflammation
- Leading to increase airway responsiveness that leads to: (Clinical triads in bolds)
- Recurrent episodes of wheezing
- Breathlessness (SOB)
- Coughing particularly at night or early morning (morning dip)
- Chest tightness
- Average daily diurnal PEF variability is >13% in children (>10% in adults)
- Often associated with widespread but variable and reversible airflow obstruction
either spontaneously or with treatment
- Physiological triad:
- Reversible bronchiolar muscle spasm
- Mucosal edema
-↑mucous production
Epidemiology:
- Most common chronic respiratory disorder in childhood
- Male : Female = 2:1 (In adult: Female > Male)
- Prevalence of asthma seems to have plateaued in Malaysia with 5.8% of children aged 6-7 years
and 8.9% of children aged 13-14% years.
- NHMS 2006 reported an asthma prevalence of 7.14% in children up to age of 18 years
- Prevalence is higher among urban and inner-city children eg. 7.3% (Muar) to 13.9% (KL)
- Responsible for 10-20% of acute admission in children aged 1-16 years
- Appear to have been a significant ↑in the incidence of asthma over the last 30 years
179
Pathophysiology:
Trigger factor
Pathogenesis:
- Very complex & NOT fully understood
- Involves a number of cells, mediators, nerves & vascular leakage which can be activated by
- Several mechanisms (commonest is exposure to allergens)
- Cellular components of inflammatory response (eg. eosinophils, T lymphocytes, macrophages
& mast cells)
2) Late phase
- Onset 4-6 hours, lasted up to 10 days
- Mast cell & alveolar macrophage release leukotriene, prostaglandin, thromboxane →
bronchoconstriction
- Chemotactic factor attracting the neutrophils, eosinophils & macrophages migration & platelet
activating factor → inflammation & edema of airway.
- Chronic changes: damage to respiratory tract epithelium → increase bronchial hyperresponsiveness
& smooth muscle hypertrophy, maintain by releasing bronchoconstrictor factor, or by local axon
reflexes thru exposed nerve fibres, lasting for days or weeks. With increasing severity & chronicity,
remodeling of the airways occurs, leading to fibrosis of the wall, fixed narrowing of the airway and a
reduced response to the bronchodilator medication.
Classification:
Intrinsic (Non-Atopic) Extrinsic (Atopic)
- Identified by bronchoprovocation test - Identified by positive skin prick test to
- Usually adulthood onset common allergens
* Less often used as all asthmatic patients show some degree of atopy
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Clinical features:
- May have multifactorial trigger factors
Symptoms Signs
Recurrent, episodic, diurnal pattern: Inspection
- Cough (nocturnal cough & early morning - Altered consciousness
exacerbation) - Respiratory distress
- Wheezing - Cyanosed
- Shortness of Breath - Dry skin, eczema
- Chest tightness - Percentile of weight & height↓
- Interval symptoms - BCG scar
- Response to asthma therapy - Mouth- oral candidiasis due to steroid puff
- Severity (no.of school missed, limitation of - Cushing features due to prolonged usage of
activity: eat, talk, walk, hx of nebulizer, steroid, myopathy, vocal cord paralysis
gas/puff) - Hyperinflated chest
(barrel-shaped or pectus carinatum)
- Recurrent chest infections - Harrison`s sulcus (anterolateral depression of
- Failure to thrive thorax at insertion of diaphragm, best seen on
sitting)
History of atopy: - Spine (asthma causes sclerosis & kyphosis)
- Eczema or dermatitis
- Allergic rhinitis(hay fever,early morning sniff) Palpation
- Allergic conjunctivitis, urticarial & - CO2 retention (warm periphery, bounding
angioedema, food & drug allergies pulse)
(absence of these conditions does not -↓chest movement
exclude the diagnosis) -↓vocal fremitus
- Family history of atopy -↑AP diameter (hyperinflated chest)
Percussion
Hyperresonance to percussion (displace liver >6
intercostal space- palpable liver, loss of cardiac
and liver dullness)
Auscultation
- Diminished air entry
- Vesicular breathing with prolonged expiratory
phase
- Generalized expiratory rhonchi
- Crepitations (In infants)
- Silent chest
* Signs of respiratory distress (nasal flaring, expiratory grunting, head bobbing, tachypnea,
suprasternal, supra-clavicular, intercostal & subcostal recession
(Presence of recession without tachypnea = in distress; Presence of tachypnea only = in distress)
* Presence of pulsus paradoxus (↓SBP >10mmHg when inspire: acute severe asthma, chronic obstructive
lung disease, pericarditis, cardiac tamponade) and silent chest indicates acute severe asthma
Diagnosis:
- Diagnosing asthma in preschool children is often difficult. Approximately half of all children
wheeze at some time during first 3 years of life.
181
A) Transient early wheezing (Episodic)
- Virus associated wheeze, episodic viral wheeze, wheezy bronchiolitis
- Due to small airways narrowing & obstruction 2` to inflammation & immune response to viral
infection
- Episodic nature, being triggered by viruses that cause common cold
-↓lung function from birth, from small airway diameter
- Risk factor: maternal smoking during/after pregnancy & prematurity
- Female, resolves by 5 years of age dt ↑ airway size
- Well between episodes, only wheeze with viral infections
C) Childhood asthma
- Clinical index to define risk of asthma in young children with recurrent wheeze
- Positive index children have 65% chance becoming asthmatic by 6 years old
- Negative index children have 95% not becoming asthmatic by 6 years old
Positive index (>3 wheezing episodes/year during first 3 years) + 1 Major criteria or 2 Minor criterias
Major criteria Minor criteria
- Eczema - Positive skin test
- Parental asthma - Wheezing without URTI
- Positive aoeroallergen skin test - Eosinophilia (>4%)
Management Plan:
- Assess asthma severity/ newly diagnosed asthma
- Choose preventer treatment (refer next page: Algorithm for long term management of asthma)
- Assess asthma control in 4-8 weeks (refer previous page: Evaluation of asthma control)
- Stepwise medication (refer next page: Algorithm for long term management of asthma)
- Monitor asthma control (refer previous page: Evaluation of asthma control)
* For any level, check compliance, technique & trigger factors
185
How to use Aerochamber:
- Shake the inhaler
- Remove the cap of inhaler
- Connect inhaler with mask spacer
- Mask spacer fully cover the mouth and nose (no gap)
- Press the inhaler to spray 1 puff of medication into it
- Ask patient hold for 20 seconds, count 10 valve flip (if valve
flip does not function, count chest expansion for 10 times)
How to clean Aerochamber:
- Rinse with water
- Do not brush (prevent electrostatic that causes particles of medications to attach to the wall
of Aerochamber and not entering patient`s airway)
- Dry in rain (not sun)
186
Pneumonia
Prof. Dr. Lucy Lum Chai See, MBBS(UM), MRCP(UK)
Definition:
- Infection of the lung parenchyma
- Infiltration of the interstitial tissue with inflammatory cells
Epidemiology:
- Incidence rate - Highest in infancy
- Remains relatively high in childhood
- Low in adult
- Increases again in old age
Aetiology:
Newborn Infancy Older children/Adult
- Bacteria from mother`s genital - Mostly viral, particularly RSV - Viral infection is rare
tract, usually during (preterm infants) - Bacteria are more common
intrapartum
- Group B β-hemolytic - RSV - Mycoplasma pneumoniae
streptococcus - Streptococcus pneumoniae - Streptococcus pneumoniae
- E.coli - Haemophilus influenzae - Chlamydia pneumoniae
- Gram -ve bacilli/ enterococci - Bordetella pertussis - Mycoplasma tuberculosis
- Proteus - Chlamydia trachomatis
- Klebsiella - Staphylococcus aureus Others:
- Listeria (most severe, a/w malnutrition) - Chlamydia psittaci
- Coxiella burnetti
- Legionella pneumophila
1-3 months Erythromycin
<1 month Penicillin, >5 years old Erythromycin +
Gentamycin 3 months - Ampicillin + Cloxa Ampicillin
5 years old /Augmentin
Aspiration pneumonia : Enteric gram -ve bacteria +/- Strep Pneumoniae, S. Aureus
Immunocompromised : Bacterial (Pneumocystis jiroveci, TB)
Viral (CMV, VZV, HSV, Measles, Adenovirus)
Fungi (Aspergillus, Candica, Histoplasma)
187
Clinical Features:
Symptoms Signs
- Fever Inspection
- Cough (sometimes with sputum production in - Grunting, air hunger, tachypnea, toxic-looking,
older children) cyanosis, nasal flaring, head retracted, recession
- Breathlessness (intercoastal, subcoastal, supraclavicular)
- Rapid & SHALLOW breathing (impression that a
child is afraid to breath deeply) Palpation
- Runny nose ↓Chest movements
- Lethargy ↑tactile fremitus
- Restless, Agitated, Irritated
Percussion
- Pleural inflammation Maybe
Dull to percussion
- Pleuritic chest pain (worsen on inspiration) absent in
- Neck stiffness (involve upper lobe) Auscultation infants
- Abdominal pain (involve lower lobe) - ↓breath sounds
- Bronchial breath sounds
- Coarse crepitations
- Pleural rub
-↑vocal fremitus
Complications:
- Parapneumonic effusion
- Empyema (infected pleural effusion)
- Usually associate with Pneumococcus (childhood)
(For adults: penicillin resistant S.aureus, gram-ve bacteria & anaerobic bacteria)
- Rx : drainage by intercostal chest drain or surgery
- Septicaemia
- Lung abscess
Assessment of severity:
- Essential for optimal management of pneumonia
- Categorized according to mild, severe, very severe based on respiratory symptoms as shown
below:
< 2 months old 2 months - 5 years old
Mild Pneumonia - Rapid breathing -
Severe - Chest indrawing - Severe chest indrawing
Pneumonia - Rapid breathing
Very severe - Not able to drink - Not feeding
pneumonia - Convulsions - Convulsions
- Drowsiness - Abnormally sleepy or difficult to wake
- Malnutrition - Fever/low body temperature
- Hypopnea with slow irregular breathing
Investigations:
- Children with bacterial pneumonia cannot be reliably distinguished from those with viral disease on the
basis of any single parameter, clinical, laboratory or chest radiograph findings.
- Chest radiograph is indicated when clinical criteria suggest pneumonia. It will not diagnose aetiological
agent. However the chest radiograph is not always necessary if facilities are not available or the
pneumonia is mild
- If recurrent pneumonia, exclude cystic fibrosis, immunodeficiency status
188
Blood - FBC (WBC)
-↑Predominance of polymorphonuclear cells suggest bacterial cause
-↓Either suggest a viral cause or severe overwhelming infection
- Blood culture & sensitivity
Remains the non-invasive gold standard for determining the previse
aetiology of pneumonia. However the sensitivity of this test is very low.
+ve blood cultures are found only in 10% to 30% of patients with
pneumonia. Blood culture should be performed in severe pneumonia or
when there is poor response to the first line antibiotics.
Nasopharyngeal aspirate - Viral isolatoin, C&S
BUSE - Hyponatraemia (SIADH)
CXR - Lobar consolidation
- Widespread bronchopneumonia
- Cavitation (less common)
Pleural Fluid - If there is significant pleural effusion diagnostic pleural tap will be
helpful
Serology - Mycoplasma pneumoniae, Chlamydia, Legionella and Moraxella
catarrhalis are difficult organism to culture, thus serology is performed
in patients with suspected atypical pneumonia. Acute phase serum titre
more than 1:160 or paired samples taken 2-4 weeks apart showing 4
fold rise is a good indicator of Mycoplasma pneumoniae infection. This
test should be considered for children aged 5 years or older.
Pulse oximetry - Assessment of oxygenation, pulse oximetry is the best measurement
for hypoxia which avoid the need for arterial blood gases. Good
indicator for severity of pneumonia.
Recurrent pneumonia
- Max 6 admissions/year, if exceeded must further investigate
- Aspiration: GERD, Vocal cord palsy
- Immunodeficiency
- Congenital cardiac disease (ASD, VSD, PDA)
- Obstruction (lymph node, vascular ring, foreign body)
-↓mucous secretion (asthma, Cystic fibrosis)
- Lung deformity (Tetralogy of Fallot)
Management:
- Divided into supportive & pharmacological measures
- Criteria for hospitalization:
- Children aged <3 months whatever the severity of pneumonia
- Fever >38.5 `C, refusal to feed and vomiting
- Fast breathing with or without cyanosis
- Associated systemic manifestations
- Failure of previous antibiotic therapy
- Recurrent pneumonia
- Severe underlying disorders (eg. Immunodeficiency)
189
Supportive Measures:
Fluids Oral intake should cease when a child is in severe respiratory distress. In severe
pneumonia, secretion of ADH is ↑ which means that dehydration is uncommon.
It is important that the child should not be overhydrated.
Oxygen Oxygen reduces mortality a/w severe pneumonia. It should be given especially
to children who are restless, tachypnoeic with severe chest indrawing, cyanosed
or not tolerating feeds. It is important to maintain the SaO2 >95%.
Temperature The rationale to use paracetamol is only to ↓ discomfort from symptoms. The
control PCM will not abolish fever.
Chest To assist in the removal of tracheobronchial secretions. Intention is to remove
physiotherapy airway obstruction,↑gas exchange and ↓the work of breathing. There is no
evidence to suggest that chest physiotherapy should be routinely done in
pneumonia.
Cough syrup It is not recommended as it causes suppression of cough and may interfere with
airway clearance. Adverse effects and overdosage have been reported.
Pharmacological Measures:
When treating pneumonia, the clinical, laboratory and radiographic findings should be considered. Other
factors include age of the child, local epidemiology of respiratory pathogens and sensitivity of these
pathogens to particular microbial agents and the emergent of antimicrobial resistance. The severity of
the pneumonia and drug costs has also a great impact on the selection of therapy. The majority of
childhood infections are caused by viruses and do not require any antibiotic. However, it is also very
important to remember that we should be vigilant to choose appropriate antibiotics especially in the
initial treatment to reduce further mortality and morbidity.
For inpatient management of children with severe pneumonia, the following antibiotics are
recommended:
1st line : β lactam dugs : Benzylpenicillin, Amoxycillin, Ampicillin, Amoxycillin-Clavulanate
2nd line : Cephalosporins : Cefotaxime, Cefuroxime, Ceftazidime
3rd line : Carbapenem, Imipenem
Others : Aminoglycosides, Gentamicin, Amikacin
If there are no signs of recovery, patients remain toxic and ill with spiking temperature for 48-72 hours, a
second line antibiotics need to be considered. If Mycoplasma or Chlamydia species are the causative
agents, a macrolide is more appropriate. A child admitted to hospital with severe community acquired
pneumonia must receive parenteral antibiotics. As a rule, in severe cases of pneumonia, combination
therapy using a second or third generation Cephalosporins and macrolide should be given.
Predominant bacterial pathogens of children and the recommended antimicrobial agents to be used:
Pathogens (β-lactam susceptible) Antimicrobial agents
Streptococcus pnuemoniae Penicillin, Cephalosporins
Haemophilus influenzae type b Ampicillin, Chloramphenicol, Cephalosporins
Staphylocccus aureus Cloxacillin
Group A Streptococcus Penicillin, Cephalosporin
Mycoplasma pneumoniae
Chlamydia pneumoniae Macrolides such as erythromycin and azithromycin
Bordetella pertussis
In children with mild pneumonia, their breathing is fast but there is indrawing of chest, antibiotics can be
prescribed orally in outpatient. The mother is advised to return in 2 days for reassessment or earlier if the
child is getting worse.
190
Viral Infection
- Primary viral pneumonia tends to be more insidious onset, less toxic and dyspnoeic
- CXR are much less impressive than bacteria pneumonia
- Radiological features tend to show a more fluffy or patchy appearance often radiated from 1 or
both hilar region.
- Usually bronchopneumonia but lobar pneumonia is still possible
- Treatment is mainstay supportive (antibiotic therapy is indicated when there is fever)
Staphylococcal infection
- Staphylococcus aureus (S.aureus) responsible for a small proportion of acute respiratory
infections in children (common in infant). Nevertheless a high index of suspicion is required
because of the potential for rapid deterioration. It is chiefly a disease of infants and has a
significant mortality rate.
- Radiological features include the presence of multilobar consolidation, cavitations,
pneumatocoeles (tension cysts), spontaneous pneumothorax, empyema and pleural effusion.
- Treatment with high dose Cloxacillin (200mg/kg/day) for a longer duration and drainage of
empyema will result in good outcome in the majority of cases.
Mycoplasma infection
- This is a very common cause of pneumonia in child >5 years old.
- Onset is usually subacute. (1 or 2 weeks)
- Symptoms include general malaise, fever, headache, irritating and paroxysmal cough
resembling pertussis. CXR are often remarkably few and less characteristic. But one is
frequently surprised at the extent of consolidation compared with the paucity of clinical sign.
- Diagnosis is established by mycoplasma serology.
- Erythromycin is the drug of choice.
Chlamydia pneumoniae
- 2-19 weeks after birth
- Conjunctivitis, URTI >1 week, afebrile
- Physical findings: Crackles, occasional rhonchi, staccato cough, tachypnea
- CXR: Hyperexpanded lung & bilateral infiltrate
- Eosinophils ↑(>400/mm3, IgM, IgG)
191
Foreign Body Aspiration
Prof. Dr. Lucy Lum Chai See, MBBS(UM), MRCP(UK)
Epidemiology:
- Majority are <4 years old
- Most death 2` to foreign body aspiration occurs in this age group.
- Right mainstem bronchus takes off at a less acute angle than left mainstembronchus,
foreign bodies tend to lodge in right airways. Thus, pathology occurs more on right lung.
Clinical features:
Symptoms Signs
- Clear histories of choking, witnessed aspiration, - Cough
physical or radiographic evidence of foreign - Localized wheezing
body aspiration - Unilateral absence of breath sounds
- Most foreign bodies are small and quickly - Stridor
expelled, some remain and causes persistent - Bloody sputum (rarely)
cough, sputum production or recurrent
pneumonia.
- Suspect foreign body aspiration when:
- Persistent wheezing unresponsive to
bronchodilator therapy
- Persistent atelectasis
- Recurrent or persistent pneumonia
- Chronic cough without other explanation
Differential diagnosis:
- Oesophageal foreign bodies (can cause persistent stridor or wheezing + dysphagia)
Diagnostic studies
- Expiratory and lateral cubitus chest radiograph:
- Reveal presence of radiopaque objects & focal air trapping, especially on expiratory film
- Fluoroscopy: for children who cannot perform expiratory views
- Rigid bronchoscopy: for strong evidence of foreign body aspiration. Best for removal of
foreign body.
- Flexible bronchoscopy: Used to locate an aspirated foreign body.
Aspiration Pneumonia
Prof. Dr. Lucy Lum Chai See, MBBS(UM), MRCP(UK)
- Defined as the inhalation of either oropharyngeal or gastric contents into the lower airways
(act of taking foreign material into the lungs)
- For it to occur, there must be a breakdown of usual defenses that normally protect the
tracheo-bronchial tree as well as pulmonary complications that result from aspiration event
- Most commonly occurs in individuals with chronically impaired airway defense mechanisms,
such as gag reflex, coughing, ciliary movement, and immune mechanisms, all of which aid in
removing infectious material from the lower airways
- Can occur in community or in a hospital/health care facility (eg. nosocomial). In both
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situations, anaerobic organisms alone or in combination with aerobic and/or microaerophilic
organisms play a role in the infection. In anaerobic pneumonia, the pathogenesis is related
to the large volume of aspirated anaerobes (eg, as in persons with poor dentition, poor oral
care, and periodontal disease) and to host factors (eg. alcoholism) that suppress cough,
mucociliary clearance, and phagocytic efficiency, both of which increase the bacterial
burden of oropharyngeal secretions
Clinical features:
- More rapid onset * History of last feeding is very important!
- May or may not be preceded by URTI (inhalation case)
Risk factors:
Introduction:
- Acute tracheobronchitis that begin with mild URTI symptoms followed by a severe paroxysmal
cough
Epidemiology:
- All ages are affected but 90% of cases occur in children <5 years of age
- About 70% of unimmunized children are affected by the age of 5 years old
- Highly contagious notifiable disease
Aetiology:
Bordetella pertussis : encapsulated gram -ve coccobacillus
Pathogenesis:
- Pathogen only for human
- Transmitted via airborne droplets, produced during the cough episode
- Attachment of the pili (filamentous hemaglutinin) to the cilia of the epithelial cell, decreased
cilia activity followed by death of the ciliated epithelial cells
- Pertussis toxin stimulates adenylate cyclase, then rise in cyclic AMP-dependent protein kinase
activity, causes a failure of lymphocytes to enter the lymphoid tissues, then a striking
lymphocytosis in the blood
Clinical features:
- Incubation period is 7-14 days (Oxford: 10-14 days)
- Symptoms may persist for 10-12 weeks
- Most contagious during first 2 weeks of cough
- May occur in the immunized child but it is almost invariably less severe
- In very young infant (<3 months) cough & catarrhal sp are less marked and the presentation is
only recurrent attack of apnoea & cyanosis, which increases mortality
Symptoms
Catarrhal stage (1-2 weeks)
- Coryzal symptoms (runny nose, conjunctivitis, malaise)
Diagnosis:
- Mainly clinical, particularly if a typical paroxysmal cough & lymphocytosis
- Confirmed by isolation of B. pertussis from the patients` nasopharyngeal secretion
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Investigation:
- per-nasal swab or sputum for culture (unsatisfactory as organisms die on the way to the lab &
slow to culture)
- Nasopharyngeal aspirates
- Agglutination/serology test (not useful for diagnosing acute infection, but convalescent
phase is confirmatory)
- Direct fluorescent antibody testing is specific but insensitive, not recommended)
- PCR (sensitive as culture but not specific)
- Blood investigation
- FBC (marked lymphocytosis >15,000 cells/mm3 or >10,000 cells/mm3)
Management:
- Admit patient to hospital if <6 months of age (risk of apnoea)
- Clearing the upper airway of mucus and O2 therapy
- Azithromycin, clarithromycin, erythromycin under 1 month age, TMX for older than 2 months
- Erythromycin to eradicate the organisms (if started during catarrhal phase, else):
- reduce the number of organism (spread) but no reduction in severity or duration of illness as
toxin has already damaged the respiratory mucosa
- risk of having side-effect: infantile hypertrophied pyloric stenosis (IHPS) -> azithromycin
- Salbutamol + corticosteroids (Oxford HOS) - ineffective
Prevention:
- Immunization reduces pertussis by 80-90% (but does not guarantee protection)
- Macrolides effective in preventing secondary cases in contacts exposed to pertussis
- Underimmunised close-contacts under 7 years of age should receive a booster dose of DTaP
(unless a booster dose has been given within preceding 3 years), whereas those 7-10 years of
age should receive Tdap.
- All close-contacts should receive prophylactic antibiotics for 5 days (azithromycin) or 7-14
days (clarithromycin or erythromycin, duration based on age)
Complications:
General - Malnutrition
CNS - Apnoea, cerebral anoxia with convulsions (young infants)
- Encephalopathy (permanent disability)
Respiratory System - Lobar pneumonia (secondary to bacterial infection, 90% of death)
- Atelectasis, Bronchiectasis (late) - secondary to mucosal plugs
- Pneumomediastinum, Pneumothorax
- Interstitial or subcutaneous emphysema
HEENT - Subconjunctival haemorrhage
- Periorbital petechiae
- Otitis media
- Sinusitis
Others - Rectal prlapse
(due to prolonged - Inguinal hernia
coughing fits) - Frenulum tear
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Cystic Fibrosis
Epidemiology:
- Most common serious genetic disorder of Caucasians.
- Carrier rate in Caucasians of 1 in 25, with 1 in 2500 affected births.
Aetiology:
- AR disorder arising from mutation in a gene on long arm of chromosome 7 which codes for
protein called Cystic Fibrosis Transmembrane Conductance Regulator (CFTR).
- Most common mutation in 70% of cases: 3-base pair deletion that removes the phenylalanine
of position 508 (ΔF508).
Pathophysiology:
- Mutations in CFTR causes defective cAMP-dependent chloride ion transport across epithelial
cells and increases the viscosity of secretions especially in respiratory tract and exocrine gland.
- There is also abnormal transport in sweat gland epithelium resulting in high concentration of
Na and Cl in sweat
Clinical features:
Respiratory tract Abnormal ions transport aross epithelial cells
↓
Reduced airway surface liquid layer, impaired ciliary function & retention
of mucopurulent secretion
↓
Increases viscosity of secretion in airway
↓
- Recurrent chest infection by:
- Staphylococcus aureus
- Haemophilus influenza
- Pseudomonas aeruginosa
- Burkholderia cepacia
↓
- Bronchiectasis and abscess formation (bronchial wall damage)
Symptoms Signs
- Recurrent, productive cough - Clubbing, HPOA
- Copious sputum, smelly & - Hyperinflation
change in odour - Coarse inspiratory crackles
- SOB - Expiratory wheezing
- Lobar collapse, Pneumothorax
- Scoliosis, Chest scars (portacath)
Exocrine gland - Pancreatic insufficiency (deficient in lipase, amylase, protease)
↓ (low fecal elastase)
Maldigestion →Malabsorption → Malnutrition → Failure to thrive (90%)
- Diabetes Mellitus (steatorrhoea)
GIT - Meconium ileus during neonatal period (10-20%) [normal: 24-48 hrs]
- Treated with Gastrograf in enema or surgery
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- Distal intestinal obstruction syndrome (adolescent/ younger adults)
- Intussusception
- Rectal prolapse (>18 months, resolves quickly on starting CREON)
- NASH (fatty liver), cirrhosis, hepatosplenomegaly, portal hypertension
- Cholesterol gallstone, pericholangitis
Joints - Cystic fibrosis-related arthropathy (episodic, <1 week, non-erosive, large
joint involvement)
- Hyperthrophic pulmonary osteoarthropathy (HPOA)
ENT - Nasal polyps
- Sinusitis
CVS - Right-sided heart failure (late, 2` to severe lung disease)
Reproductive - Males are infertile (absent vas deferens)
- Pubertal delay
Management:
- Multidisciplinary (involved paediatrician, physiotherapist, dietitian, nurse, primary care team
and patient`s parents)
- Aims to ensure optimum physical & emotional growth & to delay onset of pulmonary disease:
- General growth & development
- Respiratory pathogens
- Requency & severity of chest infections & lung function
- Nutrition & GI symtoms
- Development of diabetes, liver or joint disease
- Psychosocial problems (school progress etc)
- Fertility & genetic counseling (later stage)
- Oxygen at home as
disease progresses *CREON contains
amylase, lipase &
*Antibiotics should protease which have
cover S. aureus, marked effect of
H. influenza & steatorrhoea and allow
Pseudomonas sp. catch up growth
Others
- Mucolytics (eg. Dnase or hypertonic saline)
- ERCP for gallstones, Liver transplant for severe liver cirrhosis
- Heart-lung transplant or bilateral lung transplant (end-stage disease, >50% survival 10 years)
- NSAIDS/ short course corticosteriods (CF-related arthropathy/HPOA)
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Cystic Fibrosis Long Case (Template)
The hinge of scoring a CF case is to really focus on the chief complaint, do not be narrow-minded
of the cause of respiratory diseases and got carried away by the underlying CF, come out with
differentials of current symptoms, identify current issues to be addressed and present relevant
past medical history of CF.
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A. History
Presenting complaint
Respiratory diseases Productive cough (younger children might not be able to expectorate),
SOB, reduced effort tolerance, fever
HOSPI: For each symptom, ask for duration, chronology of each happening and correlate them with
one another
Associated symptoms Onset: Acute / gradual
URTI symptoms: Runny nose, red eyes, ear discharge, sore throat, horse
crying voice
Cough: Productive or non-productive, sputum volume, colour, blood
Fever: Pattern, documented temperature, relieve with medication
Pain: Pleurisy chest pain
SOB: Cyanosis, intercostal recession, quantify reduced effort tolerance,
orthopnoea, PND
Allergens/ irritants: Wheeze, diurnal variation, precipitating factors such as
cold, fur, dust
TB symptoms: Chronic cough, night sweat, LOW, LOA, sick contact,
crowded place
Progression Progressively worsening over the past few days / years, similar or worse
than previous episodes, frequency in a month / year
Severity Disturbed sleep, poor feeding, inactivity
Past Complications Pneumothorax, moderate-to-large haemoptysis, allergic
bronchopulmonary aspergillosis (ABPA)
Past investigations Sputum colonisation, chest X-ray, pulmonary function tests, overnight
oxymetry
Home management Exercise, Chest physiotherapy (frequency, type and by whom), PEP mask;
antibiotics (nebulised/ oral/ parenteral), saline, bronchodilators,
corticosteroid; venous port access
Systemic review
Gastrointestinal disease - Rectal prolapse (feeling of something coming out during defecation, pain
upon defecation)
- Symptoms of intestinal obstruction, vomiting, abdominal pain,
constipation
Endocrinology diseases - Symptoms of DM (found to be hyperglycemic), polyuria, polydipsia,
polyphagia
- symptoms of pancreatic insufficiency, pale oily stool, poor weight gain,
failure to thrive
Joint diseases - Large joint pain
CVS diseases - Palpitation
Reproductive system - Breast pubic hair and external genitalia maturation delay
Past medical history
Diagnosis Initial symptoms, investigations and management prior to diagnosis,
diagnosis (when, where, how)
Progression Hospitalisation details (frequency, duration, usual treatment)
Complications Frequent respiratory disease
Antibiotic resistant infection
Venous port: thrombosis, infection, haemorrhage, embolism, loss of
venous access and needle phobia
Follow up Outpatient clinics attended (where, how often, routine tests performed:
weight, nutrition, sputum, spirometry, OGTT, LFT, pancreatic function test,
HRCT )
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Gestational history
Antenatal diagnosis Antenatal diagnosis of child with CF with known parental genetic status/
previous CF siblings
Birth history
Complications Perinatal meconium ileus
Developmental milestone
Developmental delay Motor developmental delay due to failure to thrive (poor bone and muscle
growth)
School performance, slow learner
Drug history
What drug Types and purpose, traditional/ self-prescribed medicine
Compliance Is the patient compliant, can patient take the drug by self, if not aided by
who
Side effects Long term oral steroid: HPT, central obesity, easy bruising
Allergies
Vaccination
Schedule vaccination up to date or ever halted due to infection episodes ; when is
the next vaccination due; early measles immunisation
Extra immunisation pneumococcal, influenza vaccines, gamma-globulin for measles contacts,
yearly influenza vaccine
Allergy history
Allergies to food or drug. Presentations of allergies. Management of
allergies (desensitization)
Diet history
Sufficient calorie intake Quantity of milk per feed, frequency of feeds per day, formula or breast
(CF patient need 120% of milk, high energy and fat diet, nasogastric tube or gastrostomy
normal energy Vitamin A,D,E,K supplementation
requirement )
Family history
Metabolic diseases HPT, DM
Hereditary diseases Consanguinity, Thalassemia, other siblings affected / screened as carrier
Social history
Smoke and alcohol Active and passive smoking, pack years – poorer prognosis
exposure Alcohol unit per week – increase risk of pancreatitis
Disease impact on patient Independence, normal social life, school performance, acceptance,
understanding and anticipation on disease, consideration of marriage, (for
male adolescent), infertility
Disease impact on family Financial constrain, discord in marriage, tension in parenting, neglect of
other children
Support Financial aid, insurance coverage, social supportive groups, information
source, counseling, training, main caretaker
Future plans Lung transplantation
B. Physical examination
Assess patients with CF for disease progression, severity and the current status of the disease. It looks
particularly at clubbing, flap, chest deformity, cor pulmonale, nutrition, puberty, diabetes, chronic liver
disease and hypertrophic pulmonary osteoarthropathy. Two very important signs are the cough and
the sputum.
General inspection Parameters Nutrition
- Weight, Height - Muscle bulk (protein); e.g. biceps,
- Head circumference quadriceps
- Percentiles - Subcutaneous fat, eg. mid-arm,
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Pubertal status (delay): breast, subscapular
pubic and axillary hair, voice, - Pallor (anaemia)
external genitalia
Peripheral stigmata of CLD,
Sick or well jaundice, anasarca
Vital signs Oedema (hypoproteineamia)
- Respiration
Use of oxygen supplement
- Pulse
Bedside adjuvants: inhaler
- Temperature
Sputum pot
- Urinalysis (glucose)
Upper limbs Nails Flap
- Clubbing - Hypercapnia
- Cyanosis - Liver failure (rare)
- Leukonychia (CLD)
Skin
Fingers - Bruising or petechiae (CLD,
- Fingertip prick marks (BSL testing) vitamin K deficiency)
- HPOA - Spider naevi (CLD)
- Scratch marks (cholestasis)
Palms
- Erythema (CLD) Muscle: bulk (palpate, if not done
- Crease pallor (anaemia) already)
Pulse
Axilla: hair, odour (Tanner staging)
- Paradoxus (severity of airway
obstruction)
- Alternans (CCF)
- Bounding (hypercapnia)
Head Eyes Mouth
- Conjunctival pallor - Angular cheilosis
- Scleral icterus - Central cyanosis (lips, tongue)
- Retinal venous dilation - State of teeth, dental hygiene
(hypercarbia) - Oral thrush
Ears Face
- Secretory otitis media - Cushingoid (systemic steriods)
- Hearing (aminoglycosides) - Acne and facial hair (pubertal
status)
Nose: Nasal polyps
Chest Inspection Palpation: Tracheal position, apex
- Chest deformity: pectus position, palpable P2
carinatum, increased AP diameter
(hyperinflation), thoracic Percussion for hyperinflation,
kyphosis consolidation
- Scars: previous pneumothorax,
bilateral lung transplant, venous Auscultation (note: may be normal
access port (eg.Port-A-Cath, even in moderately severe CF)
Hickman) - Air entry
- Tanner stage of breast - Breath sounds
development - Vocal resonance
- Harrison's sulcus - Adventitious sounds
- Chest expansion - Crackles
- Cough: moist, productive, request - Wheezes
sputum - Loudness of second heart sound
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- Perform peak flow measurement if (pulmonary hypertension)
meter available (limited usefulness) - Gallop rhythm (cor pulmonale)
Abdomen Inspection Palpation
- Distension (poor abdominal - Liver ptosis (chest hyperinflation);
musculature with protein-calorie liver edge—is it firm, or is it bumpy
malnutrition, ascites with CLD) (cirrhotic)?
- Scars (e.g. gastrostomy, previous - Hepatomegaly (fatty liver with
meconium ileus, hepatobiliary malabsorption or corticosteroid
surgery for common bile duct use, CCF with cor pulmonale)
stenosis, fundoplication) - Splenomegaly (portal
- Venous access port (e.g. Infuse-A- hypertension)
Port) - Faecal masses (DIOS can present
- Prominent abdominal wall veins as a right iliac fossa mass)
(CLD) - Herniae
- Needle marks (diabetes mellitus) - Assess for ascites (fluid thrill,
- Tanner stage of pubic hair shifting dullness)
- Striae (corticosteroids)
- Examine genitalia
-Inspect anus for rectal prolapse
- Tanner staging
- Hydrocoele
Lower limbs Inspection Gait examination
- Toe clubbing - Peripheral neuropathy (vit E
- Bruising (vit K deficiency, CLD) deficiency)
- Joint swelling (arthropathy) - Cerebellar ataxia (vitamin E
deficiency)
Palpation: Ankle oedema
- Proximal muscle weakness
(hypoproteinaemia)
(corticosteroids)
C. Discussion
1. What is the differential diagnosis of recurrent lung infection?
- Bronchiectasis
- Congenital heart disease (paeds), heart failure causing pulmonary oedema / pleural effusion
acts as a breeding ground for bacteria
2. Why patient has to take nebulized saline and Ventolin?
- To clear respiratory secretions
- Ventolin acts as bronchodilator
3. What is the prognosis of cystic fibrosis?
- Median survival age is 36 years old
- 90% mortality due to respiratory disease, followed by liver cirrhosis
- Poorer prognosis if:
- Female sex (teenage and young adult age period);
- Pancreatic insufficiency;
- Complications, including CFRD or CFLD, or ABPA;
- Abnormal chest X-ray 12 months after diagnosis;
- Lung infection with B. cepacia;
- Age of acquisition of chronic pulmonary infection with P. aeruginosa under 6 years;
- Fall-off in growth curves
- Recurrent haemoptysis;
- Pneumothorax;
- Onset of cor pulmonale;
- Cigarette smoke exposure;
- Poor socio-economic status;
- Non-CF-clinic care.
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Bronchopulmonary Dysplasia (Chronic lung disease of prematurity)
Pathology:
- Chronic lung damage as a result of:
- Pressure & volume trauma (from artificial ventilation)
- Oxygen toxicity
- Infection (Pertussis, RSV)
- Accumulation of lung secretion
Clinical features:
- Chest hyperinflation, intercoastal & subcoastal recession
Chest X-ray of bronchopulmonary
- Crepitations on auscultation
disease showing hyperexpanded lungs
- Oxygen requirement (on any oxygen supply) with diffuse fibrosis. A nasogastric tube
Investigations: is in situ.
Management:
Non- Pharmacological Pharmacological
- Artificial ventilation - Surfactant therapy
- Some may need long-term home O2 - Reduces duration of ventilation & reduces
- Others wean to cPAP, followed by BPD in ELBW group infants
additional ambient O2 - Corticosteroid (if ventilator dependent)
- Facilitate early weaning from ventilator
- Decrease O2 requirement
- May have long-term adverse effect on neuro-
developmental outcome (eg. CP),
hypertension, hyperglycaemia, hypertrophic
cardiomyopathy.
- Diuretics (if ventilator dependent)
Complications:
- Intercurrent infection
- Cor pulmonale or pulmonary hypertension
- Respiratory failure
- Air leaks, subglottic stenosis, tracheal stenosis (complication from ventilation)
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PART VI
GASTROENTEROLOGY
Acute Gastroenteritis (AGE)
Definition:
- Gastroenteritis is the inflammation of stomach & intestine
(hallmark: increased stool frequency with alteration in stool consistency)
- Acute gastroenteritis (<2 weeks duration)
- Chronic gastroenteritis (>2 weeks duration)
Epidemiology:
- Major cause of paediatric morbidity & mortality around the world, especially in developing
world. Dehydration is the most frequent & dangerous complication (ORS is life-saving)
- Related to malnutrition, poor hygiene, poor socioeconomic status, education level and bottle
feeding
Aetiology:
Virus Bacteria Parasite
- Rotavirus (most common) Enteroinvasive (Bloody diarrhoea) - Entamoeba histolytica
- Winter months epidermic - Campylobacter jejuni - Giardia lambdia
- Age btw 6 months & 2 years (commonest of bacterial origin) - Cryptosporidium spp
- Shigella - Cyclospora cayetanensis
- Salmonella
- Enteropathogenic E. coli (EPEC)
- Yersinia
Enterotoxigenic (Watery diarrhoea)
- Vibrio cholerae
- Enterotoxigenic E. coli (ETEC)
(commonly ask in OSCE station) - Bacillus cereus
- Adenovirus (40, 41) - Clostridium perfringens &
- Norovirus (Norwalk virus) difficile
- Coronavirus - Staph. aureus
- Astrovirus
- Pararotavirus
* Cholera & ETEC infection: profuse, rapidly dehydration diarrhea
* Campylobacter jejuni: severe abdominal pain
* Shigella & salmonella: dysentery, abdominal pain, tenesmus
Pathophysiology
- Acquired by person to person spread or ingestion of contaminated food and drink
- Colonisation of the gut by enteropathogens may or may not cause clinical symptoms
- When virulence of the organism > protective factor of the gut,
- Definitive clinical sequence of event is through invasive or enterotoxin route
- Mucosal injury & inflammation - interfering w fluid, electrolyte imbalance & gut absorption
Clinical feature:
- Diarrhoea (acute onset)
- Increased stool frequency, fluidity & volume compared to normal
- Stool weight >250g/day
- Greenish +/- mucus +/- blood or musty colour (invasive bacterial infection)
- Vomiting (acute onset)
- Abdominal pain and distention
- Fever, lethargy, dizzines (systemic manifestation)
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Physical Examination:
- Assess hydration status (<5% dehydration there is no reliable clinical findings)
- Electrolyte imbalances:
- Acidosis: tachypnoea (Kussmaul breathing)
- Potassium depletion: hypotonia, weakness
- Hypocalcaemia: neuromuscular instability
- Hypoglycaemia: lethargy, coma, convulsions
Investigations:
Blood - FBC (leukocytosis)
- BUSE + creatinine (for dehydration & electrolyte imbalance)
- Hypo/hypernatremia, hypochloremia
- BUN: creatinine (disproportionate high in severe dehydration)
- Serum bicarbonate (low in metabolic acidosis)
- RBS (poor intake resuls in relative hypoglycaemia)
Stool - Stool for rotavirus antigen (eg. Rotaclone)
- Stool C&S (Salmonella, Shigella, Yersinia, Campylobacter)
- Stool red cells & leucocytes
- Stool ova & cyst
Others - ABG (metabolic acidosis)
- Urine osmolality (increased in dehydration)
Complications:
Renal - Oliguria (<200 ml/m2/day or <0.5 ml/kg/hr)
- If pre-renal AKI, urine osmolality>500, urine Na<10 mmol/L, urine urea
>250 mmol/L, urine:plasma osmolality ratio >1.3
- Urgent IV volume re-expansion, if no recovery of renal function, give
minimal maintenance fluid + losses only, without potassium, dialysis is
necessary if persistent hyperkalemia and uncorrected acidosis, recovery is
seen with polyuric phase of ATN
- Hypovolemic shock
- Electrolyte imbalance
- Metabolic acidosis
- Renal venous thrombosis (haematuria+renal mass)
- Haemolytic uraemic syndrome (haemorrhagic colitis by S.dysenteriae, E.coli
- Acute onset of miroangiopathic haemolytic anaemia, thrombocytopenia,
acute renal impairment, multisystem involvement)
CNS - Convulsions
- Hypernatraemia, hypoglycaemia, febrile convulsions, other electrolyte
disturbance, cerebral haemorrhage
- Usually associate with Shigella infection
GIT - Prolonged diarrhoea (>14 days)
Diagnosis:
- Clinical diagnosis, however AGE is diagnosis of exclusion (after excluding other differential
diagnosis as diarrhoea and vomiting are non-specific symptoms in young children)
206
Differential diagnosis:
Systemic infection - Septicemia
- Meningitis
Local infection - Respiratory infection
- Otitis media
- UTI
- Hepatitis A
Surgical cause - Pyloric stenosis
- Intussusception
- Acute appendicitis
- Necrotising enterocolitis
- Hirchsprung`s disease
Metabolic disorder - Diabetic ketoacidosis (DKA)
Renal disorder - Haemolytic uraemic syndrome (HUS)
Others - Coeliac disease
- Lactose intolerance
- Cow`s milk protein intolerance
- Adrenal insufficiency
Management:
- AGE wil lead to various degree of dehydration. According to APLS protocol, assessment of the
state of perfusion of child is the first step in management
- Identify whether child in shock (tachycardia, weak peripheral pulses, delayed capillary refill
time >2s, cold peripheries, depressed mental state with/without hypotension)
- If child is in shock, proceed to treatment Plan C immediately. Else, assess the degree of
dehydration using WHO chart as followed:
Assess
Look at general Well, alert Restless or irritable Lethargic or
condition of child unconscious
Look for eyes No sunken eyes Sunken eyes Sunken eyes
Offer child fluid Drinks normally Drinks eagerly, thristy Nor able to drink or
drink poorly
Pinch abdomen skin Skin goes back Skin goes back slowly Skin goes back very
immediately slowly (>2s)
Classify & Decide
Mild dehydration (<5%) Moderate dehydration Severe dehydration
IMCI: No signs of (5-10% dehydrated) (>10% dehydrated)
dehydration ≥2 above signs ≥2 above signs
IMCI: Some signs of
dehydration
Treat
Plan A Plan B Plan C
Give fluid and food to Give fluid and food for Give fluid for severe
treat diarrhoea at home some dehydration dehydration
Rehydration fluid:
Deficit = % dehydration x Weight (kg) + maintenance fluids + continuing losses
- Use 5% dextrose/0.45% saline (or 5% dextrose/0.9% saline) depending on plasma sodium & calculated
today body sodium. If severe acidosis (pH<7.0) treat with bicarbonate (half the deficit)
- Eg. 10 kg child with 5% dehydration has loss 5/100 x 10000 g = 500 ml of fluid deficit
207
208
Initial fluids for resuscitation of shock:
- 20 ml/kg of NaCl 0.9%
- Hartmann solution as a rapid IV bolus
- Repeated if necessary until patient is out of shock or if fluid
overload is suspected
- Review patient after each bolus
- Calculate the fluid needed over the next 24 hours:
- Fluid for Rehydration (also called fluid deficit) + Maintenance
(minus the fluids given for resuscitation)
- Fluid for Rehydration: percentage dehydration X body weight (g)
- Maintenance fluid (NaCl 0.45 / D5%)
- 1st 10 kg = 100 ml/kg
- 10-20 kg = 1000 ml/day + 50 ml/kg for each kg above 10 kg
- >20 kg = 1500 ml/day + 20 ml/kg for each kg above 20 kg
- Example:
A 6-kg child is clinically shocked and 10% dehydrated as a result of
gastroenteritis
- Initial therapy:
- 20 ml/kg for shock = 6 × 20 = 120 ml of 0.9% saline given as a
rapid IV bolus
- Estimated fluid therapy over next 24 hours:
- Fluid for Rehydration: 10/100 x 6000 = 600 ml
- 100ml/kg for daily maintenance fluid = 100 × 6 = 600 ml
- Rehydration + maintenance = 600 + 600 =1200 ml
- Start with infusion of 1200/24 = 50 ml/h
- The cornerstone of management is to reassess the hydration
status frequently (eg. at 1-2 hourly) and adjust the infusion as
necessary
- Start giving more of the maintenance fluid as oral feeds eg. ORS
(about 5 ml/kg/hour) as soon as the child can drink, usually after 3
to 4 hours for infants, and 1-2 hours for older children. This fluid
should be administered frequently in small volumes (cup and
spoon works very well for this process)
- Generally normal feeds should be administered in addition to the
rehydration fluid, particularly if the infant is breastfed
- Once a child is able to feed and not vomiting, oral rehydration
according to Plan A or B can be used and the IV drip reduced
gradually and taken off.
209
D) Indications for admission to Hospital:
- Moderate to severe dehydration
- Need for intravenous therapy (as below)
- Concern for other possible illness or uncertainty of diagnosis
- Substantial difficulties exist in giving ORS including intractable vomiting, ORS refusal or
inadequate ORS intake
- ORS treatment fails including worsening diarrhoea or dehydration despite adequate volume
- Patient factors (eg. young age, unusual irritability/drowsiness, worsening symptoms)
- Caregivers not able to provide adequate care at home
- Social or logistical concerns that may prevent return evaluation if necessary
* Lower threshold for children with obesity due to possibility of underestimating degree of dehydration.
H) Pharmacological agents
- Antimicrobials
- Should not be used routinely
They are reliably helpful only in children with bloody diarrhoea, probable shigellosis and
suspected cholera with severe dehydration
- Antidiarrhoeal medications
- The locally available diosmectite (Smecta®) has been shown to be safe and effective in
reducing stool output and duration of diarrhoea. It acts by restoring integrity of damaged
intestinal epithelium, also capable to bind to selected bacterial pathogens and rotavirus.
Other anti diarrhoeal agents like kaolin (silicates), loperamide (anti-motility) & diphenoxylate
(anti-motility) are not recommended
- Antiemetic medication
- Not recommended, potentially harmful
- Probiotics
- Probiotics has been shown to reduce duration of diarrhoea in several randomized controlled
trials. However, the effectiveness is very strain and dose specific. Therefore, only probiotic
strain or strains with proven efficacy in appropriate doses can be used as an adjunct to
standard therapy
- Zinc supplements
- It has been shown that zinc supplements during an episode of diarrhoea reduce the duration
and severity of the episode and lower the incidence of diarrhoea in the following 2-3
months. WHO recommends zinc supplements as soon as possible after diarrhoea has started.
Dose up to 6 months of age is 10 mg/day, age 6 months and above 20mg/day, for 10-14 days.
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Dehydration
212
Principle of Management:
- If possible, use enteral (oral) route for fluids instead of intravenous fluid (IV)
- If IV fluid therapy is required, maintenance fluid reuirement should be calculated based on
weight (Holliday & Segar formula)
- Indications for prescribing IV fluid:
- Circulatory support in resuscitating vascular collapse
- Replacement of previous fluid & electrolyte deficit
- Maintenance of daily fluid requirement
- Replacement of ongoing losses
- Severe dehydration with failed NG tube fluid replacement (eg. ongoing profuse losses,
diarrhoea or abdominal pain)
- Certain co-morbidities, esp GIT (eg. short bowel or previous gut surgery)
A) Resuscitation
Crystalloids 0.9% NaCl
Ringer`s lactate @ Hartmann`s solution
Colloids Gelafundin, Voluven
4.5% albumin solution
Blood products Whoe blood, blood components
- Fluid deficit (can cause impaired tissue oxygenation eg. clinical shock, should be corrected with
fluid bolus of 10-20 ml.kg)
- Always reaccess circulation (give repeated boluses if necessary)
- Identify cause of circulatory collapse (blood loss, sepsis) for alternative resuscitation fluid
- Fluid bolus of 10ml/kg in selected condition (DKA, intracranial patholgy or trauma)
- Avoid hypotonic solution in resuscitation (risk of causing hyponatraemia)
- Blood glucose: treat hypoglycaemia with 2ml/kg of 10% Dextrose solution
- Measure Na, K, glucose at outset & at least each day from then on. More frequent in ill-patient
or those with co-morbidities. Rapid result can be done with blood gases measurement
- Consider septic work-up or surgical consult in severely unwell patients with abdominal
symptoms (eg. gastroenteritis)
B) Maintenance
- Volume of daily fluid intake, includes insensible losses (from breathing, perspiratoin, stool) &
allows excretion of daily production of excess solute load (urea, creatinine, electrolyte) in urine
- Most children can be safely managed with 0.45% NaCl with added glucose depending on
glucose requirement (0.45% NaCl in 5% glucose or 0.45% NaCl in 10% glucose)
- 0.18% NaCl with 5% glucose should NOT be used as maintenance fluid, restricted to specialist
to replace ongoing loses of hypotonic fluids (area of high dependency, renal, liver, ICU)
- In SIADH maintenance fluid requirement should restrict to 2/3 of normal recommendation
- Isotonic solution (eg. 0.9% NaCl +/- glucose) should be given for high risk of hyponatraemia
with careful monitoring to prevent iatrogenic hyponatraemia in hospital, these include:
- Peri-or post-operative
- Require replacement of ongoing losses
- Plasma Na at lower normal range (definitely if <135 mmol/L)
- Intravascular volume depletion
- Hypotension
- CNS infection, head injury, chronic disease (CF, DM, pituitary deficits)
- Bronchiolitis, sepsis, excessive gastric/diarrhoea losses, salt-wasting syndrome
213
- Calculation of maintenance fluid:
Weight Total fluids Infusion rate
First 10 kg 100 ml/kg 4 ml/kg/hour
Subsequent 10 kg 50 ml/kg 2 ml/kg/hour
All additional kg 20 ml/kg 1 ml/kg/hour
Example: A child of 29 kg will require
- 100 ml/kg for first 10 kg 10 x 100 = 1000 ml
- 50 ml/kg for second 10 kg 10 x 50 = 500 ml
- 20 ml/kg for additional kg 9 x 20 = 180 ml
Total = 1680 ml (Infusion rate = 1680/24 = 70 mls/hour)
C) Deficit
- Replaced over a time period that varies according to child`s condition
- Rate of rehydration should be adjusted with ongoing clinical assessment
- Use an isotonic solution for replacement of deficit (eg. 0.9% NaCl)
- Reassess clinical status & weight at 4-6 hours, continue if satisfactory (If child lose weight,
increase fluid; if gain excessive weight, decrease fluid rate)
- Replacement is rapid in most cases of AGE (by oral or NG), but should be slower in DKA,
meningitis, much slower in hypernatraemic states (aim to rehydrate over 48-72 hours, serum
Na should not fall by >0.5 mmol/L/hr)
Example: 10 kg child who is 5 % dehydrated
Water deficit = 5% dehydration (5% of body water) x body weight (kg) x 1000 ml
= 500 mls (Infusion rate = 500mls/24 hours = 21mls/hour)
D) Ongoing losses
- Includes from drains, ileostomy, profuse diarrhoea
- Best measured & replaced (Any fluid losses >0.5 ml/kg/hr needs to be replaced)
- Calculation may base on each previous hour or each 4 hour period depending on situation
(eg. 200ml loss over previous 4 hours will replace with rate of 50ml/hr for next 4 hours)
- Can be replaced with 0.9% NaCl or Hartmann`s solution. Fluid loss with high protein content
leads to low serum albumin (eg. burns) can be replaced with 5% human albumin
B) Potassium disorders
- Daily potassium requirement: 1-2 mmol/kg/day
- Normal [K]:
- At birth - 2 weeks : 3.7-6.0 mmol/L
- 2 weeks - 3 months : 3.7-5.7 mmol/L
- Beyond 3 months : 3.5-5.0 mmol/L
Hyperkalaemia Hypokalaemia
- Serum [K] > 5.5 mmol/L - Serum [K] < 3.0 mmol/L or [Na] > 3.4 mmol/L
Causes: Causes:
- Dehydration - Sepsis
- Acute renal failure - GI losses (eg. diarrhoea, vomiting)
- Diabetic ketoacidosis - Iatrogenic
- Adrenal insufficiency (eg. diuretic therapy, salbutamol, amphotericin B)
- Tumour lysis syndrome - DKA
- Drugs - Renal tubular acidosis
(eg. oral K supplement, K-sparing diuretics, ACEi) - Hypomagnesaemia (refractory hypoK)
ECG changes: ECG changes: (when K+<2.5 mmol/L)
- Tall, tented T waves - Prominent U wave
- Prolonged PR interval - ST depression
- Prolonged QRS complex - Flat, low or diphasic T waves
- Loss of P wave, wide biphasic QRS - Prolonged PR interval (severe hypoK)
- Sinoatrial block (severe hypoK)
Management: Management:
- Stop all K+ supplementation - Identify and treat underlying condition
- Stop medication causing hyperkalaemia - Unless symptomatic, K+ of 3.0-3.4 mmol/L is
- Cardiac monitoring generally not supplemented but rather
- Exclude pseudo-hyperkalaemia (recheck venous) monitored in the first instance
- If child unstable, symptomatic, abnormal ECG, - Oral supplementation
K>7mmol/L - Oral KCl (max of 2 mmol/kg/day in divided dose
- Discuss for dialysis is common but more may be required in
- IV calcium practice)
- Nebuliser Salbutamol - IV supplementation (1g KCl = 13.3 mmol KCl)
- IV insulin with glucose - KCl is always given by IV infusion, NEVER by
- IV bicarbonate bolus injection
- +/- PR/PO Resonium (K+ binder) - Max concentration via peripheral vein is 40
- If child stable, normal ECG, K+>6, ≤7 mmol/L: mmol/L (concentration up to 60 mmol/L can be
- Nebuliser salbutamol used after discussion with senior medical staff)
- IV insulin with glucose - Max infusion rate of 0.2 mmol/kg/hr (in non-ICU
- +/- IV bicarbonate if acidosis setting)
- +/- PR/RO Resonium - IV correction (1g KCl = 13.3 mmol KCl)
- If child stable, asymptomatic, normal ECG, - K+<2.5 mmol/L may be associated with
5.5 ≤ K+≤ 6 mmol/L significant CVD compromise, in emergency, IV
- Consider treatment if necessary KCl infusion may be given:
- +/- Nebuliser Salbutamol - Dose: Initially 0.4 mmol/kg/hr into central vein
- +/- IV bicarbonate if acidosis till K+ level is restored
- +/- PR/RO Resonium - Ideally this should occur in ICU setting
As a general rule, maximum potassium infusion rate is 1
ampoule per hour (13.3mmol or to be exact should not
exceed 10mmol)
216
Up to 20mmol/h is allowed but required continuous ecg
monitoring and might cause thrombophlebitis
Gastroesophageal Reflux Disease (GERD)
Introduction:
- Gastro-oesophageal reflux (GER)
- Involuntary passage of gastric contents into oesophagus with/without regurgitation and vomiting
- Normal physiological process occurring several times per day in healthy children
- Generally associated with transient relaxations of the lower oesophageal sphincter independent of
swallowing, which permits gastric contents to enter the oesophagus.
- Gastro-oesophageal reflux disease (GERD) is present when
- Reflux of gastric contents causing troublesome symptoms or complications due to frequent or
persistent GER, producing esophagitis-related symptoms or extraesophageal presentations (eg.
respiratory symptoms or nutritional effects)
Epidemiology:
- Common in the first year of life due to: (mostly resolve spontaneously by 1 year of age)
- Maturation of lower esophageal sphincter
- Upright posture
- Introduction of more solid diet
Anti-reflux Mechanism:
- Presence of LES, below the diaphragm (increased intra-abdominal pressure reinforce LES tone)
- Oblique entry of esophagus to the stomach
- Secondary peristaltic wave in oesophagus clears the refluxed material
- Swallowed saliva neutralises the refluxed acid
Pathophysiology:
Infants Older Children/ Adults
- Functional immaturity of LES - Reduced esophageal clearance of acid due to
- Episodes of inappropriate relaxation poor esophageal peristalsis
- Short intra-abdominal esophageal length - Exacerbated by sliding hiatus hernia (Trapping
- Predominantly fluid diet of acid within hernial sac)
- Horizontal posture - Reduced esophageal mucosal resistance
- Delayed gastric emptying
- Inflammation of LES by exposure to acid, pepsin & bile
Clinical features:
Infants Older Children/ Adults
- Frequent vomiting & regurgitation* - Heartburn (retrosternal chest pain)
- Crying, poor sleeping, irritability - Aggravated by stooping, bending & lying down
- Feeding refusal, poor weight gain, sour burps - Vomiting, regurgitation, dysphagia
- Extra-oesophageal symptoms (aspiration - Acid & water brash
pneumonia, URTI, choking, coughing, wheezing) - Odynophagia, hoarseness of voice
* Regurgitation is an involuntary retrograde - Symptoms of anaemia (due to blood loss)
propulsion of stomach content via gastroesophageal - Extra-oesophageal (recurrent pneumonia,
junction to the mouth. chronic sinusitis, laryngitis, dental erosions)
Risk factors:
- Sliding hiatus hernia - Thoracic stomach
- Cerebral palsy - Coeliac disease
- Bronchopulmonary dysplasia (in preterm) - Raised ICP
- Post-surgery (oesophageal atresia, - UTI
diaphragmatic hernia) - Congenital heart disease
- Cystic fibrosis - Fictitious or induced illness
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Warning signals: (requiring investigations in fants with recurrent regurgitation or vomiting)
Symptoms of GI obstruction Systemic/neurologic disease Non-specific symptoms
- Bilous vomiting - Hepatosplenomegaly - Fever
- GI bleeding (haematemesis, - Bulging fontanelle - Lethargy
haematochezia) - Macro/microcephaly - Failure to thrive (FTT)
- Consistent forceful vomiting - Seizures
- Onset of vomiting after 6 - Genetic disorders
months of life (eg. Trisomy 21)
- Constipation - Other chronic disorders
- Diarrhoea (eg. HIV)
- Abdominal tenderness,
distension
Complications:
General - Failure to thrive
- Feeding problems
- Apnea in preterm infants
- Faltering growth
- ALTE (Apparent life threatening event)* contraversial
SIDS (Sudden infant feath syndrome)
Head - Sandifer`s syndrome
(dystonic movement of head and neck, spasmodic torticollis)
Oesophagus & stomach - Oesophagitis (dysphagia, odynophagia, hematemesis, pain)
- Peptic stricture (associate with oesophagitis)
Respiratory system - Aspiration pneumonia
Social - Smelly mouth due to regurgitation
Investigations:
24 hour pH measurement - Monitor pH for 24 hours
(Gold standard) (Normal ≤ 4%, abnormal > 4%)
Endoscopy with biopsy - Look for oesophagitis, peptic stricture, Barrett`s esophagus,
enteropathy in older children, gastritis or PUD
Barium swallow and meal - Look for underlying anatomical abnormalities of oesophagus,
stomach or duodenum (eg. hiatus hernia, malrotation, oesophageal
stricture)
Others - CXR, urine, C&S, Hb and iron studies, faecal occult blood.
* Raised ICP may cause reflux as well
Management:
Conservative Operative
Feeding modification - Nissen fundoplication (fundus of stomach is
- Small volume, frequent feeds wrapped around the intra-abdominal
- Head prop up to 30o after feeding oesophagus)
- Thickening of feeds (Nestargel, Carobel, carob
seed flour) - Reserved for patient who:
- Fail to respond to medication
Pharmacological - With esophageal stricture
- Antacid (Ranitidine & Omeprazole) - With recurrent aspiration pneumonia
- Alginate & Antacid combination (Gaviscon)
- Motility stimulator (Metoclopramide)
- Prokinetic agents (Cisapride)
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Inflammatory Bowel Disease
Definition:
- Chronic, idiopathic, immune-mediated, inflammatory disease involving the gastrointestinal
(GI) tract
- Two subtypes: Crohns Disease (CD) & Ulcerative Colitis (UC)
Epidemiology:
- In the pediatric population, Crohn`s disease is more common than UC, with the majority of
children diagnosed in adolescence, although some are much younger
- Prevalence is about 9/100,000 population. Thus, it is estimated that there are about 2000
existing cases in Malaysia
- Worldwide distribution, ↑incidence of IBD in developed countries than developing countries
- Most common onset of IBD is during preadolescent/adolescent & young adulthood
- Bimodal distribution of age: early onset at 10-20 years, smaller peak at 50-80 years of age
- Approximately 25% of patients present <20 years of age, may begin as early as 1st year of life
- Children with very early onset (<6 yr) & <1 yr have ↑incidence of monogenetic cause of IBD
- Monozygotic twins affected more than dizygotic twins in development of IBD (CD > UC)
- Associated genetic disorders: Turner syndrome, Hermansky-Pudlak syndrome, glycogen
storage disease type 1b & immunodeficiency diseases
Pathology:
- Ulcerative colitis (UC) is characterized by diffuse colonic mucosal inflammation that begins at
anal verge and extends proximally. It is limited to the colon, although distal ileal involvement
(backwash ileitis) may occur
- Crohns disease is characterized by transmural inflammation that may involve any segment of
intestinal tract from the mouth to the anus
Aetiology:
- Multifactorial with probable contributions from genetics and the environment
- There is a high incidence of disease among first- degree relatives.
- Defective IBD1 gene cause reduced immune tolerance to luminal bacteria, a process mediated
by proinflammatory cytokines including tumor necrosis factor-α (TNF-α), interleukin-1 (IL-1),
IL-6, interferon-γ, and IL-23
219
Clinical Features:
Symptoms Signs
Intestinal Manisfestation: General:
- Per rectal bleeding (mucus, pus-filled, UC>CD) - Right/ Left lower quadrant abdominal pain
- Diarrhoea (nocturnal, differentiate from irritable - Generalized abdominal fullness
bowel syndrome) - Oral Ulcer
- Abdominal pain - Clubbing
- Tenesmus, urgency - Pyrexia
- Steatorrhoea - Severe anaemia (fulminant colitis, >5 bloody
- Constipation (less common,in those with stools/day for 5 days in UC or due to poor intake)
proctitis) - Failure to Thrive (underplotted in Growth Chart)
Systemic: Extraintestinal: (more common in UC than CD)
- Fever - Erythema nodosum (red, raised, tender nodules
- Weight Loss located along the anterior shins)
- Anorexia, malaise, easy fatigability - Pyoderma gangrenosum (deep necrotic ulcers
- Growth failure (inadequate calorie, suboptimal often on the legs)
absorption/excessive nutrient loss, LOA, use of - Jaundice (sclerosing cholangitis, chronic active
steriods during treatment) hepatitis)
- Episcleritis, uveitis, and iritis
Extraintestinal Manisfestation:
- Liver tenderness
- Arthralgia
- Secondary amenorrhoea (active disease)
- Arthritis (non-deforming)
- Pubertal delay (Tanner staging)
- Skin rashes
- Perianal disease (tag, fistula, fissure, abcess)
- Eye involvement
- Pneumaturia, faecaluria (enterovesical vaginal)
Complications:
1) Intestinal:
- Stricturing & adhesion (luminal narrowing, pre-stenotic dilation, intestinal obstruction)
- Perianal/perirectal fistulae → abscesses, sinus tract (incomplete fistula ending in a `cul-de-sac`)
- Severe hemorrhage, toxic megacolon or perforation
- Long-term: colonic malignancy
2) Extra-intestinal:
Musculoskeletal - Peripheral arthritis, granulomatous monoarthritis, synovitis, periosteitis
- Sacroiliitis, ankylosing spondylitis, RA (HLA-B27 association)
- Finger clubbing, Hypertrophic osteoarthropathy
- Osteoporosis, osteomalacia (due to malabsorption, malnutrition,
inadequate calcium and vitamin D intake, chronic steroid use, inactivity,
and chronic inflammation)
- Rhabdomyolysis, pelvic osteomyelitis, recurrent multifocal osteomyelitis
Skin & mucous - Oral lesions, cheilitis, aphthous stomatitis, glossitis
membrane - Granulomatous oral Crohn disease, peristomatitis vegetans
- Inflammatory hyperplasia fissures & cobblestone mucosa (CD)
Dermatologic - Erythema nodosum, Pyoderma gangrenosum, Polyarteritis nodosa
- Sweet syndrome, Metastatic Crohn disease
- Perianal skin tags
- Epidermolysis bullosa acquisita
Ocular - Conjunctivitis, uveitis, iritis, episcleritis, scleritis
- Retrobulbar neuritis, Chorioretinitis with retinal detachment
- Crohn`s keratopathy, retinal vascular disease
Bronchopulmonary - Chronic bronchitis with bronchiectasis/ neutrophilic infiltrate
220
- Fibrosing alveolitis, Pulmonary vasculitis, bronchiolitis obliterans
- Eosinophilic/granulomatous lung disease, Tracheal obstruction
Cardiac - Pleuropericarditis
- Cardiomyopathy, endocarditis, myocarditis
Malnutrition - ↓ food intake (IBD, dietary restriction)
- Malabsorption (IBD, bowel resection, bile salt depletion, bacterial
overgrowth)
- Intestinal losses (electrolytes, minerals, nutrients)
- ↑ caloric needs (inflammation, fever)
Haematologic - Anaemia (iron-deficiency-blood loss, chronic disease, VitB12 deficiency)
- Anaphylactoid purpura (CD)
- Hyposplenism
- ↑ risk of arterial & venous thrombosis with stroke, MI, PVD
- AIHA, ↑ activation of coagulation factors, activated fibrinolysis
Renal & genitourinary - Urinary crystal formation (nephrolithiasis, uric acid, oxylate)
- Hypokalemic nephropathy, Renal amyloidosis
- Inflammation (retroperitoneal/perianal/psoas abscess, ureteral fibrosis)
- Fistulation (enteroenteric, enterocolonic, enterovesical, enterovaginal,
enterocutaneous)
- Glomerulitis, membrane nephritis, nephrotic syndrome
Hepatobiliary - Pancreatitis secondary to medications (sulfasalazine, 6-MCP,
azathioprine, parenteral nutrition)
- Granulomatous pancreatitis, sclerosing cholangitis with pancreatitis
- Primary sclerosing cholangitis, cholelithiasis, autoimmune hepatitis,
cholecystitis (immune-mediated)
- Hepatic abscess, hepatic granuloma
- Pericholangitis, carcinoma of bile ducts, NASH
Endocrine - Growth failure (more in CD), delayed sexual maturation
- Thyroiditis
Neurological - Peripheral neuropathy, meningitis, vestibular dysfunction
- Pseudotumour cerebri
- Cerebral vasculitis, migraine
Investigations:
Baseline - FBC (anemia, thrombocytosis, leukocytosis: toxic megacolon)
- ↑ESR, ↑CRP
- Hypoalbuminaemia (↓nutritional status)
- ↑AST/ALT (autoimmune hepatitis), ↑GGT,↑ALP,↑TSB (primary sclerosing
cholangitis, cholelithiasis)
Diagnostic Antibody screening, need to check for both:
(need to couple the - Anti-neutrophil cytoplasmic antibody (p-ANCA)
findings with history, PE - Anti-Saccharomyces cerevisiae antibody (ASCA)
and HPE from biopsy) p-ANCA +ve, ASCA -ve suggestive of UC
p-ANCA - ve, ASCA +ve suggestive of CD
Upper endoscopy + colonoscopy or wireless capsule endoscopy
- Erythema, aphthous ulcers, cobblestone appearance, pseudopolyps,
and mucosal friability in Crohn`s Disease
- Signs of inflammation starting in the rectum, extending proximally in a
continuous fashion, longitudinal ulcers in Ulcerative Colitis
Mucosal biopsy
- Inflammatory infiltrates with crypt distortion and crypt abscesses
consistent with chronic active inflammation are diagnostic for IBD.
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Others - Stool studies for bacteria, parasites & viruses (infectious diarrhoea)
- CT scan used in emergency (acute abdomen, ischaemic colitis, mesenteric
ischaemia)
- Faecal calprotectin (↑ indicates GI inflammation, specific marker)
Classifications:
Ulcerative colitis
1) Monstreal classification based on extent (E) & severity (S)
E1 (proctitis) Inflammation limited to rectum
E2 (left-sided, distal) Inflammation limited to splenic flexure
E3 (pancolitis) Inflammation extends to proximal splenic flexure
S0 (remission) No symptoms
S1 (mild) ≥ 4 stools/day (with/without blood), absence of systemic
symptoms, normal inflammatory markers
S2 (moderate) 4 stools/day, minumum signs of systemic symptoms
S3 (severe) ≥ 6 bloody stools/day, PR ≥ 90bpm, temp ≥ 37.5`C, Hb <10.5g/dL,
ESR ≥ 30 mm/hour
Crohn`s disease
1) Montreal classification based on age (A), location (L) & behaviour (B)
Age at Diagnosis A1: Less than 16 years old
A2: Between 17-40 years old
A3: Over 40 years old
Location L1: Ileal
L2: Colonic
L3: Ileocolonic
L4: Isolated upper GI
Behaviour B1: Non-stricturing, non-penetrating
B2: Stricturing
B3: Penetrating
P: Perianal disease
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2) Lémann score
- New technique to
score & study
intestinal damage in
Crohn disease
- Disease phenotypes
often change as
duration of disease
lengthens
(inflammatory
becomes structuring/
penetrating)
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Differential diagnosis:
- Irritable bowel syndrome
- Infectious colitis
- Bacteria (Campylobacter jejuni, Yersinia enterocolitica, C. diffile, E. coli O157:H7, Shigella)
- Parasites (Entamoeba histolytica, Giardia lamblia)
- AIDS-associated enteropathy (Cryptosporidium, Isospora belli, CMV)
- Lactose intolerance
- Coeliac disease
- Drug-induced colitis (NSAIDS)
- Hyperthyroidism
- Neuroendocrine tumor
Management:
Medical - Aminosalicylates, including sulfasalazine and mesalamine (inhibiting the
cyclooxygenase and lipoxygenase pathways of arachidonic acid metabolism,
which alters mucosal prostaglandin production). Given orally or rectal suppository.
- Systemic corticosteroids such as oral prednisone. Corticosteroid dependence,
defined as recurrent symptoms when the dose is gradually tapered, is a common
occurrence and may require an increased dose or additional therapy with
immunomodulators.
- Budesonide is a synthetic steroid, fewer side effects and less adrenal suppression
than prednisone. For short term therapy.
- Antibiotic therapy, eg. metronidazole and ciprofloxacin for complications of
Crohns disease, such as C. difficile infection and perianal fistulae.
- Immunomodulators eg. methotrexate, 6-mercaptopurine (6-MP) and
azathioprine for active disease (S/E: leucopenia, thrombocytopenia, hepatitis,
infection, pancreatitis, and allergic reaction)
- Infliximab is a humanized anti-TNF-α antibody used to treat severe and fistulizing
IBD (first-line therapy in conjunction with corticosteroids)
Surgical - Indications for surgery:
- Failed medical intervention
- Symptomatic patients
- Bowel stricture or obstruction
- Uncontrollable GI bleeding
- Intraabdominal abscess, perianal abscess, and fistula
- Types of surgery:
- Small bowel resection (as limited as possible to prevent short bowel syndrome)
- Colectomy (intractable disease, complication of therapy, fulminant colitis)
- Abscess drainage
- Seton placement for perianal abscess (not completely remission)
Nutritional - In children with growth failure, exclusive enteral nutrition therapy with special
therapy formulas is prescribed.
- Formulas are best tolerated by nasogastric tube because most formulas are not
very palatable.
Psychosocial - Family support, social workers, individual psychologic counseling
support - Ensure parent understand disease manifestations & management
- Encourage patient to participate fully in age-appropiate activites (↓ during periods
of exacerbation)
Surveillance - Begin after 8-10 years of disease to detect dysplastic changes from biopsy
colonoscopy - Immediate colectomy is needed if suggest of progression to colon cancer (esp UC)
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Prognosis:
- There is no cure for IBD
- Goal of therapy is maintenance of long-term remission, normal growth & nutritional status
- Once a child has had UC for 8-10 years, general risk of colon cancer is 1% per year, and by 20
years may be up to 25%
- If a child has continuous disease, or a frequently relapsing course, risk of malignancy is greater
than in those with less severe disease
- In IBD patients, there is an overall increased risk of lymphoma in those exposed to biological or
immunomodulator therapy
Inflammatory Bowel Disease Long Case (Template)
A. History
General profile (Age, Gender, Ethnicity)
History taken from caretaker/parent
Presenting complaints
(Reason for admission)
HOPI - Present according to current condition, remember to rule out other differential diagnosis. If
presenting complaint is related to IBD, focus on IBD under HOPI not under past-medical section
Gastrointestinal symptoms Weight loss, growth, abdominal pain (site, interference with sleep,
precipitation by eating), anorexia, nausea, vomiting, odynophagia or
dysphagia , diarrhoea, urgency, tenesmus, incontinence, rectal bleeding,
fistulae perirectal disease (CD)
Extraintestinal symptoms - General (rashes eg. erythema nodosum: CD, fever, pubertal delay)
(systemic) - Mouth involvement (aphthous ulcers)
- Liver involvement (chronic active hepatitis)
- Joint disease (arthralgias, spondylo-arthropathies)
- Visual problems (uveitis), vascular complications (vasculitis)
- Renal tract involvement (nephrolithiasis)
- CVS (hypertension, myocarditis, pericarditis)
- Neurological problems (peripheral neuropathy)
- Haematological disease (anaemia)
- Musculoskeletal weakness (vasculitic myositis, steroid-induced
myopathy)
- Hepatobiliary (jaundice, pancreatitis)
- Extraintestinal neoplasia (lymphoma)
- Others (amyloidosis, thromboembolic disease - cerebral, retinal)
Progression of Disease
1. Initial presentation, symptoms, when, where and how diagnosed, response to treatment
2. Details of subsequent hospitalisations (frequency, indications, usual length of stay, usual outcome,
doctors involved, clinics attended, previous hospitalisations, past surgery)
3. Complications of the disease
4. Complications of treatment
5. Monitoring of the disease: how often seen in clinic, usual investigations performed, how often seen
by local doctor
Past-Medical & Surgical History
Past-Medical - Other than associated conditions of IBD
Past-Surgical - Any other operation done
Drug History
Drugs - Current medication, change in medication, compliance, control
- Drug allergy
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Family History
Parent & siblings - Inflammatory bowel disease, ankylosing spondylitis, rheumatoid arthritis
Paediatrics History
Birth history - Neonatal anaemia? IUGR? G6PD deficiency?
Immunisation history - Completed immunisation?
Developmental history - Any developmental delay?
- Delayed pubertal staging
Dietary - Any enteral/parenteral nutrition needed
- Food allergy
Social History
Disease impact on the - Schooling (which stream, level), Academic performance (rank, best
child subject), able to take part in physical class/sports?
- Problems of chronic disease: energy levels, behavioural problems,
chronic hospitalisation, altered self-image, school absence, depression,
feeling of missing out due to disease exacerbations and energy levels
- Psychosocial (depression, low self-esteem & relationship)
- Cigarette smoking (exacerbates CD)
- Steroid effects, short stature, delayed sexual development
- Body image, pubertal anxieties (in teens)
Disease impact on the - Occupation of caretakers
family - Financial considerations (financial burden of multiple hospitalisations,
surgical procedures)
- Social support group available
- Social worker, parent support groups, psychologist, online `chat groups`
for teenagers
Understanding of disease - Perception of disease
- Compliance with medications
Summary
- Summarise patient (name,age,gender) with presenting complaint & underlying IBD
- Provisional diagnosis and differential diagnosis
- Current functional status & Complications from IBD
B. Physical Examination
General inspection:
- Parameters (weight, height, percentiles, growth chart)
- Tanner staging
- Nutritional status (muscle bulk, subcutaneous fat, peripheral oedema)
- Pallor
- Jaundice
- Cushingoid appearance
- Abdominal scars and stoma
- Joint swelling (especially lower limbs)
- Skin rashes (erythema multiforme, erythema nodosum, pyoderma gangrenosum)
Upper limbs:
- Clubbing (especially CD)
- Palmar crease/nailbed pallor (anaemia from dietary deficiency, iron loss in gut, folate malabsorption,
vitamin B12 malabsorption, chronic disease, or side effects of salazopyrine)
- Arthritis (wrists, elbows)
- Palpable epiphyseal enlargement (vitamin D deficiency)
Head & Neck:
- Cushingoid facies
226
- Conjunctival pallor (anaemia)
- Conjunctivitis scleral icterus (sclerosing cholangitis, chronic active hepatitis)
- Iritis
- Corneal xerosis or clouding (vitamin A deficiency)
- Cataracts (if on steroids)
- Aphthous stomatitis
Abdomen:
- Scars
- Stoma
- Striae (if on steroids)
- Tenderness Mass (matted loops or abscess)
- Hepatomegaly (sclerosing cholangitis, chronic active hepatitis)
- Ascites (protein deficiency, protein- losing enteropathy in CD)
- Enlarged kidneys (hydronephrosis in CD from ureteral compression by inflammatory mass or fibrosis)
- Fistulae (CD)
- Gluteal wasting
- Perianal disease (anal fissures, fistulae, abscesses, anal tags)
- Rectal examination (blood, pus on glove)
Lower limbs:
- Joint swelling (knees, ankles)
- Tibial bowing (vitamin D deficiency)
- Erythema nodosum, pyoderma gangrenosum
- Toe clubbing
C. Discussion
- Refer previous pages for detailed investigation and management in IBD.
- Mainstay of management can be catogorised into medical, surgical, nutritional & psychosocial
intervention. Discuss on the complications which would be faced by patient in future and necessary
management as a whole.
227
Hirschsprung Disease
Epidemiology:
- Incidence 1 in 5000 live births
- Site of involvement:
- 75% confined to rectosigmoid
- 10% involvement of entire colon
Aetiology:
- Failure of ganglionic cell precursors to migrate into the distal bowel during fetal life
- Absence of ganglion cells from the myenteric and submucosal plexus (Meissner & Auerbach
plexus) of large bowel (due to failure of migration from the neural crest)
- This results in sustained contraction at aganglionic segment which is narrow and contracted
segment while distention and dilation of colon proximal to it.
Clinical features:
Symptoms Signs
Neonatal: - Distended abdomen
Early - Rectal examination
- Failure to pass meconium within first 24 hrs - Empty, contracted rectum clenches around
examiner`s finger (snug anal sphincter)
Late
- On finger withdrawal:
- Constipation from birth
- a gush of liquid stool expelled with flatus
- Abdominal distention
- Bilious vomiting
* May occur due to delay in diagnosis because
Children: temporary relief of obstruction as a result of
- Chronic constipation dilatation caused by rectal examination
- Abdominal distention
- Growth failure
Classification:
Short-segment Long-segment
- 5 males : 1 female - 1 male : 1 female
- Affects rectum and sigmoid - Extends above sigmoid
- 10-15% associate with Down`s syndrome
Complication:
- Hirschsprung enterocolitis
- Present during first few weeks of life: fever, foul-smelling diarrhoea, megacolon
- Severe and life-threatening
- Affected areas become thin & inflamed and may perforate
- Sometimes due to Clostridium difficile infection
Investigations:
Abdominal X-Ray - Dilatation of bowel
Rectal suction biopsy - Absence of ganglion cells in submucosal plexus
(1 & 3 cm above dentate line) - Excessive acetylcholinesterase (nerve trunk hyperplasia)
(Gold standard)
Anorectal manometry & - For surgeon to determine length of aganglionic area
barium study - Determine absence/presence of rectosphincteric reflux
- Not for diagnosis
228
Management:
- Mainly surgical resection of the involved colon
- Initial colostomy above the aganglionic segment, followed weeks later by a transanal pull-
through excision of aganglionic bowel and creation of primary colorectal anastomosis without
laparotomy (limited to rectosigmoid involvement)
229
Intussusception
Definition:
- Invagination of a segment of proximal bowel into the distal bowel in a `telescopic` manner
Epidemiology:
- Incidence is 1:1000 (Male : Female = 3 : 2)
- Commoner in children (2 months-2 years) than adults, peak at 6-9 months
Risk factor:
- Hypertrophy of Peyer`s patches (Lymphoid hyperplasia)
- Polyps
- Meckel`s diverticulum (eg. Peutz-Jeghers` syndrome, AD, hereditary intestinal polyposis)
- Intramural hematoma (eg. in Henoch Schonlein Purpura)
- Lymphosarcoma
Anatomy:
Common sites Parts of intussusception
- Ileocaecal - Intussuscipien (receiving part)
- Ileo-ileal - Intussusceptum (prolapse part)
- Ileo-ileocolic
- Jejunoileal
- Jejuno-jejunal
Pathophysiology:
- Intussusception progresses leading to prolonged obstruction
- As intussuscepted bowel is pulled further and further into downstream intestine by motility,
mesentery is pulled, stretched and compressed
- Venous outflow from intussusceptum is obstructed, leading to oedema, congestion & bleeding
- Third space fluid loss and `currant jelly` stools result
Clinical features:
Symptoms Signs
- Paroxysmal colicky abdominal pain - Abdominal distension
- Knees draw up, cry & appear pale - Sausage-shaped mass (RUQ or epigastrium)
- Colicky pain every 15-20 minutes - Signs of shock (tachycardia, hypotension)
- Bilious vomiting (prolonged obstruction) - Digital PR
- Refuse feeding, lethargy - Presence of blood or mucus
- Redcurrant jelly stool (blood + mucus)
(pathognomonic)
* Normal in between bouts of attacks
Complications:
- Small bowel obstruction (commonest)
- Mesenteric ischemia
- Perforation
- Peritonitis
- Sepsis
- Hypovolaemic shock (due to pooling of fluid in gut)
230
Investigations:
Imaging Plain abdominal X-ray
- Typical gas distribution (crescent gas at the apex)
- Small bowel obstruction (distended small bowel + absence of gas in distal
colon or rectum)
USS & barium enema
- `doughtnut` or `target` appearance (layers of bowel wall of the end - on
intussusception)
- Present of free intraperitoneal fluid
Doppler Ultrasound (not routinely done)
- Check for bowel viability
Management:
- Fluid resuscitation (if patient in shock)
Conservative Operative
- Hydrostatic pressure or enema/air reduction - Laparoscopic or laparotomy (25%)
- Air insufflation - Open reduction
- 75% successful - Gentle retrograde reduction of the
- Partial or incomplete reduction may intussusceptum
warrant a repeat attempt after 4-6 hours - Surgical resection of bowel (10%)
- Indicated in failed open reduction or
gangrenous bowel
* Traction should not be applied to the proximal bowel
Prognosis:
- Rapid recovery with resumption of oral feeding within 24-48 hours.
- Risk of recurrence: 1-2 %
- Mortality low if treatment started soon, high if resection is required (development of
gangrenous bowel)
231
Pyloric Stenosis
Definition:
- Hypertrophy of longitudinal & circular smooth muscle of pylorus causing gastric outlet
obstruction (GOO)
Risk factor:
- Boys ( Male : Female = 4 : 1)
- First born
- Family history (particularly on the maternal side)
Clinical features:
Symptoms Signs
- Usually presents 2-7 weeks of age, irrespective
at - Do Test feed
of gestational age - For examination
- Calm the hungry infants
- Projectile vomiting
Inspection
- Not bile-stained
- Gastric peristalsis from left to right
- Increases in frequency & severity with time
Palpation
- Constant hunger (even after vomiting) - Pyloric mass or olive at the right upper quadrant
- Refuse only when markedly dehydrated (empty the air with nasogastric tube for
- Weight loss or poor weight gain examination if overdistension)
- In delayed presentation Auscultation
- Succussion splash (shake the infant`s abdomen)
Investigations:
Blood - BUSE: Low Cl (hypochloremia) & Low K+(hypokalemia)
- Serum HCO3-: Metabolic alkalosis (HCO3- increase to 25-35 mEq/L)
Radiology - Abdominal USS: Demonstrating hypertrophic pylorus
- Barium meal: Only perform when in doubt, grossly enlarged stomach
which empties slowly
Management:
Supportive Operative
- Correct fluid & electrolyte imbalance with IV fluid - Ramstedt`s pyloromyotomy
- Chloride and potassium should be replaced - Can be performed by laparotomy/laparoscopically
- Muscle of the pylorus is cut (NOT mucosa)
- Child can be fed the next day, discharge after 2-
3 days post-operatively
Ramstedt`s pyloromyotomy
232
Malrotation & Volvulus
Introduction:
- Intestinal malrotation: Any variation caused by interruption of typical intestinal rotation and fixation
during fetal development
- Can occur at a wide range of locations leading to various acute & chronic presentations
- Most common type: Incomplete rotation predisposing to midgut volvulus (defined as abnormal twisting
of bowel at a focal point along its mesentery, different aetiology if occur in adult)
Common sites:
- Duodenojejunal flexure failing to rotate adequately to left around superior mesenteric vessels
- Caecum failing to rotate and descend on the right which may predispose to volvulus
Presentation:
Types Pathophysiology Presenting symptoms
Obtruction without Due to crossing of Ladd`s bands across - Bilious vomiting
compromised blood duodenum - Abdominal distension
supply - PR bleeding (late sign)
Obstruction with Due to volvulus of midgut around superior - Abdominal pain
compromised blood mesenteric vessels, supplying whole midgut - Abdominal distension
supply beyond ampulla of Vater to proximal 2/3 of
transverse colon → mesenteric ischaemia
Investigation:
Plain Abdominal X-Ray - All small bowel is to the right
- Distended stomach + proximal duodenum with rest of the abdomen
being gasless
Barium meal - Duodenojejunal junction to the right of the spine
- Duodenal obstruction often with spiral or corkscrew appearance
- Presence of small bowel mainly on the right side
Management:
Conservative Operative
- Fluid resuscitation & electrolyte correction - Reduction of volvulus
- Orogastric/nasogastric tube with 4 hourly - Resection of bowel (if gangrenous) with division
aspiration of Ladd`s band
- Antibiotics (if septic)
233
Meckel`s Diverticulum
Investigations:
- Technetium scan/ Meckel scan (increase uptake by ectopic gastric mucosa 70%)
- Ultrasound, barium enteroclysis, video capsule endoscopy (visualise diverticula)
- Surgical exploration
Extra Notes:
Treatment: Omphalocele/Exomphalos (anterior abdominal wall defect
- Surgical resection in which intestine, liver & other organs remain outside
with membranous sac covering.
Gastrochisis (anterior abdominal wall defect which
abdominal contents freely protrude without membranous
Mesenteric Adenitis sac covering)
Introduction:
- Non-specific, self-limiting inflammation of mesenteric lymph nodes in RLQ
- Most common in children & adolescents (occasional encountered in adults)
- Yersinia enterocolitica is considered most common pathogen in temperate Europe, North
America & Australia, more common in boys
Aetiology:
- Viral or bacterial (Yersinia enterocolitica, Helicobacter jejuni, Campylobacter jejuni, Salmonella
spp, Shigella spp)
Clinical features:
- Acute abdominal pain (differential diagnosis of acute appendicitis)
- Often associate with systemic symptoms and signs including fever, headache, pharyngitis and
cervical lymphadenopathy
Management:
- Investigation (USS look for enlarged LNs, ileal/ileocaecal wall thickening>3mm over >5cm bowel)
- Symptomatic management (self-limiting)
- Conservative treatment
- Persistent right iliac fossa pain warrants surgical exploration to identify cause
234
PART VII
UROLOGY
Renal Anomalies
Introduction:
- Frequent cause of renal failure in children (30% of ESRF)
- 3 categories based on the stage of primary abnormality in renal embryologic development:
Primary abnormality Examples
Failure to form a functional nephron - Renal agenesis
(renal parenchymal malformation) - Multicystic dysplastic kidney (MCDK)
Failure of migration of developing - Renal ectopy (Pelvic/ Thoracic kidneys)
kidney to appropriate destination - Abnormal fusion (Horseshoe kidney)
Defects of urinary collecting system - Double ureters (Duplex collecting system)
- Posterior urethral valves (PUV)
- The changes of renal parenchyma (hydronephrosis, dysplasia) are often secondary to
obstructive uropathy or urinary reflux disease
- Almost all abnomalies are detectable on antenatal ultrasound screening
- Inherited conditions include Polycystic Kidney Disease (PKD) are result of specific genetic
mutations detectable at birth or later in life
235
A) Polycystic Kidney Disease (PKD)
- Group of genertically inherited conditions in which cyst formation and renal parenchymal
replacement occur anytime from fetal life
- Pathogenesis: ciliary dysfunction (PKD proteins are localised to cilia/basal body), loss/abnormal
cilia in the kidney are associated with cyst development
- 2 major forms: Autosomal Recessive (ARPKD) or Autosomal Dominant (ADPKD)
Autosomal Recessive Polycystic Kidney Disease Autosomal Dominant Polycystic Kidney Disease
- Commonly prenatal, neonatal, infantile, - Variable but commonly adulthood
juvenile, adolescence for age of presentation (40-50 years old)
(Presents early)
- Abnormal gene on short arm of Chr6 encodes - Abnormal PKD1 encodes Polycystin 1 (85%)
for Fibrocystin (polyductin) protein - Abnormal PKD2 encodes Polycystin 2 (15%)
- May associate with Potter sequence - May associate with Tuberous sclerosis (PKD1-
(oligohydramnios with lung hypoplasia, limb & TSC2 gene, contiguous gene syndrome)
facial abnomalities)
- Renal cysts are in radial pattern - Renal cyst are anywhere in kidney, varying size
- Cysts arise from collecting ducts & - Cysts arise from all types of tubules
perpendicular to cortical surface
- Presentation: mass at birth, interferes birth, - Presentation: flank pain, renal colic, mass,
respiration, renal failure haematuria, UTI, hypertension, renal failure
- Association: Biliary obstruction, congenital - Association: Liver cysts, pancreas cyst, vascular
hepatic fibrosis with portal hypertension, liver cyst (Berry aneurysm)
failure (cystic biliary dysgenesis) - Extrarenal manifestation are uncommon in child
- Complications: Oesophageal varices, GI bleeding - Complications: ESRF, stroke, male infertility
hypersplenism with thrombocytopenia, liver
failure, cholelithiasis, ascending cholangitis
- USS: Large kidneys (external surface lobulated), - USS: Progressive bilateral development &
increased echogenicity of parenchyma, loss of enlargement of focal cysts (increase size &
corticomedullary differentiation, macrocyst number with age), external surface smooth
- Diagnosis: - Diagnosis:
- +ve USS findings with - >1 cyst in child
- Absence of renal cysts in both parents - Parent with ADPKD
- Previously affected siblings
- Consanguinity
- Hepatic fibrosis
- Renal cysts do not communicate.
- Disease may present at any age, including prenatally.
- Gene defect leads to malfunction of the ciliary body.
- Both kidneys are usually enlarged, usually bilateral (except early diagnosis of ADPKD in childhood
with positive family history)
236
B) Horseshoe Kidney
- Most prevalent fusion abnormality of developing kidney
- Commonly occurs at lower poles, 2 separate excretory
urinary system are maintained
- Isthmus may be located at/ lateral to midline (symmetric or
assymetric horseshoe kidney)
- May contain actual parenchyma or a fibrous band
- Physiology: Kidneys arrest embryologic ascension towards
dorsolumbar position usually between 4th to 9th weens POG
- Pathology: Inferior mesenteric artery holding isthmus and
preventing further rostral migration
- Blood supple is variable & may come from iliac arteries/
aorta, sometimes hypogastric & middle sacral arteries
- May occur isolated or associate with Turner, trisomy 18, less common (trisomy 13, 21)
- Associate with bicornuate/ septate uterus (girls) & hypospadias, undescended testis (boys)
- Most are asymptomatic & diagnosed incidentally by USS
- Symptoms: Pain, haematuria, obsturction, UTI, hydronephrosis (80%), urolithiasis (20%)
- Due to VUR, obstruction of collecting system or UPJ by external ureteric compression
- Patient with isolated case have slightly higher risk of developing Wilms tumour
- Investigation: Renal USS (hydronephrosis), MCUG (identify VUR), DTPA (obstruction)
- Management: Antibiotics & Surgical correction
C) Duplex collecting system
- Defined as 2 pyelocaliceal system within one renal
unit (both ureters may either drain separately or
jointly over a single orifice into bladder)
- Unilateral or bilateral (15-40%), associate with
congenital genitourinary tract abnormalities
- Common, 0.2% of live births
- Mostly asymptomatic, incidental finding
- Occurs when 2 ureteral buds arise from Wolffian duct
- Complete duplication:
- Upper renal unit: drains ectopically in bladder,
urethra (urinary dribbling,incontinence), vagina, uterus
- Lower renal unit: drains into ureteric insertion
- Investigations: renal USS, MCUS (identify VUR,
ureterocele, obstructive uropathy)
- Complications:
- Upper pole: Urinary obstruction from ectopic insertion
(hydronephrosis), ureterocele
- Lower pole: Urinary reflux (from maldevelopment of
ureter`s valve mechanism)
- Management: Surgical correction
D) Renal agenesis & Multicystic dysplastic kidney (MCDK)
- Renal agenesis: absence of both kidneys
- MCDK: failure of union of uteretic bud (which form ureter, pelvis, calyces, collecting ducts) with
nephrogenic mesenchyme (large fluid-filled cysts without renal tissue/ connection to bladder)
237
Renal agenesis & MCDK (Non-functioning kidneys)
238
Renal Assessment
240
Definition:
Lower UTI Collective terms involving cystitis & urethritis
Upper UTI Collective terms involving pyelonephritis & renal abscess
Urosepsis Bacterial infection in urinary tract invade bloodstream to cause
septicaemia
Significant bacteriuria ≥105 cfu/mL of a single species of organism
Asymptomatic bacteriuria ≥105 cfu/mL of single species of organism without UTI symptoms
Sterile pyuria 5 ≤104 cfu/mL, presence of pus cells with/without UTI symptoms or
pure/mixed growth of bacteria (seen in partially treated UTI, TB,
calculi, tumour)
Contaminated urine sample ≤104 cfu/mL or mixed culture
Recurrent UTI Same strain organism with rapid reinfection after cessation of
therapy within 2 weeks
Catheter-associated UTI Presence of UTI symptoms, ≥103 colony forming units of ≥1 bacterial
(CA-UTI) species in a single catheter urine specimen or in MSU from a patient
whose urethral, suprapubic or intermittent catheter removed within
previous 48 hours
Epidemiology:
- Occurs in 1% of boys & 1-3% of girls before age of 11 (50% have recurrence within a year)
- First year (M>F = 2.8-5.4:1), beyond 1-2 years (F>M = 10:1)
- In girls, first UTI is usually by age of 5, with peaks during infancy & toilet-training
- Comprises of 5% of febrile illness in early childhood
- Majority of cases of CKD in child are 2` to VUR or obstructive nephropathy which usually
associate with recurrent UTI
Aetiology:
E. coli - Commonest (85-90%), virulence depends on:
- Cell wall antigens (O,K,H antigens)
- Possession of endotoxins (haemolysin)
- P.fimbriae mediate attachment → pyelonephritis
Proteus - Common in boys, presence under prepuce
- Predisposes to formation of phosphate stone by urea-splitting mechanism →
ammonia → alkalising urine
Pseudomonas - Usually associated with structural abnormality in urinary tract affecting
drainage or catheter insertion (CA-UTI)
Klebsiella - More commonly found in hospital-acquired UTI due to their resistance to
antibiotics favours their selection in hospital
Enterococus - In neonate, UTI is due to haematogenous spread
- In older child, UTI is due to ascending spread (bowel organism colonise
periurethral area & adherence to uroepithelial cells)
S. saprophyticus - Present for both gender, more in adolescent girls (prone to be sexually active)
S. epidermidis - Associate with UTI in hospitalised patients (esp those with AIDS)
241
Risk factors:
- Divided into host defence mechanism & pathogen virulence
Host Pathogens
- Anatomy difference (female) - Bacterial infection
- Vesicoureteric reflux (developmental anomaly) - Enteric flora enter urinary tract via urethra
- Incomplete bladder emptying - Common organisms:
- Infrequent voiding, leads to bladder enlargement - E. coli
- Vulvitis - Proteus
- Hurried micturition - Pseudomonas
- Obstructive uropathy (constipation) - Pathogenicity (P fimbriae, capsular antigens,
- Neuropathic bladder (CP, spinal bifida) urease, haemolysin)
- Facilitation of entry of organism - Parasitic infection
- Uncircumcised male - Pinworm infestation
- Catheterisation - Fungi infection
- Surgery/instrumentation (cystoscopy) - Candida albican
- Behavioral activity - Immunocompromised patient
- Toilet training - Viral infection (rare)
- Wiping from back to front in girls - CMV, rubella (asymptomatic shedding in
- Tight clothing (underwear) congenitally-infected babies)
- Sexual activity - Adenovirus, BK virus (haemorrhagic cystitis in
- Pregnancy marrow transplant)
- Anatomy anomaly (labial adhesion)
Clinical features:
Newborn/Infant Older children
- Non-specific symptoms - May have specific urinary symptoms
- Fever, lethargy, irritability - Fever (chills & rigors), lethargy
- Vomitting - Frequency, secondary enuresis
- Diarrhea - Urgency/ hesistancy
- Prolonged jaundice - Dysuria/ scalding micturition
- Poor feeding, FTT - Suprapubic pain (cystitis) or loin pain
- Complications: - Cloudy & smelly urine
- Febrile convulsion (>6 months) - Anorexia, vomiting, diarrhea
- Irritability, photophobia, headache (meningitis) - Febrile convulsion
- Septicaemia
* Sometimes it is difficult to localise the site of infection whether upper or lower UTI
* The presence of UTI should be considered in children <2 years old with unexplained fever
* Pyelonephritis is normally presented with fever, loin pain while in cystitis, there is no fever, loin pain
Physical examination:
- General examination, growth, blood pressure
- Abdomen : Distended bladder, ballotable kidneys, other masses, genitalia, perineal hygiene
- Back : Spina bifida
- Lower limbs : Deformities, wasting of muscles (Neurogenic bladder)
Diagnosis:
An accurate diagnosis is extremely important as a false diagnosis of UTI will lead to unnecessary
interventions that are costly and potentially harmful. The quality of urine sample is of crucial
importance. Diagnosis is made when:
- Bacterial culture of ≥105 cfu/ml of a single organism OR
- Symptomatic + bacterial culture of 102 -104 cfu/ml of a single organism
242
Collection of urine:
Adhesive bag urine Applied to the perineum after careful washing, although there may
specimen be skin contamination. Positive culture should be confirmed with a
clean catch or suprapubic aspiration specimen
Clean catch specimen In a child who is bladder-trained. Sampling into a waiting clean pot
when the nappy is removed (recommended method)
Urethal If there is urgency in obtaining a sample and no urine has been
catheterisation passed, high sensitivity & specificity, lower risk of introducting
infections
Suprapubic aspiration Gold standard of obtaining an uncontaminated urine sample and
(SPA) any growth from SPA specimen is significant. It is usually done in
infants <1 year old, but also applicable in children up to 4-5 years
of age. Method : With the child lying in supine position, a fine
needle attached to a syringe is inserted directly into bladder 1-2 cm
above symphysis pubis under USS guidance (98% success rate) in
the midline. Urine is usually obtained at a depth of 2-3cm). It may
be used in severely ill infants requiring urgent diagnosis and
treatment, but considered invasive (increasingly replaced by
urethral catheter sampling)
Good method
- Suprapubic aspirate
- Catheter specimen
- Mid-stream specimen
- Clean catch specimen
- Bag urine specimen
Poor method
Investigations:
U-FEME + C&S - Should be microscoped and cultured straight away
- If there is delay in culture :
a) Refrigerate at 4`C (to prevent overgrowth of contaminating bacteria)
b) Add bacteriostatic agent (eg. Boric acid 1.8% or dipslides)
- UFEME diagnosis : Pyuria (>10 pus cell)
* Presence of WBC alone is not reliable (may lyse during storage or present
in febrile child without UTI in balanitis/vulvovaginitis)
- Culture diagnosis :
- ≥105 cfu/ml of single organism (90% specificity)
- Mixed organisms in the absence of WBC → Contamination
- For urine microscopy, WCC >10/ml (uncentrifuged) or >5/hpf (centrifuged)
is considered abnormal, can be false -ve in immunocompromised
Blood - FBC (leukocytosis, neutrophilia, ↑ESR, ↑CRP): non-specific for UTI
- ↑WCC >20,000-25,000/mm3 (suggestive of renal abscess)
- ↑Serum procalcitonin (pyenephritis, high risk of renal scarring)
- Blood culture (before initiating antibiotics)
Imaging - USS (reveal dilatation of upper tracts, renal size & major anomaly)
- MCUG (detect VUR or infravesical obstruction eg. posterior urethral valve)
(USS is done urgently, - 99mTc DMSA (uptake defect in early phase indicates inflammation, uptake
others for later stage) defect 6 months later indicates permanent scarring)
- MAG3 (only use in ureter dilatation without reflux, look for RAS, obstruction)
243
Studies show that 3 parameters in urinalysis (leukocyte esterase, nitrite, microscopy) carry highest sensitivity
and specificity in diagnosing UTI.
Management:
- After first proven UTI, antiobiotic therapy should be started without delay after collection of
satisfactory urine specimen, together with ultrasound of kidney & urinary tract
- In patients with high risk of serious illness, it is preferable that urine sample should be obtained
first; however treatment should be started if urine sample is unobtainable.
- Oral antibiotic is satisfactory in a non-toxic child. The usual choices include trimethoprim
or cephalosporin. Agents that are excreted in the urine but do not achieve therapeutic
concentrations on the blood stream (eg. Nalidixic acid or nitrofurantoin) should not be used
to treat UTI in febrile infants and young children with likely renal involvement
- Patients with toxic appearing/unable to retain oral intake should receive parenteral antibiotic
- Duration of treatment: 7-14 days. Always review antibiotic when urine C&S results are available
- Repeat urine culture after 2 days of treatment. Bacteriuria is almost always eradicated within
24-48 hours of introducing effective treatment. Change antibiotic if bacteriuria persists.
- Children treated for UTI should continue antibiotic at prophylactic dosage while awaiting
hospital referral and imaging studies
Prevention of UTI
- Aim : - To ensure washout of organism that ascend into the bladder
- To reduce the presence of aggressive organism
- High fluid intake to produce a high urine output
- Regular voiding
- Ensure complete bladder emptying (double micturition)
- Prevention of constipation
- Good perineum hygiene
- Antibiotic prophylaxis
- Lactobacillus acidophilus (probiotics to encourage colonisation of gut to reduce number of
pathogenic organisms which potentially cause invasive disease
244
Factors predisposing to renal scarring/damage
- Antenatal renal anomality
- Infant & boy
- Delayed treatment of UTI, recurrent UTI
- Septicemia
- Severe grades of reflux
- Host susceptibility, bacterial virulence
Antibiotic prophylaxis:
- Should not be routinely recommended in infants and children following first time UTI as
antimicrobial prophylaxis does not seem to reduce significantly the rates of recurrence of
pyelonephritis, regardless of age or degree of reflux.
- However, antibiotic prophylaxis may be considered in the following:
- Infants and children with recurrent symptomatic UTI
- Infants and children with vesico-ureteric reflux grades of at least grade III
245
Recommendations for imaging
Previous guidelines have recommended routine radiological imaging for all children with UTI.
Current evidence has narrowed indications for imaging as below:
Ultrasound Recommended in
- All children less than 3 years of age
- Children above 3 years of age with poor urinary stream, seriously ill
with UTI, palpable abdominal masses, raised serum creatinine, non
E coli UTI, febrile after 48 hours of antibiotic or recurrent UTI
Should be done urgently TRO obstruction or pus collection
DMSA scan Recommended in infants and children with UTI with any of the
following features:
- Seriously ill with UTI
- Poor urine flow
- Abdominal or bladder mass
- Raised creatinine
- Septicaemia
- Failure to respond to suitable antibiotics within 48 hours
- Infection with non E. coli organisms
MCUG Routine MCUG after first UTI should not be recommended, may be
considered in:
- Infants with recurrent UTI
- Infants with UTI and the following features:
- poor urinary stream, seriously ill with UTI, palpable abdominal
masses, raised serum creatinine, non E. coli , UTI, febrile after 48
hours of antibiotic treatment
- Children less than 3 years old with the following features:
- Dilatation on ultrasound
- Poor urine flow
- Non E. coli infection
- Family history of VUR
Done when children is free from infection, usually 6 weeks after an
acute infection
Others DTPA scan (Tc-99m diethylene-triamine-penta-acetic acid scan)
MCUG in older children (depend on USS findings)
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Further Management
This depends upon the results of investigation
Normal renal tracts - Prophylactic antibiotic not required
- Urine culture during any febrile illness or if the child is unwell
Renal scarring without VUR - Repeat DMSA 6-12 months later to ensure defect is a real scar
and not pyelonephritis
- Repeat urine culture only if symptomatic
- Assessment includes height, weight, blood pressure and
routine tests for proteinuria
- Children with a minor, unilateral renal scarring do not need
long-term follow-up unless recurrent UTI or family history or
lifestyle risk factors for hypertension
- Annual BP surveillance for life
- Annual renal function test and UFEME (for proteinuria) if
bilateral or severe scarring
- Children with bilateral renal abnormalities, impaired renal
function, raised blood pressure and or proteinuria should be
managed by a nephrologist
- Close follow up during pregnancy
Vesicoureteric reflux (VUR) - Refer VUR topic
Posterior urethral valve - Refer urologist/surgeon
Renal dysplasia, hypoplasia - May need further imaging to evaluate function and drainage.
or evidence of obstruction - Refer surgeon if necessary.
- Monitor renal function, BP, and growth parameters
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Vesicoureteric Reflux (VUR)
Definition:
- Retrograde flow of urine from the bladder up to the ureter and collecting system
Aetiology:
Primary VUR Secondary VUR
- Congenital incompetence of ureterovesical (UV) - Distal bladder obstruction (BOO)
junction (commonest) - Increased intravesicular pressure from cystitis or
- Ureter is displaced laterally and enter directly acquired bladder obstruction
into the bladder rather than at an angle - Posterior urethral valve (urethral obstruction)
- Shorten intramural course - Neuropathic blader (50%)
- Familial (30-40% in first-degree relatives) - Voiding dysfunction
- Duplication of ureters with/without ureterocele
- May obstruct upper collecting system
- Often lower pole of duplicated renal unit
- Post-UTI (temporary) or recurrent UTI
Clinical features:
- Commonest radiological abnormality in children with UTI (30-40%)
- Children with VUR are at risk for further episodes of pyelonephritis with potential for increasing
renal scarring and renal impairment (Reflux nephropathy)
ESRF (End stage
renal failure)
Recurrent Progresssive
VUR
UTI renal
Hypertension
* Backflow of urine from the renal pelvic into the papillary collecting duct → high risk of renal scarring
Investigations:
Renal ultrasound (RUS) - Evaluate urinary tract for hydronephrosis, scarring
Micturating cystourethrogram - Detect urethral/ bladder abnormalities
(MCUG) - Detect VUR
- Provides additional anatomic detail as compared to NCG
- Indicated when RUS reveals findings suggestive of VUR or there is a
recurrence of febrile UTI
Radionuclide cystogram (NCG) - Same as MCUG but able to detect mild VUR with less radiation
Dimercaptosuccinic acid - Reliable test for diagnosis of acute pyelonephritis
(DMSA) - Detection of renal scarring
Nuclear renal scanning - Identify renal scarring
Complications:
Incomplete bladder emptying - Urine return into bladder after voiding
- Predisposes to UTI
Pyelonephritis - Particularly if there is intrarenal reflux
Chronic kidney disease (CKD) - Occur when voiding pressure is high & transmitted to renal papillae
- Segmental glomerulosclerosis with interstitial scarring → shrunken,
poorly functioning segment of kidney (if severe & bilateral) → renal
failure & HPT
Hypertension - Renal scarring causing decreased renal function, fluid retention
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Classification of VUR Severity (International Reflux Study Committee)
Management:
- Most reflux resolves spontaneously with time (grade 1 to 2 - 80%; grade 3 - 50%; grade 4 - 25%)
- Studies have not shown any significant difference in outcome between both medical & surgical
intervention
Medical Surgical
- Long-term prophylactic antibiotic therapy - Ureteral reimplantation/ dextranomer/
- TMX or nitrofurantoin hyaluronic acid copolymer (Deflux procedure)
- Maintain sterile urine until - Very successful minimally invasive correction of
- At least 4-5 years old (based on fact that new mild to moderate VUR
scars have only rarely been seen to develop - Considered if:
after 4-5 years but optimal duration is not yet - Antibiotic prophylaxis fails to prevent
well-defined) breakthrough infection
- Reflux has resolved spontaneously - New scar formation
- Useful in children with high-grade VUR or - Non-compliance to medical prophylaxis
recurrent symptomatic UTI - Persisting high grade (4 to 5) VUR beyond 2
years especially in girls
- Immediate treatment for any breakthrough
infection
- Periodic urine culture (approximately every 3
months) to detect asymptomatic bacteriuria as
well as culture when a fever is present
Additional
- Advice on general measure to prevent recurrent UTI
- Follow up patients with renal scarring (refer UTI section)
- Sibling screening (High risk group would be siblings younger than 5 years of age, evidence of AD)
* For mild reflux (grade 1 and 2), discontinuing prophylaxis after age 2 years. If DMSA scan shows
scarring; repeat 1 year later. If DMSA scan normal, can discharge.
Medical management is the treatment choice for
- All infant (regardless of the reflux grade)
- Older children with mild to moderate VUR (grade 1-3) who can be maintained infection-free
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Haemolytic Uraemic Syndrome (HUS)
Introduction:
- Characterised by triad: microangiopathic haemolytic anaemia, thrombocytopenia, renal injury
- Important cause of AKI in children (occurs in <5 years of age but can occur in older child)
- Most common type is associated with prodromal diarrhoeal illness (D+HUS)
Aetiology:
- Contamination of meat, fruit, vegetables or water with verotoxin(VT)-producing E.coli O157:H7
or Shigella → inactivate ADAMTS13→microthrombi→ haemorrhagic enterocolitis → HUS
- Atypical HUS (without prodromal diarrhoea) is more severe than D+HUS, can be 2` to infection
(Strep Pneumoniae, HIV), genetic & acquired defects in complement regulation, medication, SLE
Clinical features:
Symptoms Signs
Prodromal phase: - Pallor (microangiopathic haemolytic anaemia)
- Diarrhoea - Irritability
- Bloody stools (enterocolitis) - Petechiae (thrombocytopenia)
- Signs of dehydration
Acute phase (7-10 days later): - Hypertension (volume overload/AKI)
- Weakness, lethargy - CNS signs: seizures (25%), encephalopathy
- Abdominal pain - Other organs:
- Oliguria/anuria (AKI) - Pancreatitis
- Haematuria - Cardiac dysfunction
- Bleeding tendency (thrombocytopenia) - Colonic perforation
* Suspect child without diarrhoea with microangiopathic syndrome as TTP (predominant CNS symptoms with
significant renal disease, recurrence is common, but difficult to distinguish from HUS in some cases)
Investigation:
Blood - Normochromic, normocytic anaemia (MAHA)
- Thrombocytopenia
- Leukocytosis
- Increased LDH, decreased hatoglobin (breakdown of RBCs)
- Elevated reticulocyte count (RR)
- LFT: Increased unconjugated bilirubin, Increased AST
- RP: Elevated creatinine
PBF - Presence of schistocytes, helmet cells, burr cells
Urinalysis - Presence of haematuria, proteinuria, pyuria, casts
Others - Positive stool culture for E.coli O157 : H7
- Positive stool test for shiga-toxin
- Elevated amylase/ lipase
- Coombs test negative
- D-dimer normal (TRO SLE, consumptive coagulopathy)
Management:
Supportive Managing complications
- Volume repletion (early hydration for diarrhoea) - Dialysis (indicated if uncorrected renal
- Control of hypertension insufficiency)
- AVOID antibiotics, antidiarrhoeal - RBC transfusion
(as they may increase risk of developing HUS) - Platelet transfusion (NOT use unless in active
haemorrhage as it might worsen thrombotic
microangiopathy)
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Proteinuria
- Defined as urine protein > 40 mg/m2/hr or >1 g/m2/day OR
- Early morning urine protein: creatinine index > 200 mg/mmol (3.5 mg/mg)
A) Physiological/ Transient Proteinuria
- Causes include:
- Orthostatic (eg. proteinuria only when standing upright, normal when recumbent)
- Exercise induced (transient)
- Febrile (transient)
B) Pathological/ Persistent Proteinuria
- Confirmed by repeated urine dipstick then quantified by 24 hrs urine collection or measuring
urine protein/creatinine ratio in an early morning sample (Protein should not >20 mg/mmol Cr)
- Causes include:
Tubular proteinuria - Hereditary tubular dysfunction
- Acquired tubular dysfunction
Glomerular disease - Minimal change disease
- Glomerulonephritis
- Abnormal glomerular basement membrane (familial nephritides)
Vascular disease - Hypertension (increased glomerular perfusion pressure)
Others - UTI - Reduced renal mass
- Drugs - Urinary calculi
- Tumours (eg. lymphoma)
- Usually asymptomatic and may appear frothy urine
- Most common symptoms of renal impairment
- Primary detection is by urine dipstick (can detect >100-200mg/L, react primarily with albumin)
Haematuria
- Indication of bleeding from anywhere in urinary tract (RBC should not present in normal urine)
- Red-coloured urine or postitive test for Hb on urine dipstick (>10 RBC/hpf) >5RBC/hpf
Macroscopic - Visible & reported as red urine by patient
- If seen at initial voiding, becomes clear later (urethra, prostate, bladder neck)
- If diffuse at voiding (bladder, ureter, kidneys) * Brown urine for glomerular
- If seen at end of voiding (prostate, bladder base)
Microscopic - Detected by urine dipstick (detection limit: 15-20,000 RBC/ml)
- Can be false +ve for haemoglobinuria or myoglobinuria
- Always followed by urine microscopy (+phase contrast) to confirm presence
of RBC (red cell cast suggestive of bleeding from kidneys, most often dt GN)
- Causes:
Non-glomerular Glomerular
- Infection (bacterial, viral, TB, schistosomiasis) - Acute GN (usually with proteinuria)
- Trauma (genitalia, urinary tract, kidneys) - Chronic GN (usually with proteinuria)
- Stones - IgA nephropathy
- Tumours - Familial nephritis (eg. Alport syndrome)
- Sickle cell disease - Thin GBM disease
- Bleeding disorders
* GBM is -ve charge & permeability depends on size &
- Renal vein thrombosis charge molecules
- Hypercalciuria
* Renal biopsy indicated when RP abnormal, persistent ↑complements, recurrent macroscopic hematuria
or significant persistent proteinuria
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Acute Glomerulonephritis (AGN)
Definition:
- Specific set of renal disease which immunological mechanism triggers inflammation and
proliferation of glomerular tissue
- Antigen-antibody complexes in the glomerular basement membrane (GBM) induces
complement activation
- Initiates glomerular proliferation and inflammatory response
Epidemiology:
Most common in the younger age group
Aetiology:
Exogenous Endogenous
- Post-streptococcal infections* - Autoimmune diseases
- Pharyngitis - Henoch Schonlein purpura
- Skin infection (eg. impetigo) - Systemic lupus erythematosus (SLE)
- Bacterial infection/Sepsis - Wegener`s Granulomatosis
- Subacute bacterial endocarditis - Polyarteritis Nodosa (PAN)
- Drugs - Hemolytic Uremic Syndrome
- Heavy Metal - IgA Nephropathy
- MembranoprolIferative GN
- Hereditary nephritis
- Goodpasture syndrome (anti-GBM ds)
* Most common cause in children (6-10 years old) & developing world, usually caused by Group A β-hemolytic
streptococci
Post-Streptococcal AGN
Pathogenesis:
- Immunological in nature
- Bacteria become trapped in the glomerulus → Acute diffuse proliferative GN
- Formation of immune complex → Deposited in the glomerular capillary (evoke inflammatory
response → Complement activation) → Damage to GBM → Hematuria & Proteinuria
- Increased glomerular cellularity restricts glomerular blood flow & therefore glomerular
filtration rate (GFR) decreases → Reduced urine output & fluid retention → Pulmonary oedema
& HTN (can lead to seizures)
Clinical Features:
- Post-streptococcal GN develops after 1-2 weeks of streptococcal infection
Symptoms Signs
Specific Cardinal Features of AGN
- Edema (Periorbital, pedal & scrotal) - Oedema
- Facial puffiness is an early sign - Hematuria (micro/macroscopic)
- Smoky or tea-coloured urine (haematuria) - +/- proteinuria
- Reduced urine output - Uraemia (azotemia)
Non-Specific - Oliguria
- Anorexia & lethargy - Hypertension
- Abdominal Pain General
Complications: - Hypertension
- SOB (pulmonary oedema) - Papilloedema (fundoscopy)
- Dizziness, headache (hypertensive encephalopathy) - Skin lesions (eg. impetigo, cellulitis)
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Complications:
CNS - Hypertensive encephalopathy
Early - Restless, drowsy
- Headache
Late - Visual disturbance
- Vomiting, nausea
- Seizures, Coma
K – Ketones (DKA)
U – Uraemia
S – Sepsis
S – Salicylates
M – Methanol
A – Aldehydes
L – Lactic acidosis
Diagnosis:
- Detailed history (evidence of a recent streptococcus infection (culture of the organism)
- Raised ASOT and low C3 level that return to normal after 3-4 weeks
- ASOT (Antibody to Streptolysin-O titre) - Post-streptococcal GN
- ANCA (Anti-neutrophil cytoplasmic antibody) - Goodpasture synd
Investigations:
Urinalysis & Culture - Hematuria (RBC distorted and fragmented)
- Proteinuria (usually trace up to 2+ but if >2+ need to consider nephrotic
syndrome)
- RBC casts (pathognomonic for AGN) & other cellular cast
- Pyuria may also be present
Bacteriological & - Raised ASOT (>200 IU/ml)
serological evidence - Increased anti-DNAse B (if available) - better serological marker of preceding
of antecedent strep. streptococcal skin infection
Infection - Throat swab or skin swab
Blood - FBC (↑WCC for evidence of infection)
- Renal Profile
- Blood urea, serum creatinine (assess renal function, ↓GFR)
- Electrolytes (look for electrolyte imbalance)
- Complement levels
- C3 level is low at onset of symptoms and normalize by 6 weeks
- C4 level is usually within normal limits in post streptococcal AGN
- Immunological markers
- Antinuclear & anti-dsDNA antibody (SLE)
- ANCA (for Wegener`s granulomatosis & polyarteritis)
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Imaging - CXR (look for cavitation in Wegener`s granulomatosis)
- Renal ultrasound & biopsy
- Indication of renal biopsy:
- Steriod-resistant, atypical presentation or severe acute renal failure
- Prior history of renal disease or family history of nephritis
- Features suggesting non post-infectious AGN as cause of acute nephritis
- Delay resolution:
- Oliguria > 2weeks
- Azotemia > 3 weeks
- Gross haematuria > 3 weeks
- Persistent haematuria > 6 months
Management:
- Divided into supportive & specific management
A) Supportive Management:
- Strict monitoring
- Fluid intake, urine output, daily weight, BP (nephrotic chart)
- Penicillin V for 10 days to eliminate β-haemolytic streptococcal infection (give erythromycin if
penicillin is contraindicated)
- Fluid restriction to control edema and circulatory overload during oliguric phase until child diureses
and BP is controlled
- Day 1 : Up to 400 mls/m2/day. Omit if child has clear signs of fluid overload eg. pulmonary oedema
- Day 2 : Till patient diureses - 400 mls/m2/day (as long as patient remains in circulatory overload)
- When child is in diuresis - free fluid is allowed
- Diuretics (eg. Furosemide) should be given in children with pulmonary oedema, it is usually needed
for treatment of hypertension
- Diet: Salt free! Protein restriction is unnecessary
- Look out for HTN and complications of Post-streptococcal AGN:
- Hypertensive encephalopathy
- Pulmonary edema (acute left ventricular failure)
- Acute renal failure
- Indication for dialysis:
- APO, Hyperkalemia, severe acidosis, uraemic symptoms
B) Specific Management:
Infection - Antibiotic (oral penicillin ×10 days) to eliminate β-haemolytic Streptococcal
infection
Edema - Diuretic eg. frusemide may be useful for treatment of hypertension and if fluid
retention has not improved with fluid restriction
Hypertension Significant hypertension but asymptomatic
① Nifedipine - Bed test and recheck BP 30 min later
② Frusemide - If BP still high, give oral nifedipine 0.25-0.5 mg/kg. Recheck BP 30 min later
③ Captopril - Monitor BP hourly ×4 hours the 4 hours if stable
④ Metoprolol - Oral nifedipine can be repeated if necessary on prn basis.
- May consider regular oral nifedipine (6-8 hourly) if BP persistently high
- Add frusemide 1mg/kg/dose if BP still not well controlled
- Other anti-hypertensives-captopril (0.1-0.5 mg/kg 8 hourly); Metoprolol 1-
4mg/kg 12 hourly
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Symptomatic/severe hypertension/hypertensive emergency/ hypertensive
encephalopathy
- Symptom/ sign: headache, vomiting, loss of vision, convulsions, papilloedema
- Emergency management is indicated to reduce BP sufficiently to avoid
hypertensive complications yet to maintain it at a level that permits
autoregulatory mechanism of vital organs to function.
- Reduce mean BP [DBP + 1/3(SBP - DBP)] by 25% over 3-12 hours then next 75%
reduction is achieved over 48 hours
Severe acute - Severe persistent oliguria or anuria with azotaemia is uncommon
kidney injury - Peritoneal dialysis
- Hemodialysis
Hyperkalemia - IV calcium gluconate
- Protect myocardium from hyperkalemia
- IV insulin with dextrose
- To drive potassium into cells
- IV sodium bicarbonate
- To connect acidosis
- Resonium (oral or rectal)
Pulmonary - Sit-up & give high flow O2 by face mask
edema - Venous vasodilator (eg. morphine) (+ metoclopramide: antiemetic)
- IV diuretics (eg. frusemide)
- IV nitrates also can be used
- If no response consider hemodialysis
When to discharge?
Criteria for discharging patients:
- Weight drop
- Renal function improved
- HTN resolved
Follow up: (if proteinuria and hematuria has fully resolved)
- Follow up for at least 1 yr at 1-3 months interval
- Do U-FEME (and renal function if initially abnormal) to evaluate recovery
- Monitor BP at every visit
Prognosis:
- Proteinuria and oedema characteristically decline rapidly by 5-10 days
- Hypertension and gross hematuria normally resolves by 2-3 weeks
- C3 returns to normal by 6-8 weeks, Microscopic hematuria persist for months to a year
- Generally EXCELLENT prognosis, self limiting disease with >95% recover completely but
minority of patient progress to renal failure disease
255
Natural history of Acute Post-Streptococcal GN:
Vasculitis
- Includes HSP, PAN, microscopic polyarteritis & Wegener granulomatosis
- Clinical features: Fever, malaise, weight loss, skin rash, arthropathy
- Diagnosis:
- ANCA(anti-neutrophil cytoplasmic Antibody)
- Renal arteriography (to demonstrate aneurysm in PAN)
- Management:
- Steroids, plasma exchange & IV cyclophosphamide
Pathophysiology:
- Believed to be an immunological event but precise pathway still unknown
- Hallmark: Heavy proteinuria
- Selective permeability to albumin of the glomerular capillary
- There are two hypotheses:
- Change in the anionic composition of the GBM (albumin is negatively charged)
- Flattening, retraction and effacement of the foot podocytes
Oedema (salt & water move to extravascular compartment due to ↑ hydrostatic pressure) +
Activation of renin-angiotensin aldosterone system
Hypovolemia → Hyperviscosity *
(↓ synthesis of antithrombin, protein C, protein S)
257
Hyperlipidaemia
- Increased cholesterol and triglyceride synthesis following increased hepatic albumin synthesis
- Urinary loss of enzyme digesting cholesterol
Clinical features:
Symptoms Signs
- Facial swelling (earliest) - Periorbital oedema
- Breathlessness (due to pleural effusions & - Scrotal, leg, sacral & pedal oedema
abdominal distension) - Ascites
- Abdominal pain & diarrhea (lethargy) - Signs of pleural effusion
- Decreased urine output - Ipsilateral reduced chest expansion
- Hypertension (<15%) - may be atypical NS - `Stony dull` to percussion
- Absent breath sounds or bronchial breath
sound just above the effusion
Complications:
Hypovolemia - Due to oedema (water and sodium moves into third space)
- Clinical Features: abdominal pain & syncope (peripheral vasoconstriction)
- Investigations:
- Low urinary sodium (<20mmol/L)
- High PCV
- SHOCK & THROMBOSIS (commonly renal vein thrombosis)
Thrombosis - Urinary losses of antithrombin increased blood viscosity
- Increased synthesis of clotting factors by steroid thrombosis
Infection - Urinary losses of immunoglobulin (susceptible to infection particularly
Pneumococcus)
- Steroid therapy (immunosuppression)
- Generalised edema - good for bacterial culture medium
- eg. Spontaneous Bacterial Peritonitis (SBP), cellulitis, URTI
Hypercholestrolemia - As explained above
Renal Failure - <5% develops RF (NOT for minimal change ds)
258
Investigations:
Blood - FBC (Hb, WCC & Hct)
- Evidence of infection & hemoconcentration
- ESR
- BUSE + Creatinine
- LFT (Look for hypoalbuminemia <25g/L)
- Serum complement level (↓C3 & C4 in AGN)
- Serum ASOT & anti-DNAse B
- Hepatitis B
Urine - Urine dipstick (albustix) for proteinuria
- 24-hour urine collection (in older children)
- U-FEME (if +ve) + C & S
- Urinary sodium concentration
- Low sodium (<20mmol/L) indicates hypovolemia
Renal Biopsy - Not indicated for idiopathic syndrome in children prior to starting corticosteroid
therapy
- Main indication is
- Steroid resistant nephrotic syndrome*
- Presence of atypical features such as persistent hypertension, gross hematuria
Imaging - Renal ultrasound/CT/MRI (TRO renal vein thrombosis if indicated)
* Define as failure to achieve remission despite 4 weeks of adequate corticosteroid therapy
Management:
1) Management of the oedematous state
Bed rest - Not required & usually not practical unless the child has gross oedema
Diet - A normal protein diet with adequate calories is recommended
- No added salt to the diet during the oedematous state
Antibiotics - Penicillin V 125mg BD (1-5 y/o); 250mg BD (6-12 y/o); 500mg BD (>12y/o) is
recommended during relapse particularly with gross oedema
Fluid status - Carefully assess the haemodynamic status
- Check for signs and symptoms which may indicate
- Hypovolaemia (abdominal pain, cold peripheries, tachycardia and poor pulse
volume, low blood pressure) OR
- Hypervolaemia (basal lung crepitations and rhonchi, hypertension)
Fluid restriction - Not usually recommended except in oedematous state
Diuretics - eg. frusemide is not usually necessary in steroid responsive nephrotic syndrome
but if required should be used with caution as it can precipitate hypovolaemia
Human albumin - 0.5-1.0 g/kg can be used in symptomatic grossly oedematous states together with
(20-25%) IV frusemide at 1-2 mg/kg to produce a diuresis
- Caution: fluid overload and pulmonary oedema with salt poor albumin infusion.
Urine output and blood pressure should be closely monitored
- Human albumin at 0.5-1.0 g/kg of 5%, 20% or 25% (which ever is available) over
one hour in those suspected to have hypovolaemia/underfilled state. Do not give
frusemide in this instant.
Chart - Input/Output chart
monitoring - Nephrotic chart
259
poor albumin is not available, other volume expanders like 5% albumin, plasma
protein derivatives or human plasma can be used
Primary - Clinical Features: fever, abdominal pain in children with frank nephrotic syndrome
peritonitis (SBP) - Investigations: Blood culture, peritoneal fluid culture (not usually done)
- Treatment: parenteral penicillin and a third generation cephalosporin
Thrombosis - Detailed investigation & adequate treatment with anticoagulation is needed
3) General Advice
- Inform regarding high probability (85-95%) of relapse.
- Home urine albumin monitoring. Urine dipstick testing of the first urine specimen in the
morning daily. Parents are advised to consult doctor if albuminuria >2+ for 3 consecutive days
- Immunocompromised status eg. steroid therapy
- Parents and children should be advised & cautioned for contact with chicken pox and measles,
and if exposed should be treated like any immunocompromised child
- Immunization: While the child is on corticosteroid treatment and within 6 weeks after its
cessation, only killed vaccines may safely be administered to the child. Live vaccines can be
administered six weeks after cessation of corticosteroid therapy
- Acute Adrenal Crisis
- This may be seen in children who have been on long term corticosteroid therapy (equivalent
to 18mg/m² of cortisone daily) when they undergo situations of stress. Prevention and
- Treatment: corticosteroids (hydrocortisone) given in 3 divided doses at 2-4 mg/kg/dose
4) Corticosteriod therapy
- Corticosteroids is effective in inducing remission of nephrotic syndrome but the most optimal
dose & duration is yet to be resolved although it has been found that longer duration results in
more prolonged remission
- Prednisolone dosage at:
- 60 mg/m²/day (maximum 80mg/day) for 4 weeks
- Followed by 40mg/ m²/EOD (maximum 60mg) for 4 weeks
- Then reduced prednisolone dose by 25% monthly over next 4 months
- 90% of children will achieve remission defined as urine dipstick is trace or nil for 3 consecutive
day within 28 days, many within 7-14 days
- Definition:
Steriod-sensitive - Age between 1-10 years old
nephrotic syndrome - No macroscopic haematuria
- Normal BP, complement, renal function
Steriod-resistant - Failure to achieve response to an initial 4 weeks treatment with prednisolone
nephrotic syndrome 60mg/m²/day
- Should be referred to a nephrologist for a renal biopsy
5) Management of relapse
- Majority of children with nephrotic syndrome will relapse.
- Definition: Urine albumin excretion >40mg/m²/hour or urine dipstix of 2+ or more for 3
consecutive days
- Treatment: Prednisolone 60 mg/m²/day until remission then 40 mg/m²/EOD for 4 weeks & off
- Breakthrough proteinuria may occur with intercurrent infection and usually does not require
prednisolone if the child has no edema remains well and the proteinuria resolves with
resolution of the infection. If proteinuria persists, treat as relapse.
260
6) Management of frequent relapse
- Definition: ≥2 relapses within 6 months of initial response or ≥4 relapses within any 12 months
- Treatment:
- Prednisolone 60 mg/m²/day till urine albumin nil/trace for 3 days (until remission)
- Prednisolone 40 mg/m²/alternate morning for 4 weeks only
- Taper prednisolone dose every 2 weeks and keep on as low alternate day dose as possible for
6 months. Should a child relapse while on low dose alternate day prednisolone, the child
should be re-induced as for a relapse.
7) Management of Steriod-dependent Nephrotic Syndrome
- Definition: 2 consecutive relapses occurring during the period of steroid taper or within 14 days
of its cessation
- Treatment:
- If the child is not steroid toxic, re-induce with steroids and maintain on as low a dose of
alternate day prednisolone as possible
- If the child is steroid toxic (short stature, striae, cataracts, severe cushingoid features)
consider cyclophosphamide therapy
8) Cyclophosphamide therapy
- Indicated for the treatment of steroid dependent nephrotic syndrome with sign of steroid
toxicity & should be started when child is in remission following induction with corticosteroids
- Dose: 2-3 mg/kg/day for 8-12 weeks
- Monitoring: FBC and U-FEME two weekly
9) Relapse post-Cyclophosphamide
- Relapses after a course of cyclophosphamide is treated as for relapses after the initial diagnosis
of nephrotic syndrome if the child does not exhibit any further signs of steroid toxicity
- Should relapse occur soon after a course of cyclophosphamide when the child is still steroid
toxic, or the child again becomes steroid toxic after multiple relapses then a paediatric
nephrology opinion should be sought
- Treatment options available include cyclosporine & levamisole
10) Steroid-resistant nephrotic syndrome
- Refer for renal biopsy, specific treatment will depend on the histopathology
- General management of nephrotic state:
- Control of edema
- Restriction of dietary sodium
- Diuretic eg. Frusemide, Spironolactone
- ACE inhibitor (eg. captopril) or ARB (eg. Losartan, Irbesartan) to reduce proteinuria
- Monitor BP & renal profile 1-2 weeks after initiation of ACE inhibitor or ARB
- Control of hypertension using anti-hypertensive of choice
- Penicillin prophylaxis
- Monitor renal function
- Nutrition: normal dietary protein content, salt-restricted diet
- Evaluate calcium & phosphate metabolism
Prognosis:
- 93%-97% respond to steroid therapy (steroid-sensitive)
- 1/3 resolve, 1/3 relapse infrequently, 1/3 relapse frequently
261
- <5% develop renal failure
Summary of Treatment of Nephrotic Syndrome:
Definitions:
Remission - Urine dipstick is trace or nil for 2 consecutive days within 28 days
Relapse - Urinary albumin excretion > 40mg/ m²/hour OR
- Urine dipstix ≥ 2+ for 3 consecutive days
Frequent relapse - ≥ 2 relapses in 6 months of initial diagnosis OR
- ≥ 4 relapses within any 12 months period
Infrequent relapse - Anything less than frequent
Steroid-resistant - Failure to achieve remission in spite of 4 weeks treatment with prednisolone at
60 mg/m2/day (standard steriod therapy)
Steroid- - ≥ 2 consecutive relapses during period of steroid tapering or within 14 days of
dependance steriod cessation
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PART VIII
HAEMATOLOGY
Haemopoiesis
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Anaemia in Children
Definition:
- Hemoglobin level below the normal range for a child of that age and gender (WHO)
Age Non-anaemic Mild anaemia Moderate anaemia Severe anaemia
6 - 59 months ≥11.0 10.0 - 10.9 7.0 - 9.9 <7.0
5 - 11 years ≥11.5 11.0 - 11.4 8.0 - 10.9 <8.0
12-14 years ≥12.0 11.0 - 11.9 8.0 - 10.9 <8.0
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Aetiology (Classification according to age groups):
Neonates
Severe Less severe
Antepartum Antepartum
- Rh isoimmunisation (usually with jaundice) - ABO incompabilities
- Twin-twin transfusion syndrome - Kell & Duffy
- Feto-maternal transfusion
- Abruptio placentae
Intrapartum/ Postpartum
- Hemorrhage
Infants or childhood
Type Examples
Haemolytic anaemia
Intracorpuscular factor Extracorpuscular factor
- Hemoglobinopathies - Autoimmune hemolytic anaemia
- Sickle cell anemia (Coomb`s test +ve)
- Thalassemia - Primary
- Red cell enzyme deficiency - Infection (CMV, HIV, viral hepatitis,
- G6PD deficiency infectious mononucleosis,
- Pyruvate kinase deficiency mycoplasma, typhoid fever,
- Red cell membrane defect malaria)
- Spherocytosis - Drug: penicillin
- Congenital dyserythropoietic - Collagen disease: SLE
anemia - Heavy metals
- Hypertension
Deficiency anaemia
- Nutritional anemia
- Iron deficiency anemia
- Folate or very rarely vitamin B12 deficiency
- Malabsorption syndrome
- Celiac disease
Blood loss
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Acute Chronic
- Trauma - Parasites (eg. hookworm)
- GIT - Bleeding disorders
- GERD - Hemophilia
- Meckel`s diverticulum - von Willebrand`s disease
- Cow`s milk protein intolerance
- Menstruation in adolescent
- Epistaxis
- Iatrogenic (eg. excessive
venesection in infants)
Clinical features:
Symptoms Signs
- Pale - Pallor, jaundice
- Lethargy & tiredness - Tachycardia, tachypnea
- Anorexia - Collapsing pulse, bounding pulse
- Reduced effort tolerance - Flow murmur
- Associate with jaundice - Bleeding site, ecchymosis
- Reduced activity - Hepatosplenomegaly
- Hematemesis, hematochezia - Lymphadenopathy
- Signs of iron-deficiency anemia:
(koilonychia, angular stomatitis, glossitis)
- Signs of cardiac failure:
(tachycardia, tachypnea, cardiomegaly,
bibasal crepitations)
Hb HPLC Findings:
Sickle-cell:
- HbS present
- No HbA
β-Thal major:
- Only HbF present
β-Thal minor:
- Increased HbA2
α-Thal trait:
- Hb HPLC normal
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Physical Findings in Evaluation of Anaemia:
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Summary for Aetiology of Anaemia:
Introduction:
- Commonest deficiency disease in the world at present.
- Commonest cause of anemia in childhood
- Prevalence is higher in poorer socioeconomic groups.
- Incidence of iron deficiency anemia in most reported series appears to be related to not age,
sex, or race, but to socioeconomic factors.
- Inadequate intake of iron is common in infants as additional iron is required for the increase in
blood volume accompanying growth and to build up the child`s iron stores
- May develop because of a delay in introduction of mixed feeding beyond 6 months of age or to
a diet with insufficient iron-rich foods, especially if it contains a large amount of cow`s milk
- Iron absorption
- Markedly increased when eaten with food rich in vitC (fresh fruit & vegetables)
- Inhibited by tannin (tea) Iron content in food:
Iron sources:
- For infants, iron may come from:
- Breastmilk (low iron content but 50% of the iron is
absorbed)
- Infant formula (supplemented with adequate iron)
- Cow`s milk (higher iron content than breastmilk, only
10% is absorbed)
- Solids introduced at weaning (eg. cereals:
supplemented with iron but only 1% is absorbed)
Aetiology:
- Chronic blood loss
- Meckel's diverticulum, peptic ulcer, ITP, parasitic infection, hemoglobinuria, polyp
- Increased demand - prematurity/low-birth weight infant and rapid rate of growth
- Frequently poor dietary intake of iron
- Impaired absorption - Malabsorption, chronic diarrhea, GI abnormalities, hookworm infection
Laboratory findings:
- Red cell indices
-↓Hb (hypochromic , microcytic RBC, Anisopoikilocytosis, +/- target cell)
-↓MCV
-↓MCH
- Low serum ferritin
- Stool for occult blood loss and ova and cyst for parasitic infections
Management:
- Nutritional counseling
- Advice on diet
- Maintain breastfeeding
- Use iron fortified cereals
- Iron supplementation
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- Oral iron medication: 6mg/kg/day of elemental iron in 3 divided doses for 6-8 weeks after
hemoglobin level is restored to normal. Syrup FAC (ferrous ammonium citrate): 1mg elemental
iron per ml. Ferrous fumarate/sulphate tablet: 200mg elemental iron per tablet.
- Consider the following for failure to respond to oral iron:
- Non-compliance
- Inadequate iron dosage
- Unrecognised blood loss
- Incorrect diagnosis
- Impaired GI absorption
- Blood transfusion: In general no transfusion required in chronic anemia unless there are signs
of decompensation (e.g.: cardiac dysfunction) and the patient is otherwise debilitated. Give
low volume packed cells (<5ml/kg) if necessary over 4-6 hours with IV furosemide (1mg/kg) in
severe anemia (Hb <4g/dL)
- For 6-year-old patients, blood transfusion is indicated if Hb< 6mg/dL or emergency. If patient's
condition is stable, consider 20ml/kg in 1 day.
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Thalassaemia
Definition:
Hemoglobinopathies are genetic disorders which result from either the synthesis or abnormal
Hb chain (Hb variant) or defective synthesis of normal Hb chain (thalassemia syndrome)
Introduction:
- Inherited defects of globin chain synthesis
- Results from alteration (absence/reduce) in the genes controlling the globin chain production
- Excess of other globin chains → Precipitate within red cell membrane → Cell death within bone
marrow (ineffective erythropoiesis) & premature removal of circulating red cell by spleen
(shortened RBC survival) → Hypochromic and microcytic anaemia
α-Thalassemia Reduced rate of α-chain synthesis (chromosome 16)
β-thalassemia Reduced rate of β-chain synthesis (chromosome 11)
* Chromosome 11 - ε,γ,β,δ ; Chromosome 16 - α,ζ
- Common presenting symptoms are pallor, lethargy, FTT & hepatosplenomegaly
Epidemiology:
- β-thal major is an inherited blood disorder presenting with anaemia at 4-6 months of age
- In Malaysia, β-thal carrier rate is estimated at 3-5%, most of whom are unaware of their carrier/
thal minor status
- Carrier rates of α-thal & HbE are 1.8-7.5% and 5-46% respectively (HbE are found more in
northern peninsular states)
- Interaction between a β-thal carrier with a HbE carrier may result in birth of patient with HbE/β-
thal or thal intermedia with variable clinical severity (moderate-severe forms behave like β-thal
major patients while the milder forms are asymptomatic)
Types of Haemoglobin:
Hb Structure Comments
Normal A α2β2 - 97% of adult haemoglobin
A1c α2β2 - ≤5% of HbA (glycosylated Hb)
A2 α2δ2 - 2% of adult haemoglobin (↑in β-thal)
F α2γ2 - Normal Hb in fetus from 3-9 months, ↑in β-thal
Abnormal chain H β4 - Found in α-thal
production Barts γ4 - Found in homozygous α-thal, incompatible with life
Abnormal chain S α2β2 - Substitution of valine by glutamate in position 6 of β chain
structure C α2β2 - Substitution of lysine by glutamate in position 6 of β chain
* There are 4 α gene & 2 β gene for globin synthesis
Epidemiology:
- Commonest in people from Mediterranean and Middle East
- Common in Chinese and Malays in Malaysia
During pregnancy, β-thalassemia major does not affect the fetus due to HbF. When a baby is born in the first 6
months of life it is gradually replaced with HbA. Thalassemic children are unable to produce enough HbA, he/she
is usually well at birth and become ill in later life. So, the HbF is increased in that patient.
Clinical features:
General - Pallor (anemia)
- Jaundice (due to hypersplenism, ↑ RBC destruction)
- Failure to thrive or retarded growth
- Delayed puberty
Thalassaemia - Skull bossing (prominent frontal & parietal bones)
facies (bony - Maxillary overgrowth
deformities) - Prominent malar eminence
(hypoxia - bone marrow expand inside the bones → bone weak & alter shape →
make more & more non-functional RBC → RBC dies easily)
GIT - Hepatosplenomegaly
- due to resumption of hematopoiesis (extramedullary hematopoiesis)
- Gallstones (↑ bile pigments) *cholecystectomy if biliary colic/obstructive jaundice
CVS - Cardiomegaly
- Recurrent leg ulcers
Hypersplenism
- Splenomegaly with normal function of bone marrow
- Pancytopenia (anaemia, leukopenia, thrombocytopenia) caused by enhanced capacity of splenic
pooling, sequestration and destruction of blood cells, leading to ↑ plasma volume
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Investigations:
Blood - FBC
- ↓Hb, MCH, MCV - hypochromic microcytic anaemia)
- ↑ Reticulocyte count (RR)
- RDW (normal in thal trait, raised in iron-deficiency, thal intermedia, thal major)
- PBF
- Anisopoikilocytosis (including fragments & tear-drop cells)
- Hypochromia, microcytosis
- Basophilic strippling
- Pappenheimer bodies & Target cells
- Iron status (TRO iron-deficiency anaemia or identify iron overload in thal major)
High performance - Precise quantification of HbA2,HbF with presumptive identification of variant Hb
liquid - Diagnostic for β-Thal in accurate determination of ↑HbA2
chromatography - HbA2 (4-9%) in heterozygosity or severe β-Thal
(HPLC) - HbA2 (3.6-4.2%) in mild β-Thal
- Correction required for HbA2 to quantify Hb subtypes (falsely lowed by iron
deficiency)
Hb Electrophoresis - Screening for abnormal Hb
- Increaed HbF (α2γ2) & HbA2 (α2δ2>4%)
- Markedly low HbA (α2β2)
- H inclusion test for α-Thal
DNA analysis - Confirmatory test by identify globin chain synthesis & structural analysis
- Diagnostic test for α-Thal
- Required when unable to confirm haemoglobinopathy by haematological tests
- Genetic counseling & prenatal diagnosis
Management:
- Algorithm for management of transfusion-dependent thalassaemia patients (CPG 2009) involves:
- Family cascade screening, Genetic counseling, Dietary advice
- Blood transfusion therapy
- Iron chelation therapy
- Monitor for complications
- Transfusion-related complications (HepB, HepC, HIV)
- Iron overload (serum ferritin, liver iron concentration, cardiac T2)
- Target-organ damage (cardiac, endocrine, hypersplenism, infections)
- Consider stem cell transplantation (when has unaffected siblings)
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1) Blood transfusion therapy
- Aim: suppress extramedullary haemopoiesis while minimising complications from transfusion
and maintaining normal well-being
β-Thalassaemia Major
- Indications:
- After completing blood investigations for confirmation of diagnosis
- Hb <7 g/dL on 2 occasions > 2 weeks apart (in absence other factors eg. infection)
- Hb >7 g/dL in β-Thal major/severe forms of HbE-β Thal if impaired growth, para-spinal
masses, severe bone changes, hepatosplenomegaly
- Transfusion targets:
- Maintain pre-transfusion Hb level at 9 -10 g/dl
- Aim to keep mean post-transfusion Hb at 13.5-15.5g/dl
- Aim to keep mean Hb 12 - 12.5 g/dl
- Not advisable to raise the post-transfusion Hb above 15.5g/dL
- High-transfusion regime (never allow to fall <10g/dL)
- Above targets allow for normal physical activity and growth, abolishes chronic hypoxaemia,
reduce compensatory marrow hyperplasia which causes irreversible facial bone changes and
para-spinal masses
- Transfusion interval:
- Usually 4 weekly interval (usual rate of Hb decline is at 1g/dl/week)
- Interval varies from individual patients (range: 2-6 weekly)
- Transfusion volume:
- Volume: 15-20mls/kg (maximum) packed red cells (PRBC)
- Round-up to the nearest pint of cross-matched blood provided
- If calculated volume is just >1 pint of blood, give 1 pint
- If calculated volume is just < 2 pints, give 2 pints
- This strategy minimizes the number of exposure to immunologically different units of blood
product and avoid wastage of donated blood
Note:
- In the presence of cardiac failure or Hb < 5g/dl, use lower volume PRBC (< 5ml/kg) at slow infusion
rate over >4 hours with IV Frusemide 1 mg/kg (20 mg maximum dose)
- It is recommended for patients to use leucodepleted (pre-storage, post storage or bedside leucocyte
filters to prevent non-haemolytic febrile reachtion by removing WBC) PRBC < 2 weeks old
- Leucodepletion would minimize non-haemolytic febrile reactions and alloimmunization by removing
white cells contaminating PRBC
β-Thalassaemia Intermedia
- Clinical diagnosis where patients present later with less severe anaemia at > 2 years of age
usually with Hb 8g/dl or more
- Severity varies from being symptomatic at presentation to being asymptomatic until later
adult life. If they require regular transfusion, follow β-Thal major transfusion regime
α-Thalassaemia (Hb H disease)
- Transfuse only if Hb persistently < 7g/dl or symptomatic
When Hb is kept in normal range by blood transfusion, there is neither bone expansion nor anaemia or
extra iron absorption, the only problem is iron overload. As child grows, more blood & shorter interval
should be given. High transfusion starts with 30% more than low transfusion, in which patient have to
increase amount of blood later due to marrow expension & hypersplenism.
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Expected Hb rise with Hct levels:
Senario 1: Patient 20kg, 360mls transfusion every 4 weeks, average Hct 60%
1) Annual blood requirement = 13 transfusion x 360ml/20kg = 234 ml/kg/year
2) Annual pure RBC requirement = 234 x 60% = 140.4 ml/kg/year
3) Annual transfusional iron loading = 140.4 x 1.08 = 152 mg/kg iron
* Usual Hct level of Malaysian packed red cell ranges from 50-75%
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2) Iron Chelation Therapy
- In most normal adults there are ~4g of iron in the body (3 g in RBC; 1g in liver storage). GIT
absorbs only ~10% in total daily diet; there is no natural way of getting rid of iron once it is in
the body, but a small amount excreted every day via skin & gut.
- This is essential to prevent iron overload in transfusion dependent thalassaemia.
- Compliance to optimal treatment is directly related to superior survival outcome, now possible
beyond the 6th decade.
- Currently 3 approved iron chelators are available:
- Desferrioxamine (DFO) - subcutaneous
- Deferiprone (DFP) - oral
- Deferasirox (DFX) - oral
i) Desferrioxamine (Desferal®)
MOA:
- It picks up iron from cells & brings it out in urine & stool & prevents the iron that is stored in
body from interfering with its normal function
- Serum ferritin level is best guide for whether the treatment is working or not
When to start?
- Usually when the child is >2-3 years old when serum ferritin reaches 1000 µg/L
- This usually occurs after 10-20 blood transfusions (250 mL pack rbc/ 1 unit of blood = contain
0.2g iron)
- In early stage, extra iron is stored in the liver (max 20g), when the storage is full, then iron is
accumulated in other organs, damaging the organs.
* Normal serum ferritin level = 100-400 μg/L
Dosage and route:
- Average daily dose is 20-40mg/kg/day, by subcutaneous (sc) continuous infusion using a
portable pump over 8-10 hours daily, 5 - 7 nights a week
- Aim to maintain serum ferritin level below 1000 μg/L
- Vitamin C augments iron excretion with Desferal
- Severely iron loaded patients require longer or continuous SC or IV infusion (via Portacath)
Complications of Desferal:
Local skin reactions - Usually due to inadequately diluted Desferal or infection
- Redness, swelling, hard tender lump
Yersinia infection - Present with fever, abdominal pain & diarrhea
- Stop desferal and treat with cotrimoxazole
Severe allergy - Rare
Desferal toxicity - High doses >50 mg/kg/day in the presence of low serum ferritin in
children
Ocular toxicity - Reduced vision, visual field and night blindness
- Reversible when Desferal is discontinued
Auditory toxicity - High tone deafness, usually irreversible
Growth retardation - Vertebral growth retardation
Skeletal lesions - Pseudo rickets, metaphyseal changes
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Complications of chronic iron overload in Thalassaemics over 10 years:
Endocrine - Growth retardation
- Impaired glucose tolerance (DM)
- Pubertal delay
- Hypothyroidism
- Hypoparathyroidism
Cardiac - Arrhythmias
- Pericarditis
- Cardiac failure
Hepatic - Liver cirrhosis (especially if with Hepatitis B/C infection)
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3) Monitoring of Patients
Monitoring Assessment & Investigations
Blood transfusion - Screening for HbsAg, Anti-HCV, Anti-HIV 6 monthly
- During each admission for blood transfusion, following should be done:
- Pre-transfusion Hb, platelet count and WBC (if on Deferiprone).
- Post transfusion Hb-1⁄2 hour post transfusion.
- Calculate the volume of pure RBC transfused based on the haematocrit
(HCT) of PRBC given (usually HCT of PRBC from blood bank is >50-55%)
- Volume of pure RBC transfused = volume of blood given x HCT of PRBC
given (eg. 600 mls x 0.55 = 330 mls)
- Annual volume of pure RBC transfused per kg body weight
- Iron balance assessment.
Growth - Weight, Height & physical examination (liver, spleen size) 3-6 monthly
Medication - Review of current medications
Iron overload - Serum ferritin 3 monthly
Cardiac assessment - Annual ECG or Holter monitoring for arrhythmias
(>10 years old) - Annual cardiac echocardiography
- Cardiac T2* MRI (1-2 yearly)
- LIC MRI 102 yearly
Drug toxicity
- Desferrioxamine - Auditory/ ophthalmology annually
- Deferiprone - FBC weekly, ALT 3 monthly
- Deferasirox - RP, urine protein monthly, ALT monthly, Auditory/opthalmo annually
Growth failure - Test for DM, hypothyroidism, delyed puberty, zinc deficiency, bone
(Evaluate growth & disorders, DFO toxicity
development) - Bone age assessment
- GH stimulation tests (in referral centre)
Delayed puberty, short - Tanner staging 6 monthly
stature & hypogonadim - LH, FSH, oestradiol or testosterone
- Pelvic USS (for girls)
- GnRH stimulation test if necessary
Hypothyroidism - Free T4 and TSH
DM - Fasting plasma glucose or OGTT
Liver iron assessment - Liver T2* MRI for non-invasive assessment of liver iron
- Liver biopsy for liver iron concentration and the assessment of hepatitis,
fibrosis or cirrhosis in selected cases and prior to bone marrow
transplantation
Osteoporosis/osteopenia - Serum calcium, phosphate, ALP
- 25-OH VitD
- Serum zinc
- Spinal radiograph (AP & lateral view)
- DEXA scan
Hypoparathyroidism - Serum calcium, phosphate, ALP
- Serum magnesium
- PTH
Hypoadrenalism - Baseline cortisol at 8-9am
- ACTH stimulation test
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4) Splenectomy
- Indications:
- Blood consumption volume of pure RBC > 1.5X normal or >200-220 mls/kg/year in those
>5 years of age to maintain average haemoglobin levels
- Evidence of hypersplenism
- Massive splenomegaly (risk of splenic rupture)
- Give pneumococcal and HiB vaccinations* 4-6 weeks prior to splenectomy
- Meningococcal vaccine required in endemic areas
- Penicillin prophylaxis for life after splenectomy.
- Low dose aspirin (75 mg daily) if thrombocytosis >800,000/mm3 after splenectomy (platelets
in blood usually high after splenectomy)
- Thromboembolic phenomenon is more common in patients with Thal intermedia, thus short-
term anti-thrombotic prophylaxis should be considered during risk periods
* Revaccination of HiB may be required after 5 years
7) Antenatal diagnosis
- Can be done by chorionic villous sampling at 9-11 weeks period of gestation.
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8) Patient and parents support groups
- Various states and local Thalassaemia Societies are available nationwide
- Provide support and education for families
- Organises fund raising activities and awareness campaigns
- Health professionals are welcomed to participate.
B) α-Thalassaemia
Epidemiology:
- Common in Asian population
Pathology:
- There are 4 α-globin genes coded by chromosome 16
- Reduced synthesis of α globin chains of Human Hb
- Clinical manifestations depend on the number of functional genes
Types of α-Thal:
Thal minor - α-thal 1-2 α globin genes deleted
(trait/carrier) - α-thal 2-1 α globin genes deleted
- Asymptomatic/ incidental finding
- Absent OR mild hypochromic microcytic anemia
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Thalassaemia Long Case (Template):
A. History
General profile
(Age, Gender, Ethnicity - HbE more likely in Malays & Chinese)
Presenting complaints (Reason for admission, consider)
- Visit to drug therapy centre for regular blood transfusion
- Admission for elective surgery (eg. splenectomy, cholecystectomy)
- Symptoms of complications (cardiomyopathy, CCF, DM, worsening anaemia, jaundice)
- May also be causes not directly related to thalassaemia
HOPI - Bring past-medical history of Thalassaemia under this section (unless presenting complaint not
related to Thalssaemia)
Diagnosis of - Age of diagnosis (antenatal/infantile/childhood)
Thalassaemia - Initial presentation (increasing pallor, FTT, jaundice, ↓ET, LOA, syncope)
- Where it was diagnosed, investigations done
- Ellicit most probable type of Thalassaemia
- β-Thal major (6-12 months)
- β-Thal intermedia/HbE (late >2 years old)
Treatment History
- Ask about age of first transfusion
- Age when chelation therapy started
- How often are transfusion needed per year (Quantify)
- Other medications (eg. Folate, VitC, B-complex, Thyroxine-short stature, Penicillin-post-splenectomy)
- Drug allergy
- Hospitalisations (other than PCT) & reasons
- Previous surgery (eg. splenectomy, cholecystectomy)
A) Blood transfusion - Blood group
- Frequency & volume (pints)
`Hb from previous transfusion range from __ to __`
- Pre & Post-transfusion Hb (maintain adequare transfusion to prevent
extramedullary erythropoiesis)
- Pre-transfusion: 9.5-11.5 g/dL
- Post-transfusion: 13.5-15.5 g/dL
`My patient was active before & after transfusion, no complications noted`
- When started? Why? When Hb <8g/dL for 2 weeks? Severe anaemia?
- Infective screening (HepB,C,HIV) every 6 months until now (-ve/+ve)
- Current serum ferritin level (normal 100-400 ng/ml)
- Control:
- Symptoms & progression of anaemia few weeks before transfusion?
- Need for any unscheduled transfusion?
- Is growth appropriate to chart?
- Symptoms of extramedullary erythropoiesis? Increasing size of mass in
abdomen?
- Complications from blood transfusion:
- Mild: Rash, itchy, ulticaria (Tx: hydrocortisone)
- Severe: Hypotension, anaphylactic shock, bronchospasm
- Complications from iron overload:
- Cardiac siderosis (CCF, cardiomyopathy) – echo yearly
- Endocrine
- Pancreas (DM) - HOPI can be elective admission for insulin therapy
- Hypogonadism (amenorrhoea,↓pubertal staging, absence pubic hair)
- Hypothyroidism (less active)
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- Short stature (GH insufficiency)
- Osteoporosis
- Liver (chronic liver disease)
B) Iron chelation cherapy - Started when serum ferritin level >1000 ng/ml after __ no. of transfusion
- Types: Desferal, Deferiprone (>5 years old), Deferasirox (2-3 years old)
- On monotherapy? If desferal, who inject the drug? Use of infusion pump?
- After chelation, target ferritin level achieved? Below 1000ng/ml?
- Vit C given? Dosage? To augment iron excretion from stool
- Compliance:
- How many bottle of infusion needed?
- Any missed day in a week/month?
- Calculate percentage of compliance per month: x/30 x 100%
- For Desferal, 20-60mg/kg/day (max 50), 8-10 hours daily, 5-7 nights/week
- Complications:
- Local skin infections (redness, swelling, pain)
- Yersinia infection (abdominal pain, fever, diarrhoea) - on antibiotics?
- Severe allergy
- Desferal toxicity (>50mg/kg/day)
- Ocular toxicity (reduced vision, night blindness)
- Auditory toxicity (high tone deafness)
- Growth retardation
- Skeletal lesions (pseudorickets, metaphyseal changes, fracture)
C) Splenectomy - When was started? >5 years old
- Why?
- Hypersplenism (pancytopenia with pooling of blood)
- ↑ splenomegaly (risk of rupture when spleen fails)
- Pre-vaccination (>2 weeks; 4-6) before surgery
- Meningococcal, Pneumococcal, Hib (If given <5 yrs old ↑ infection risk)
- Post-surgery
- Lifelong penicillin (↓streptococcal infection)
- Low dose aspirin (antiplatelet): prevent thrombosis (thrombocytosis
after splenectomy)
- Complications:
- Requires ICU monitoring (infections), discharge after how many day?
Past-Medical & Surgical History
Past-Medical - Other than associated conditions of thalassaemia
Past-Surgical - Splenectomy
Drug History
Drugs - Any supplementation (folic acid?)
- Drug allergy
Family History
Parent - Parent genetic status, do they know they are carriers? Consanguinity?
- Genetic counseling done before?
- Draw family tree
Siblings - Any affected? If yes, on any treatment? Severity?
- If not affected, possibility of stem cell transplant?
Paediatrics History
Birth history - Neonatal anaemia? IUGR? G6PD deficiency?
Immunisation history - Completed immunisation?
Developmental history - Any developmental delay?
- Abnormal pubertal staging
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Dietary - Any restricted diet (less intake of iron, red meat, peanut butter, curry
powder, use of iron pan)
- Food allergy
Social History
Disease impact on the - Schooling (which stream, level), Academic performance (rank, best
child subject), Amount of school missed, Behaviour, conduct, Able to take part
in physical class/sports?
- Body image, pubertal anxieties (in teens)
- Psychosocial (depression, low self-esteem & relationship)
Disease impact on the - Occupation of caretakers
family - Financial considerations (cost of Desferal+pump) expensive
- Social support group available
Summary
In summary, my patient is a (age/race/gender) who has (β-Thal major/HbE β-Thal/HbH), who is
- Transfusion-dependent
- Clinically thalassaemia major/intermedia
- Ongoing problems/issues include _____ & reason for hospitalisation is ______.
- Complications (without evidence of iron overload)
B. Physical Examination
General inspection:
- Bronze-skin
- Short stature
- Attached PCT, oxygen, IV lines (infusion of medication)
- Thalassaemic facies (frontal bossing, maxillary overgrowth, malar eminence)
- Pallor (conjunctival, nailbed, palmar crease)
- Jaundice (scleral jaundice, generally appear jaundice)
Abdomen:
- Desferal scars (pigmented, round, no lipodystrophy)
- Surgical scars (open/laparoscopy)
- Hepatomegaly +/- Splenomegaly
Chest:
- Apex beat displaced?
- Flow murmur?
- Signs of CCF?
Others:
- Signs of CLD
- Signs of hypothyroidism (dry,scaly hair, hyporeflexia etc)
- Screen visual acuity
- Tanner staging (if parent allows)
C. Discussion
- Refer previous pages for detailed investigation and management in Thalassaemia.
- Mainstay of management should include blood transfusion, iron chelation therapy, splenectomy (if
hypersplenism), genetic counseling & screening, dietary advices and management for complications.
Bone marrow transplant should depend on patient`s siblings.
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Haemostasis
Clinical features:
History Most likely aetiology
(overlap considerable)
- Easy bruising (ecchymoses) Coagulation defects, platelet or
vascular
- Petechiae (skin & mucous membranes)
- Mucosal bleeding:
- Gum bleeding
- Epistaxis Platelet disorders
- Haematuria
- Menorrhagia
- Internal bleeding (GIT, intracranial, intramuscular)
- Bleeding into joints (haemarthroses) with minor injuries
- Bleeding into muscles Coagulation defects
- Excessive bleeding after trauma (eg. surgery, dental
extractions)
Examination
- Skin (Petechiae: ~1-2mm spots; Purpura: <1cm, varying shape & Ecchymoses: >1cm, varying shape)
- Mucous membrane (Palatal petechiae, gum bleeding)
- Assymetrical joint deformities (due to haemarthroses)
APTT
(Heparin)
PT/INR
(Warfarin,
liver damage)
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Investigation of clotting disorders:
Test Mechanism Abnormal in DIC
FBC & PBF Platelet morphology & count
Bleeding time Abnormalities of other blood cells, Prolonged in
measures platelet plug formation in vitro thrombocytopenia, platelet
function disorders & von
Willebrand disease
Prothrombin time (PT) Measures factors VII, X, V, prothrombin & Prolonged in liver disease,
fibronogen (extrinsic & common vitamin K dependent clotting
pathyways) (INR=1) factors; Used to monitor
Normal=10-14s warfarin therapy
Activated partial Measure factos V, VIII, IX, X, XI, XII, Used to monitor heparin
thromboplastin time prothrombin & fibrinogen (intrinsic & therapy
(APTT) common pathways)
Normal=30-40s
Thrombin clotting time Normal=14-16s Abnormal in fibrinogen
(TT) deficiency or thrombin
inhibition
Coagulation factors Specific assays of individual clotting Clotting factor deficiencies (eg.
factors haemophilia)
Abnormal in DIC
Fibrinolysis tests Detection of fibrinogen or fribrin Decrease in enhanced
degradation products (FDPs), fibrinolysis
Plasminogen & plasminogen activator
raised
A) Disorders of Vasculature
- Clinical features are generally mild, with skin & mucous membrane bleeding (bruising,
petechiae). All screening tests are normal including the bleeding time.
- Aetiology:
Inherited - Ehlers-Danlos syndrome
- Hereditary haemorrhagic telangectasia
- Marfan`s syndrome
Acquired - Easy bruising syndrome
- Vasculitis (eg. Henoch-Schonlein purpura (HSP))
- Infection (eg. meningitis)
- Vitamin C deficiency (scurvy)
- Drugs (eg. steroids)
B) Platelet disorders
- Include thrombocytopenia & platelet dysfunction
1) Thrombocytopenia (when platelet count <150 x 109/L)
Classification Platelet count x 109/L Risk
Severe <20 Risk of spontaneous bleed
Moderate 20-50 Risk of excess bleed during operation or trauma
Low risk of spontaneous bleed
Mild 50-150 Low risk of bleed during operation or trauma
- Clinical features: Bruising, Petechiae/ecchymoses, Purpura, Mucosal bleeding (epistaxis, gum),
GIT bleeding, Haematuria, Intracranial haemorrhage)
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- Aetiology:
1) Increased platelet consumption/destruction
Immune - ITP
- SLE
- Alloimmune neonatal thrombocytopenia
Non-immune - Haemolytic Uraemic Syndrome (HUS)
- Thrombotic Thrombocytopenic Purpura (TTP)
- DIVC
- Congenital heart disease
- Giant haemangioma (Kasabach-Merritt syndrome)
- Hypersplenism (liver disease, haemolytic disease)
2) Decreased platelet production
Congenital - Fanconi`s anaemia
- Wiskott-Aldrich syndrome
- Bernard-Soulier syndrome
- Thrombocytopenia with absent radius (TAR syndrome)
Acquired - Aplastic anaemia (cytotoxic drugs)
- Leukaemia, Lymphoma
- Dengue, HIV
- Drug-induced (penicillin, heparin)
- Radiation
2) Platelet Dysfunction
- Platelet count is normal but bleeding time is prolonged & specific platelet function tests are
abnormal. They may be inherited or acquired.
- Aetiology:
Congenital - Glanzmann`s thromboasthenia (rare)
Acquired - Drugs
- Aspirin (Inhibition of cyclo-oxygenase)
- Heparin (Platelet segregation & secretion inhibited)
- Myeloproliferative disease
- Uraemia
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- In haemophilia, APTT is prolonged in moderate and severe haemophilia but may not show
prolongation in mild haemophilia. PLT & PT are normal. When APTT is prolonged, proceed to do
FVIII antigen level. If this is normal, only then proceed to assay the Factor IX level. Once the level
has been measured, then the haemophilia can be classified as below.
Classification of haemophilia and clinical presentation
Factor level Classification Clinical presentation
<1 % Severe Spontaneous bleeding, risk of intracranial haemorrhage
1-5 % Moderate Bleeding may only occur with trauma, surgery or dental
5-25 % Mild procedures
- Further Investigations
- HbsAg, anti-HBS, anti-HCV, HIV serology
- RP, LFT, Platelet aggregation (if high suspicion of platelet defect)
- Diagnosis of carrier status for genetic counseling
- Mother of a newly diagnosed son with haemophilia
- Female siblings of boys with haemophilia
- Daughter of a man with haemophilia
- Once a child is diagnosed to have haemophilia, check the viral status at diagnosis & then
yearly. This is because treatment carries the risk of acquiring viruses. All haemophiliacs should
be immunized against Hepatitis B.
- Treatment
- Treatment of severe haemophilia should be prophylactic to prevent arthropathy & ensure
best quality of life possible. Dosage of prophylaxis is usually 25-35 U/kg of FVIII concentrate,
given every other day or 3x/week. For FIX, the dosage is 40-60 U/kg, given every 2-3 days.
However, this form of management is costly & requires central venous access.
- On demand treatment is another option for inadequate clotting factors are. It consists of
replacing the missing factor: FVIII con-centrates (Haemophilia A), FIX concentrates
(Haemophilia B). FFP & cryoprecipitate ideally SHOULD NOT be used (high risk of viral
transmission). Dose of factor replacement depends on the type & severity of bleed.
- Dose of factor required can also be calculated using the formulas below
- Units of FVIII: (% rise required) x (weight in kg) x 0.5
- Units of FIX: (% rise required) x (weight in kg) x 1.4
- Percentage of factor aimed for depends on the type of bleed
- For haemarthroses, 30-40 % is adequate
- For soft tissue or muscle bleed aim for 40- 50 % level.
(there is potential to track and cause compression/compartment syndrome)
- For intracranial bleeds or patients going for surgery, aim for 100%
- Infuse FVIII by slow IV push at a rate not exceeding 100 units/min in young children
- FVIII is given every 8-12 hours. Factor IX is given every 12 - 24 hours.
- Duration of treatment depends on type of bleed:
- Haemarthroses 2-3 days
- Soft tissue bleeds 4-5 days
- Intracranial bleeds or surgery 7-10 days.
- Veins must be handled with care. Never perform cut-down unless in an emergency
as it destroys the vein.
287
- Complications:
- Joint destruction
Recurrent haemarthroses into same joint will destroy the joint causing osteoarthritis &
deformity, this can be prevented by prompt & adequate factor replacement
- Acquisition of viruses (Hepatitis B, C or HIV)
Immunisation and regular screening recommended.
- Inhibitors:
These are antibodies directed against the exogenous factor VIII or IX neutralizing the clotting
activity. Can develop at any age but usually after 10-20 exposure days. Suspected when there
is lack of response to replacement therapy despite high doses. Treatment requires `bypassing`
the deficient clotting factor. Currently 2 agents are available - Recombinant activated FVII
(rfVIIa or Novoseven) & FEIBA. Immune tolerance induction is also another option.
Haemophilia A & B:
288
- Management:
- FVIII concentrate infusions containing vWF (severe)
- DDAVP & fibrinogen inhibitors (milder)
- Management:
- Treat underlying cause
- Supportive therapy on ICU (blood, FFP, fibrinogen, PLTs)
- Protein C concentrates given in meningococcal sepsis DIC
Haemostasis Test:
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Autoimmune Thrombocytopenic Purpura (AITP)
Epidemiology:
- Commonest cause of thrombocytopenia in childhood
- Usually affects children aged 2-10 years old
Aetiology:
Acute AITP Chronic AITP
- Post viral infection - Usually idiopathic
- Usually presents after 1-2 weeks after a - Associated with autoimmune disorders
viral infection - SLE
- Thyroid disease
- Chronic lymphatic leukemia
- Viral infections (e.g. HIV)
- Drugs (e.g. that cause AHA)
*AHA = autoimmune haemolytic anaemia (e.g. quinine, penicillin, methyldopa)
Pathogenesis:
- Thrombocytopenia results from an immune-mediated destruction of circulating platelets (due
to anti-platelet autoantibody) within the reticuloendothelial system (especially spleen)
- ↓platelet counts accompanied by a compensatory↑megakaryocytes (platelet precursors) in
bone marrow
Classification:
Acute AITP Chronic AITP
- 1 or 2 weeks of duration - >6 months duration
- Usually occurs in children - Usually occurs in adults/teenagers
- Male: Female = 1: 1 - Male: Female = 1: 3
- History of viral infection - Usually no history of viral infection
- Rapid onset of purpura - Associated with autoantibodies (60-70%)
- Self-limiting illness (95%) & only 5%
becomes chronic
Clinical features
Symptoms Signs
- History of fever (post viral infection) - Petechiae & purpura
- Bleeding tendencies, easy bruising - Superficial bruising (ecchymoses)
- Mucosal bleeding (e.g. gum bleeding) - No hepatosplenomegaly
- Epistaxis, PR bleed, haematemesis, - No lymphadenopathy
- Haematuria - Intracranial bleeding (rare; 0.1-0.5%)
- Menorrhagia (after puberty) - Positive tourniquet test (Hess test)
*Spontaneous bleeding usually occurs when platelet counts <20 x 109/L
290
Investigations:
- Diagnosis is principally based on on the history, physical examination, full blood count &
examination of peripheral smear
- Diagnosis by exclusion (should exclude other causes of thrombocytopenia)
Blood - FBC
- Normal Hb & WBC
- ONLY thrombocytopenia (<150 x 109/L or <100 x 109/L)
- But look for other associated blood parameters disorders (e.g. pancytopenia)
- FBP
-↓amount and ↑size of platelet
- Prolonged bleeding time (normal:≤11 mins, not practised nowadays)
Biopsy - Bone marrow aspiration (controversial)
- Threshold for performing a bone marrow aspiration must be low
- Indicated if there is:
- Presence of atypical features e.g. organomegaly, significant lymphadenopathy,
abnormal blood counts or suspicious peripheral blood picture
- Before starting steroid therapy (to avoid partially inducing an undiagnosed
acute leukemia)
- Not responding to IV Ig therapy
- Persistent thrombocytopenia beyond 6 months
- Thrombocytopenia recurs after initial respond to treatment
*Others tests maybe indicated when there is atypical presentation from the history, physical
examination, FBC or PBF (eg. Antinuclear factor, Coomb`s test, ultrasound of abdomen, HIV testing)
Management:
- Not all children with diagnosis of acute ITP need hospitalization (80% is acute, benign, self-
limiting)
- Hospitalization is indicated if:
- Severe life-threatening bleeding (e.g. ICH) regardless of platelet count
- Platelet count <20,000 with evidence of bleeding
- Platelet count <20.000 without bleeding but inaccessible to health care
- Parents request for admission
- Most of childhood ITP remit spontaneously with 70% achieves platelet count >50,000 by the
end of 3rd week
- Careful observation and monitoring platelet count without specific treatment is appropriate for
patients with
- Platelet count >20,000 without bleeding
- Platelet count >30,000 with only cutaneous purpura
- Treatment is indicated if there is:
- Life threatening bleeding episode (e.g. ICH) regardless of platelet count
- Platelet count <20,000 with mucosal bleeding
- Platelet count <10,000 with any bleeding
- Choice of treatment
- Oral prednisolone 4mg/kg/day for 7 days, then taper and discontinue at 21 days
- IV Methylprednisolone 30mg/kg/day for 3 days
- IV Immunoglobulin 0.8g/kg/dose for 1 day or 250mg/kg for 2 days
- IV Anti-Rh(D) Ig (50-75mg/kg) in Rhesus positive patients → may cause haemolytic anemia
- All are effective in raising platelet count quicker compared to no treatment with IVIG quickest
291
- However no direct evidence indicates that any of these treatments reduce bleeding
complications or mortality from ITP. No influence on progression to chronic ITP.
- Side effects of IVIG is common (15-75% incidence) and include fever, flushing, headache,
nausea, aseptic meningitis and transmission of Hepatic C (older preparation).
- Steroids should not be continued, however, if there is no response or if there is a rapid relapse
after withdrawal. The considerable risks of long term side effects in a growing child outweigh
benefits of either too frequent high dose pulses or any attempt to titrate the platelet count
against a regular lower steroid dose.
- Platelet transfusion are reserved for life threatening haemorrhage (↑platelet only for few
hours)
- Treatment should not be directed at increasing platelet count above a preset level but rather
on the clinical status of the patient.
Chronic ITP
- Persistent thrombocytopenia after 6 months of onset (20%)
- Wide spectrum of manifestations varying from mild symptomless low platelet counts through
intermittent relapsing symptomatic thrombocytopenia to the rare stubborn and persistent
symptomatic and haemorrhagic disease
- Management
- Every opportunity should be given for disease to remit spontaneously as the majority will do
so if given enough time
- Revisit the diagnosis to exclude other causes of thrombocytopenia (Immunodeficiency,
lymphoproliferative or collagen disorders or HIV infection).
- Asymptomatic children can be left without therapy and kept under observation.
- Symptomatic children may need short course of treatment to tide them over the relapse
which include:
- Intermittent pulses of IVIg
- Intermittent anti-Rh(D) antibody treatment for those with Rhesus D positive
- Intermittent pulses of steroid
- Care must be taken with any pulse of steroid strategy to avoid treatment-related steroid side
effects. Aware of immunosuppression eg. risk of severe varicella
- No justification for long term continuous steroids
- Splenectomy is indicated when:
- Persistence of disease after 12 months with
- Bleeding symptoms and
- Platelet count <10,000/µL to 30,000/µL (ages 8-12 years)
- No response or only transient success with intermittent IVIg, anti-D or pulse steroids
- No contra-indications to surgery. Operative mortality <1%
- Over 70% rate of complete remission post splenectomy
- Pre-splenectomy immunization against pneumococci, haemophilus influenza type b and
meningococci infection mandatory 2 weeks before surgery
- Post-splenectomy penicillin prophylaxis
- Post-splenectomy failure or relapse, consider: danazol, vincristine, azathioprine,
cyclophosphamide, alpha-interferon, stahphylococcal protein A immunoadsorption,
cyclosporine, cholchicine or dapsone.
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Henoch-Scholein Purpura (HSP)
Epidemiology:
- Usually occurs at age between 3-10 years old
- Twice as common in boys
- Peak during the winter months
Pathophysiology:
- Aetiology of HSP is unknown.
- Postulations:
Genetic predisposition & Antigen exposure
- Increase circulating IgA levels and disruption
in IgG synthesis
- IgA & IgG interact to produce complexes that
activate complement
- Deposited in affected organ
- Precipitate inflammatory response with vasculitis
*HSP and IgA nephropathy are related disorders. Both illnesses have elevated serum IgA levels and
identical findings on renal biopsy
Clinical Features:
Symptoms Signs
- Preceded by URTI - Characteristic rash (1 clinical features in
st
Complications:
Abdomen Others
- Intussusception (intramural haematoma) - Hypertension
- Ileus - CNS involvement
- Protein-losing enteropathy
- Nephrotic/nephritis syndrome
- Deteriorating renal function
- Orchitis
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Diagnosis:
- Clinical diagnosis and not based on laboratory evaluation
Investigations:
- Routine laboratory test results are usually within reference ranges.
- Some laboratory studies TRO other diagnoses and in evaluating renal function
- Urinalysis: Hematuria/ proteinuria are present in 10-20% of patients
- Platelet count and coagulation studies:
- Platelet count is usually in the reference range but may be elevated; the platelet count
should not be low in HSP. A normal platelet count rules out idiopathic thrombocytopenic
purpura (ITP). A normal platelet count and normal coagulation studies (eg., PT, aPTT, FDP)
rule out thrombotic thrombocytopenic purpura (TTP).
- Lipase: A normal lipase level makes acute pancreatitis very unlikely.
- FBC and differential: WBC count may be in the reference range or elevated. Eosinophilia is
sometimes present.
- Erythrocyte sedimentation rate: Sedimentation rate may be in the reference range/ elevated.
- BUN and creatinine levels: May be elevated from renal involvement of HSP/ from dehydration.
- Abdominal ultrasound may be better than barium enema to diagnose intussusception.
- IgA level (elevated in >50%)
Management:
- Very limited data are available on the treatment of Henoch-Schonlein purpura. Fortunately,
most patients recover quickly in several weeks without treatment.
- Treat any suspected infection
- Supportive therapy for rash, arthalgia, fever & malaise
- For renal disease:
- Standard treatment of nephritic or nephrotic syndrome (see below)
- Renal biopsy (if severe hypertension or rising creatinine)
- Non-steroidal anti-inflammatory drugs (NSAIDs)
- Helps joint pain and do not seem to worsen the purpura. However, NSAIDs should be used
cautiously in patients with renal insufficiency. Clinicians often use corticosteroids to treat
abdominal pain, subcutaneous edema and nephritis, but few prospective placebo-controlled
studies have demonstrated their effectiveness.
- Prednisolone in a dose of 1 mg/kg/day for 2 weeks and then tapered over 2 more weeks
- Shown to improve gastrointestinal and joint symptoms. Although this regimen did not
decrease the incidence of renal disease, it did lessen the severity of nephritis in some patients.
Other treatment regimen have included IV or oral steroids with or without any of the
following: azathioprine, cyclophosphamide, cyclosporine, dipyridamole, plasmapheresis, high
dose IV immunoglobulin G (IVIg), danazol, or fish oil.
Prognosis:
- HSP is generally a benign disease with an excellent prognosis.
- More than 80% of patients have a single isolated episode lasting for a few weeks.
- Approximately 10-20% of patients have recurrences.
- Fewer than 5% of patients develop chronic HSP.
- Abdominal pain resolves spontaneously within 72 hours in most patients.
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Sickle Cell Anaemia
Introduction:
- AR, common sickle cell syndromes include HbSS, HbSC and HbS-β-thal, others are rare variants
- Hb phenotype must be identified as clinical complications differ in frequency, type and severity
- Sickle cell Hb (HbS) is Hbα2βs2, single amino acid substitution (valine for glutamic acid at
codon 6 on β-chain → HbS crystallise and form a gel in deoxygenated state → normally soluble
when reoxygenated (reversible HbS) and able to enter microcirculation
- HbS is insoluble in low oxygen tension → polymerises as long fibers (sickle-shaped) → block
microcirculation → microinfarction → pain and dysfunction
- HbS releases oxygen in tissure more readily than HbA (OxyHb dissociation curve shift to right)
- 2 common clinical conditions:
- Sickle cell anaemia HbSS (homozygous disease, 85-95% HbS, 5-15% HbF, no HbA)
- Sickle cell trait HbSA (carrier, heterozygous disease, 40% HbS, 60% HbA)
295
Sickling crises:
- Most episodes of crises last between 5-7 days
Splenic - Life-threatening, hyperacute ↓Hb 2` to splenic pooling of RBC and sickling
sequestration crisis within spleen (moderate to massive splenomegaly, RR↑), hypovolemic shock
- ↑infection risks from encapsulated organisms
- Transient, continue for 3-4 hours and may last for one day
- Management: Blood transfusion, Prophylactic antibiotics, Vaccination
Vaso-occlusive - Occurs in any organ with clinical symptoms of pain or organ dysfunction (due to
crisis restriction in blood flow → ischaemia → pain & necrosis)
- i) Acute chest syndrome
- Vaso-occlusive crisis within lungs with evidence of new infiltrate on CXR
- Defined by ≥2 of: chest pain, fever, CXR: pulmonary infiltrate/focal abnormality
- 2nd most common complication, 25% of death in sickle cell patients
- Associated with infection and infarction, atelectasis, fat embolism
- Initial complaint of chest pain, develops cough, ↑RR, ↑HR, hypoxia and
progressive respiratory distress in later stage
- PE: ↓breath sounds, dullness on percussion
- Management:
- Early recognition and prevention of arterial hypoxemia
- Oxygen, fluids, analgesics (use wisely), antibiotics, bronchodilators, RBC
transfusion (rarley exchange transfusion)
- Incentive spirometry may help ↓incidence of acute chest crisis presented with
chest or abdominal pain ↓ development of atelectasis
- ii) Pain crisis (most common type of vaso-occlusive event)
- Microvascular painful infarcts of muscle, bone, bone marrow, lung, intestines
- Usually localises to long bones of arms/legs but may occur in smaller bones of
hands or feet in infancy (dactylitis) or in abdomen
- Usually last 2-7 days
- Crises within femur → avascular necrosis of femoral head or chronic hip disease
- Management:
- Fluids, analgesics (usually narcotics & NSAIDS), oxygen if hypoxic
- Priapism can occur in boys (between 6-20 years old)
- Experiences sudden, painful onset of turnescent penis that will not relax
- Management: Administration of oxygen, fluids (due to renal medullary
infarction which results in loss of ability to concentrate urine), analgesia,
transfusion (achieve HbS <30%, often by partial exchange transfusion)
Aplastic crisis - Acute and reversible worsening of patient`s baseline anaemia
- Presented with pallor, tachycardia, fatigue
- Usually triggered by parvovirus B19 infection (invades RBC precursors,
multiplying and destroying RBC, almost complete cessation of RBC production
for 2-3 days)
- Reticulocytopenia, rapid RBC turnover (↓Hb)
- Management: Supportive, blood transfusion (sometimes)
Haemolysis crisis - Acute accelerated ↓Hb (RBC break down at faster rate)
- Common in patient with coexistent G6PD deficiency
- Management: Supportive, blood transfusion (sometimes)
296
B) Sickle trait
- Heterozygote expression of sickle Hb gene eg. HbSA
- HbS makes up 30-40% of Hb, appears partially protect against falciparum malaria
- Usually asymptomatic with no anaemia
- Sickling can occur in severe hypoxia, haematuria is the commonest symptom
- Special care is needed with general anaesthetics and pregnancy
- Diagnosis is made by Sickledex test and Hb electrophoresis
Investigations:
Blood - FBC (Hb 6-8 g/dL usually)
- PBF (sickle cells, target cells, Howell-Jolly bodies)
Sickledex test - Specific test to identify sickle cells (HbS blood will sickle)
Hb electrophoresis/ - To detect relative quantities of HbS, HbF, HbA
Isoelectric focusing/
High-performance
liquid chromatography
Guthrie test - Newborn screening for sickle cell disease at birth
Management:
General - Folic acid 5 mg OD
- Oral penicillin daily (due to autosplenectomy)
- Triple vaccination (Pneumococcal, Hib, meningococcal)
- Regular influenza vaccination
- Avoid precipitating factors
Crises - Admit to hospital
- Check FBC, film, reticulocytes, BUSE, LFT, CRP
- CXR if respiratory symptoms/signs, ECG if chest pain
- MSU and blood cultures if infection suspected
- Strong analgesia (usually IV opiates)
- Fluid (IV, 50% above usual formula)
- Oxygen (by CPAP if necessary eg. sickle chest syndrome)
- Bed rest and keep warm
- Monitor closely (SPO2, PR, BP, RR, pain & nausea)
- IV antibiotics if infectoin present or suspected
- Transfusion if necessary (multiple may be needed)
- Exchange transfusion (↓proportion of sickle cells, indicated in severe painful
crises, neurological damage, sequestration, sickle chest syndrome,
priapism)
Surgery - Transfusions are performed pre-operatively for major surgery to ↓HbS
fraction
to <30%
- Anaesthetic care is taken to keep patient warm, well oxygenated and
hydrated, pain-free and acidosis avoided
New therapies - Bone marrow transplant or Haematopoietic Stem Cell Transplant (for severe
disease, using a haploidentical sibling match, curative)
- Hydroxyurea (↑HbF, ↓frequency of crises as early as 1 year of age)
297
PART IX
ONCOLOGY
Oncology Overview
Cancers in Paediatrics:
- Neuroblastoma
- Nephroblastoma (Wilms tumour)
- Rhabdomyosarcoma
- Bone tumours
- Retinoblastoma
- Germ cell tumours
- Liver tumours (Hepatoblastoma)
- Brain tumours
- Childhood histiocytosis syndrome
- Leukaemia (Refer subsequent chapter) *Most common!
- Lymphoma (Refer subsequent chapter)
A) Neuroblastoma
- Tumour arising from neural crest cells of the sympathetic nervous system, may develop in
- Adrenal gland (50%)
- Sympathetic chain (50%): anywhere from cranial fossa to the coccyx)
- Clinical features:
- Usually <5 years old
- Abdominal mass
- Metastatic symptoms (70%): Bone pain, Proptosis, periorbital bruising, massive
hepatosplenomegaly, skin, nodules, lymphadenopathy, weight loss, pallor, malaise
- Investigations:
- Urinary catecholamine metabolites (↑vanillylmandelic acid (VMA) and homovanillic acid (HVA)
- CT/MRI scan
- Meta-iodobenzylguanidine (MIBG) scan: cathecholamine precursor, will outline metastases
- Tissue biopsy (or positive bone marrow): necessary to confirm diagnosis & define molecular
features that determines prognosis & therapy
- Management:
- Treatment depends on child`s age, tumour stage & biology (presence/absence of amplification
of MYCN oncogene)
- Low-risk tumours (managed with surgical resection +/- chemotherapy (Subtype-Stage 4S
resolves without therapy; cure rate >90%)
- High-risk tumours (More aggressive chemotherapy, high-dose chemo with stem cell rescue,
local radiotherapy & differentiation treatment*; cure rate 10-40%) * Use of retinoic acid derivatives
to force cells to diffentiate past a point of development so that they lose capacity to grow quickly/spread)
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B) Nephroblastoma (Wilms tumour)
- Tumour of embryonic renal precursor cells, incidence is 7.8/million
- Clinical features:
- Mean age 3 years, 5% with bilateral disease at presentation
- Abdominal mass (most common presentation), abdominal pain & vomiting
- Hypertension, haematuria
- Associations: genitourinary abnormalities, overgrowth disorders (hemihypertrophy, Beckwith-
Wiedemann syndrome), aniridia, Chr11 short arm deletion involving ½ Wilms gene (eg. W1T)
- Investigations:
- Imaging (Abdominal USS, CT/MRI scan, AXR, CXR-metastasis)
- Urinalysis (haematuria)
- Staging:
I - Completely resected disease of kidney only
II - Disease beyond kidney but completely resected
III - Residual disease post-surgery or nodal involvement
IV - Metastatic disease (usually lung)
- Management: (age-dependent)
- Primary nephrectomy then chemotherapy (USA)
- Initial chemotherapy, nephrectomy (Standard in UK, Europe)
- Radiotherapy used as part of combined strategy for local residual post-surgery & pulmonary
metastatic disease
- Prognosis: (histology, disease stage, tumour size, child`s age)
- Favourable histology (89-98%, 2-year survival)
- Poor histology (17-70%, 4-year survival)
C) Rhabdomyosarcoma
- Tumour of primitive mesenchymal tissue (which striated muscle arises from), may occur
anywhere, but commonest sites are: head & neck, genitourinary tract, extremities
- Clinical features:
Head & neck tumour - Proptosis, Facial swelling
- Nasal obstruction, blood-stained nasal discharge
Genitourinary tract tumour - Urinary tract infection (UTI), Dysuria
- Blood-stained vaginal discharge
- Associations: NF-1, Beckwith-Wiedermann syndrome
- Management: (site, resectability, stage, location, histology, metastases)
- Initial surgical resection then chemotherapy
- If unresectable initially, chemotherapy, second look surgery +/- radiotherapy
- Prognosis: localised standard risk histology disease has 70% 5-year survival
D) Bone tumours
- Incidence: 5.6/million
(whites>blacks, M>F),
- Most commonly
present in adolescent
- Two most common:
- Osteosarcomas
- Ewing sarcoma
299
E) Retinoblastoma
- Tumour arising in the retina. Annual incidence: ~4/million
- May be unilateral (75%) or bilateral (always hereditary)
- AD, incomplete penetrance, hereditary (40%), sporadic (60%)
- Clinical features:
- White pupillary reflex (leucoria): picked up on developmental checks
- Squint (any new squint in child should be investigated, though it is an unusual finding)
- Decreased vision
- Proptosis, raised ICP, orbital pain (advanced disease)
- Management:
- Local therapy (radiotherapy, photocoagulation/cryotherapy)
- Enucleation of eye (if unavoidable)
- Chemotherapy (reduce tumour volume prior to local therapy/if residual/metastatic cancer
- Optimised treatment which minimises radiotherapy to improve visual sparing & reduce
incidence of future secondary tumours
- Prognosis:
- Overall survival is >90%. Poor survival if extensive/metastatic disease. Familial cases have
increased incidence of 2` malignancies (osteosarcoma, soft tissue sarcoma, melanoma)
G) Liver tumours
- Primary:
- Benign (hemangioma)
- Malignant
- Hepatoblastoma
(refer next page)
- HCC
- Secondary/Metastatic:
- Wilms tumours
- Neuroblastoma
300
H) Hepatoblastoma
Introduction:
- Occurs predominantly in children <3 yr of age, median age of diagnosis is 1 yr
- Aetiology unknown, associate with familial adenomatous polyposis (FAP), Beckwith-
Wiedemann syndrome, hemihyperplasia, Gardner syndrome & other somatic overgrowth
syndromes (increased IGF-2 expression 2` to genetic mutations/ epigenetic changes
- All children with Beckwith-Wiedemann syndrome or hemihyperplasia should be routinely
screened with AFP levels & abdominal ultrasounds
- Prematurity & low birthweight is associated with ↑incidence, risk ↑ as birthweight ↓.
Epidemiology:
- Primary hepatic malignancies in children are rare (<2% of all pediatric malignancies)
- Hepatoblastoma accounts for majority of cases (75% of primary liver tumors)
- Approximately 100 new cases of hepatoblastoma are diagnosed each yr in US
- Usually of an advanced stage, yet adjuvant chemotherapy & total hepatectomy with
transplantation provide cure and long-term survival for the majority of patients
- Survival >85% (reported by International Society of Pediatric Oncology)
Pathogenesis:
- Arises from precursors of hepatocytes, histologically classified as whole epithelial type,
containing fetal/embryonal malignant cells (either as a mixed or pure elements)
- Mixed type contains both epithelial & mesenchymal elements
- Histologic classification has a direct correlation with clinical outcome
- Pure fetal subtype predicts a more favorable outcome
- Small cell undifferentiated subtype has normal AFP levels, predicts worse outcome
Clinical features:
- Usually presents as a large, asymptomatic abdominal mass
- Arises from right lobe 3x more often than left, usually unifocal (large, firm mass)
- Fatigue, fever, weight loss, anorexia, vomiting & abdominal pain as the disease progresses
- Rarely, it presents with hemorrhage 2` to trauma/spontaneous rupture
- Metastatic spread most commonly involves regional lymph nodes & lungs
Diagnosis:
Blood - Anaemia
- Thrombocytosis (30%)
Liver biopsy - Biopsy of liver tumour to establish diagnosis
AFP - Used in diagnosis & monitoring of hepatic tumors
- Elevated in almost all hepatoblastomas
LFT - Bilirubin & liver enzymes usually are normal
Hepatitis B & C - Usually negative in hepatoblastoma
screening
Imaging - AXR, USS to characterise the hepatic mass
- USS to differentiate malignant hepatic masses from benign vascular lesions
- CT or MRI to define extent of intrahepatic tumor involvement & potential
for surgical resection
- CT thorax to look for metastatic lesions
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Management:
- Complete resection is the definitive cure
- Max 85% resectability, hepatic regeneration noted within 3-4 months post-surgery
- Treatment is based on surgery & systemic chemotherapy using:
- Cisplatin+ vincristine+5-fluorouracil/doxorubicin
- Liver transplant is a viable option for unresectable hepatoblastoma with good long-term
survival
- Pretransplant medical condition is important predictor of outcome
- Transplant is much more effective as primary surgery than as salvage therapy
- Alternative treatment options currently under investigation include other systemic
chemotherapy agents such as carboplatin, ifosfamide, etoposide, and irinotecan
- Other treatment approaches include transarterial chemoembolization, cryoablation, and
radiofrequency ablation.
Prognosis
- Survival rates >90% in low-stage tumors (with surgery & adjuvant chemotherapy)
- Survival rates is ~60% for unresectable tumour at diagnosis
- Survival rates of ~25% for metastatic disease with complete regression by chemotherapy &
surgical resection of tumour & isolated pulmonary metastatic disease
- Long-term chemotherapy S/E: cardiac toxicity with doxorubicin, renal & ototoxicity with
cisplatin
*Consider continuation of
chemotherapy or living-related liver
transplantation if cadaveric liver
transplant not available in a timely
fashion
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I) Brain tumours
- In children, always primary.
- Divided into supratentorial & posterior fossa
(infratentorial)
- Infant <2 years : Equal frequencies of infra &
supratentorial tumours
- 2-12 years : 2/3 posterios fossa (infratentorial)
- Clinical features:
Signs of raised ICP - Morning headache, drowsiness, vomiting (esp on waking)
- Diplopia, strabismus, papilloedema (late sign)
- Nystagmus (horizontal, vertical or rotatory)
- Bulging fontanelle, macrocephaly
- Behavioral/ personality change
- Head tilting & nuchal rigidity
- Cranial nerve palsies (IV & VI)
Focal neurological signs - Complex partial seizures
- Ataxia (cerebellar tumours)
- Hemiparesis
- Endocrinopathies (eg. diabetes insipidus)
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J) Childhood Histiocytosis Syndrome
- Group of disorders involving proliferation of histiocytic cells in bone marrow of dendritic cell or
monocyte-macrophage systems
- Most are benign proliferations, some malignant. Classified based on histology:
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Leukaemia
Definition:
- Uncontrolled & abnormal hyperproliferative immature WBC, leading to bone
marrow failure & body organ infiltrated OR
- Malignant neoplasm of haemopoetic stem cell characterized by diffuse replacement of bone
marrow with neoplastic cells & leukemic cells infiltrate liver, spleen, lymph node & other tissues
Epidemiology:
- Acute leukemia is the single most common form of malignancy in children
- Incidence rate in west Malaysia ~ 3/4 per 100,000 children below the age of 13 years old
- About 70% of leukemia are ALL & about 18% is non-lymphoblastic leukemia
- CML is relatively rare in childhood
Aetiology:
- Most commonly, the aetiology is unknown
- Genetic factors
- Increased incidence in patients with chromosomal disorders (eg. Down`s syndrome, ataxia
telangiectasia, Wiskott-Aldrich syndrome & identical twins with affected parents)
- Chromosomal abnormalities:
Philadelphia chromosome in CML (95%) & sometimes ALL
- A long arm of chr22 is shortened by reciprocal translocation to long arm of chr9
- Environmental factor
- Chemicals (eg. benzene compounds used in industry)
- Drugs (eg. chemotherapy with chlorambucil & procarbazine)
- Radiation exposure (eg. nuclear generators & Rx for Hodgkin`s disease)
Pathogenesis:
- Clonal proliferation by successive divisions from a single abnormal stem/progenitor cell
- Blast cells fail to differentiate normally (non-functional cell) but are capable to further divide
- Accumulation of these cells results replacement of normal haemopoetic precursor cells of bone
marrow -> Bone marrow failure
- Immature cell with rapid infiltration to the body organ, may result in death
Classification:
- Classified on the basis of:
- Type of cell involved, Maturity of cells
- Either acute or chronic
Acute Leukemia Chronic Leukemia
- Very immature cells (blast cells) - Initially, mature leukocytes
- Rapidly fatal course - Relatively indolent course
- Subdivided into: - Subdivided into:
- Acute myeloid leukemia (AML) - Chronic myeloid leukemia (CML)
- Acute lymphoblastic leukemia (ALL) - Chronic lymphoblastic leukemia (CLL)
- Acute lymphoblastic leukaemia (ALL) (75%): peak incidence age 4 years
Acute myeloid leukaemia (AML) (20%): stable incidence <10 years, increase in adolescence
Chronic myeloid leukaemia (CML) (3%)
Juvenile CML and the myelodysplastic syndromes (2-3%, rare)
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A) Acute Lymphoblastic Leukaemia
- Arises from early cells in the lymphoid series
- Genetic association with Down syndrome, hyperdiploidy, translocation (eg. t(9:22) Philadelphia
chromosome (poor risk)
Classification of ALL:
Clinical Features:
Organ Symptoms or Signs
General - Malaise & anorexia
Bone Marrow - Anemia: pallor, lethargy
- Thrombocytopenia: brusing, petechiae & nose/gum bleed
- Neutropenia: infection, Fever, Mouth ulcer
- Bone or joint pain: Limping)
Reticulo-endothelial system - Hepatosplenomegaly
- Lymphadenopathy
- Superior mediastinal obstruction
Other organ infiltration - CNS: headaches, vomiting, convulsions & nerve palsies
- Testis: Testicular enlargement
- Kidney: Acute renal failure
Investigations:
FBC, PBF - Anaemia (normochromic, normocytic)
- Blasts present (normally only found in bone marrow_
- WCC↓, normal or ↑
- Platelet ↓
CXR - Mediastinal mass (in T-ALL)
CSF - Blasts seen if CSF involvement
Renal function & uric acid - Impaired renal function with raised uric acid (if renal
infiltration or tumour lysis syndrome)
Special classification test - Chromosomal analysis
- Immunocytochemistry, immunophenotyping
- Ig & T-cell receptor gene rearrangement studies
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Management:
Induction of remission - Aim to kill rapidly most tumour cells to enter remission phase
- Combination therapy for 4 weeks, remission rate is 95%
- Multiagents: vincristine, danorubicin, L-asparaginase, steriod (pred/dexa)
Consolidation of - Blocks of intensive chemotherapy to consolidate remission
remission - To bring down tumour burden to very low level
- Improves cure rate BUT high risk for complications (toxicity)
- Multiagents: Ara-c, cyclophosphamide, etoposide
- CNS prophylaxis (crosses BBB), eg. intrathecal chemotherapy (MTX)
(previously used high-dose MTX & CNS radiotherapy but associate with
adverse neuropsychological side effects)
Intensification - 2-3 blocks of intensive multiagent chemotherapy to clear submicroscopic/
minimal residual disease
Maintenance - 2/3 years chemotherapy(outpatient) usually with oral 6-MP, MTX, vincristine
chemotherapy & prednisolone or dexamethasone
- Modest intensity continue over 2 years (girls) or 3 years (boys)
- Co-trimoxazole given throughout regimen to prevent Pneumocytic carinni
infection
Management of Relapse:
- Intensive chemotherapy (and cranial irradiation CNS relapse): high dose chemo +/- total body
irradiation (TBI). BMT may offer best chance of cure
- Relapse usually attacks CNS (polyphagia), testes (painless unilateral swelling), bone marrow
(pancytopenia)
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Remission criteria:
- <5% blasts in the bone marrow OR absence of blast cells in the PBF
- Restoration of normal peripheral blood counts
- Absence of extramedullary involvement
- Child is physically well or normal
Prognostic indicators:
Ph+, 11q23
Clinical features:
Organ Symptoms or Signs
Bone marrow failure - Same as in ALL: WCC may be ↑, ↓ or normal
Others - Gum hypertrophy (esp M4 & M5)
- DIC (M3)
- Chloroma (localised mass of leukaemic cells, eg. skin,
retro-orbital epidural)
- Bone pain (less common than in ALL)
Classifications:
**
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Investigations:
Same as ALL. Bone marrow must contain ≥30% blast cells (blasts may contain Auer rods)
Management:
Induction of - Chemotherapy(eg. danorubicin,cytosine arabinoside,thioguanine/etoposide
remission - >80% achieve remission. If not achieved then BMT is necessary.
Consolidation - Same as induction regimen
- Intrathecal chemo (+/- irradiation) if CNS leukaemia at diagnosis/CNS relapse
Further consolidation - Total 4-5 courses of multiagent chemotherapy (eg. etoposide, cystosine
arabinoside, m-amascrine)
- BMT is usually only considered after relapse of AML in children
Management of Relapse:
- Treated with intensive chemotherapy (and intrathecal chemotherapy & cranial irradiation in
CNS relapse). BMT offers best chance of cure.
- Common site: bone marrow (CNS rarely)
Prognosis:
- Overall cure rate is 60-70%. Cure rates depend on types (highest for M3 AML) & decrease with
increasing age.
Principle of Management:
1) General
- Correction of anaemia & thrombocytopenia by blood & platelet transfusion
- Treat infection with IV antibiotics
- Prevention of acute tumour lysis syndrome (ATLS) by giving adequate hydration & allopurinol
* ATLS resuls from massive release of cellular breakdown products consequent of tumour cell death from effective
treatment, biochemical disturbances: hyperkalemia, hyperuricaemia, hypocalcaemia, hyperphosphataemia.
2) Chemotherapy
- Acts in different ways BUT end-result is inhibit process of cell division
- Not only affect tumour cell but also normal dividing cells:
- Bone marrow suppression: anaemia, thrombocytopenia & neutropenia leads to infection
- Gastrointestinal tract ( mucositis causing mucosal ulceration)
- Germinal epithelium (sterility that may be irreversible)
- Other SE of chemotherapy:
- Loss of hair (alopecia)
- Nausea & vomiting (particularly for cisplastin because its direct action on brainstem CTZ)
- Antiemetics (metoclopramide & domperidone)
- Serotonin 5HT3 antagonists (ondansetron & granisetron)
- May cause cancer, particularly acute leukemia years after Rx
- Given in interval to allow recovery of normal cell function between the cycles & minimize S/E
3) Radiotherapy
- Damages nuclear DNA thus impairs ability of cells to divide
- Complications: (depends on radiosensitivity of normal cell in radiation path)
- Lethargy & anergy (loss of energy)
- Skin damage (erythema & desquamation)
- GIT (nausea, mucosal ulceration & diarrhoea)
- Testes (sterility), Bone marrow (anaemia, leucopenia)
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Clinical Presentation of Leukaemia (Summary):
310
Haemalogical malignancy according to age distribution:
Pre-school (<5 years old) School-aged Adolescence
- Acute lymphoblastic leukaemia - Acute lymphoblastic leukaemia - Acute lymphoblastic leukaemia
(ALL): peak incidence (ALL) (ALL)
- Non-Hodgkin lymphoma - Hodgkin lymphoma
- Neuroblastoma - Brain tumours Malignant bone tumours
- Wilms tumour Soft tissue sarcomas
- Retinoblastoma
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- Tachypnoea, cyanosis or cough (radiation-/chemotherapy-induced pneumonitis, or pulmonary
infection)
Skin:
- Pallor: anaemia from marrow suppression (most agents), or bone marrow relapse of leukaemia (or
development of secondary leukaemia)
- Bruises: thrombocytopenia from marrow suppression (most agents) or (rare) coagulopathy from
L-asparaginase, or bone marrow relapse of leukaemia
- Dermatitis (MTX, 6-MP, 6-TG)
- Hyperpigmentation (chronic GVHD from BMT)
- Desquamation (bleomycin)
- Jaundice (MTX, 6-MP, 6-TG, bleomycin, radiation to liver)
- Pigmented naevi (increased by most agents)
Manoeuvres:
- Gait: full examination for evidence of neuropathy (VCR), spasticity (leukoencephalopathy), cerebellar
ataxia (L-asparaginase), antalgic limp (marrow relapse of leukaemia), or proximal myopathy (steroids);
also may detect evidence of cerebral tumour (second malignancy)
- Romberg`s test (neuropathy from VCR)
Back:
- Effects on bony skeleton (XRT, steroids, GVHD, MTX, BMT, endocrinopathy; poor mineral density,
growth anomalies, avascular necrosis); effects on paraspinal soft tissues (XRT, steroids, GVHD; muscle
weakness, hypoplasia, impaired mobility)
- Inspect (look for scars, any vertebral masses - secondary malignancy)
Upper limbs:
- Inspect (look for scars - previous diagnostic or curative surgery)
- Asymmetry (limb radiation, hemihypertrophy)
- Contractures (limb XRT, chronic GVHD)
- Peripheral stigmata of chronic liver disease (MTX, 6-MP, radiation to abdomen)
- Palmar crease pallor (marrow suppression)
- Pulse (bradycardia; untreated hypothyroidism from XRT to thyroid, or busulphan, BMT, MIBG)
- Blood pressure (elevated from steroids, bleomycin, MTX nephrotoxicity, radiation nephritis, renal
damage from GVHD; low from adrenal insufficiency from XRT to adrenal area, BMT)
HEENT:
- Alopecia (reversible: ADR, bleomycin, CPA, daunorubicin, VCR; irreversible: post-BMTx; busulfan;
cranial XRT + anthracycline given close together)
- Scars (previous diagnostic, curative or debulking surgery)
- Midfacial hypoplasia, small nose, chin (XRT to head and neck → altered growth bone/soft tissue)
- Conjunctival pallor (marrow suppression, various agents)
- Scleral icterus (bleomycin, MTX, 6-MP, 6-TG, radiation to liver)
- External ocular movements for evidence of cranial nerve palsy (CNS relapse of leukaemia, VCR
neuropathy)
- Cataracts (corticosteroids, radiation to eyes)
- Papilloedema (CNS relapse of leukaemia)
- Hearing impairment/hearing aid (XRT, cisplatin, carboplatin, antibiotics)
- Mouth dry (salivary gland dysfunction from XRT)
- Mucositis (MTX, 6-MP, 6-TG, actinomycin D)
Chest:
- Scars (previous diagnostic, curative or debulking surgery)
- Praecordial assessment for cardiomegaly (cardiomyopathy) from anthracyclines (the `rubicins`) or
radiation (mediastinal XRT), pericarditis (reversible—from mediastinal XRT), evidence of congestive
cardiac failure (from cardiomyopathy), abnormal rhythms
- Full respiratory examination for tachypnoea, cough or crackles due to interstitial pneumonitis or
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pulmonary fibrosis (bleomycin, busulphan, MTX, CPA, XRT, GVHD), pulmonary infection (opportunistic
viruses, bacteria/fungi if still on chemotherapy)
- Assess bony tenderness at sternum, clavicles, spine (marrow relapse: leukaemia, 2` leukaemia)
Abdomen:
- Scars (previous diagnostic, curative or debulking surgery)
- Prominent veins (chronic liver disease from MTX, 6-MP or XRT to abdomen)
- Hepatomegaly (MTX, 6-MP or relapse of leukaemia or Iymphoma)
- Splenomegaly (relapse of leukaemia or Iymphoma)
- Testicular enlargement (relapse of leukaemia)
Lower limbs:
- Effects on bony skeleton (XRT, steroids, GVHD, MTX, BMT, endocrinopathy; poor mineral density,
growth anomalies, avascular necrosis; effects on large joints); effects on soft tissues (XRT, steroids,
GVHD; muscle weakness, hypoplasia, impaired mobility)
- Asymmetry (limb radiation, hemihypertrophy)
- Contractures (limb XRT, chronic GVHD from BMT)
- Ankle oedema (from cardiac, liver or renal disease; see above)
- Bony (tibial) tenderness (marrow relapse of leukaemia)
- Functional assessment if:
- any asymmetry or contractures suggestive of radiation to limb, or
- scars from resection of tumour with potential neurological or vascular complications, or
- amputation: examine function with prosthesis; check how well it fits, any loosening, or infection
Urinalysis:
- Blood (CPA-induced cystitis)
- Proteinuria (radiation nephritis)
- Glucose (corticosteroids)
C. Discussion
- Refer previous pages for detailed investigation and management in leukaemia.
- Mainstay of management can be catogorised into chemotherapy, radiotherapy & psychosocial
intervention. Discuss on the complications which would be faced by patient in future and necessary
management as a whole.
ADR = adriamycin; BMT = bone marrow transplantation; CNS = central nervous system; CPA = cyclophosphamide;
GVHD = graft-versus-host disease; MIBG = radioactive iodine metaidobenzoguanidine; MTX = methotrexate;
6-MP = 6-mercaptopurine; 6-TG = 6-thioguanine; VCR = vincristine; XRT = radiotherapy.
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Lymphoma
A) Hodgkin Lymphoma
Hodgkin lymphoma
- Malignancy of lymphoid tissue, Reed-Sternberg (RS) cells & Hodgkin cells seen on histology
- B-cell malignancy, but exact origin of the malignant cells is unclear
- Has bimodal age distribution (adolescents & >50 years), M:F = 2:1
- Clinical features:
Lymphadenopathy - Painless, firm lymph nodes
- Cervical, supraclavicular, axillary, inguinal
- Mediastinal (cough, airway compression), retroperitoneal
`B` symptoms - Fever `Pel-Epstein`
- Night sweats
- Weight loss
Other constitutional - Fatigue, pruritis, anorexia symptoms
Extranodal involvement - Hepatosplenomegaly, bone pain, skin deposits, SVC obstruction
- Bone marrow failure (rare)
Investigations:
- Careful clinical examination is essential
Lymphadenopathy - FBC:
- Anaemia (normochromic, normocytic)
- Neutrophils↑, eosinophils ↑
- ESR↑ (used to monitor disease progression)
- LDH↑, LFT↑ (both indicates poor prognosis)
Lymph node biopsy - For diagnosis & histological classification
CT chest/abdomen/pelvis - For staging
Others (if necessary) - Bone marow aspirate
- Bone scan, MRI scan
- Liver biopsy
Management:
Stages IA and IIA Radiotherapy only or chemotherapy (ABVD)
Advanced disease Chemotherapy, e.g. adriamycin (doxorubicin), bleomycin, vinblastine,
dacarbazine (ABVD) ± Radiotherapy
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Management of Relapse:
Alternative combination chemotherapy, e.g. MOPP, and autologous stem cell transplant
Prognosis:
Stage I and II - >90% 5-year survival
Stage IIIA - >80% 5-year survival
Stage IIIB and IV - >70% 5-year survival
B) Non-Hodgkin Lymphoma
- Arises from abnormal T or B lymphocytes
- Children have high-grade diffuse disease & it is associated with congenital immunodeficiency
disorders. There are several classifications.
- Clinical features:
These vary depending on the site of the primary.
Systemic symptoms - Fever, night sweats, weight loss
Organ involvement - Abdomen (31%): abdominal distension, nausea, vomiting, acute
abdomen, hepatosplenomegaly
- Mediastinum (26%): dyspnoea, pleural effusions, SVC obstruction
- Oropharyngeal: stridor, sore throat
- Lymph nodes: painless hard lymph nodes. Most commonly cervical.
- Bone marrow: bone marrow failure features
- CNS: headache, CN palsies, raised ICP
- Oher organ: skin deposits, testes mass
Investigations:
Excision biopsy or fine Lymph node or other mass
needle aspirate
Bloods - FBC (anaemia, neutropenia, lymphoma cells, platelet↓)
- U&E↑, uric acid↑, bone profile
- LDH↑ (prognostic indicator)
Bone marrow aspirate or - Involvement in around 20%
trephine
CSF - Look for CNS involvement
Imaging CT scan chest/abdomen/pelvis and bone scan
Special tests - Chromosome analysis, immunological markers
Staging:
- Same as Hodgkin lymphoma, though it is less clearly related to prognosis than histological type
- Staging system for NHL reflects tumour volume more than degree of spread from primary site.
Murphy Staging System for NHL:
316
Management:
- Depends on the grade of malignancy.
- High-grade T cell malignancy seen in children is usually treated with multiagent
chemotherapy, like the ALL protocols.
- Relapses are treated with intensive chemotherapy, radiotherapy, autologous/ allogeneic SCT.
Prognosis:
- Limited stage disease > 90% cure
- Stage III and IV 70% cure
C) Burkitt Lymphoma
- Unusual B-cell lymphoma that is related to Epstein-Barr virus infection
- Endemic in Africa (jaw involvement classically seen) & sporadic in developed countries
(abdominal involvement seen).
Clinical features:
- Massive jaw lesions
- Abdominal extranodal involvement
- Ovarian involvement
Specific investigations:
- Lymph node biopsy: few histiocytes among masses of lymphocytes (`Starry sky` appearance)
- Cell culture for EBV
- Chromosome analysis: t(8:14) is usually present
Management:
- Intensive chemotherapy (four cycles), with SCT if relapse. Recently good results to treatment
have been obtained (70% cure).
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PART X
INFECTIOUS DISEASES
Dengue fever
Introduction:
- Common in Malaysia & other tropical countries (SEA, India & Africa)
- Arthropod-borne viral infection
Aetiology:
- Caused by flavivirus
- There are 4 distinct serotypes of dengue viruses: DEN-1, 2, 3, 4.
- In Malaysia, all 4 strains are present (thus increased risk for severe dengue)
- Secondary infection is the major risk factor for severe dengue due to antibody-dependent
enhancement theory
- All producing a similar clinical syndrome
- Homotypic immunity is lifelong but heterotypic immunity against other serotypes lasts only
few months (partial & transient protection)
- Incubation period is 4-7 days (range 3-14 days) * CPG Dengue 2009
- Vector is Aedes aegypti & Aedes albopictus mosquitoes (day-biting mosquitoes)
- Other risk factors for severe dengue include viral virulence, host genetic background, T-cell
activation, viral load & auto-antibodies.
Classification:
Dengue Virus
Infection
Asymptomatic Symptomatic
Undifferentiated
Dengue Fever Severe Dengue
fever
Note:
- DHF term is no longer being used (since 2009) as it suggests that hemorrhage is the cardinal
manifestation, whereas plasma leakage leading to shock is the most specific feature of severe dengue &
most important for clinical management:
- Some patients with severe clinical syndromes requiring medical intervention do not meet all criteria
for DHF.
- Classification is difficult when patients meet some but not all four diagnostic criteria, especially if
pivotal clinical laboratory data are unavailable.
- Diagnostic criteria for DHF have been inconsistently applied in epidemiologic & scientific reports.
- Reporting limited to DHF according to WHO classification scheme underestimates disease burden of
dengue illness
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Dengue Fever Severe Dengue
Criteria for Dengue with or without warning signs : Criteria :
Probable dengue Warning signs Severe plasma leakage
- Live/travel to dengue endemic - Abdominal pain or tenderness - Shock (DSS)
area. Fever & 2 of the following: - Persistent vomiting - Fluid accumulation with RDS
- Nausea, vomiting - Clinical fluid accumulation Severe bleeding
- Rash - Mucosal bleeding - Evaluated/defined by clinician
- Aches & pains - Lethargy, restlessness
Severe organ impairment
- Torniquet test positive - Hepatomegaly (>2cm)
- Liver: AST/ALT ≥ 1000
- Leukopenia - Lab: increase Hct concurrent
- CNS: Impaired consciousness
- Any warning sign with rapid decrease in PLT
- Heart & other organs
Pathogenesis:
- Classic dengue primarily occurs in non-immune, non-indigenous adults and children.
- Haemorrhagic & shock manifestations- represent a hypersensitivity phenomenon as a result of
a second attack of dengue infection (2 different dengue serotypes in an immune host. The first
infection produces the benign illness but sensitises the pts, so that if a second infection occur
within 6 months, a devastating immune reaction is provoked. (Type IV hypersensitivity-delayed
type). There is activation of complement system, coagulation and fibrinolytic cascades. Shock
may be mediated by massive release of histamine and vasoactive amines from mast cell. A mild
degree of functional capillary damage(leakage),consumptive coagulopathy,thrombocytopenia,
hypocellularity of bone marrow and liver damage.
Clinical features:
Phases Symptoms Signs
Febrile - Prodromal symptoms for 2 days - Fever rising to 39.5 - 41.4`C
Characterized by a - High grade, continuous fever lasting (documented)
sudden developing 2-7 days associate with chills & rigors - By 2-3 days later, temp returns to
high grade fever - Facial flushing near normal & symptoms disappear
- Myalgia, arthralgia and headache - Remission for 2 days followed by
- Skin rash (transient macular in 1st 2 return of fever & symptoms (Saddle-
days, maculopapular , petechial and back fever)
scarlet morbiliform at trunk, palm & - Conjunctival & scleral congestion
sole) `Islands of white in sea of red” - Tenderness upon pressure on eye
- Sorethroat, injected pharynx & - Positive Torniquet test
conjunctival injection
- Retro-orbital pain & lacrimation
Critical/ - Drop in temperature, sweating - Cool extremities
Defervescense - Generalised body ache, loss of taste - Prolonged capillary refill time
Characterized by a - Palpitation - Hypotension & tachycardia (early)
rapid drop in - SOB, respiratory distress - Relative bradycardia (late)
temperature - Bleeding tendency - Tachypnoea (↑RR: >20/min)
coinciding with
- Signs of intravascular volume
increased capillary Warning signs (Red flags):
depletion (Hypotension with
permeability - Abdominal tenderness
narrowed pulse pressure)
- Persistent vomiting
- Lymphadenopathy
- Clinical fluid accumulation
- Clinical fluid accumulation (Pleural
- Mucosal bleeding
effusion, pericardial effusion, sacral
- Restlessness or lethargy
edema, pedal edema, ascites)
- Tender hepatomegaly
- Mucosal bleeding
- Lab (↑Hct with ↓PLT)
- Tender hepatomegaly
319
- Oliguria/anuria
- Kussmaul`s respiration
- Bowel ischaemia (severe
hypovolemia, ↓blood supply to GIT)
Recovery Patient generally improves, however some may have classical rash and
Plasma leakage stops generalized pruritus
and ECF reabsorption
320
Differential Diagnosis:
A) During febrile phase B) During critical phase
Clinical Differential diagnoses Clinical Differential diagnoses
syndrome Syndrome
Flu-like - Influenza Acute - Acute appendicitis
syndrome - Measles abdomen - Acute cholecystitis
- Chikungunya - Viral Hepatitis
- Adenovirus - Diabetic Ketoacidosis
- Infectious mononucleosis Shock - Septic shock (septicaemia)
- Acute HIV seroconversion Respiratory - Diabetic ketoacidosis
distress - Renal Failure
Rash - Rubella (Kussmaul`s - Lactic acidosis
- Measles breathing)
- Scarlet fever Leucopenia & - Acute leukemia
- Meningococcal infection thrombocyto- - Immune thrombocytopenia
- Chikungunya penia ± purpura (ITP)
- Drugs bleeding - Thrombotic Thrombocyto-
penic purpura (TTP)
Diarrhea - Rotavirus - Malaria / Leptospirosis /
- Food poisoning Typhoid / Typhus
- Bacterial sepsis
Neurological - Meningoencephalitis - SLE
manifestation - Febrile seizures - Acute HIV seroconversion
- In clinical practice, the following classification of dengue fever is proposed, DHF is no longer used.
Dengue Fever Without increased vascular permeability
Severe Dengue Plasma leakage (↑ vascular permeability and fragility)
Evidence of pleural effusion or ascites or haemoconcentration >20%
321
Investigations:
Blood - FBC
- Thrombocytopenia, neutropenia, ↑Hct (Haemoconcentration)
- LFT (transaminitis, usually AST>ALT)
- PT/aPTT (DIC)
- BUSE, Creatinine (hydration status, electrolyte imbalance)
Virology IgM detection 4 days after onset of symptoms & up to 3 months in primary
dengue. 3 days after onset of symptoms & sometimes
hindered by large scale IgG production in secondary
dengue
IgG detection 10 days after onset of symptoms in primary dengue. 3 days
after onset of symptoms in secondary dengue
Rapid IgM detection 5 days after onset of symptoms & up to 2 months
NS1 & IgM/IgG Useful in early stage of infection (D3 onwards) & up to
Combo Kit seroconversion period (up to 2 weeks onwards). In event of
both NS1 & IgM are non-reactive while IgG is reactive, case
can be interpreted as secondary dengue
Viral Isolation - 1-5 days of onset of symptoms in primary dengue
(cell culture, - 1-4 days after onset of symptoms in secondary dengue
mosquitoes) - Most definitive diagnostic test, limited availability
- If patient dies soon after admission, liver biopsy specimen
sent in viral transport media may be useful in confirming
diagnosis
Viral RNA RT-PCR - 1-5 days of onset of symptoms in primary dengue
(conventional/real - 1-4 days after onset of symptoms in secondary dengue
time) - Indicated when there is a diagnostic problem (use of PCR
reaction to detect dengue RNA)
Viral antigen (NS1) - 1-7 days of onset of symptoms in primary dengue
- 1-5 days after onset of symptoms in secondary dengue
Critical phase often occurs after D3 of fever (or earlier) or around defervescence with a rapid ↓ temp. Clinical
deterioration often occurs during critical phase with plasma leakage or organ dysfunction. Evidence of plasma
leakage includes raised HCT, haemodynamic instability, fluid accumulation in extravascular space or
hypoproteinaemia. Abdominal pain, persistent vomiting/diarrhoea, restlessness, altered conscious level, clinical
fluid accumulation, tender liver/ mucosal bleed are the clinical warning signs of dengue infection with high
possibility of rapid progression to severe dengue.
Management:
A) Severe dengue without shock
- Must be admitted
- IV cannula & encourage pts to drink fluid, ORS, fruit-juices (banana, papaya)
- Encourage oral fluids. IV fluids using ½ NS + D5% if unable to take orally & patients with
evidence of plasma leakage
- Paracetamol for fever. Avoid NSAIDs. (causing gastrointestinal bleeding, Reye`s syndrome)
- Monitoring
- Clinical (circulation): pulses, Temp, PR, RR and BP
- I/O chart
- Urine SG
- Hct, platelet, Hb (8-12 hourly)
- Observations are continued till temperature returns to normal for 1-2 days. Critical period
occurs during transition from febrile to afebrile phase (usually after third day)
- Haemoconcentration usually precedes changes in pulse pressure and rate. ↑ in haematocrit >
20% reflects a significant plasma loss & indicate need for IV fluid.
B) Severe dengue with shock (Dengue Shock Syndrome)
- Admit to ICU
- Obtain IV access
- Resuscitation with Fluid Therapy
- 0.9% NaCI/Hartmann`s solution at 10-20 ml/kg, run as rapidly as possible. Dose is repeated till
peripheral circulation, pulse volume and BP return to normal. 2-3 boluses may be needed in
profound shock.
- If no definite improvement and haematocrit remains high, use colloids eg. haemecel or
gelafundin
- If no definite improvement and haematocrit is low or has ↓ transfuse blood, it signifies
bleeding, occult or obvious.
- Avoid Dextrose containing solution during initial resuscitation. Circulation and fluid therapy
must be assessed frequently.
- Monitor:
- Vital signs, peripheral perfusion
- BP hourly till stable
- PCV or HCT
- Urine output
- Platelet count 6 hoursly
- BUSE and serum creatinine
- ABG
- Fluid maintenance:
- Following fluid resuscitation, continue with 0.45% saline 5% Dextrose at 1-2 times
maintenance, guided by haematocrit, urine output and vital signs.
- In general, the duration of vascular permeability lasts 1-2 days following onset of shock, after
which further infusion of more fluids may result in pulmonary oedema & pleural effusion.
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- Electrolyte and metabolic disturbances:
- Hyponatremia and metabolic acidosis occur in DSS. Isotonic fluids and restoration of tissue
perfusion correct both problems. Correct hypoglycaemia that may occur in liver failure.
- Transfusion of blood and blood products:
Blood transfusion Indication:
Significant haemorrhage
Persistent shock despite crystalloid replacement in presence of low
or declining haematocrit. Fresh whole blood is preferable.
Platelet concentrate Indication:
Platelet count <50,000/mm3 with bleeding
Platelet count < 10,000-20,000/mm3
Dose: 10-20 ml/kg or 4units/m2 BSA over 1 hour
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Additional Notes (Adult Dengue):
- NS1 Ag test should be done immediately after blood is drawn to prevent false -ve result.
- NS1 can be postive up to D9 of fever, but usually don`t send for checking after D5.
- NS1 if positive after D5, it`s a prognostic feature that patient might go into severe dengue.
- IgM -ve at D7, should perform IgG test instead.
- Aware of severe organ dysfunction can occur even in recovery phase, eg. encephalitis/carditis
- Prolonged dengue fever (>6 days) means prolonged viraemia or comcomitant sepsis.
- Proper I/O charting with CBD in severe dengue are advisable.
- Aware of secondary haemophagocytosis occurrence in severe dengue. Suspect when Hct,
acidosis improved after fluid resuscitation but patient condition deteriorates. Investigation
includes ferritin, TG, fibrinogen. Treatment is steriod.
- Papaya products or sup ketam in relieving condition, no evidence but be neutral to patients.
- Encourage fluid intake 2-3L/day.
- Colloid usage in decompensated shock/ when patient requires 2nd round of fluid resuscitation
- Maintanence drip is calculated based on 2ml/kg/hour. Give 1.2-1.5 L x maintanence in patients
who cannot tolerate orally
- Usage of adjusted body weight, not ideal body weight in calculation.
- Manage patient as a whole, do not give repeated graded fluid bolus therapy for one single
warning symptoms.
- If patient no improvement with fluid resuscitation, think of myocardial dysfunction, order echo.
Management will be cut down IV drip and start inotropes early.
NOTE: Information about DHF is for introductory purpose. This term and its classification no longer
applies in Malaysia clinical practice.
WHO case definition of DHF:
- ALL of the following criteria must be present:
- Fever (High grade and continuous for 2-7 days duration)
- Haemorrhagic diathesis / Positive tourniquet test except in shock
- Thrombocytopenia (less than 100,000/mm3)
- Haemoconcentration (HCT 20% or more relative to baseline) or evidence of plasma leakage
- Other clinical manisfestation suggestive of DHF
- Hepatomegaly
- Circulatory disturbances (cool extremities, capillary refill >2s), low pulse volume, tachycardia)
- Fall in haematocrit following volume replacement.
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Measles (Rubeola)
Introduction:
- Highly contagious disease
- Characterised clinically by a typical prodome followed by a general maculopapular eruption
Epidemiology:
- Has a global distribution
- Since the introduction of an effective vaccine (MMR), incidence of measles has reduced
dramatically.
- Disease incidence has risen again, appearing in cluster among unvaccinated population
- In many developing countries, measles remain one of the leading causes of childhood mortality
(overcrowding, malnutrition & immunodeficiency)
- Occurs almost exclusively in children (Infants <6 months are partially protected by maternal
antibody)
Aetiology:
- Caused by paramyxovirus - measles virus which contains ssRNA within a lipoprotein envelope
- Transmitted by direct contact with infected droplets & contaminates fomes (close contact)
- Single serotype; lifelong immunity occur in individual who had the disease
- Human is the only natural host
Pathogenesis:
- Infection is transmitted via respiratory droplets, which can remain active & contagious, either
airborne or on surfaces, for up to 2 hours.
- Initial infection & viral replication occur locally in tracheal & bronchial epithelial cells.
- After 2-4 days, measles virus infects local lymphatic tissues, perhaps carried by pulmonary
macrophages.
- Following the amplification of measles virus in regional lymph nodes, a predominantly cell-
associated viremia disseminates the virus to various organs prior to the appearance of rash.
Clinical features:
- Incubation period is 8-14 days
- 2 distinct phase:
- Infectious pre-eruptive & catarrhal stage (early, eruption of measles surface)
- Non-infectious eruptive or exanthematous stage (late, maculopapular rash)
- Period of infectivity
- 1 or 2 days prior to rash to 6 days after (8 days overall)
Infectious Stage:
Prodromal Symptoms Prodromal Signs
- High grade fever - Koplik`s spots (pathognomonic early stage)
- Coryza, Dry cough, Conjunctivitis - Tiny white spot on an erythematous base
- Enanthem (an eruption upon a mucous - On buccal mucosa (opposite 2nd molar tooth)
surface) - Appear on D2 & D3 of clinical illness
- Miserable & ill-looking - Begins to fade as cutaneous rash appears
- Malaise, Headache, Irritability
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Non-infectious Stage:
Signs What is the difference
- Discrete erythematous maculopapular rash between an exanthem
- Consistently appear on D3 or D4 after the onset of fever and an enanthem?
- Starts on the nape of the neck Any skin rash associated
- Spreads upward to involve the face (behind ears & foreheads) with a viral infection is
- Spread downward to involve the trunk, limb, soles, palms called an exanthem. If
- There is tendency for rash (confluent & blotchy) the rash occurs on
- Eruption begins to fade -> desquamate & pigmentation will mucosal surfaces, it is
called an enanthem.
follow in second week
Investigations:
- Diagnosis is usually clinical & a rise in the antibody titre
- Definitive diagnosis can be determined by viral isolation in cell culture & immunofluorescence
of viral antigen
Differential Diagnosis:
- Rubella
- Roseola enterovirus
- Adenovirus
- Infectious mononucleosis
- Toxoplasmosis
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- Superimposed infection with S. pneumoniae, H. influenza, S. aureus
- Fever may persist, cough became worse, tachypnoea, cyanosis,
respiratory failure
- Giant cell (Hecht`s pneumonia)
- Rare & seen in immunodeficiency
- Fatal pneumonia
- Bronchitis
CVS - Myocarditis
GIT - Gastroenteritis, Diarrhoea
- Hepatitis, Appendicitis
Pregnant mother - Spontaneous abortion
- Premature delivery
Eyes - Keratitis
- Corneal scarring
- Blindness
Haematological - Hemorrhagic measles
- Thrombocytopenia
Management:
- Patient should be isolated & require hospitalisation
- Management is symptomatic and there is no antiviral therapy
- Maintenance of the fluid intake & nutritional state + relief the fever
- Immunocompromised should be given antiviral (eg. ribavirin)
- Vitamin A (in developing countries) which may modulate immune response
- Antibiotics in patient with secondary bacterial infection (eg. otitis media)
Prevention:
- Vaccine is given to immunize
- 6 months in Sabah & Sarawak (Measles)
- 12 months in peninsular (MMR)
- Also give to susceptible contacts within 3 days of exposure
- Why not injected from birth? Because maternal antibody in the child can neutralise the virus
and reduce the immune response (reduce immunogenicity of vaccine)
Clinical course:
329
Mumps
Epidemiology:
- Has a worldwide distribution & particularly prevalent in crowding, urban community
- Incidence has declined dramatically because of MMR vaccine
- There has been a rise in non-immunised child & unvaccinated young adults
- Predominantly a disease of childhood/school-aged: 90%; rarely in early infancy presumably the
result of persisting maternal antibody
Clinical features:
- Incubation period averages 18 days (14-21 days)
- Period of infectivity (7 days)
- 2-3 days before the onset of parotitis & 3 days afterwards
Investigations:
- Diagnosis is based on clinical
- Virus can be isolated from urine, saliva, throat swab or CSF (mumps meningitis)
- If in doubt, measure serum antibody titer (raised
- However definitive diagnosis can be made from viral isolation in cell culture & serology of viral
antigen (complement fixation test or hemagglutination inhibition test)
Differential Diagnosis:
- Coxsackie A infection
- Bacterial suppurative parotitis
- Sialectasis
- Mastoiditis
- Orchitis
- Epididymitis
- Drug reaction (thiazide diuretics)
330
Complications:
Neurological - Meningoencephalitis
-Most frequent complication
- CSF: Pleocytosis (result in ↑cell in CSF)
- Cx: Meningeal irritation, ↑ ICP (hard to differentiate from other viral
meningitis)
- Recovery is gradually & fully
- Transient hearing loss
CVS - Myocarditis
GIT - Hepatitis
- Pancreatitis (raised plasma amylase)
- Rare in the childhood
Reproductive organs - Orchitis ± epididymitis
- Rare prepubertal males; 2/3 of patients if after puberty
- Painful swelling (3-4x the original size)
- If involved bilateral -> infertility
(Fibrosis of tunica albuginea -> resist expansion -> causing pressure
necrosis of spermatocytes)
- Oophoritis
Others - Arthritis
- Mastitis
Management:
- Management is symptomatic
- Pain relieve with analgesics (eg. paracetamol)
- Adequate nutrition (soft & fluid food) & mouth hygiene
- Bed rest is guided
- There is no antiviral therapy
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Rubella (German Measles)
Introduction:
- Common communicable disease, often occurring in the endemic waves
- Affecting the school age child, adolescent & young adult
Aetiology:
- ssRNA virus (Togaviridae family): spherical & enveloped fragile virus (moderately contagious)
- Transmitted via respiratory droplet & transplacentally
- Single serotype; lifelong immunity occur in the individual who had the disease
Clinical features:
- Incubation period is 14-21 days (infectious from 1 week before & after rash)
Symptoms Signs
- Low-grade fever, malaise & headache - Forchheimer spots
- Skin rash - Petechial lesios on soft palate
- D1: From face rapidly spread to whole body - Suggestive NOT diagnostic
- Entire body may cover with discrete - Characteristic lymphadenopathy
erythematous macules (immune-mediated) - Suboccipital
- D3: rash will fade on the trunk only - Post-auricular
- D4: the rash will disappear rapidly - Posterior cervical groups
- Conjunctivitis - Maculopapular rash
- Splenomegaly
* Symptoms are mild or absent in children <5 years old
Complications:
Neurological - Encephalitis
CVS - Myocarditis
Bone - Arthritis (or arthralgia)
Blood - Thrombocytopenic purpura
- Haemorrhagic manifestations
*Complication is rare in the childhood
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Head - Microcephaly
- Mental retardation
- Rubella retinopathy (eg. cataract, glaucoma)
- Sensorineural deafness
CVS (congenital heart - Patent ductus arteriosus (PDA)
disease) - Ventricular septal defect (VSD)
Investigations:
- Diagnosis is usually clinical + a rise in antibody titre (4 fold rise in IgG)
(confuse with other viral exanthema & drug eruption)
- Definitive diagnosis is tissue culture from nasopharyngeal secretion or serology test
(haemagglutination test or enzyme immunoassay ELISA)
- Viral isolation/PCR in throat swab, synovial fluid
- Congenital: IgM in fetal blood, virus isolation/PCR in amniotic fluid
Management:
- Symptomatic treatment
- No antiviral therapy
Prevention:
- Live attenuated rubella vaccine
- Rationale: prevent congenital rubella by controlling post-natal rubella, vaccinating:
- 12 months old baby, 6 years old school entry
- Female of childbearing age (include screening in pregnancy)
- People with exposure risk (eg. healthcare workers, teachers)
- Contraindicated in pregnant woman
- 95% efficacy, long-term protection
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HHV infections
- 8 known human herpesviruses:
Common name Subtypes Site of Latency
Herpes simplex virus (Herpes) HHV-1, HHV-2 Sensory neurons
Varicella-Zoster virus (Chickenpox, Shingles) HHV-3 Sensory nerve ganglia
Epstein-Barr virus (EBV) HHV-4 B-lymphocytes
Cytomegalovirus (CMV) HHV-5 Monocytes/neutrophils
Human herpesvirus 6, 7 (Roseola infantum) HHV-6, HHV-7 Lymphocytes
Kaposi`s sarcoma-associated herpesvirus HHV-8 Unknown
- Hallmark of herpesviruses: Latency is established in post-infection and there is long-term
persistence of the virus within the host, usually in a dormant state, after certain stimuli,
reactivation of the infection may occur.
Management
- Acyclovir to treat severe symptomatic skin, ophthalmic, cerebral & systemic infections
- IV fluids (ensure adequate hydration)
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Herpes Simplex Infections (HHV-2)
Introduction:
- Accounts for 90% of primary genital herpes, 70-85% of neonatal herpes
- Infants with HSV infections are more likely to born prematurely (40% infants <38 weeks POG)
- Transmission:
- Ascending infection (acquired from mother with reactivated infection) (<5%)
- Passage through birth canal at delivery - genital herpes (33-50%)
Clinical features:
- Normal at birth, symptomatic at D5-10 of life
- Disseminated disease with multi-organ involvement (usually first week of life)
- Mostly liver, lung or localised infection to skin, eyes, mouth
- Considered in any infants with fever, sepsis, liver dysfunction, irritability, -ve bacteriologic
cultures, abnormal CSF findings, seizures
- Symptoms may overlap, skin lesions are late findings
- Often severe, a delay in treatment results in significant morbidity and mortality
Diagnosis:
- Viral culture from any skin vesicle, nasopharynx, eyes, urine, blood, CSF, stool or rectum
- +ve culture obtained from these sites >48 hours after birth indicate intrapartum exposure
- PCR (sensitive to detect HSV DNA in blood, urine, CSF)
Management:
- Parenteral acyclovir (neonatal HSV infections)
- Best outcome is observed in infants with disease limited to skin, eyes & mouth
- Elective LSCS is indicated when a mother with active genital herpes goes into labour
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Chickenpox (Varicella Zoaster/ HHV-3)
Introduction:
- Common, highly infectious, benign disease
- Affects all age but peak in 2-8 years old (maternal antibody protection is uncertain)
- Life-long immunity after recovery
Aetiology:
- Caused by primary infection with varicella zoster virus (VZV): enveloped, icosahedral, dsDNA
- Highly infectious during viral shedding (2 days before & 7 days after onset of rash)
- Incubation period is 10-23 days, peak occurrence: 5-10 years
- Human is the only natural host
Pathophysiology:
- Spread via
- Respiratory droplets, discharge from ruptured lesions on skin or conjuctivae
- Intrauterine infection (rare)
- Replicates in the nasopharynx & upper respiratory tract → disseminates by primary viraemia &
infects regional lymph nodes, liver, spleen and other organs
- Secondary viraemia follows → cutaneous infection with vesicular rash
- After resolution, virus persists in latent infection in dorsal root ganglia cells
Clinical Features:
Symptoms Signs
- Low grade fever - Characteristic vesicular rash *
- Headache & malaise - Appears as crops of small macules → papules →
- Skin rashes or eruption vesicles → pustules → dry up, scab & crust
- Appears in crops for 3-5 days formation → fall off within 1-3 weeks
- Start on head and trunk - Pruritus may be intense (scratching→scarring)
- Trunk is site of maximum lesions (D2 illness) - Scarring does not occur as a rule unless
- Progress to peripheries (involve all body parts) complicated by secondary infection**
* Adults patients tend to be more severe (severe chickenpox symptoms with ↑risk of developing complications)
** Watch for the child with chickenpox whose fever initially settles, but recurs a few days later: more likely to be due
to secondary bacterial infection. If new lesions appear beyond 10 days, suggests defective cellular immunity.
Complications:
Skin - Secondary bacterial infection
- Purpura fulminans
- Haemorrhagic lesions (immunocompromised)
- Mortality rate up to 20%
Head - Corneal lesions
- Stroke
CNS - Cerebellitis, Aseptic meningitis
- Generalised encephalitis
CVS - Myocarditis
Respiratory - Pneumonia (immunocompromised, adult)
GIT - Acute glomerulonephritis
- Hepatitis
Musculoskeletal - Arthritis
- Osteomyelitis
Blood - DIC (immunosuppressed)
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Rare but severe complications:
Secondary bacterial - Staphylococci, Group A streptococcal or other organisms
infection - Further complications eg. toxic shock syndrome and necrotizing fasciitis
- Should be considered where there is onset of new fever or persistent high
fever after the first few days
Encephalitis - Usually generalized, occurring early during the illness
- Prognosis is good compared to encephalitis caused by HSV
- Most characteristic is a VZV-associated cerebellitis
- Ataxic with cerebellar sign
- Usually resolved within a month
Purpura fulminans - Consequence of vasculitis in the skin and subcutaneous tissues
- Pathophysiology: After VZV infection→ Antiviral antibodies cross-react and
inactivate protein S → Dysregulation of fibrinolysis → Increased risk of clotting
Stroke - Very rare but can occur
- Same explanation as purpura fulminans
Investigations:
- Usually clinical diagnosis, lab test confirmation is usually unnecessary
- Definite diagnosis
- PCR (diagnostic)
- Genotyping (distinguish vaccine & wild-type strains, available through CDC)
- Immunofluorescent (using monoclonal antibodies) or culture of vesicular fluid (detects
varicella-specific antigens)
- Serology (demonstration of 4-fold antibody increase of acute & convalescent sera)
Management:
- Majority of cases are mild cases, only symptomatic treatment is required
- Oral acyclovir is not recommended in otherwise healthy children with varicella
Symptomatic relief - Non-aspirin antipyretics, cool baths
- Careful hygiene
Antiviral - Accelerates cutaneous healing, hasten resolution of acute neuritis, ↓risk of
(Higher dose for VZV post-herpetic neuralgia
infections than that for - IV acyclovir within 24 hours of rash onset to prevent severe complications
HSV) in immunocompromised individual
- Acyclovir or Valacyclovir in those at ↑risk of severe varicella:
- Unvaccinated individuals >12 years
- Chronic cutaneous or pulmonary disease
- On short-course, intermittent, aerolised corticosteriods
- On long-term salicylate therapy
- Oral famciclovir & valacyclovir (greater oral bioavailability than acyclovir,
recommended in adults)
- Acyclovir is recommended in children or as alternative therapy in adults
Human varicella zoster - Immunocompromised (deficient T-lymphocyte function following contact
immunoglobulin (VZIG) with chickenpox or if maternal chickenpox shortly before or after delivery)
Antibiotics - Indicated when secondary bacterial infection occurs, either local/systemic
High-risk individuals:
- Newborns (preterm, exposed to maternal varicella within 5 days prior/2 days post-delivery)
- Patients with congenital or acquired immunodeficiency (eg. HIV)
- Patients on corticosteriods or immunosuppresive drugs (previous 3 months)
- Recipients of bone marrow transplant
337
Clinical Course of Chickenpox:
338
Ebstein-Barr Virus infection (EBV, HHV-4)
Introduction:
- EBV has particular tropism for B lymphocytes and epithelial cells of the pharynx
- Major cause of infectious mononucleosis syndrome (glandular fever)
- Also involved in Burkitt lymphoma, lymphoproliferative disease in immunocompromised hosts
and nasopharyngeal carcinoma
- Transmission route is via oral contact with droplets or saliva (kissing disease)
Clinical features:
- Can be asymptomatic or manifests as glandular fever/ infectious mononucleosis
- Glandular fever:
- Common in adolescent and may persist for 1-3 months
- Symptoms are caused by host immune response to infection rather than virus itself
- Majority subclinical (fever, malaise)
- Tonsillopharyngitis (may be exudative) - Poor feeding
- Cervical lymphadenopathy - Breathing may be compromised
- Petechiae on soft palate
- Splenomegaly (50%) & Hepatomegaly with hepatitis (10%)
- Maculopapular rash
- Jaundice
Investigations:
PBF - Atypical lymphocytes/numerous large T cells
Monospot test - Positive indicates presence of heterophile antibodies
- This test often negative in young children with this disease
EBV serology - Seroconversion with production of IgM and IgG to EBV antigens
Differential Diagnosis:
- Diagnosis is usually made clinically
- TRO other causes of infectious mononucleosis (CMV, Toxoplasmosis)
- TRO other causes of pharyngitis (Group A Streptococcus, other viruses)
Management:
- Symptomatic treatment
- Corticosteroid if airway compromised
- Penicillin if group A streptococcus grown from tonsils
(Avoid ampicillin or amoxicillin which may cause a generalised florid maculopapular rash in
children EBV)
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Cytomegalovirus infection (CMV, HHV-5)
Introduction:
- Most common congenital infection, affecting 3-4/1000 live births in the UK
- In Europe, 50% of pregnant women are susceptible to CMV infection
- ~1% of susceptible women have 1` infection during pregnancy, 40% of their infants infected
- Mode of transmission:
- Transplacental (mother to fetus)
- Oral or genital (salivary or genital secretions)
- Blood transfusion (blood products)
- Organ transplantation
- Breastfeeding
Clinical features:
Infected infants - 90% are normal at birth and develop normally
- 5% have clinical features at birth:
- Mononucleosis syndrome with pharyngitis & lymphadenopathy
- Petechiae, purpura
- Hepatosplenomegaly, hepatitis, jaundice, thrombocytopenia
- Neurodevelopmental disabilities
- Sensorineural hearing loss
- Cerebral palsy
- Epilepsy
- Cognitive impairment, Mental retardation, Developmental delay
- Microcephaly, intracranial/periventricular calcifications, chorioretinitis
- SGA (small for gestational age)
- Blueberry muffin appearance (dermal erythropoiesis)
- 5% develop problems later in life, mainly sensorineural hearing loss
Infected pregnant - Usually asymptomatic or mild non-specific illness
woman
Immunocompromised - Retinitis
host (esp organ - Pneumonitis
transplant individual) - Bone marrow failure
- Encephalitis
- Hepatitis
- Colitis
- Oesophagitis
Investigations:
PBF - Atypical lymphocytes
Monospot test - Negative indicates absence of heterophile antibodies
Viral isolation (from - Diagnostic, must be taken within first 3 weeks after birth
urine or saliva) - Rapid culture using centrifugation & monoclonal antibody: result in 24 hours
Serology - Strong IgM anti-CMV antibody titre
PCR - Detect CMV DNA in urine
Management:
- Ganciclovir or Foscarnet (both have serious side-effects)
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Exanthem Subitum/Roseola Infantum (HHV-6, HHV-7)
Introduction:
- Both are closely related and have similar presentations
- HHV-6 more prevalent
- Mostly by the age of 2
- Transmission: oral secretion
Clinical features:
- High fever with malaise for few days, followed by generalized macular rash
- Exanthem subitum (17-30%)
- Uvulo-palatoglossal junctional ulcers, diffuse macular rash on face, trunk
- Infectious mononucleosis-like illness
- Frequently clinically misdiagnosed as measles or rubella
- Another frequent occurrence is when infants seen by GP during febrile stage are prescribed
antibiotics, when rash appears, it is erroneously attributed to an allergic reaction to the drug
- Commonly cause febrile convulsion
Diagnosis:
- Serology (Look for IgG seroconversion, IgM less reliable)
- PCR (but ubiquitous)
Complications:
- Acute febrile convulsions
- Encephalitis
Management:
- Symptomatic
- Ganciclovir or Foscarnet
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Erythema Infectiosum (Fifth disease or slapped-cheek syndrome)
Introduction:
- Caused by Parvovirus B19 (ssDNA) which only infects human erythroblastoid red cell precursors
in the bone marrow → Binds to P antigens (erythrocyte precursors, endothelial cells, fetal
myocardial cells)
- Occur at any time, although outbreaks most common during spring. Mainly in schools
- Transmission:
- Respiratory secretions from viraemic patients
- Vertical transmission from mother to fetus (transplacental)
- Transfusion of contaminated blood products
Clinical features:
- Acute, self-limited (4-8 days) cessation of RBC production, ↓Hb
- Dangerous in patient with red cell disorders, immunodeficient foetus (<20 weeks)
Asymptomatic - Common, ~5-10% of preschool children & 65% of adults have antibodies
- Mild, subclinical in most people
Erythema infectiosum - Most common, with a viraemic phase (non-specific prodrome)
- Fever, malaise, headache and myalgia
- Followed by a characteristic rash a week later on the face (`slapped-cheek`),
- Progressing to a maculopapular, `lace`-like rash on the trunk & limbs
(immune-mediated)
- Complications are rare in children
- Polyarthropathy
- Common in adults, 1-3 weeks or longer
- Acute, symmetrical, involving small joints
Aplastic crisis - Most serious complication of parvovirus infection
- Occurs in children with chronic haemolytic anaemias, ↑RBC turnover (eg.
sickle cell disease or thalassaemia) and in immunodeficient children (eg.
malignancy) who are unable to produce an antibody response to neutralise
the infection
Fetal disease - Transmission of maternal parvovirus infection→ Hydrops fetalis and death
- Severe anaemia, though majority of infected fetuses will recover
- Pure red cell aplasia
- Chronic infection in immunocompromised (eg. HIV) → chronic anaemia
- Management: IVIGs to improve immunity
Investigations:
Serology - IgG seroconversion
- IgM from serum, foetal blood
PCR - From serum, tissue, amniotic fluid, synovial fluid for Parvovirus B19 DNA
Virus isolation - Virus difficult to grow and culture
Management:
- No vaccine
- Infection control practices for chronic infection of Parvovirus B19
- Supportive, blood transfusion (severe anaemia in aplastic crisis)
- Immunoglobulins (Igs) to improve immunity in pure red cell aplasia
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Hand foot mouth disease (HFMD)
Introduction:
- Acute viral illness presents as a vesicular eruption in the mouth, hands, feet, buttocks, genitalia
- Self-limiting, mild systemic involvement, clinical improvement is observed after approximately
3-5 days; cutaneous & mucosal lesions resolve in 7-10 days
- More common in children <5 years old
Aetiology:
- Coxsackie virus A type 16 (CVA16) - most common EV subgroup of HFMD
- Also associated with coxsackievirus A5, A7, A9, A10, B2, and B5 strains
- Enterovirus 71 (EV-71) - outbreaks of HFMD with associated neurologic involvement
Pathogenesis:
- Faecal-oral route or contact with skin lesions/ oral secretions (highly contagious esp first week)
- Viral replicate in oropharynx → Pass into bowel to replicate in lymphatic tissue
- Viraemia & dissemination to target organs (CNS, skin, heart), rarely in HFMD
- Excreted in pharynx & faeces for weeks (spread via close contact, air droplets, faecal contact)
Clinical features:
Symptoms Signs
Prodromal phase: (Incubation period : 1 week) - Pyrexia, injected throat
- Fever - Tender, erythematous, blanching vesicular rash
- 38-39`C, may present for 1-2 days (usually not itchy)
- Anorexia, malaise, irritability, headache - Signs of dehydration (painful mouth ulcers)
- Sore throat (pharyngitis)
- Poor feeding (loss of appetite) - Associated systemic involvement is rare, mostly
limited to cutaneous manifestation
Exanthematous phase: (75%)
- Neurological involvement: (0.1/1000 EV-71 cases)
- Painful vesicular rashes
- Aseptic meningitis, encephalitis
- Over hands, feet, buccal mucosa, hard
- Acute cerebellar ataxia
palate, tongue, sometimes buttock, genital area
- Acute flaccid paralysis, GBS
- Initial macular lesions rapidly progress to
- Acute transverse myelitis
erosive vesicles surrounded by erythematous
- Neurogenic pulmonary oedema
halo or base
- Benign intracranial hypertension
Diagnosis:
- Clinical diagnosis
- Virus culture (throat swab, saliva, vesicle fluid, stool)
- Serologic testing is less helpful (eg. acute and
convalescent antibody levels)
- Polymerase chain reaction (PCR)
Management:
- Supportive management
- No specific antiviral agent or preventive vaccination
- Adequate fluid intake
- Direct analgesia (spray, mouthwash)
- Antipyretic/analgesic (acetaminophen, Ibuprofen) *AVOID using aspirin in children
- Antihistamine
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PART XI
NEONATOLOGY
Congenital Hypothyroidism
Introduction:
- Clinical syndrome resulting from deficiency of thyroid hormone activity
- Results in generalised slowing of all bodily function (↓basal metabolic rate)
- Hypothyroidism occuring during the critical period of brain growth (<2 years old)
- Retards physical growth, development, irreversible intellectual retardation
- Delayed maturation of foetal lungs and bones
- After CNS maturation has completed (>2 years old), hypothyroidism is reversible on treatment
- Ocurs in 1/2000-4000 live births (In Malaysia 1:3666)
- Can be congenital or acquired hypothyroidism (↓free T4) depending on level:
- Primary hypothyroidism (due to thyroid gland failure, 90% cases)
- Secondary hypothyroidism (due to deficiency of TSH)
- Tertiary hypothyroidism (due to deficiency of TRH)
Physiology:
- Fetal thyroid gland produces `reverse T3` (derivative of T3 which is largely inactive)
- After birth, TSH surge occurs (marked increase in circulating T3 & T4 levels
- TSH declines to normal adult range within a week
- Physiological, no thyroxine is necessary
- Pre-term infants usually have normal TSH but ↓ circulating T4 in the first few weeks of life
Aetiology:
A) Congenital
Dysgenesis - Can either partially or completely not develop
- Athyreosis (30%) - Normally, thyroid gland migrates from a position at foramen caecum
- Hypoplastic (10%) (sublingual) to its normal site below the larynx
- Ectopia (60%) - If this does not occur
- It remains as lingual mass
- Formation of thyroglossal cyst (maldescent & athyrosis)
Dyshormonogenesis - AR, inborn error of thyroid hormone synthesis (eg. Pendred`s syndrome)
- Common in consanguinuous marriage
TRH deficiency - Abnormalities of hypothalamus
TSH deficiency - Usually associated with panhypopituitarism
- Growth hormone deficiency (hypoglycaemia)
- ACTH deficiency (micropenis, undescended testis)
- Isolated TSH deficiency is rare (<1%)
Iodine deficiency - Commonest worldwide, endemic crenitism
- Usually related to maternal iodine deficiency
Maternal diet (pregnancy) - Maternal goitrogen ingestion (broccoli, cabbage, soybeans, spinach etc.)
- Drugs (propylthiouracil, methimazole, iodides, amiodarone, lithium etc.)
Newborn:
No goiter:
- Dysgenesis, Iodide exposure
- TSH deficiency
- TRH deficiency
With/without goiter:
- Dyshormonogenesis
- Maternal diet during pregnancy
- Iodine deficiency (endemic goiter)
344
B) Acquired
Autoimmune - Hashimoto thyroiditis (autoimmune or lymphocytic thyroiditis)
- Family history is present in 25-35% of patients
- Autoimmune process targeted against thyroid gland with lymphocytic
infiltration, lymphoid follicle and geminal center formation preceding
fibrosis & atrophy
- Typically occurs after 6 years of age, peak incidence: adolescent (F>M)
- Asssociate with T1DM, adrenal insufficiency, hypoparathyroidism
- Predisposition in Trisomy 21 and Turner syndrome
Surgery - Following thyroidectomy (after thyrotoxicosis or other thyroid surgery)
TSH deficiency - Pituitary tumour
- Following chemotherapy or radiotherapy
Iodine deficiency - Endemic goiter
Infiltrate diseases - Sarcoidosis, lymphoma
Drugs - Goitrogenic drugs (leads to goiter but not necessary hypothyroid state)
Clinical features:
- Divided into congenital & acquired (juvenile hypothyroidism)
- Difficult to differentiate from normal in the first month of age (more prominent with ↑ age)
345
1) Congenital: (Incidence=1/4000 live births, relatively common)
Symptoms Signs
General: General:
- Lethargy, inactive (excessive sleepiness) - Pale, cold & mottled, dry skin
- Failure to thrive (FTT) - Acrocyanosis
- Poor feeding - Hypothermia, bradycardia, respiratory distress
- Developmental delay
GIT:
- Delayed relaxation of reflex
- Prolonged jaundice
- Abdominal distension Head & Neck:
- Constipation - Large anterior and posterior fontanelle with
delay closure
- Coarse, puffy facies, thick lips, large tongue
- Low hair line with sparse, brittle hair
- Wrinkled forehead & depressed nasal bridge
- Periorbital oedema (myxedema)
- Hoarse cry
- Goiter (occasionally)
Abdomen:
- Umbilical hernia or potbelly
Investigations:
Blood - Guthrie test (neonatal heel-prick screening test)
- Raised TSH (>21mU/L in primary hypothyroidism)
- Low serum T4 level
Thyroid scan - Evaluate anatomy of thyroid (diffuse/multinodular goiter or normal)
Others - Hormonal panel (Indicated if secondary hypothyroidism, look for
panhypopituitarism)
- MRI (look for pituitary-hypotahalamic anatomy in secondary or tertiary
hypothyroidism)
- FBS, serum PTH, cortisol (If suspect for autoimmune polyglandular
syndrome in Hashimoto`s thyroiditis)
- Serum anti-thyroid peroxidase (TPO), anti-thyroglobulin antibodies both
raised in Hashimoto`s thyroiditis
346
Management:
B) Follow-up
- Monitor growth parameters and developmental assessment.
- Recommended measurements of serum FT4 and TSH by American Academy of Pediatrics:
- At 2 and 4 weeks after initiation of T4 treatment
- Every 1 to 2 months during the first 6 months of life
- Every 3 to 4 months between 6 months and 3 years of age
- Every 6 to 12 months thereafter until growth is completed
- After 4 weeks if medication is adjusted
- At more frequent interval when compliance is questioned or abnormal values are obtained.
- Ongoing counseling of parents is important due to serious consequences of poor compliance
347
Screening for Congenital Hypothyrodism:
348
Neonatal Hepatitis Syndrome
Introduction:
- Intrahepatic inflammation and cholestasis of multiple aetiologies (idiopathic, infectious
hepatitis or intrahepatic bile duct paucity) which leads to prolonged jaundice in neonates
- Infants may have IUGR & hepatomegaly at birth (in contrast to biliary atresia)
- Liver biopsy non-specific, showing gaint cell hepatitis
- Comprises of:
- Congenital infections
- Inborn errors of metabolism
- α1-antitrypsin deficiency
- Galactosaemia
- Tyrosinaemia (Type 1)
- Errors of bile acid synthesis
- Progressive familial intrahepatic cholestasis (PFIC)
- Cystic fibrosis
- Lipid & glycogen storage disorders (eg. Niemann-Pick, Gaucher disease, von Gierke`s disease)
- Perioxisomal disorders (eg. Zellweger syndrome)
- Intestinal failure-associated liver disease (associate with long-term parenteral nutrition)
- Alagille syndrome (intrahepatic biliary hypoplasia)
A) α1-Antitrypsin Deficiency
Introduction:
- AR disorder with deficiency of protease inhibitor α1-antitrypsin <2g/L (normal: 1.5 - 3.5 g/L)
- Protease inhibitor(Pi) is coded on chromosome 14 (liver disease associate with PiZZ phenotype)
- Functions to inhibit various protease, protects tissue from enzymes of inflammatory cells (esp
neutrophil elastase)
- Its absence/deficiency leads to dis-inhibition of elastase → elastin breakdown (COPD)
- Mutation in SERPINA1 gene → protein misfolding & impaired secretion → liver cirrhosis
Clinical features:
Liver cirrhosis Pulmonary disease
- Occurs in infancy & childhood - Usually manifests in adult
- Prolonged jaundice (>2 weeks of life) - Emphysema will lead to COPD
- Bledding tendency (↓ vitamin K) - Predominant lower-lobe involvement with
- Haemorrhagic disease of newborn bullae formation
- Gum bleeding, bruising - Advise to avoid active & passive smoking
- Intracranial haemorrhage - Smoking directly inactivate α1-antitrypsin &
- Hepatomegaly increase inflammatory reaction in airways
- Splenomegaly (2` to cirrhosis with portal - Bronchiectasis (end-result of COPD)
hypertension) - Increased risk of developing asthma
- Leads to chronic liver disease & hepatocellular
carcinoma (in adults)
Other associated conditions
- Vascular (ANCA +ve vasculitis, abdominal & intracranial aneurysm, arterial fibromuscular dysplasia)
- Renal (proliferative GN, IgA nephropathy), Intestine (pancreatitis, IBD, SSC)
- Skin (necrotizing panniculitis, systemic vasculitis, psoriasis, ulticaria, angioedema)
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Investigations:
Serum α1-antitrypsin - Less than 2 g/L (10-20% of normal) signifies low antitrypsin
Liver biopsy - Periodic acid Schiff +ve with diastase-resistance globules &
polymerised α1-antitrypsin in periportal hepatocytes, Kupffer cells
Phenotyping - Isoelectric focusing (IEF) to determine exact phenotype of patient
(diagnostic) - PiMM (100% normal serum α1-antitrypsin)
- PiMS/PiSS/PiMZ/PiSZ/P (40-80% of normal serum α1-antitrypsin)
- PiZZ (10-15% of normal serum α1-antitrypsin)
DNA analysis - Antenatal diagnosis via chorionic villus sampling at 11-13 POG
Imaging (for later age) - CXR (hyperlucency suggestive of emphysema)
- HRCT (widespread abnormal hypoattenuated areas, lack of lung tissue)
Others - Spirometry for lung function test (obstructive)
Management:
- 3 progression:
- Cholestatic jaundice gradually subsides before 6 months (30%)
- Develop cirrhosis in later age
- Liver failure in early infancy
- Liver transplant (indicated for patients with chronic liver disease)
- IV α1-antitrypsin augmentation therapy (indicated for emphysema, not appropriate for CLD)
B) Galactosaemia
Introduction:
- AR, very rare metabolic disorder which affects ability to metabolize galactose, accumulating
galactose 1-phosphate to toxic level
- Classical galactosaemia (Type 1): deficiency in galactose-1-phosphate-uridyl transferase (GALT)
Clinical features:
Symptoms Signs
- Poor feeding (FTT) - Developmental delay
- Vomiting - Cataracts
- Prolonged jaundice - Hepatomegaly
- Lethargy (hypoglycaemia) - Signs of shock (hypotension, tachycardia)
* Symptoms worsened on feeding milk to baby
Complications:
Early Late
- Gram-negative sepsis (rapidly fatal) - Developmental delay, learning difficulty
- Shock - Cataracts
- Haemorrhage - Chronic liver failure, Ascites
- DIC - Premature ovarian failure (1` amenorrhoea)
Investigations:
Screening Diagnostic
- Antenatal screening (amniocentesis/CVS) - Dried blood spots for total blood galactose &
- Detection of urine galactose (reducing sugar) Galactose-1-phosphate-uridyl transferase (GALT)
(can be +ve in lactose formula feeding or in RBC * Recent blood transfusion might mask dx
breastfeeding)
Management:
- Galactose or lactose-free diet (delay progression of liver disease BUT learning difficulty &
ovarian failure may occur in later age
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C) Other Neonatal Hepatitis Syndrome
Citrin deficiency - Important treatable cause of neonatal hepatitis among Asians
- Investigations MAY yield elevated total blood galactose but normal GALT)
eg. in 2` galactosaemia
- Elevated plasma citrulline (in plasma amino acids & acylcarnitine profile)
- Treatable with lactose free formula with medium chain triglyceride (MCT)
supplement
Note: Use lithium heparin container to send plasma amino acids
Tyrosinaemia type I - Treatable with NTBC (2-(2-nitro-4-trifluoromethylbenzoyl)-1,3-
cyclohexanedione)
- Urine organic acids specifically looking for presence of succinylacetone is
highly specific. Take particular attention of sending urine organic acids
frozen and protected from light (i.e. covered plain urine container) to
maintain the accuracy of the test
Neonatal - Needs TRO in infants presenting with liver failure within first weeks of life
Haemochromatosis - Significantly elevated serum ferritin (few thousands) is characteristic
- Diagnosis is confirmed by presence of iron deposits in extra hepatic tissue,
eg. lip tissue (iron deposits in minor salivary glands). Buccal mucosa biopsy
can be safely performed even in severely coagulopathic infants where liver
biopsy is contraindicated
- Treatment with combination of immunoglobulins, desferral and anti-oxidant
cocktails is potentially life saving (avoid liver transplant which at present not
an option for neonatal onset liver failure)
- Antenatal IVIg prevents recurrence in subsequent children
Long-chain fatty acid - Associated with cardiomyopathy
oxidatio disorders - Diagnostic test is blood acylcarnitine
Congenital disorders - Multisystem disease, protein-losing enteropathy
of glycosylation - Diagnostic test is transferrin isoform analysia
(CAG)
Wilson disease - Clues involve detection of KF rings under slit-lamp, neurological symptoms or
haemolysis
- Diagnostic test involves serum/urine copper, ceruloplasmin
Primary bile acid - Suspect if cholestasis, low GGT and low cholesterol
synthesis disorder - Serum bile acids is a good screening tool (ensure patient is not on
ursodeoxycholic acid <1 week prior to sampling)
- Definite diagnosis: urine bile acids analysis (available at specialized lab in UK)
- Treatment with cholic acid (not ursodeoxycholic acid) - excellent outcome
Peroxisomal - Cholestasis may be part of the manifestation
biogenesis disorders - Clues involve severe hypotonia, cataract, dysmorphic, knee calcification
- Plasma very long chain fatty acids (VLCFA) is elevated
Niemann Pick C - Clues involve hypotonia, opthalmoplegia, hepatosplenomegaly
- Diagnostic test is bone marrow examination
Mitochondrial - Suspect in presence of other neurological signs eg. rotatory nystagmus,
depletion syndrome hypotonia and elevated blood lactate. Metabolic/genetic consult for further
diagnostic evaluation
Infective causes - Septicaemia, Urinary tract infection (UTI)
- Herpes simplex, Hep B virus infection
- Consider in infants with liver failure within first few weeks of life
- IV Acyclovir therapy while waiting Herpes IgM results to be justified
- Can potentially present as early infantile liver failure but incidence is rare
- Presence of HbsAg, HBV-DNA (high viral loads) confirms the diagnosis
351
Alagille syndrome - Consider in infants who have cardiac murmurs or dysmorphism
- One of the parents is usually affected (AD inheritance, variable penetrance)
- Might not have typical dysmorphic features at birth due to evolving its nature
- Important screening tests include:
- Slit eye lamp examination (look for posterior embryotoxon, also help to
rule out other aetiologies in neonatal hepatitis syndrome, eg. retinitis in
congenital infection, cataract in galactosaemia)
- Vertebral x ray (look for butterfly vertebrae)
- Echocardiography (look for branched pulmonary artery stenosis, ASD,
valvular pulmonary stenosis
- Gene test (JAG1 gene mutation which can be done at IMR - EDTA container)
- Diangnostic tests include liver biopsy and DNA study
Idiopathic Neonatal - Follow up with LFT fortnightly
Hepatitis Syndrome - Watch out for liver failure and bleeding tendency (vitamin K deficiency)
- Repeat Hepatitis B and C virus screening at 6 weeks
- Most infants with idiopathic neonatal hepatitis in the absence of physical
signs of chronic liver disease usually make a complete recovery
Progressive familial - Reduced or normal GGT except in PFIC type III
intrahepatic - Diagnostic test include liver biopsy and DNA study
cholestasis (PFIC)
Cystic fibrosis (Refer topic Cystic Fibrosis)
Causes of Jaundice:
352
Neonatal Jaundice
Definition:
- Yellowish discoloration of skin, mucous membrane & sclera*
- Clinically detectable when the serum bilirubin levels are >85μmol/L (5 mg/dL)
* reliable site to look for jaundice, rich in elastin which has special affinity to bilirubin
Adult Term newborn
Hyperbilirubinaemia >17 μmol/L (1 mg/dL) D3-4 of life: >6 mg/dL
End of first week: 2-3 mg/dL
Clinical jaundice >50 μmol/L (3 mg/dL) >85 μmol/L (5 mg/dL)
Aetiology:
<24 hours 24 hours-2 weeks >2weeks (Prolonged)
Unconjugated - Haemolytic disorders - Physiological jaundice - Congenital
- ABO incompatibity - Prematurity hypothyroidism
- Rhesus incompability - Breastmilk jaundice - Infection (UTI,
- G6PD deficiency - Breastfeeding jaundice septicaemia, meningitis)
- Pyruvate kinase - Haemolysis - Breastmilk jaundice
deficiency (ABO, G6PD) - Haemolysis
- Polycythaemia - Upper GI obstruction
- Haemorrhage - Impaired enterohepa-
(bruising, haematoma) tic circulation
- Crigler-Najjar Syndrome
- Septicaemia
Conjugated - TORCHES infections - TORCHES infections - Biliary atresia
(congenital (congenital) - Choledochal cyst
- Neonatal hepatits
syndrome (IEM,
galactosemia, α1-
antitrypsin deficiency)
- TORCHES infections
- Metabolic (A1ATD etc)
- Post-TPN
Characteristic features:
Unconjugated hyperbilirubinaemia Conjugated hyperbilirubinaemia
- Fat-soluble (able to cross blood brain barrier) - Water soluble (cannot cross blood brain barrier)
- Presents normally in plasma - Presents normally in bile
- Indirect Van den Bergh reaction - Direct Van den Bergh reaction
- Clinical features: - Clinical features:
- Dark stool - Tea-coloured/dark urine
- Neurological manifestation (if severe) - Pale stool
- Acute Bilirubin Encephalopathy (ABE)
(drowsiness, poor feeding, hypotonia followed
by hypertonia affecting extensor muscles,
opisthotonos, torticollis)
- Kernicterus
(athetoid cerebral palsy, paralysis of upwards
gaze, sensorineural hearing loss)
- Bilirubin-induced Neurologic Dysfunction (BIND)
(abnormal gait, fine tremors, fine and gross
motor incoordination)
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Risk factors (of developing severe NNJ):
- Prematurity (common among babies delivered <37 POG, degree of hepatic immaturity)
- Low birth weight (ELBW babies have adverse neurodevelopmental outcome: mild-moderate
CP, blindness, severe bilateral central hearing loss or poor mental/ psychomotor development)
- Jaundice in the first 24 hours of life
- Mother with blood group O or Rhesus negative
- G6PD deficiency
- Rapid rise of total serum bilirubin (>6 mg/dL/day or 103 μmol/L/day)
- Sepsis, Acidosis, Asphyxia
- Excessive weight loss (in first 3 days after birth)
- Lactation failure
- Exclusive breastfeeding (dehydration)
- High predischarge bilirubin level
- Cephalohaematoma or bruises
- Babies of diabetic mothers (macrosomic, insulin resistance)
- Family history of severe NNJ in siblings
- Gastrointestinal tract obstruction (↑ enterohepatic circulation)
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Infections - Most common is due to UTI, meningitis, septicaemia Treat underlying
- Unconjugated hyperbilirubinaemia due to: cause with
- Poor fluid intake appropriate
- Haemolysis antibiotics
- ↓ hepatic function
- ↑ enterohepatic circulation
- Investigations: depending on suspected infections
Crigler-Najjar - Rare, absent or deficient of enzyme UDP-glucuronyl - Exchange transfusion
syndrome transferase, history of consanguinity important (immediate)
- Type 1 (UGT1A1 undetectable, no response with - Phototherapy
phenobarbital, higher bilirubin, ↑kernicterus risk) (12hours/day)
- Type 2 (UGT1A1 low but detectable, response with - Heme oxygenase
phenobarbital) inhibitor
- Unconjugated hyperbilirubinaemia - Phenobarbital
(Type 2)
- Liver transplant
Haemorrhage - Due to birth trauma eg. vantouse delivery - Stop the source of
- Causing cephalohaematoma, subaponeurotic bleeding
haematoma - Surgical intervention
Polycythaemia - Excessive breakdown of RBC due to abnormally high - Phlebotomy for 1`
concentration fo RBC polycythaemia
- Precipitating factors: - Treat 2`
- Antepartum - GDM, PIH polycythaemia
- Maternal hypoxia depending on 2`
- Interpartum - delayed cord clamping, not sterile cause
delivery environment
- Twin-twin transfusion (recipient)
- IUGR
C) Prolonged jaundice >14 days in full-term baby (or >21 days in preterm baby)
Condition Description Management
Congenital - Refer Topic Congenital Hypothyroidism Early diagnosis is
hypothyroidism important, treatable!
Infections - Refer Section B above (UTI, septicaemia, meningitis) -
Breastmilk jaundice - Refer Section B or Topic on Infant feeding (pg. 51) -
Haemolysis - Refer Section A (haemoglobinopathy) -
Biliary atresia - Refer Topic on Biliary atresia (pg. 354) Early diagnosis is
important, treatable!
Choledochal cyst - Refer Topic on Choledochal cyst (pg. 356) -
Neonatal hepatitis - Refer Topic on Neonatal hepatitis syndrome (pg. 335) -
syndrome
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2) Acute Bilirubin Encephlopathy (ABE) Assessment
i) Term babies
- Serious consequences of NNJ: ABE, choreoathetoid cerebral palsy, hearing impairment & death
- Bilirubin-indiced neurological dysfunction (BIND) score may be used in babies with severe NNJ
to assess severity & progression of ABE
BIND Date: Date:
Clinical Signs
Score Time: Time:
Mental Status
Normal 0
Sleepy but arousable; decreased feeding 1
Lethargy, poor suck and/or irritable/jittery with strong suck 2
Semi-coma, apnoea, unable to feed, seizures, coma 3
Muscle Tone
Normal Persistent mild to moderate hypotonia 0
Mild to moderate hypertonia alternating with hypotonia, beginning arching 1
of neck and trunk on stimulation 2
Persistent retrocollis and opisthotonus - bicycling or twitching of hands and 3
feet
Cry Pattern
0
Normal
1
High pitched when aroused
2
Shrill, difficult to console
3
Inconsolable crying or cry weak or absent
Management:
- Indications for hospital referral:
- Jaundice within 24 hours of life or rapid rising TSB > 6mg/dL/day (103mol/L/day)
- Jaundice below umbilicus (corresponding to serum bilirubin 200-250 μmol/L)
- Jaundice extending to soles of feet (urgent, may require exchange transfusion)
- Family history of significant haemolytic disease or kernicterus
- Any unwell infant with jaundice, clinical symptoms/signs of sepsis
- Prolonged jaundice of >14 days
- Refer infants with conjugated hyperbilirubinaemia urgently to hospital
- Refer infants with unconjugated hyperbilirubinaemia only if jaundice not resolve or a
definitive cause found
- TSB levels for Phototherapy & ET in babies ≥35 weeks POG:
A) Phototherapy
- Purpose:
- Prevent potentially dangerous indirect bilitubin level (converts into lumirubin which is water
solube to be excreted with faeces via intestine)
- Decrease the need for exchange transfusion
- Benefits:
- Non-invasive
- Highly convenient and inexpensive
- Needs minimum medical & nursing condition
- Causes prolonged reduction in bilirubin levels
- Many types of devices:
- Fluorescent tubes, Light Emitting Diode (LED), fibreoptic and halogen bulbs
- Effective phototherapy depends on:
- Blue light range (spectrum: 400 - 500 nm)
- Irradiance of minimum of 15μW/cm2/nm for conventional phototherapy
- Irradiance of minimum of 30 μW/cm2/nm for intensive phototherapy
- Distance of the light source not exceeding 30-50 cm from the baby
- Gestational age of baby (small, premature baby responds very rapidly)
- Birth weight of baby
- Aetiology of jaundice
- Bilirubin at the initiation of phototherapy
i) Types of Phototherapy
a) LED phototherapy
- Similar clinical efficacy as non-LED for term babies
- Shorter duration of phototherapy compared to non-LED for pre-term babies
- LED phototherapy does not induce significant alterations on transepidermal water loss and
cerebral blood perfusion when compared to conventional phototherapy
b) Fibreoptic phototherapy
- Less commonly used compared with conventional/LED phototherapy
- Common fibreoptic phototherapy used: Biliblanket and Wallaby II
- Similar clinical efficacy as conventional phototherapy in terms of duration of phototherapy
and % serum bilirubin change in 24 hours for preterm babies
- Less efficacy in comparison to conventional phototherapy for term babies
c) Intensive phototherapy
(Refer Section iii below)
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ii) Overview for Phototherapy
- Phototherapy lights should have a minimum irradiance of 15 μW/cm2/nm
- Measure intensity of phototherapy light periodically using irradiance meters
- Position light source 35-50 cm from top surface of the infant (when conventional fluorescent
photolights are used)
- Expose infant adequately, cover infant`s eyes
- Monitor serum bilirubin levels as indicated
- Monitor infant`s temperature 4 hourly to avoid chilling or overheating
- Ensure adequate hydration and good urine output. Monitor for weight loss.
- Adjust fluid intake (preferably oral feeds) accordingly
- Routine fluid supplementation is not required with good temperature homeostasis
- Allow parental-infant interaction
- Discontinue phototherapy when serum bilirubin is below phototherapy level
- Turn off photolights and remove eyepads during feeding and blood taking
- Once the baby is on phototherapy, visual observation as a means of monitoring is unreliable.
Serum bilirubin levels must guide the management
- In infants without haemolytic disease, the average increase of bilirubin level in rebound
jaundice after phototherapy is < 1 mg/dl (17 μmol/L). Hospital discharge need not be delayed
to observe for rebound jaundice, in most cases no further measurement of bilirubin is
necessary.
iii) Intensive Phototherapy
- Irradiance in the blue-green spectrum of at least 30 μW/cm2/nm measured at infant`s skin
directly below center of the phototherapy unit
- Indications for intensive phototherapy (KIV exchange transfusion):
- Total bilirubin >300 umol/L
- Early onset jaundice (First 24 hours)
- Rapidly rising jaundice (more than 8.5μmol/L/hr)
- If TSB does not decrease/ continues to rise in an infant receiving intensive phototherapy, this
strongly suggests hemolysis
iv) Failed Phototherapy
- Defined as an inability to observe a decline in bilirubin of 1-2 mg/dl (17-34 μmol/L) after 4-6
hours or to keep the bilirubin below the exchange transfusion level
- Do an immediate exchange transfusion if infant shows signs of acute bilirubin encephalopathy
(hypertonia, retrocollis, opisthotonus, fever, high pitch cry) or if TSB is ≥5 mg/dL (85 μmol/L)
above exchange levels stated above
- Use TSB. Do not subtract direct or conjugated bilirubin
- During birth hospitalisation, ET is recommended if TSB rises to these levels despite intensive
phototherapy
- Infants who are of lower gestation will require phototherapy & ET at lower levels (please check
with specialist)
v) Intravenous Immunoglobulins (IVIG)
- High dose IVIg (0.5-1 gm/kg over 2 hours) reduces the need for exchange transfusions in Rh &
ABO hemolytic disease.
- Give as early as possible in hemolytic disease with positive Coombs test or where the serum
total bilirubin is increasing despite intensive phototherapy.
- Dose can be repeated in 12 hours PRN. If ET is already indicated, IVIG should be given after ET.
362
vi) Practical Considerations:
- Phototherapy should be commenced when total serum bilirubin reaches the phototherapy
threshold for neonatal jaundice
- Irradiance of phototherapy units (non-LED) should be regularly checked
- Overhead phototherapy is preferred to underneath phototherapy
- Use of reflecting curtains shortens the duration of phototherapy and achieves a faster
reduction of TSB
- Effectiveness of reflecting curtains in phototherapy depends on the material and type of
curtain used, but use of curtains may impair observation of the babies
- Effective phototherapy is achieved with optimal irradiance and adquetely exposed body
surface area rather than the number of phototherapy units
- Babies should be placed in the supine position with adequate exposure (prone position is
associated with ↑risk of sudden infant death syndrome)
- Phototherapy should be started at a lower threshold in preterm & LBW babies
- LED phototherapy is preferred in preterm babies
- Babies should be regularly monitored for vital signs including temperature & hydration status
- Babies should be adequately exposed
- Babies` eyes should be covered to prevent retinal damage
- Breastfeeding should be continued
vii) Discontinuation of Phototherapy
- When bilirubin <threshold levels & has been falling for 24 hours (<185μmol/L or 11mg/dL on 2
successive determinations
- After cessation of phototherapy, bilirubin should be monitored for 2 successive days to detect
any rebound
- In infant without haemolytic disease, average bilirubin rebound after phototherapy is <1mg/dL
(17μmol/L)→discharge & no further bilirubin measurement is necessary
- If phototherapy is initiated early & discontinued before infant is 3-4 years old, additional
ambulatory follow up may be necessary
viii) Bronze baby syndrome
- Baby turns into dark bronze colour with macular rash due to exposure to phototherapy
- There is always evidence of obstructive jaundice & hepatic dysfunction
- Plasma & urine of baby shows characteristic absorption spectrum at 416 nm
- The dark colour fades within 2-3 months without any permanent ill-effects on baby
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B) Exchange Transfusion (ET)
- Procedure whereby infant`s blood is withdrawn & gradually replaced by donor blood
- Kernicterus has a 10% mortality and 70% long term morbidity
- Neonates with significant neonatal jaundice should be monitored closely & treated with
intensive phototherapy
- Mortality within 6 hours of ET ranged from zero death to 3-4/1000 exchanged term infants.
Causes of death includes kernicterus itself, necrotising enterocolitis, infection and procedure
related events.
i) Indications
- Double volume exchange
- Lower TSB & reduce risk of brain damage associated with kernicterus
- Hyperammonimia
- To remove bacterial toxins in septicaemia
- To correct life-threatening electrolyte and fluid disorders in acute renal failure
- Partial exchange transfusion
- To correct polycythaemia with hyperviscosity
- To correct severe anaemia without hypovolaemia.
ii) Preparation of Infant
- Signed Informed Consent from parent
- Ensure resuscitation equipment is ready and available
- Stabilise and maintain temperature, pulse and respiration
- Obtain peripheral venous access for maintenance IV fluids
- Proper gentle restraint
- Continue feeding the child; Omit only the LAST feed before ET
(If <4 hours from last feed, empty gastric contents by NG aspiration before ET)
iii) Type of Blood to be used
- Rh isoimmunisation (ABO compatible, Rh -ve blood)
- Other conditions (Cross-match with baby and mother`s blood)
- In Emergencies if blood type unkown (rarely): `O` Rh -ve blood
iv) Procedure
- Volume to be exchanged is 2x the infant`s total blood volume (2 x 80mls/kg)
- Use (preferably irradiated) Fresh Whole Blood preferably < 5 days old or reconstituted Packed
Red Blood Cells and FFP in a ratio of 3:1
- Connect baby to a cardiac monitor
- Take baseline observations (either via monitor or manually) and record down on the Neonatal
Exchange Blood Transfusion Sheet.
- Following observations are recorded every 15 minutes: apex beat, respiration, SPO2.
- Doctor performs the ET under aseptic technique using a gown and mask
- Cannulate the umbilical vein to a depth of NOT >5-7cm in a term infant for catheter tip to be
proximal to the portal sinus (for push-pull technique ET through UVC)
- Aliquot for removal and replacement:
- 5-6 mls/ kg (not more than 5-8% of blood volume)
- Maximum volume/cycle: 20 mls for term infants, not exceed 5 ml/kg for ill or preterm infants
- At the same time the nurse keeps a record of the amount of blood given or withdrawn and
medications given
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v) Isovolumetric or continuous technique
- Indication: when UVC cannulation is not possible eg. umbilical sepsis, failed cannulation
- Blood is replaced as a continuous infusion into a large peripheral vein while simultaneously
removing small amount blood from an arterial catheter at regular intervals, matching the rate
of the infusion closely
- eg. in a 1.5 kg baby, total volume to be exchanged is 240 mls. Delivering 120mls an hour
allowing 10 ml of blood to be removed every 5 mins for 2 hours
- Care and observation for good perfusion of the limb distal to the arterial catheter should be
performed as per arterial line care
vi) Practical consideration:
- Pre-warm blood to body temperature using a water bath
- Avoid other methods eg. placing under radiant warmer, massaging between hands or placing
under running hot water, to minimise preprocedure hemolysis of donor blood. Shake blood
bag gently every 5-10 cycles to prevent settling of RBC
- Rate of exchange: 3-4 min/cycle (1 minute `out`, 1 minute `in`, 1-2 minute `pause` excluding
time to discard blood and draw from blood bag)
- Syringe should be held vertical during infusion `in` to prevent air embolism
- Total exchange duration should be 90-120 minutes utilising 30-35 cycles
- Begin the exchange with an initial removal of blood, so that there is always a deficit to avoid
cardiac overload
- Routine administration of calcium gluconate is not recommended
- Remove the UVC after procedure unless a second ET is anticipated and there was difficulty
inserting the UVC
- Continue intensive phototherapy after the procedure
- Repeat ET may be required in 6 hours for infants with high rebound SB
- Feed after 4 hours if patient is well and a repeat ET not required
- If child is anemic (pre-exchange Hb <12 g/dL) give an extra aliquot volume of blood (10 mls/kg)
at the end of exchange at a rate of 5 mls/kg/hr after the ET
- If the infant is on any IV medication, re-administer the medication after ET.
Investigations:
Pre-exchange Post-exchange
- Serum bilirubin (Discard initial blood remaining in UVC before
- FBC, capillary blood sugar, BUSE sampling)
- Blood C & S (via peripheral venous blood, UVC to - Serum bilirubin
reduce contamination) - FBC, capillary blood sugar
- HIV, Hepatitis B (baseline) - Serum electrolytes, Calcium
- Others (Serum calcium, blood gases) - Others (as indicated)
Post-ET Management:
- Maintain intensive phototherapy (prevent rebound immediately after ET)
- Monitor vital signs: Hourly for 4 - 6 hours and 4 hourly subsequently
- Monitor capillary blood sugar: Hourly for 2 hours following ET
- Check serum Bilirubin: 4 - 6 hours after ET
Follow up:
- Long term follow-up to monitor hearing and neurodevelopmental assessment
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Complications of ET:
Catheter-related Haemodynamic problems Electrolyte/Metabolic disorders
- Infection - Overload (cardiac failure) - Hyperkalemia
- Haemorrhage - Hypovolaemic shock - Hypocalcaemia
- Necrotising enterocolitis - Arrhythmia (catheter tip near - Hypoglycaemia/
- Air embolism sinus node in the right atrium) hyperglycaemia
- Vascular events
- Portal, splenic vein thrombosis
(rare)
Where Hbw is reflection of the Hb removed during partial ET: Hbw = [Hb desired + Hb initial]/2
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ii) Follow up:
- All infants discharged <48 hours after birth should be seen by a healthcare professional in an
ambulatory setting, or at home within 2-3 days of discharge.
- For infants with risk factors for severe neonatal jaundice, early follow up to be arranged to
detect rebound jaundice after discharge.
- Infants with serum bilirubin >20 mg/dl (340 μmol/L) and those who require exchange
transfusion should be followed for neurodevelopmental outcome. Do a Hearing assessment
(using BAER, not OAE) at 0-3 months of corrected age.
- Infants with hemolytic diseases not requiring ET should be closely followed up for anaemia
until the risk of ongoing hemolysis is minimal
Kernicterus
Pathophysiology:
- Neurotoxicity due to deposition of unconjugated bilirubin
- No definite bilirubin level, ↑risk when TSB >20mg/dL (or 340 μmol/L)
- Occurs when [unconjugated bilirubin] exceeds albumin-binding capacity of bilirubin →
unconjugated bilirubin (which is fat-soluble) → cross blood-brain barrier (BBB) → most
commonly deposited in basal ganglia (esp globus pallidus, subthalamic nuclei, hippocampus,
substantial nigra), various cranial nuclei (esp CNIII, VII, VIII) can be involved
- BBB is more permeable to bilirubin during:
- Sepsis
- Prematurity
- Immature CNS & BBB
- Lower albumin level
- ↑risk of developing anoxia, hypercapnia, acidosis
- Hypercapnia (respiratory acidosis ↑bilirubin deposition in brain)
- Hyperosmolarity (dehydration)
- Low albumin due to displacing drugs (eg. sulphonamide, diazepam)
Phases of Kernicterus:
Phase 1 - Non-specific: Stupor(drowsy), Hypotonia, Poor sucking
Phase 2 - Hypertonia/spasicity of extensor muscles:
- Retrocollis (arching of neck) & Opithotonus (backward arching of the trunk)
- Fever, fits
Phase 3 - Disappearance of hypertonia (end of 1st week of kernicterus)
Phase 4 - Seizure, coma, spasticity,deafeness, mental retardation
- Extrapyrimidal (choreoathetosis, athethoid CP) may develop usually after 2 years →
Speech disturbance, Facial grimacing, Drooling, Poor feeding
- High frequency sensorineural hearing loss (due to brainstem injury)
Clinical features:
Acute kernicterus (Reversible) Chronic kernicterus (Irreversible)
- Lethargy - Dystonia
- Poor feeding - Cerebral palsy (athetoid)
- Irritability - Mental retardation
- Seizure - Delayed motor skills
- Coma - Learning difficulty
- Hypertonia - Sensorineural hearing loss (auditory neuropathy)
- GERD
Clinical Features:
Symptoms Sign
- Yellowish discolouration of skin/mucosa - Jaundice
- Cholestatic: - FTT
- Pale, acholic stool & dark/tea-coloured urine - Hepatomegaly
- Splenomegaly (portal hypertension
Complications:
- Liver cirrhosis (due to backflow of bile)
- Portal hypertension (presents as distended abdominal veins, caput medusa, UGIB)
- Fat malabsorption:
- Vitamin A (night blindness)
- Vitamin D (scurvy)
- Vitamin E (truncal, limb ataxia, lack of coordination of muscles)
- Vitamin K (haemorrhagic disease of newborn, bleeding disorders)
- Chronic liver failure (death within 2 years)
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Investigations:
Blood - FBC (↓Hb - anaemia of chronic disease)
- LFT (↑TSB, predominant ↑direct/conjugated bilirubin, ↑ALP, ↑↑GGT)
- Coagulation profile - ↓VitK-dependent clotting factors (II, VII, IX, X) secondary to
vitamin K deficiency
- Prothrombin time ↑
Imaging Abdominal ultrasound
- Detect abdominal polysplenia and vascular malformations (fetal BA)
- Gallbladder either is not visualized or as microgallbladder in biliary atresia
dilatation of intrahepatic bile ducts
- Triangular cord sign (cone-shaped fibrotic mass cranial to the bifurcation of the
portal vein)
- Gallbladder ghost triad (atretic gallbladder <19mm, irregular/lobular contour,
lack of smooth/complete echogenic mucosal lining with indistinct wall)
Hepatobiliary scintigraphy (sensitive but not specific)
- Technetium99-labeled iminodiacetic acid derivatives (TIBIDA/ HIDA scan
- Need to wait 5 days before the procedure for pre-treatment with phenobarbital
to ↑biliary secretion (less practical, limited usefulness)
- Demonstrates relatively good hepatic uptake with no evidence of excretion into
bowel at 24 hours
Diagnostic Percutaneous liver biopsy
- Detects bile ductular proliferation, presence of
bile plugs, portal/perilobular edema and fibrosis,
with intact basic hepatic lobular architecture
- Features of neonatal hepatitis may be present
- Diagram on the right shows bands of fibrous
tissue with bile duct proliferation suggestive of
extrahepatic biliary obstruction of biliary atresia
Others Exploratory laparotomy & direct cholangiography
- Determine the presence & site of obstruction
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Types of Choledochal Cyst:
Clinical features:
Symptoms Sign
Charcot`s triads: General:
- Yellowish discolouration of skin/mucosa - Cholestatic jaundice (intermittent)
- Pale, acholic stool, dark urine
Children:
- Intermittent abdominal pain (RUQ)
- Abdominal mass (RUQ)
- Fever & rigors
- Ascending cholangitis, pancreatitis
Investigations:
- Abdominal ultrasound, Endoscopic ultrasound (EUS)
- Radionuclide scan (TIBIDA/ HIDA scan)
- Abdominal CT/MRCP
- Endoscopic Retrograde Cholangiopancreatography (ERCP)
Complications:
Childhood - Cholangitis
- Caused by complete/partial obstruction due to ascending infections of biliary tree,
- Complications: septicaemia, liver abscess
- Maglinancy (cholangiocarcinoma: 2% risk in residual CBD)
- Hepatic damage
Adulthood - Liver abcess
- Liver cirrhosis, Portal HPT
- Recurrent pancreatitis
Management:
- Surgical excision of cysts with formation of roux-en-Y anastomosis to the biliary duct
- Liver transplantation (in severe case involving intrahepatic ducts)
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Neonatal Jaundice Long Case (Template)
A. History
General profile (Age, Gender, Ethnicity)
History taken from caretaker/parent
Presenting complaints
(Reason for admission)
HOPI - Present according to current condition, remember to rule out other differential diagnosis.
Assess in terms of severity, probable cause of NNJ
Jaundice Ascertain cause & risk factors:
- Age of onset of jaundice
- What is the initial total - Rapid rise of serum bilirubin (if serial serum bilirubin results available)
bilirubin and the >0.5 mg/dL/hour
progress of it? - First presenting symptoms, how diagnosed, what interventions were done
- What treatment has previous, under follow up in which hospital, any previous/ recent
been carried out on admission due to similar complaint
him? For how long? Birth History
- How long has he been - Gestational age: Prematurity
hospitalized and the - Low birth weight
total bilirubin upon - Bruising (eg: Cephalohaematoma)
discharge? Antenatal History
- Any congenital - Mother`s blood group, Rh status
abnormalities for the - Diabetic mother is a risk factor
child? - Maternal genitourinary infections/ TORCHES
- Where does the Family History
jaundice manifest in - G6PD (Infant + family) and other haemolytic anaemia
the child clinically? - Previous infants with NNJ
- Consanguinity
- Metabolic diseases
Dietary History
- Feeding method:
- Breastfeeding (breast milk jaundice)
- Lactational failure (breast feeding jaundice)
- Excessive weight loss (Risk factor)
- Poor fluid intake: Dehydration worsens NNJ
- Food allergy
Associated symptoms Pale stool, dark urine, bleeding tendencies, failure to thrive, prolonged
(Obstructive jaundice) jaundice, abdominal distention/pain
Severity - Signs of kernicterus/ acute bilirubin encephalopathy (ABE): Apnoea,
lethargy, poor feeding, seizures
- Signs of acute liver failure: encephalopathy, alternate periods of
irritability and confusion with drowsiness
- Any future planning or management told by doctor eg. liver transplant
Systemic review
Gastrointestinal disease Symptoms of intestinal obstruction: vomiting, abdominal pain, constipation
Endocrinology diseases Congenital hypothyroidism
Past-Medical & Surgical History
Past-Medical - Other than associated conditions of NNJ
Past-Surgical - Any other operation done previously (eg. Kasai)
Drug History
Drugs - Current medication, change in medication, compliance, control
- Drug allergy
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Paediatrics History
Immunisation history - Completed immunisation?
- Any delay in immunisation? Side effects?
Social History (if appropriate)
Disease impact on the - Schooling (which stream, level), Academic performance (rank, best
child subject), able to take part in physical class/sports?
- Problems of disease: energy levels, behavioural problems, frequent
hospitalisation, altered self-image, school absence, depression, feeling of
missing out due to disease exacerbations and energy levels
- Psychosocial (depression, low self-esteem & relationship)
- Body image, pubertal anxieties (in teens)
Disease impact on the - Occupation of caretakers
family - Financial considerations (financial burden of multiple hospitalisations,
surgical procedures)
- Social support group available (funding for operations)
Understanding of - Perception of disease
disease - Compliance with medications & follow up
Summary
- Summarise patient (name, age, gender) with presenting complaint & underlying cause of NNJ
- Provisional diagnosis and differential diagnosis
- Relevant history to be included
- Current functional status & Complications from NNJ
B. Physical Examination
General inspection Parameters General Condition
- Weight - Ill-looking (severe NNJ/ infections)
(If age beyond - Height - Cephalo-caudal progression of
expected for NNJ, - Head circumference jaundice severity (usually inaccurate)
consider CLD) - Growth charts - Lethargic, presence of hypotonia
(kernicterus)
Vital signs
- Presence of cephalohaematoma,
- Respiratory rate
petechiae, purpura, ecchymosis
- Pulse rate
- Dysmorphic features
- Temperature
- Signs of hypothyroidism: coarse
- Urinalysis (IEM)
facies, dry skin, hypotonia
Hydration status - Abdominal scars: Kasai procedure
(capillary refill time, skin turgor) - Specific odours during crises (IEM)
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Chest Praecordium Chest
Congenital heart disease Auscultate: evidence of cystic fibrosis
C. Discussion
1. Investigations :
- Total serum bilirubin
- G6PD status
- Others as indicated:
- Infant`s blood group, maternal blood group, Direct Coombs` test (indicated in Day 1 jaundice and
severe jaundice)
- Full blood count, reticulocyte count, peripheral blood film
- Blood culture, urine microscopy and culture (if infection is suspected)
2. Indications for hospital admission.
- Jaundice within 24 hours of life.
- Jaundice below umbilicus (if till level of the sole of the feet - likely to need exchange transfusion)
- Rapid rise of total serum bilirubin (TSB) of more than 8.5 µmol/L/hour (>0.5 mg/dl/hour).
- Prolonged jaundice of more than 14 days - other causes/conditions need to be excluded eg. neonatal
hepatitis, biliary atresia.
- Family history of significant haemolytic disease or kernicterus
- Clinical symptoms/signs suggestive of sepsis
3. Management
- Refer Notes in previous session or Paediatric Protocol
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Acute Respiratory Distress Syndrome (Hyaline Membrane Disease)
Introduction
- Occurs primarily in premature infants
- Incidence is inversely related to gestational age and birthweight
- Occurs in 60-80% of infants <28 wk, 15-30% of those between 32 & 36 weeks, rarely in those
>37 weeks of gestational age
Risk factors:
Increased Decreased
- Preterm - Chronic or pregnancy-associated hypertension
- Maternal diabetes - Maternal heroin use
- Multiple births - Prolonged rupture of membranes
- LSCS, precipitous delivery - Antenatal corticosteroid prophylaxis
- Fetal asphyxia, cold stress
- Previously affected siblings
Aetiology:
- Acquired (any factors which reduce surfactant production, refer Risk factors above)
- Familial (due to abnormal surfactant protein B & C genes/ ABC transporter 3 gene), eg :
- Alveolar capillary dysplasia
- Acinar dysplasia
- Pulmonary lymphangiectasia
- Mucopolysaccharidosis
- Congenital alveolar proteinosis (congenital surfactant protein B deficiency)
Pathophysiology:
- Surfactant deficiency (decreased production and secretion) as the primary cause, it results in:
- High surface tension
- Failure to attain adequate FRC
- ↑tendency of atelectasis in affected lungs (refer below)
- Physiologically, ↑phospholipids are synthesized & stored in type II alveolar cells with ↑POG →
surfactant are released into the alveoli → reduce surface tension & help maintain alveolar
stability by preventing the collapse of small air spaces at end-expiration
- Due to immaturity, surfactant production is insufficient to meet postnatal demands
- Surfactant is present with high concentrations in fetal lung homogenates by 20 POG, but it
does not reach surface of the lungs until later (appears in amniotic fluid between 28-32 POG)
- Matured pulmonary surfactant are present usually after 35 POG
- Hallmark: Alveolar atelectasis, hyaline membrane formation & interstitial edema
- Less compliant lungs → ↑ pressure is required to expand alveoli & small airways
- Preterm chest wall (highly compliant, less resistance) → ↑ tendency of lungs to collapse
- At end-expiration, volume of thorax & lungs tends to approach residual volume→ atelectasis
(perfused but not ventilated) → hypoxia
- ↓ lung compliance, small tidal volumes, ↑physiologic dead space & insufficient alveolar
ventilation → hypercapnia (respiratory acidosis)
- Combination of hypercapnia, hypoxia & acidosis → pulmonary arterial vasoconstriction with
↑R>L shunt via foramen ovale, ductus arteriosus & within the lung
- Progressive injury to epithelial & endothelial cells from atelectasis (atelectrauma), volutrauma,
ischemic injury & oxygen toxicity → effusion of proteinaceous material into alveolar spaces
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Contributing factors in the
pathogenesis of hyaline membrane
disease. Potential `vicious circle`
perpetuates hypoxia and
pulmonary insufficiency.
Clinical features:
- Usually appear within minutes of birth, may not be recognized for several hours in larger
premature infants until rapid, shallow respirations become more obvious
Symptoms Signs
- Fatigue, lethargy - Tachyonoea, tachycardia
- Breathing difficulty, dyspnoea - Nasal flaring & grunting
- Disinterest in surroundings - Head bobbing
- Poor cry - Use of acessory muscles
- Rapid, shallow breathing (↓tidal volume) - Intercoastal, suprasternal & subcostal retractions
- Cyanosis
- Diminised, harsh, tubular breath sounds
- Fine crepitations (deep inspiration)
- Apnoea, irregular respiration (ominous signs)
- Oliguria, ileus, oedema (untreated)
Complications:
- Interstitial emphysema
- Pulmonary haemorrhage
- Intraventricular haemorrhage (IVH)
- Bronchopulmonary dsyplasia (in chronic lung disease or with severe RDS)
- From intubation: Pneumothorax, air leaks, bradycardia during intubation, subglottic stenosis
Diagnosis:
- Clinical diagnosis based on clinical course, CXR & blood gases (acid-base values)
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Investigations:
Blood - Neutropenia (suggests early-onset sepsis)
ABG - Hypoxaemia (initial stage)
- Hypoxaemia, hypercapnia & variable metabolic acidosis (later stage)
CXR - Fine, reticular, granular lung parenchyma (typical develop on 1st day)
- Air bronchograms (more prominent early in left lower lobe due to superimposed
cardiac shadow)
Echocardiography - Indicated when no response to surfactant replacement
with colour-flow - Cyanotic heart disease can mimic RDS both clinically & radiographically
imaging
Lung profile - Lecithin : Sphingomyelin ratio and phosphatidylglycerol determination
- Indicated for atypical cases of RDS, performed on a tracheal aspirate
- Helpful in establishing a diagnosis of surfactant deficiency
Prevention:
- Avoidance of unnecessary/poorly timed early LSCS (<39 weeks) or induction of labor
- Appropriate management of high-risk pregnancy and labor (including administration of
antenatal corticosteroids)
- Prediction of pulmonary immaturity with possible in utero acceleration of maturation
- Antenatal and intrapartum fetal monitoring may decrease the risk of fetal asphyxia
- Administration of antenatal corticosteroids to women before 34 POG:
- ↓incidence, mortality of RDS & overall neonatal mortality
- ↓need for and duration of ventilatory support and admission to a neonatal ICU
- ↓incidence of severe IVH, necrotizing enterocolitis & neurodevelopmental impairment
- Postnatal growth is not adversely affected
- Not increase risk of maternal death, chorioamnionitis, or puerperal sepsis
- Recommended for all women in preterm labor who are likely to deliver within 1 week
- Act synergistically with postnatal exogenous surfactant therapy
- Betamethasone & dexamethasone have both been used antenatally. Betamethasone may
reduce neonatal death to a greater extent as compared to dexamethasone
- Administration of surfactant into the trachea of symptomatic premature infants immediately
after birth (prophylactic) or during the 1st few hourr of life (early rescue) showed reduced air
leak and mortality from RDS.
- CPAP started at birth is as effective as prophylactic or early surfactant and is the approach of
choice for the delivery room management of a preterm neonate at risk for RDS.
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Management:
- Main indications for intervention:
- Inadequate pulmonary exchange of oxygen and carbon dioxide
- Metabolic acidosis and circulatory insufficiency
- Early supportive care of premature infants includes:
- Treatment of acidosis, hypoxia, hypotension & hypothermia may lessen severity of RDS
- Therapy requires careful and frequent monitoring of heart and respiratory rates, oxygen
saturation, Pao2, Paco2, pH, serum bicarbonate, electrolytes, glucose, hematocrit, blood
pressure, and temperature. Arterial catheterization is frequently necessary
- Goal of treatment: Minimize abnormal physiologic variations & superimposed iatrogenic
problems as most cases are self-limiting. Treatment of infants with RDS is best carried out in
neonatal ICU
A) General Management
The general principles for supportive care of any premature infant should be adhered to,
including developmental care and scheduled `touch times.`
- Place infant in an incubator or radiant warmer to avoid hypothermia and minimize oxygen
consumption (core temperature maintained between 36.5 and 37`C)
- Calories and fluids should initially be provided intravenously
- Electrolytes should be added on D2 in most mature infants & on D3-7 in more immature ones
- Fluid volume is increased gradually over the 1st week
- Excessive fluids (>140 mL/kg/ day) contribute to development PDA and BPD
B) Oxygen therapy
- Warm humidified oxygen should be provided at a concentration initially sufficient to keep
arterial oxygen pressure between 50-70 mm Hg (91-95% saturation) in order to maintain
normal tissue oxygenation while minimizing the risk of oxygen toxicity
- CPAP reduces collapse of surfactant-deficient alveoli and improves both FRC and ventilation-
perfusion matching
- Infants with respiratory failure or persistent apnea require assisted mechanical ventilation
- Reasonable measures of respiratory failure are:
(1) arterial blood pH <7.20
(2) arterial blood Pco2 of 60 mm Hg or higher
(3) oxygen saturation <90% at SPO2 of 40-70% & CPAP of 5-10 cm H2O
- Infants with persistent apnea also need mechanical ventilation
- Goal of mechanical ventilation: Improve oxygenation & elimination of CO2 without causing
pulmonary injury or oxygen toxicity
- A strategy to minimize ventilator-associated lung injury is the use of CPAP instead of
endotracheal intubation. The decreased need for ventilator support with the use of CPAP may
allow lung inflation to be maintained but may prevent volutrauma from overdistention and/or
atelectasis.
- Permissive hypercapnia
- Strategy for the management of patients receiving ventilatory support in which priority is
given to the prevention or limitation of lung injury from the ventilator by tolerating relatively
high levels of Paco2 rather than maintenance of normal blood gas values
- Implemented during CPAP and mechanical ventilation
- Volume-targeted ventilation allows the clinician to set a tidal volume that may prevent
volutrauma & decrease the rates of pneumothorax and BPD
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- High-frequency ventilation (HFV)
- Achieves desired alveolar ventilation by using smaller tidal volumes & higher rates (300-1,200
breaths/min or 5-20 Hz)
- May improve elimination of carbon dioxide and improve oxygenation in patients who show
no response to conventional ventilators and those who have severe RDS, interstitial
emphysema, recurrent pneumothoraces, or meconium aspiration pneumonia
- Most frequently used HFV: High-frequency oscillatory ventilation (HFOV) and high-frequency
jet ventilation
C) Surfactant replacement therapy (SRT)
- Immediate effects of SRT:
- Improved alveolar-arterial oxygen gradients
- Reduced ventilatory support, increased pulmonary compliance
- Improved chest radiograph appearance
- In neonates with RDS who fail CPAP, treatment with endotracheal surfactant should be
initiated immediately after intubation
- Repeated dosing is given every 6-12 hr for a total of 2 to 4 doses, depending on preparation
- Exogenous surfactant should be given by a physician who is qualified in neonatal resuscitation
and respiratory management
- Additional onsite staff support required includes nurses and respiratory therapists experienced
in the ventilatory management of preterm infants
- Appropriate monitoring equipment (radiology, blood gas laboratory, pulse oximetry) must also
be available
- Complications of SRT: transient hypoxia, hyper- capnia, bradycardia and hypotension, blockage
of the endotracheal tube, and pulmonary hemorrhage
D) Pharmacological therapy
- Systemic corticosteroids indicated for:
- Infants with RDS
- Selectively treat infants who continue to require respiratory support
- Those in whom BPD develops
- Mortality and/or BPD at 36 weeks decrease with moderately early (7-14 days) administration of
corticosteroids
- Short-term adverse effects: hyperglycemia, hypertension, GI bleeding, perforation,
hypertrophic obstructive cardiomyopathy, poor weight gain, poor growth of the head,
↑incidence of periventricular leukomalacia
- Long-term adverse effects: neurodevelopmental delay and cerebral palsy in infants randomly
assigned to receive systemic corticosteroids
- Administration of inhaled steroids to ventilated preterm infants during the 1st 2 weeks after
birth reduced the need for systemic steroids and tended to decrease rates of death/BPD at 36
weeks without an increase in adverse effects
- Inhaled nitric oxide has been evaluated in preterm infants with hypoxemic respiratory failure
- Decreases the need for extracorporeal membrane oxygenation (ECMO) in term and near-term
infants with hypoxic respiratory failure or persistent pulmonary hypertension of the neonate
- Methylxanthines appear to have a large effect on reducing extubation failure
- Sodium bicarbonate (1-2 mEq/kg, may be administered over 15-20 min through a peripheral or
umbilical vein, emergency basis through an umbilical venous catheter) to treat metabolic
acidosis in RDS (result of perinatal asphyxia, hypotension or when an infant has required
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prolonged resuscitation. Possible side effects include skin sloughing from infiltration,
increased serum osmolarity, hypernatremia, hypocalcemia, hypokalemia & liver injury
- Empirical antibiotics therapy is indicated until results of blood cultures are known (due to
difficulty of distinguishing GBS or other bacterial infections from RDS. Penicillin or ampicillin
with an aminoglycoside is suggested, though choice of antibiotics should be based on the
recent pattern of bacterial sensitivity in the hospital where the infant is being treated
Prognosis:
- Antenatal steroids, postnatal surfactant use & improved modes of ventilation have resulted in
low mortality from RDS (~10%)
- Mortality increases with decreasing gestational age
- Optimal results depend on availability of experienced and skilled personnel, care in specially
designed & organized regional hospital units, proper equipment & lack of complications eg.
severe asphyxia, intracranial hemorrhage or irremediable congenital malformation
- Surfactant therapy has reduced mortality from RDS by approximately 40%
- Although 85-90% of all infants surviving RDS after requiring ventilatory support with
respirators are normal, the outlook is much better for those weighing >1.5kg
- Long-term prognosis for normal pulmonary function in most infants surviving RDS is excellent
- Survivors of severe neonatal respiratory failure may have significant pulmonary &
neurodevelopmental impairment
- Prolonged ventilation, IVH, pulmonary hypertension, cor pulmonale & oxygen dependence
beyond 1 year of life are poor prognostic signs
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PART XII
ENDOCRINOLOGY
Type 1 Diabetes Mellitus (T1DM)
Introduction:
- Diabetes in children is almost invariably type I diabetes mellitus.
- The incidence of type II diabetes mellitus is on the increasing trend among young people due
to obesity
Aetiology:
- Pancreatic β-cell destruction leading to absolute insulin deficiency, can be idiopathic/immune-
mediated (HLA-DR3, DR4 association with autoimmune disease)
- Genetic susceptibility + Precipitating environmental insult (microbial, chemical, dietary)
Clinical features:
Early Late
- Polydipsia - Vomiting, Dehydration
- Polyuria - Abdominal pain
- Weight loss - Hyperventilation due to acidosis
- Enuresis (secondary) - Drowsiness, coma
Diagnosis:
Criteria for Diagnosing Diabetes Mellitus
Clinical symptoms of Diabetes
PLUS
Random plasma glucose concentration more than or equals to 11.1 mmol/L (≥200 mg/dL)
(Random is defined as any time of day without regard to time since the last meal)
OR
Fasting plasma glucose more than or equals to 7.0 mmol/L (≥126 mg/dL)
(Fasting is defined as no calorie intake for at least 8 hours)
OR
Single 2-hour Post-prandial Glucose more than or equals to 11.1mmol/L (≥200 mg/dL) during an oral
glucose tolerance test (OGTT)
(Using a glucose load containing the equivalent of 75g anhydrous glucose dissolved in water or
1.75g/kg of body weight to a maximum of 75g) -WHO
Investigation:
Blood - FBS (for daily self-monitoring or by parent on glucose level)
- HbA1c (for monitoring of glycaemic control)
- Blood ketone (when difficult to obtain urine ketone or when urine ketone
reading is large, ↑ suggestive increased risk of ketoacidosis)
Autoantibody - Glutamic acid decarboxylase antibody (GADA)
screening - Insulin antibody (IAA)
(Only present in T1DM) - Insulinoma-associated protein-2 antibody (IA-2A)
- Zinc transporter 8 antibody (ZnT8)
C-peptide - To differentiate between Type 1 or 2 in newly diagnosed DM
- Low in Type 1 DM, normal to high in Type 2 DM
- To differentiate hypoglycaemia due to exogenous insulin use or insulinoma
- Low in exogenous insulin, high in insulinoma
Others - Microalbuminuria (suggestive of early stage of renal impairment)
- Fasting serum lipid (detect dyslipidaemia in DM)
- Sweat test (TRO CF-related diabetes if suspected)
- TFT (screen for autoimmune thyroid disease)
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Management:
A) Principle of insulin therapy:
Daily Insulin dosage
- Daily insulin dosage varies between individuals and changes over time.
- The correct dose of insulin for any individual is the dose that achieves the best glycaemic
control without causing obvious hypoglycaemic problems, and achieving normal growth
(height and weight)
- Dosage depends on many factors such as: age, weight, stage of puberty, duration and phase
of diabetes, state of injection sites, nutritional intake and distribution, exercise patterns, daily
routine, results of blood glucose monitoring (BGM), glycated haemoglobin (HbA1c) and
intercurrent illness
Guidelines on dosage:
- During the partial remission phase, total daily insulin dose is usually 0.5IU/kg/day.
- Prepubertal children (outside partial remission phase) usually require insulin of 0.7-1.0
IU/kg/day
- During uberty, requirements may rise to 1-2IU/kg/day.
- The total daily dose of insulin is distributed across the day depending on the daily pattern of
blood glucose and the regimens that are used.
Types of insulin:
Type Examples Onset of Action Peak Duration
Rapid-acting NovoRapid, 5-15 mins 30-60 mins 3-5 hours
insulin Humalog
Short-acting Actrapid, 30 mins 2-3 hours 3-6 hours
insulin (regular) Humilin R
Intermediate- Insulatard (NPH) 2-4 hours 4-12 hours 12-18 hours
acting insulin Humulin N
Long-acting Levemir (Detemir), Determir Determir Determir
insulin Lantus (Glargine) 1-2 hours 6-8 hours 6-23 hours
Glargine Glargine Glargine
1 hour No peak 24 hours
B) Frequently-used regimens:
Twice Daily Regimens
- 2 daily injections of a mixture of a short or rapid acting insulin with and intermediate-acting
insulins (before breakfast and the main evening meal)
- Approximately 1/3 of the total daily insulin dose is short acting insulin and 2/3 intermediate-
acting insulin
- 2/3 of the total daily dose is given in the morning and 1/3 in the evening
Three injections daily
- A mixture of short, rapid and intermediate-acting insulins before breakfast;
- A rapid-acting analogue/regular insulin alone before afternoon snack/ the main evening meal
- And an intermediate-acting insulin before bed
Basal-bolus Regimen
- Of the total daily insulin requirements, 40-60% should be basal insulin, the rest pre-prandial
rapid-acting or regular insulin.
- If using regular insulin, inject 20-30 min before each main meal (breakfast, lunch, and the main
evening meal); if using rapid-acting insulin analogue inject immediately before or after each
main meal (eg: breakfast, lunch, and the main evening meal)
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- Basal cover is given once daily at bedtime. However sometimes twice daily injections may be
needed (the other dose usually before breakfast).
- Insulin pump regimens are regaining popularity with a fixed or a variable basal dose and bolus
doses with meals.
- Patient should learn about carbohydrate counting to adjust dose of pre-prandial insulin.
Insulin Glargine
- Usually given once a day. However if needed, it can be given twice a day.
- When converting from NPH to Glargine, the total dose of basal insulin needs to be reduced by
approximately 20% to avoid hypoglycaemia. Then, the dose should be individually tailored.
Insulin Detemir
- Most commonly given twice daily in children
- When changing to Detemir from NPH, the same doses can be used to start with.
C) Monitoring of glycaemic control
Self-monitoring of blood glucose (SMBG)
- The frequency of SMBG is associated with improved HbA1c in patients with type 1 dabetes
- Timing of SMBG
- At different times in the day to show levels of BG.
- To confirm hypoglycaemia and to monitor recovery; and
- During intercurrent illness to prevent hyperglycaemic crises.
- The number and regularity of SMBG should be individualized depending on:
- Availability of equipment
- Type of insulin regimen
- Ability of the child to identify hypoglycaemia.
Note:
- Successful application of intensified diabetes management with multiple injection therapy or
insulin infusion therapy requires frequent SMBG (four to six times a day) and regular, frequent
review of the results to identify patterns requiring adjustment to the diabetes treatment plan.
- However, each child should have their targets individually determined with the goal of
achieving a value as close to normal as possible while avoiding severe hypoglycaemia as well as
frequent mild to moderate hypoglycaemia.
Target Indicators of Glycaemic control
Level of control Ideal (non-diabetic) Optimal (diabetic)
Clinical assessment
Raised Blood Glucose (BG) Not raised No symptoms
Low BG Not low Few mild, no severe
hypoglycaemia
Biochemical assessment
SBGM values, mmol/L
AM fasting or preprandial 3.6-5.6 5.0-8.0
Plasma glucose (PG), mmol/L
Postprandial PG 4.5-7.0 5.0-10.0
Bedtime PG 4.0-5.6 6.7-10.0
Nocturnal PG 3.6-5.6 4.5-9.0
HbA1c <6.05 <7.5
H) Diet
- A balance and healthy diet for age is required with dietician involvement.
- Carbohydrate counting should be taught to patients. Insulin dosage should match the
carbohydrate intake.
I) Exercise
- Regular exercise and participation in sport should be encouraged.
- Plan injection sites according to the activity eg. inject insulin in the arm if plan to go cycling
- Approximately 1.0-1.5g carbohydrates/kg body weight/hour should be consumed during
strenuous exercise if a reduction in insulin is not instituted.
- If pre-exercise blood glucose levels are high (>14mmol/L) with ketonuria or ketonaemia,
exercise should be avoided. Give approximately 0.05 IU/kg or 5% of total daily dose and
postpone exercise until ketones have cleared.
- Hypoglycaemia may be anticipated during or shortly after exercise, but also possible up to 24
hours afterwards, due to increased insulin sensitivity.
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- Risk of post exercise nocturnal hypoglycaemia is high and particular care should be taken if
bedtime blood glucose <7.0mmol/L
J) Diabetic Education
- At diagnosis - Survival skills:
- Explanation of how the diagnosis has been made and reasons for symptoms.
- Simple explanation of the uncertain cause of diabetes. No cause for blame.
- The need for immediate insulin and how it will work.
- What is glucose? Normal blood glucose levels and glucose targets.
- Practical skills: insulin injections; blood and/or urine testing, reasons for monitoring.
- Basic dietetic advice.
- Simple explanation of hypoglycaemia.
- Diabetes during illnesses. Advice not to omit insulin – prevent DKA.
- Diabetes at home or at school including the effects of exercise.
- Psychological adjustment to the diagnosis.
- Details of emergency telephone contacts.
K) Medic alert
- Wear the medic alert at all times as this may be lifesaving in an emergency.
- Obtain request forms for a medic alert from the local diabetes educator.
M) School
- The school teachers should be informed about children having diabetes so that some flexibility
can be allowed for insulin injections and mealtimes.
- Symptoms and treatment of hypoglycaemia should be informed so that some emergency
measures can be commenced at school.
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O) Evaluation for complications
- Microalbuminuria: 2/3 urine collections should be used as evidence of microalbuminuria
defined as:
- Albumin excretion rate (AER) 20-200mcg/min or AER 30-300 mg/day
- Albumin/creatinine ratio (ACR) 3.5-35mg/mmol (males) and 4.0-35mg/mmol (females) on first
morning urine specimen; Random ACR is higher
- Albumin concentration (AC) 30-300mg/L (on early morning urine sample).
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MODY Characteristics MODY Characteristics
MODY1 - 5%, mutation in HNF-4α gene MODY4 - Rare, mutation in IPF-1 gene
- Onset <25 yrs age - Onset post-pubertal
- Severe hyperglycaemia - Moderately severe diabetes
- OHA/insulin often required - Microvascular complications: rare
- Microvascular complications:
high risk/frequent
MODY2 -10-63% mutation in glucokinase gene MODY5 - Rare, mutation in HNF-1β/TCH2 gene
- Altered glucose sensing by β-cell - Onset post-pubertal
- Onset early childhood/ incidental - Severe diabetes
- Milf hyperglycaemia - Associated renal insufficiency
- Diet therapy alone - Microvascular complications:
- Complications: rare unknown
MODY3 20-70%, HNF-1α gene MODY6 - Rare, mutation in NeuroD1/β2 gene
- Onset adolescence <25 yrs - Onset post-pubertal
- Severe hyperglycaemia - Severe diabetes
- OHA//insulin often required - Microvascular complications:
- Microvascular complications: unknown
high risk/frequent
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Type 1 Diabetes Mellitus Long Case (Template)
A. History
General profile (Age, Gender, Ethnicity)
History taken from caretaker/parent
Presenting complaints
(Reason for admission)
HOPI - Present about DM in detailed, remember to rule out other differential diagnosis based on
symptoms of presenting complaint
Initial symptoms Early symptoms preceding the classic triad, lack of weight gain, nocturia,
behaviour change, altered school performance, changed vision
(blurring), tempo of onset (developing over days, weeks or months pre-
diagnosis)
Symptoms associated with Vomiting, abdominal pain, clouding of consciousness
ketoacidosis
Immediate pre-diagnosis Polydypsia, polyuria, weight loss despite polyphagia
symptoms
Details on intervention Where, when and how the diagnosis was made, length of hospital stay,
education given, treatment in hospital, treatment at discharge
Progression of Disease
1. Details of subsequent hospitalisations (frequency, indications, usual length of stay, usual outcome)
2. Complications of the disease: for example, eye problems with cataracts, retinopathy, joint problems
with limited joint mobility (LJM), severe hypoglycaemic reactions
3. Complications of treatment (e.g. fat atrophy or hypertrophy, insulin allergic reactions); degree of
control (number of episodes of ketoacidosis, frequency of hypoglycaemic symptoms)
4. Monitoring of the disease: how often seen in clinic, usual investigations performed, how often seen
by local doctor
5. Changes in management: for example, increase in insulin administration from daily to twice daily,
twice daily with additional short/ultra-short-acting or basal bolus regimen, use of insulin pump,
altered dosages due to occult nocturnal hypoglycaemia, changeover from human insulin to
analogues
6. At what age did the patient begin to administer his or her own insulin?
Paediatrics History
Birth history - GDM?Polyhydraminos? IUGR? G6PD deficiency?
Immunisation history - Completed immunisation?
- Influenza vaccine (recommended)
Developmental history - Any developmental delay?
Dietary - Any dietary control (avoid high glycaemic index food)
- Food allergy
Social History
Disease impact on the child - Self-image, reaction of school friends
- Coping with giving insulin, dietary restrictions, exercise
- Amount of school missed, academic performance, favourite subjects
Disease impact on the - Occupation of caretakers, employment status
family - Financial considerations
- Concern regarding future complications
- Genetic counseling
Social supports - Malaysia Diabetes Association (MDA)
- Access to social worker, government benefits obtained
Coping - Who attends the clinic with the patient
- Level of education of the child and parents
- Contingency plans for intercurrent illnesses or severe hypoglycaemia
causing loss of consciousness
- Access to local doctor/paediatrician/hospital
- Peer pressures, risk-taking behaviours
Summary
- Summarise patient (name,age,gender) with presenting complaint
- Provisional diagnosis and differential diagnosis
- Current functional status & Complications from DM
B. Physical Examination
Positioning:
- Initial inspecition standing, then lying, ensure adequate exposure (undressed)
General inspection:
- Parameters (weight, height, percentiles, growth chart)
- Well/unwell
- Hydration status
- Attached IV lines
- Tanner staging
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Hands:
- Fingertip pricks
- Trophic changes
- Cutaneous infections
- Limitation of joint mobility
Blood Pressure:
- Hypertension (nephropathy)
- Hypotension (Addison`s disease)
- Postural hypotension (autonomic neuropathy, dehydration)
Eyes:
- Inspection (squint, cataract, contact lenses, visual acuity)
- Eye movement, pupillary reaction, Red reflex
- Fundoscopy for fundus, retinopathy, optic atrophy (DIDMOAD)
Mouth:
- Hydration
- Ketotic breath
- Oral candidiasis
Thyroid:
- Inspection (swallowing)
- Palpation, Auscultation
Abdomen:
- Injection sites, fat atrophy, hypertrophy
- Distension (coeliac disease)
- Hepatomegaly
- Tanner staging
- Perianal candidiasis
Lowe Limb:
- Injection sites, fat atrophy, hypertrophy, trophic changes
- Candidiasis
- Necrobiosis lipoidica
- Reflexes, Sensation, Light touch, Vibration
Urinalysis:
- Glucose, Ketones
- Protein, Blood
Thyroid:
- Inspection (swallowing)
- Palpation, Auscultation
Others:
- Hearing (DIDMOAD)
- ENT & Chest (Infection precipitating presentation)
- Request insulin dosages & glucometer readings
C. Discussion
- Refer previous pages for detailed investigation and management in DM.
- Mainstay of management should be lifestyle modifications, followed by insulin therapy or OHA (in
Type 2 DM). Discuss on the complications which would be faced by patient in future and necessary
management as a whole.
Extra Notes:
Wolfram syndrome (DIDMOAD)
- Rare genetic disorder due to endoplasmic reticulum dysfunction
- DIDMOAD: Diabetes Insipidus, Diabetes Mellitus, Optic Atrophy, Deafness
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PART XIII
DYSMORPHISM
Angelman Syndrome
Introduction
- Complex genetic disorder which primarily affects the nervous system
- Inherited from mother (paternal imprinting with loss of maternally inherited genes) at chr15
- Characterised by severe intellectual & developmental disability, sleep disturbance, seizures,
jerky movements (esp hand-flapping), frequent laughter or smiling, usually a happy demeanor
- There are 4 known genetic mechanism:
- Molecular deletion involving 15q11.2-q13 critical region (deletion positive)
- Paternal uniparental disomy (UPD)
- Imprinting defects
- Mutations in the ubiquitin-protein ligase E3A gene (UBE3A)
Clinical features:
- Delayed development (by the age of 6-12 months)
- Severe speech impairment *
- Ataxia
- Behavioural uniqueness :happy, excitable personality
- Intellectual disability *
- Most affected children also have epilepsy* and microcephaly
- Characteristic facies:
- Flat occiput, Occipital groove, Strabismus
- Protruding tongue, tongue thrusting, suck/swallowing
disorder, frequent drooling (feeding problems)
- Truncal hypotonia during infancy
- Constipation
- Fascination with water
- Hypopigmented skin, light hair and eye color
- Abnormal sleep-wake cycles and diminished need for sleep
- Scoliosis
* Throughout life
Diagnosis:
- Baseline brain MRI, EEG (seizure, TRO focal neurological deficit)
- Musculoskeletal examination (scoliosis, gait impairment, muscular hypotonia, refer orthopedic)
- Ophthalmology examination (strabismus, visual acuity, evidence of ocular albinism)
- Developmental evaluation (whether speech therapy, physiotherapy should be indicated)
- Dietary evaluation (evaluate GERD in infants & young children, ensure optimal nutritional state)
Management:
- Supportive management:
- Antiepileptic drugs (seizures)
- Night-time wakefulness (sedatives)
- Scoliosis (thoraco-lumbar jackets or surgical intervention)
- Surveillance:
- Scoliosis (annual clinical examination)
- Obesity (evaluate for excessive appetite)
- Drugs to avoid (carbamezapine, vigabatrin, tiagabine as they may exacerbate seizures)
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Cornelia de Lange
Introduction
- aka Amsterdam dwarfism or Bushy syndrome
- Very rare genetic disorder (~1/10,000) present from birth but not always diagnose at birth.
- Causes severe developmental anomalies, physical and intellectual derangement.
Etiology
- Usually caused by de novo mutations in NIPBL (50%), SMC1A (5%), SMC3 (<1%) gene.
Clinical Features
- Low birth weight (<2.5kg)
- Small stature and delayed growth (FTT)
- Global developmental delay
- Feeding difficulty
- Regurgitation, GERD
- Projectile vomiting
- Swallowing difficulty
- Severe mental retardation
- Hirsutism, diaphragmatic hernia, aspiration pneumonia
- Upper limbs abnormalities
- Proximally placed thumbs
- Clinodactyly (Incurved fifth fingers)
- Craniofacial abnormalities:
- Microcephaly (average adult HC: 49cm)
- Synophrys (thick, brushy eyebrows meet at midline)
- Long curly eyelashes, arched eyebrows
- Small, upturned nose and thin downturned lips
- Low-set ears
- Long philtrum
- Cleft palate, small widely-spaced teeth
- Micromelia (small hands and feet)
- Hearing impairments
- Visual impairments (ptosis, nystagmus, hypertropia)
- Speech delay
- Seizures
- Congenital heart defects (PS, VSD, ASD, COA)
- Hypoplastic genitalia, undescended testes
- Behavioral problems
- Austistic, aggression
- Self-destructive behaviours, strong preference to a structured routine
Diagnosis
- Clinical diagnosis : frequent underdiagnosed or misdiagnosed.
- Genetic study (NIPBL and SMC1A) : referral to genetics specialist
Management
- Interdisciplinary approach (speech, occupational, physical therapist, teachers, physician,
parent)
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Dandy Walker Syndrome
Introduction
- Congenital brain malformation involving cerebellum and fluid-filled spaces around it
- 1/10,000-30,000 newborns, most cases are sporadic
- Classical malformation includes:
- Complete/partial agenesis of cerebellar vermis
- Cystic dilatation of fourth ventricle (non-communicating hydrocephalus)
- Enlargment of posterior fossa (with upward displacement of lateral sinuses, tentorium)
- Dandy-Walker malformation, variant & mega cisterna magna representing a continuum of
developmental anomalies on a spectrum known as Dandy-Walker complex
- Associated with hydrocephalus (may not develop till adulthood), absence of corpus callosum,
neuronal migration abnormalities (spina bifida, proencephaly, holoprosencephaly,
syringomyelia, Dermoid cysts)
- Known to be due to genetic cilliopathies (dysfunctional ciliary mechanism in cells)
- Strong association with PHACES syndrome (Posterior fossa malformation-Hemangiomas-
Arterial anomalies-Cardiac defects-Eye abnormalities-Sternal cleft & Supraumbilical raphe
Syndrome: cutaneous condition with multiple congenital abnormalities)
- Seen in chromosomal abnormalities (especially trisomy 18)
Clinical features:
- Developmental delay, especially motor skills (eg. crawling, walking, coordination)
- Progressive enlargement of skull (↑head circumference)
- Symptoms of ↑ICP (irritability, vomiting, convulsion)
- Signs of cerebellar dysfunction (nystagmus, lack of muscle coordination, ataxia)
- Muscle stiffness, hypertonia, muscle spasm
- Facial palsy (late childhood or adulthood)
- Spastic paraplegia
- Seizures
- Hearing & vision problems (rare)
- Abnormal breathing pattern, hypertelorism, cataracts, retinal dysgenesis, choroid coloboma
- Intellectual disability (mild to severe), normal intellectual will have learning difficulties
- Occipital encephalocele (sac-like protrusion of brain via opening at back of skull)
- Syndactyly, polydactyly, cardiac anomalies, orofacial deformities & cleft palate
- Retrocerebellar arachnoid cyst (cystic formation near the internal base of skull)
Diagnosis:
- Prenatal diagnosis by ultrasound, amniocentesis for fetal karyotype abnormalities
- MRI to show hydrcephalus, large CSF fluid cyst in posterior fossa, thinned occipital bone,
hypoplastic cerebellar hemispheres with winged appearance, ventriculomegaly, absence of
foramen of Lushka and Magendie
Management:
- Shunt to reduce intracranial pressure (eg. endoscopic third ventriculostomy)
- Occupational therapy, Physiotherapy for improvement in motor function
- Speech therapy
- Specialised education
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DiGeorge Syndrome (22q11.2 deletion)
Introduction
- aka velocardiofacial syndrome, conotruncal anomaly
face syndrome, Takao/Strong syndrome, thymic hypoplasia
Epicanthic folds
- AD, 1/4000
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Goldenhar Syndrome
Introduction
- aka oculoauriculo-vertebral (OAV) spectrum
- Characterized by incomplete development of ear,
nose, soft palate, lip, and mandible.
- Symptoms vary greatly and may be mild or severe.
- Frequency of 1/3,000-5,000 live births, M>F
- Hemifacial microsomia variant, with presence of
benign eyeball or eyelid tumours
- Usually affects one or both side of the face, impacting the right side more severely.
Etiology
- Unknown, related to branchial arch development issue late in the first trimester
- Possible cause: Embryonic blood vessel in the baby`s developing face accidentally burst,
creating two growth-related problems:
- Notable slow-down in the blood flow to either one or both sides of face, preventing those
structures from growing at a normal rate
- Formation of a group of blood clots, interfere growth
- Sporadic, multifactorial
Clinical Features
- Underdeveloped facial muscles
- Underdeveloped cheekbones
- Eye problems: small openings, benign growths, missing upper eyelid tissue, crossed eyes
- `Flat` larger than normal upper jaw
- Extremely small lower jaw
- Small, malformed, and/or absent ears and/or ear canals
- Underdeveloped, absent or fused vertebrae
- Underdeveloped organs or heart, kidney, and lung defects
- Cleft lip and/or palate
- A missing eye
- Hearing loss (unilateral/bilateral), vision and breathing problems
- Fusion of the bones of the neck
- Curvature of the spine (Scoliosis)
- Abnormal ribs
- Preauricular skin tags, strabismus
Management
- Grafting to correct the cheek bones
- Jaw surgery
- Eye surgery
- Ear reconstruction (Ocular dermoid debulking)
- Staged orthodontics and palatal closure
- Speech therapy and hearing aids
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Marfan Syndrome
Introduction:
- Autosomal dominant condition caused by defective fibrillin-1, a protein important to the
integrity of connective tissue. The defect found at the FBN1 gene on chromosome 15, which
codes for the connective tissue protein fibrillin.
Clinical Features:
Cardiac manifestation (manifesting in childhood in 25% of those affected, progressively worsen in 1/3 of
these children)
- Dilatation of the ascending aorta, with or without regurgitation & involving at least sinuses of Valsalva
- Dissection of the ascending aorta
- Mitral valve prolapse, with or without regurgitation
- Dilatation of main pulmonary artery in the absence of other anatomic cause (< 40 years)
- Calcification of the mitral valve annulus (< 40 years)
- Dilatation or dissection of the descending thoracic or abdominal aorta (<50 years)
Skeletal manifestation
- Pectus carinatum / pectus excavatum
- An increased arm span-to-height ratio > 1.05
- A positive Walker-Murdoch sign (Figure b)
- Steinberg sign (Figure a)
- A thoracolumbar scoliosis
- Progressive collapse of the hindfoot, leading to pes
planovalgus deformity
- A protrusio acetabuli of any degree
- High arched palate, with dental crowding
- Facial appearance (dolichocephaly, malar
hypoplasia, enophthalmos, retrognathia, down-slanting palpebral fissures)
- A reduced upper-to-lower segment ratio (distance from the head to the pubic symphysis /distance of
the pubic symphysis to the sole of < 0.85 )
Others
- Associated with ectopia lentis, spontaneous pneumothorax and lumbosacral ectasia.
Mnemonics: MARFANS
M - Mitral valve prolapse, Mental retardation (not present), Myopia (upward dislocation of lens),
Microfibrillin protein - Fibrillin 1
A - Aortic root dilatation (dissection & aneurysm), Aortic regurgitation
R - Retinal detachment
F - Fibrillin 1 gene, Chr15, Flat feet (Pectus excavatum, high-arched palate, hammer toes)
A - Arachnodactyly, Astigmatism, Air in lung (Pneumothorax)
N - Nitroprusside test –ve, Near-sightedness
S - Subluxation of lens (upward dislocation), Scoliosis, Speech disorders (due to high-arched palate &
small jaws), Sleep apnoea, Spinal cord - dural ectasia (widening of ballooning of dural sac
surrounding spinal cord
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Noonan Syndrome
Introduction:
- AD, associated with mutation in four genes PTPN11(12q24.1), KRAS, SOS1, RAF1
- Almost all have some cardiac defect (Dysplastic (often stenotic) pulmonary valve (PTPN11),
hypertrophic cardiomyopathy (HCM)
- Phenotypic features: Dysmorphic facial features, short stature, webbed neck & skeletal
anomalies (male version of Turner`s syndrome)
Management:
- Surgical intervention (complete excision of valve, resection of the RV outflow muscle & outflow
tract patch) - Dysplastic pulmonary valves (valvular obstruction)
- Cardiac transplant - Symptomatic HCM
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Prader-Willi Syndrome
Introduction:
- Rare (1/25000-1/10000)
- Deletion or unexpressed (partial deletion) on paternal chromosome 15 (genetic imprinting
whereby maternal copy is silenced, paternal copy is non-functional), opposite to Angelman.
- Characteristic features include hypotonia, short stature, incomplete sexual development,
cognitive disabilities, behavioral problems, chronic hunger (life-threatening obesity)
Clinical features:
Infancy - Reduced fetal movement, abnormal lie (often breech or Caesarean birth)
- Occasional polyhydramnios
- Lethargy, hypotonia
- Poor feeding (poor muscle tone affecting sucking reflex)
- Hypogonadism
Childhoods - Developmental delay, speech delay, poor physical coordination
- Excessive sleeping, Sleep disorders
- Strabismus `crossed eyes`, esotropia
- Hyperphagia(age 2-8, proceed to adulthood, oppose to infancy poor feeding)
- Excessive weight gain, Obesity
- Delayed puberty
- Short stature
- Extreme flexibility
Adulthood - Infertility (male & female), hypogonadism (sparse pubic hair)
- Obesity, hypotonia, extreme flexibility
- Learning disabilities (borderline intellectual functioning)
- Prone to DM, decreased bone density
Physical appearance - Prominent nasal bridge
- Small hands, feet with finger tapering
- Soft skin (easily bruised)
- Excessive fat (esp central obesity)
- High, narrow forehead
- Thin upper lip, downturned mouth
- Almond-shaped eyes
- Light skin & hair (relative to family)
- Lack of complete sexual maturity
- Frequent skin picking
- Striae
- Delayed motor development
Neurocognitive - Learning & attention difficulties (borderline to mid IQ)
- Speech poorer than comprehension (due to hypernasality)
- Extreme & insatiable appetite (morbid obesity)
- High pain tolerance (unaware of appendicitis, cholecystitis until later)
Diagnosis:
- Initially based on clinical diagnosis, currently via genetic testing (DNA-based methylation
testing to detect absence of paternal region on chr15q11-13)
Management:
- No cure, symptomatic treatment include physiotherapy (muscle tone), speech & occupational
therapy, daily recombinant GH injections (linear growth & increased muscle mass)
- Positive airway pressure machine (OSA 2` to obesity), weight reduction (if possible)
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Russell-Silver Syndrome
Introduction:
- Primordial dwarfism, growth disorder in both male & female
- Unknown aetiology, but 10% associate with maternal uniparental disomy (UPD)
- Classical presentation: IUGR/SGA, triangular-shaped face, fifth finger clinodactyly
Clinical features:
- IUGR combined with SGA at birth
(birth weight/length ≥2 SD below the mean for gestational age)
- Feeding problems (disinterested feeding, inadequate feeding with difficulty)
- Hypoglycaemia
- Excessive sweating as a baby (esp at night), greyness or pallor of skin
- Triangular-shaped face with a small jaw, pointed chin (tends to lessen slightly with age)
- Blue tinge to white of the eyes in young children
- Head circumference normal/ disproportionate to small boy size
- Wide & late-closing fontanelle
- Clinodactyly
- Body asymmetry (one side of body grows more slowly than other)
- Continued poor growth with no `catch up` into normal centiles on growth chart
- Hypotonia, striking lack of subcutaneous fat
- GERD, constipation (sometimes severe)
Diagnosis:
- Mainly based on clinical diagnosis
- No definitive tests to clearly determine though some
genetic markers are confirmed in
significant number of individuals
Management:
- Ensure adequate caloric intake
- Enteral feeding if unable to tolerate orally via PEG Triangular-shaped face
(percutaneous endoscopic gastrostomy)
- Physiotherpy (limb-length discrepancy or scoliosis)
- Growth hormone therapy (injection daily from age of 2 years old through teenage years)
- Improving self-esteem & interaction with other children
- Assists in muscular development & managing hypoglycaemia
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Turner Syndrome
Introduction:
- One of the most common chromosomal abnormalities (1 in 2000 female infants)
- Caused by the absence of one set of genes from the short arm of one X chromosome, 2/3 loss of
paternal X chromosome. (XO syndrome)
- It can be mosaic karyotype
Clinical Features:
- Short stature
- Webbed neck
- Nevi
- Infertility
- High arched palate with dental crowding
- Low hairline
- Skeletal defect (hip dislocation,
scoliosis)
- Hypertension (sometimes associate with
coarctation of aorta)
- Hypoplastic/hyperconvex nails
- Ovarian failure with no breast
development (No menstruation)
- Eyes (ptosis, strabismus, cataract &
amblyopia) and ears (otitis media)
- Cardiovascular malformation (hypoplastic left heart, coarctation of aorta, bicuspid aortic heart
valve)
- Learning disabilities, attention deficit hyperactivity disorder
- Associated with hypothyroidism, Crohns Disease and Ulcerative Colitis
Investigation:
- Prenatally diagnosed by amniocentesis or chorionic villous sampling. Obtain a karyotype by
one of these methods if ultrasonography of a fetus reveals a nuchal cystic hygroma, horseshoe
kidney, left-sided cardiac anomalies, or nonimmune fetal hydrops. Highly suggestive if the
human chorionic gonadotropin (HCG), estradiol, or alpha-fetoprotein (AFP) level is elevated
during pregnancy
- Standard 30-cell karyotype analysis is required for diagnosis of Turner syndrome, in order to
exclude mosaicism. Diagnosis is confirmed by the presence of a 45,X cell line or a cell line with
deletion of the short arm of the X chromosome (Xp deletion).
- Assess both LH and FSH levels prior to initiating estrogen replacement therapy.
Management:
- Estrogen replacement therapy starts at 12-15 years
- Human growth hormone stimulate growth of linear bone, skeletal muscle, and organs.
- Osteoporosis is common due to short stature & ovarian failure needed to be corrected with
minerals & vitamins supplement.
400
William`s Syndrome
Introduction:
- AD, deletion of a region of chromosome 7 causing elastin gene haploinsufficiency (very rare)
- Children with this condition are friendly, outgoing, gregarious (approach stranger readily)
Clinical features: (Mneumonics: WILLIAMS HYPERCALCAEMIA)
- Williams-Beuren Syndrome Critical Region (WBSCR); chromosome locus 7q11.2
- IQ (average 50-60), Impaired vision (reduced stereopsis)
- Low tone (hypotonia), Low pitched or hoarse voice, vocal cord paralysis, Lax joints (joint
hypermobility)/Loquacious, over-friendly, excessively empathic
- Impaired feeding (difficulty with food textures, vomiting)
- Appearance: broad brow, bitemporal narrowness, medial eyebrow flare, short palpebral fissures,
epicanthic folds, blue stellate iris, short nose, full nasal tip, full cheeks, malar hypoplasia, long
philtrum, full lips, wide mouth, small jaw, prominent earlobes
- Mitral valve prolapse (MVP)
- Supravalvular aortic stenosis (SVAS), Spine (scoliosis, kyphosis), Sternum (excavatum)
- HYpercalcaemia, hypercalciuria, hypertension
- Peripheral pulmonary arterial stenosis (PPW), Puberty early (but not precocious)
- Elastin arteriopathy (SVAS, PPS, aortic insufficiency, stenosis of mesenteric arteries),
Endocrine (hypothyroidism, T1DM in adults, Elfin face
- Renal anomalies (nephrocalcinosis, pelvic kidney, renal artery stenosis)
- Chronic otitis media (50%), Characteristic personality (over-friendly, people-orientated)
- Audiological problems: high-frequency sensorineural hearing loss, hyperacusis
- Linear growth failure, Loquacious personality
- Cognitive (good verbal short-term memory, language, poor visuospatial construction)
- ADHD/Anxiety (somatisation can lead to abdominal pain)
- Eyes (hypotelorism, strabismus (50%), amblyopia, refractive errors)
- Malocclusion, microdontia, enamel hypoplasia, widely spaced teeth, missing teeth
- Intestinal problems (constipation, diverticulosis, coeliac disease)
- Abdominal pain (reflux oesophagitis, cholelithiasis, diverticulitis, ischaemic bowel disease)
Investigation:
- Fluorescent in situ hybridization (FISH) -
detection of deletion in 7q11.23 region of chr7
Management:
- No cure, symptomatic treatment:
- Treat hypercalcaemia
- Physical therapy (joint stiffness, hypotonia)
- Developmental & speech therapy (enhance
social skills)
- Dietary assessment (manage constipation &
urinary problem)
- Hearing assessment, Eye check-up
- Inguinal hernia examination
- CVS assessment
401
Index
Aspiration Pneumonia 192-193 Childhood Asthma 179-186
A . Asplenia 32,295 Childhood Histiocytosis Syndrome 304
ABO Incompatibility 354 Asthma 178-186 Choanal Stenosis/Atresia 167
Absence Musculature Syndrome 238 Asymmetrical Tonic Neck Reflex 38 Choledochal Cyst 370-371
(Prune Belly syndrome) (ATNR)/Tonic Labyrinthine Reflex Chronic
Absence Seizure 115 Asymptomatic Bacteriuria 240 Gastroenteritis 205
Acoustic Neuromata 125 Atonic Seizure 97,115 Glomerulonephritis 251
Acquired Hypothyroidism 346 Atopic asthma 180 Kidney Disease (CKD) 248
Acute Atrial Septal Defect (ASD) 117,122 Suppurative/Serous Otitis 166
Adrenal Crisis 260 Attention deficit hyperactivity 34,37, Media (CSOM)
Bacterial Meningitis 85 disorder (ADHD) 82,401 Citrin Deficiency 351
Bilirubin Encephalopathy (ABE) 353,367 Autistic Spectrum Disorder 34,37 Clinodactyly 79,392,
99,101 Autoimmune Diseases 86,136, 399
Bronchiolitis 175 245,252, Clotting Disorders 286-288
Chest Syndrome 296 290-292, Coagulation Defects 284
Cystitis 240,245 Polyglandular Syndrome 346 Coarctation of Aorta 139-140,
Epiglottitis 173-174 Thrombocytopenic Purpura 290-292 130,157,
Gastroenteritis (AGE) 205-211 Thyroid Disease 345 400
Glomerulonephritis (AGN) 252-256 α1-Antitrypsin Deficiency 349-350 Common Cold (Coryza) 165
Haemorrhagic Cystitis 240 Complement System, 319,286
Kernicterus 353, 367 B . Coagulation & Fibrinolytic
Lobar Nephronia (Nephritis) 240 Bacterial Tracheitis 172 Cascade
Lymphoblastic Leukemia (ALL) 306-307 (Pseudomembranous Croup) Congenital
Myeloid Leukemia (AML) 308-310 Barbinski or Plantar Reflex 38,39 Adrenal Hyperplasia 21,46
Otitis Media 166 Becker`s Muscular Dystrophy 129 Disorders of Glycosylation (CAG) 351
Post-Streptococcal GN 252-256 Beri-beri 57 Dyserythropoietic Anemia 265
Pyelonephritis 240 Bifidus Factor 50 Genitourinary Tract 237,299
Renal Failure 216,254, Biliary Atresia 368-370 Abnormalities
306,364 Bilirubin-induced Neurologic 359 Heart Disease 130-148,
Respiratory Distress Syndrome 375,380 Dysfunction (BIND) 157, 175
Rheumatic Fever 149-150 Bitot Spots 57 Hepatic Fibrosis 236
Tracheobronchitis 170-172 Blalock-Taussig Shunt 142 Hypothyroidism 344-348
Tumour Lysis Syndrome (ATLS) 216,306 Blinking Reflex 39 357
Adenoma sebaceum 126 Block and Pencil test 36 Incompetence of Ureterovesical 248
(angiofibromata) Bone Marrow Transplant (BMT) 283,297 Infections 340,353,
Adrenarche 21 Bone Tumours 299 356
Alagille Syndrome 352 Brain Tumours 303 Malformation 235,34,
Alport Syndrome 251,256 Breast 99,130
Anaemia 265-270 Development 3,4,21 Muscular Dystrophy 128-129
Aplastic 242,265 Feeding 50-53 Nephrotic Syndrome 257-262
296,308 Breastfeeding Jaundice 52,356 Obstructing Posterior Urethral 238
Autoimmune Haemolytic 221,265 Breast-Milk Jaundice 51,52, Membrane (COPUM)
Chronic Disease 266 353,357 Prothrombotic Condition 289
Cooley`s 272 Broad-based Gait 22,25 Red Cell Aplasia 264-265
Diamond-Blackfan 265 Bronchiectasis 197,198, 349 Rubella Syndrome 332-333
Fanconi 242,265 Bronchiolitis 175-178 Talipus Equinovarus 12
296,308 Bronchiolitis obliterans 176 Toxoplasmosis 22,123
Folate/Vitamin B12 deficiency 57, 265 Bronchopulmonary Dysplasia 60,204, 328,339
Haemolytic 250,265 220,376 Constipation 53,220,
Hypochromic, Microcytic 273 Bronze Baby Syndrome 363 346,391
Iron Deficiency 60,271, Brudzinski`s sign 73 Cornelia de Lange 392
269-270 Brushfield Spots 76 Corrected age 45
Megaloblastic 57,356 Bruxism 81 Cow`s Milk Protein Allergy 53
Microangiopatic (MAHA) 250 Burkitt Lymphoma 317 Cranial Meningocele 119
Normochromic, Normcytic 250,306 Craniorachischisis Totalis 119
Sickle Cell 295,297 C . Craniotabes 58
Anencephaly 119 Cafe-au-lait spots 125,397 Crigler-Najjar Syndrome 353,357
Angelman Syndrome 391 Catarrhal 194,195 Crohn`s Disease 219-227
Ann Arbor Staging 315 Catch-up Growth formula 49 Croup 170-172
Anorexia 54 Catheter-associated UTI 241 Cerebrospinal fluid (CSF) 93,123
Antiepileptic 117 Coeliac Disease 54,265 Cushing Reflex 124
Aortic Regurgitation 141 Cerebellar sign 25,27 Cushing Syndrome 262
Aortic Stenosis (AS) 117,125 Cerebellopontine angle 125 Cyanosis 131
Apnoea 60,167-68 syndrome Cyanotic Heart Disease 141-148
194, 372 Cerebral Palsy 99,108 Cystic Fibrosis 196-203,
Arbovirus 96 Cervical Spine Instability 78,79 46,352
Arterial Switch 131 Charcot`s Triads 371 Cytomegalovirus infection (CMV) 123,140,
Arteriovenous shunt 15 Chickenpox (VZV/HHV-3) 336-338 334,360
Artrioventricular Septal Defects 117,131
(Complete AVSD)
402
D . Evoked optoacoustic emission 35 Gingivostomatitis 334
Dandy Walker Syndrome 393 (EOAE) Glandular fever 339
Deferasirox (Exjade®) 277 Ewing sarcoma 299 Glasgow Coma Scale (GCS) 11,13,22
Deferiprone/ L1 277 Exanthem subitum 341 Glenn or semi-Fontan operation 145
(Ferriprox®/Kelfer®) Exchange transfusion 364-366 Glomerular filtration rate (GFR) 239
Dehydration 199-203 Exercise-induced asthma 163,178 Glucose-6-phosphate 7,244,268,
Dengue Fever 305-312 Exomphalos 234 dehydrogenase (G6PD) 354,355,
Denver`s Guide 41-43 Extracorporeal membrane 72,379 deficiency 366
Dermatitis 56,168, oxygen (ECMO) Glycogen storage disorders 48,219,349
300 Eyes 39,76,212 Gower`s sign 23,128
Desferrioxamine (Desferal®) 276 Gross motor development 8,40,103
Developmental Assessment (DA) 34-44 F . Gross Motor Function Measure 103
Developmental Delay 33,37,47 Facial nerve palsy 26,125 (GMFM)
Developmental Milestones 40-42 Factor V Leiden mutations 289 Growth 10,19,45,
Diabetes Mellitus (DM) 381-390 Failure to thrive 45-49 49,56,80
DiGeorge Syndrome 394 Fanconi anaemia 265,268 Growth hormone deficiency 344,394
Dimercaptosuccinic acid (DMSA) 239,246 Fanconi syndrome 58 Growth hormone treatment 45,400
Scan Febrile convulsion 109-112 Guthrie test 4
Disseminated Intravascular 289 Female puberty 4
Coagulation (DIC) Femoral pulses 13,65,139 H .
Doll`s eye reflex 39 Fetal alcohol syndrome 37,130 Haematological disorders 263-317,
Down Syndrome 45,75-84, α-fetoprotein (AFP) 400 206,237
117,131 Fibrinolysis 221,285, Haematuria 240,252,
Duchenne`s muscular dystrophy 128-129 289,337 254,256
Duke`s Criteria 143 Fifth disease 342 Haemoglobin (Hb) 263,264,
Duodenal Atresia 76,84 Fine motor skills 8,40,101 271
Duplex Collecting System 237 Flat feet (pes planus) 79 Haemoglobinopathies 254,255
Dysdiadochokinesia 25,27 Floppy infant 22,397 Haemolytic anaemia 206,250,
Dysmorphism 391-401 Fluids 213-215 268,290,
Fluorescent in situ hybridisation 77,394, 295,342
E . (FISH) 401 Haemolytic disease of newborn 264
Echocardiography 130,131 Foetus 29,342 Haemolytic uraemic syndrome 250
Eczema 182,334 Folic acid supplements 62,297 (HUS)
Eisenmenger syndrome 13 Follicle-stimulating hormone FSH 21,78,278 Haemophilia 287-288
Electroencephalography (EEG) 98,116 Fontan operation 145 Haemophilus infection 32,85,166,
Emergencies (PALS) 68-74 Foreign body inhalation/ 192 173,187,
Encephalitis 96-98 obstruction 190,196,
Encephalocele 119,393 Formula-feeding 52-53 Haemopoiesis 263
Encephalopathy 96-98 Fractures 58,59,304 Haemostasis 284-289
Endocarditis 155-159 Fragile X syndrome 34,37 Hand, foot and mouth disease 343
Endocrine and metabolic 381-390 Frontal seizures 114 Harrison sulcus 58,164,181
disorders Fundoscopy 156,252, HbH disease 272
Endoscopy 124,218, 390,386 HbSAg 32,275,278
221,234 Fungal infections 83,85,89 280,287,
Endotracheal balloon occlusion 174,193, FVIII concentrate 286-289 351
378 Hearing assessment 35
Enteral feeding 56 G . Heart failure 131,132,
Enterococcus faecalis 155,158 G6PD deficiency 355 138,139,
Enteroviruses 96,85,343 Gait 22-23 152,187
Enuresis 168,242, Galactosaemia 350 Heart murmur 131
381 Galactose 350 Hemiplegia 87,101-02
Epicanthic folds 76,397 Gallstones 197,198, Henoch Schonlein purpura 293-294
394,401 272,295, Hepatitis 301,368,
Epidermolysis bullosa 220 356,360 349-352
Epididymitis 330 Gamma glutamyl transferase 221,351, Hepatocellular carcinoma 349,360
Epididymo-orchitis 330 (GGT) 352,360, Hepatomegaly 19
Epidural anaesthesia 93 369 Hepatoblastoma 299,300-
Epiglotitis 173,174 Gastritis 218,223 302,351
Epilepsies 113-118 Gastroenteritis 205-211 Hereditary spherocytosis 355
Epinephrine 171 Gastroesophageal reflux 217-218 Hernia 60,93,195,
Episodic viral wheeze 182 Gastroschisis 234 217,345,
Epstein-Barr virus (EBV) 339 Gastrostomies 56,105, 374,392
Erythema infectiosum 342 106,203 Herpes simplex encephalitis 334
Erythema multiforme 31,226 Gaucher`s disease 349 Herpes simplex virus 334-335
Erythema nodusum 47,220, Genetic counselling 198,273, Herpetic whitlows 334
223,225, 283,287 Hirschsprung disease 228-229
227 Genetic linkage 396 History taking 6-10
Erythromycin 151,165, Germ cell tumour (GCT) 300 HIV 7,96,163,
187,195 German Measles (Rubella) 332-333 321,341
Erythropoiesis 263 Gestational diabetes 7,99,130 Hodgkin disease 315-317
Escherichia coli 85 Giant-cell pneumonia 329 Horseshoe kidney 237
403
Human herpes virus (HHV) 334 Urology 247 K .
Human normal immunoglobulin 31 Immunisation 28-32 Kartagener`s syndrome 16
(HNIG) Immunodeficiency 48,163, Kasai procedure 370
Human papillomavirus (HPV) 28 189,316, Kawasaki disease 160-162
vaccine 394 Kayser-Fleischer rings 18
Human varicella zoster 337 Immunoglobulin 157,162, Kernicterus 367
immunoglobulin (VZIG) 294,337, Ketoacidosis 216,321,
Hyaline membrane disease 375-380 342,362 384,388,
Hydrocephalus 123-124 Immunoreactive trypsinogen 4,197 Kidneys and urinary tract
Hygiene hypothesis allergy 179 (IRT) disorders
Hyperactivity 100,1178, Impairment Acute kidney injury 206,250
279,400 Hearing 34-35 Chronic kidney disease 241,248
Hyperbilirubinaemia 253-274 Speech and language 34-35 Dialysis 206,250,
Hypercholesterolaemia 257,345 Impetigo 29,252 254,255
Hypercyanotic spells 142 Imprinting Enuresis 168,242,
Hyperexpanded chest 191,204 Inborn errors of metabolism 351-352 236-237
Hypergonadotropic 77,278, Infant feeding 50-53 Haematuria 250,251,
hypogonadism 281,398 Breast-feeding 50-52 252,256
Hyperkalaemia 72,216 Formula feeding 52-53 284,290,
Hyperlipidaemia 258 Weaning 53 299, 381
Hypernatraemic dehydration 214-215 Infantile Palpable kidneys 20
Hyperoxia test 131 Hypertrophic pyloric stenosis 195 Klebsiella 85,173
Hyperphosphataemia 309 Liver failure 236 187,241
Hypertension 124,134, Obesity 53 Kwashiorkor 55,56
139,152, Polyarteritis 160
204,254 Spasm 115 L .
Hyperthyroidism 7,83,224 Infants Lactose intolerance 53,120,
Hypertrophic cardiomyopathy 159,397 Premature 60-62 207,211
Hypoalbuminaemia 161,257 Sudden infant death syndrome 363 Langerhans cell histiocytosis 304
Hypocalcaemia 58,206, (SIDs) Laryngotracheobronchitis 170-172
309 Infectious mononucleosis 165,339 (croup)
Hypoglycaemia 60,113, Infective Endocarditis (IE) 155-159 Laser therapy 386
206,383- Inflammatory bowel disease 219-227 Laxatives 120,245
384 Inguinal hernia 60,185 Lead poisoning 37,264
Hypogonadism 77,298,281 Insulin 198,255, Learning difficulties 37,77,
Hyponatraemic dehydration 215 383,383 128,347
Hypoparathyroidism 277-278 Interferon 219,292 Left-to-right shunt 133-137
Hypoplastic left heart syndrome 146 Intestinal obstruction (IO) 197,220, Leukaemia 305-310
Hypospadias 84,237, 230,233, Life-threatening 68,184,
394 234 197,295,
Hypotension 10,61,212, Intracranial pressure 87,122, 296
320,390 303,331 Limping 82,102,
Hypothermia 55,69,73, Intrahepatic biliary hypoplasia 349 306
275,346 Intrarenal reflux 347,348 Liver disorders
Hypothyroidism 344-348 Intrauterine growth restriction 7,312 Acute liver failure 372
Hypotonic cerebral palsy 101-102 Intravenous immunoglobulin 291,292, Cirrhosis 197,349,
Hypovolaemia 61,72,257, (IVIg) 342,362 368,370-1
258,366 Intussusception 230 Neonatal hepatitis syndrome 349-352
Hypoxic-ischaemic 60,99,101 Ipratropium bromide 176 Tumours 300-302
encephalopathy (HIE) Iron-deficiency 268-270, Liver transplantation 302,357,
273 370,371,
I . Irritable bowel syndrome 220,224 Lumbar puncture 93-94
Idiopathic Isonatraemic 215 Lyme disease 96
Agranulocytosis 277 Isoniazid 86,366 Lymphadenopathy 160,268,
Generalised epilepsy 115 315,319,
Giant cell hepatitis 360 J . 332
Giant cell pneumonia 329 Jaundice 349-374 Lymphomas 315-317
Neonatal hepatitis syndrome 349-352 Jejunum 56,370
Seizure 94,117 Joint 306,320 M .
Thrombocytopenic purpura 290-292 Pain 31,82,149, Macrocephaly 7,107,303
IgA nephropathy 251,349 150,156 Magnetic resonance imaging 88,98,103,
Ileocaecal valve 230,234 160,293 (MRI) 108,278
Ileostomy 214 Swelling 150,160, Malabsorption 46,54-
Ileus 203,227 56,196
Paralytic 60,211 Juvenile Malformation 34,99,123,
Meconium 196-198 Absence epilepsy (JAE) 118 168,393
Iliac fossa pain 234 Myoclonic epilepsy (JME) 118 Malignancy
Imaging Hypothyroidism 345 Bone tumours 299
Brain tumour 303 Idiopathic arthritis 264,266 Brain tumours 303
Inflammatory bowel disease 222,227 Germ cell tumours 300
Neurology 127 Langerhans cell histiocytosis 304
404
Leukaemia 305-310 Night blindness 57,368 Pneumomediastinum 195
Liver tumours 300-302 Niridazole 366 Pneumonia 187-193
Lymphomas 315-317 Noonan Syndrome 397 Polycythaemia 134,142,
Nephroblastoma (Wilms) 299 357,366
Neuroblastoma 303 O . Polyhydramnios 389,398
Retinoblastoma 300 Obesity 53,79,168, Prednisolone 29,261,
Rhabdomyosarcoma 299 398 291,294,
Malnutrition 54-56,196 Obstructive sleep apnea (OSA) 81,167-68 307
Malrotation 233 Obstructive jaundice 353-374 Preterm infant 7,102,359
Mantoux test 88,92,183 Ocular albinism 391 Prevention of acute tumour lysis 309
Marasmus 55 Ocular dermoid debulking 395 syndrome (ATLS
Marfan`s syndrome 396 Ocular toxicity 276,282 Prevention of contracture 129
Medium-Chain Acyl-CO-A 4 Oedema, pedal 131,252, Prevention of arterial hypoxemia 296
Dehydrogenase Deficiency 258 Prevention of UTI 244
(MCADD) Oedema, pulmonary 133152, Protein intolerance 46,210
Measles 327-329 252-253, Protein-energy malnutrition 55,56
Meckel`s diverticulum 234 343 Proteinuria 251
Meconium aspiration 7,99 Oesophageal atresia 217 Pruritus 18,31,320,
Meconium ileus 197-198, Omphalocele 234 336
196 Oophoritis 331 Pulmonary atresia 130,142
Meningitis 85-92 Oral ulcer 220,334 Pulmonary haemorrhage 60,376
Meningocele 119-120 Orchitis 31,293, Pulmonary stenosis 138
Meningococcal infection 87,92 330,331 Pyruvate kinase deficiency 355
Mesenteric adenitis 234 Osmotic fragility test 356
Methicillin-resistant 158 Osteomyelitis 220,295, R .
Staphylococcus areus (MRSA) 336 Rabies 86
Methotrexate 224,314 Ostium primum & secundum 135 Radioactive iodine 314
Metronidazole 224 Otitis media 166-167 Rash 335
Microcephaly 7,292,333 Oxygen toxicity 204,375, Rectal prolapse 197,200,
Micturating cystourethrogram 243,246, 378 203
(MCUG) 247,248 Oxygen therapy 378 Reflexes (Primitive) 38,39
Midstream urine (MSU) 241,243 Refractive error 81,100,
Mitochondrial disorder 94,351, P . 297,401
360 Painful crisis 296 Renal failure 235,236,
MMR vaccine 28,30, Painful defecation 229 248,262
327,329 Painful infarcts 296 Renal disorder 235-262
Moraxella caterrhalis 166,189 Painful mouth ulcer 334,343 Respiratory acidosis 367,378
Mosaicism, Down syndrome 76 Painful swelling 331 Respiratory distress 16,164
Multicystic dysplastic kidney 235,237 Painful vesicular rashes 343 Respiratory distress syndrome 60,375-80
(MCDK) Pale urine 368,371 Respiratory failure 68,129,
Mumps 330-331 Pale oily stool 200 379,380
Murmurs 14,131 Paediatrics Advanced Life 68-74 Respiratory infection 163-164
Muscular dystrophy 129 Support (PALS) Respiratory syncytial virus 163,165,
Musculoskeletal disorders Paediatrics Basic Life Support 63-67 166,170,
Abnormal posture 24,35,99, (PBLS) 179,187
102,106 Pancreatitis 250,331 Retinoblastoma 300
Arthritis 150,220 Papilloedema 87,122, Retinopathy of Prematurity 380
Limp 82,102 252,303 Reye's syndrome 94,98
Mutation analysis 197,360 Papules 304,336 Rhesus incompatibility 291,292,
Myasthenia gravis 193 Parainfluenza virus 96,170 353,354
Mycobacterium tuberculosis 89,92,307 Paraldehyde 112 Rheumatic fever 149-154
Mycoplasma pneumoniae 163,187, Paralysis 109,120, Rhinitis 172,181
191,295 295,343 Rhodopsin 57
Myelomeningocele 86,120 Paramyxovirus 327 Rhonchi 170,175,
Myocarditis 150,221, Parotid gland 55,330 181,182,
332,329, Patent ductus arteriosus 137 191
331,336 Pectus carinatum & carinatum 14,17,181, Rickets 57-59
Myopathy 22,23,313 202,396 Rifampicin 32,92,174
Myopia 77,105, Pellagra 57 Rotavirus 305,321
107,396 Pendred's syndrome 344 Rubella 332-333
Penicillin 91,190,265 Russel-silver (dwarf) 399
N . Percentile charts 10
Naevus 127 Peritonitis 230,231, S .
Nasal congestion 175 258,260 Saddle anaesthesia 121
Neck stiffness 97,98,188 Periventricular leukomalacia 60,99,379 Saddle-back fever 319
Necrotising enterocolitis 50,60,364 Pharyngitis 165 Saddle gap 76,84
Neglect 10,46,104, Phenobarbitone 117,357 Salicylates 150,162,
201 Phenylketonuria 4,52 253,337
Nephroblastoma 299 Phototherapy 361-363 Salmonella 205-206,
Nephrotic syndrome 257-262 Physiotherapy 190,198 234,295
Neuropathy, peripheral 57,221 Platelet transfusion 250,292 Scarlet fever 149,321
405
Seizures 109,118 167
Septic shock 87,321 Tonsilitis 163,167
Serology 157,195, Toxic shock syndrome 337
340,342 Transposition of great arteries 143,144
Shingellosis 205,211, Trisomy 21 75-84
224,250 Truncal hypotonia 391
Shock 10,70,319, Truncus arteriosus 13
324,350 Tuberculosis (TB) 89,92,307
Short stature 45,47,77, Twin-twin transfusion syndrome 265,357
281,282
397,400 W .
Sickle cell anemia 295-297 Wegener granulomatosis 253-257
Sleep disturbances 186,388, Werdnig-Hoffmann disease 193
391 Wheezing 182
Spastic diplegia 101 Whooping cough 194-195
Spastic hemiplegia 102 Williams syndrome 401
Spastic monoplegia 102 Wilms` tumour 299,300
Spastic paraplegia 102,393 Wilson disease 18,351
Spastic tetraplegia 102 Wiskott-Aldrich syndrome 286,305
Speech disorder 34,35
Splenomegaly 84,156, X .
295,296, X- linked recessive inheritance 128,256,
368,339 286,355
Spina bifida 120-122
Squint 35,76,300 Y .
Saphylococcal infection 85,163, Yersinia enterocolitica 205,224,
187,190- 234,276,
191,196, 282
337
Status epilepticus 111 Z .
Steven-johnson syndrome 117 Ziehl-Nielson stain 92
Strawberry tongue 160 Zinc deficiency 278
Streptococcus pneumoniae 163,165, Zinc Transporter 8 Ab (ZnT8) 381
187,190
253
Stridor 164,170-
171,192
Sturge-weber syndrome 127
Subacute sclerosing 328
panencephalitis
Subdural haematoma 95
Sulphonamides 355,367
Swallowing difficulty 100,105,
392,394
Sydenham chorea 150
Syphilis 93,275
Systemic lupus erythematosus 252,256
T .
Talipus equinovarus 12
Tantrum 82
Temperature control 62,73,
112,190
Temporal lobe
Sign 27
Seizure 114
Testes
Mass 316
Painless unilateral swelling 307
Stages 2,20
Undescended 392
Testicular
Anomalies 84
Enlargement 4,314
Size 20
Tetralogy of Fallot 141,142
Thalassaemia
α-Thalassaemia 280
β-Thalassaemia 272-283
Toe-heel gait (tiptoe walk) 102
Tonsillectomy 158,166,
406