Tce - Medscape

21/1/2020 https://emedicine.medscape.com/article/1163653-print 21/1/2020 https://emedicine.medscape.
com/article/1163653-print
Abnormal postresuscitation pupillary reactivity: Correlates with a poor 1-year outcome
emedicine.medscape.com
Isolated internuclear ophthalmoplegia secondary to traumatic brainstem injuries: Has a relatively benign prognosis[4]
Cranial nerve (CN) VI palsy: May indicate raised intracranial pressure
Head Injury CN VII palsy: May indicate a fracture of the temporal bone, particularly if it occurs in association with decreased hearing
Hearing loss: Occurs in 20–30% of patients with head injuries[5]
Dysphagia: Raises the risk of aspiration and inadequate nutrition[6]

Updated: Oct 01, 2018
Author: David A Olson, MD; Chief Editor: Stephen A Berman, MD, PhD, MBA Focal motor findings: Include flexor or extensor posturing, tremors and dystonia, impairments in sitting balance, and
primitive reflexes; may be manifestations of a localized contusion or an early herniation syndrome
Overview See Clinical Presentation for more detail.
Diagnosis
Practice Essentials Bedside cognitive testing
Head injury can be defined as any alteration in mental or physical functioning related to a blow to the head (see the image In the acute setting, measurements of the patient's level of consciousness, attention, and orientation are of primary importance.
below). According to the Centers for Disease Control and Prevention (CDC), more than 50,000 individuals die from traumatic
Some patients acutely recovering from head trauma demonstrate no ability to retain new information. Mental status
brain injuries each year in the United States. Almost twice that many people suffer permanent disability. In the United States in
assessments have validated the prognostic value of the duration of posttraumatic amnesia; patients with longer durations of
2013, about 2.8 million emergency department (ED) visits, hospitalizations, or deaths were associated with TBI—either alone or
posttraumatic amnesia have poorer outcomes.[7]
in combination with other injuries.[1, 2]
In the long-term setting, the following bedside cognitive tests can be employed:
Mini-Mental State Examination
Luria "fist, chop, slap" sequencing task: To rapidly assess motor regulation
Antisaccade task: Impaired in patients with symptomatic brain injury; the sensitivity of this test in detecting brain injury
has been questioned[8]
Letter and category fluency: To provide information about self-generative frontal processes.
Untimed Trails B test: Allows further qualitative testing of frontal functioning
Laboratory studies
Sodium levels: Alterations in serum sodium levels occur in as many as 50% of comatose patients with head injuries[9] ;
hyponatremia may be due to the syndrome of inappropriate antidiuretic hormone (SIADH) or cerebral salt wasting;
elevated sodium levels in head injury indicate simple dehydration or diabetes insipidus
Magnesium levels: These are depleted in the acute phases of minor and severe head injuries
Coagulation studies: Including prothrombin time (PT), activated partial thromboplastin time (aPTT), and platelet count;
these are important to exclude a coagulopathy
Blood alcohol levels and drug screens: May help to explain subnormal levels of consciousness and cognition in some
patients with head trauma
Renal function tests and creatine kinase levels: To help exclude rhabdomyolysis if a crush injury has occurred or marked
This 50-year-old woman with epilepsy seized and struck her head. Her initial Glasgow Coma Scale score was 12. Her scan rigidity is present
shows prominent right temporal bleeding. She recovered to baseline without surgery.
Neuron-specific enolase and protein S-100 B: Although earlier studies suggested that elevated serum levels may
correlate with persistent cognitive impairment at 6 months in patients with severe or mild head injuries, current opinion
Signs and symptoms considers these tests no longer useful.[10, 11]
The Glasgow Coma Scale (GCS) is the mainstay for rapid neurologic assessment in acute head injury. Following ascertainment In 2018, a commercially available blood test for mild brain injury was approved by the FDA.[12] This test reportedly
of the GCS score, the examination is focused on signs of external trauma, as follows: identifies 98% of patients with abnormal head CT scans.
Bruising or bleeding on the head and scalp and blood in the ear canal or behind the tympanic membranes: May be clues Imaging studies
to occult brain injuries
Computed tomography scanning: The main imaging modality used in the acute setting
Anosmia: Common; probably caused by the shearing of the olfactory nerves at the cribriform plate[3]
https://emedicine.medscape.com/article/1163653-print 1/39 https://emedicine.medscape.com/article/1163653-print 2/39

21/1/2020 https://emedicine.medscape.com/article/1163653-print 21/1/2020 https://emedicine.medscape.com/article/1163653-print
Magnetic resonance imaging: Typically reserved for patients who have mental status abnormalities unexplained by CT Gross structural changes in head injury are common and often obvious both on autopsy and conventional neuroimaging. The
scan findings skull can fracture in a simple linear fashion or in a more complicated depressed manner, in which bone fragments and pushes
beneath the calvarial surface. In patients with mild head injury, a skull fracture markedly increases the chance of significant
Electroencephalography intracranial injury.
Although certain electroencephalographic patterns may have prognostic significance, considerable interpretation is needed, and Both direct impact and contrecoup injuries, in which the moving brain careens onto the distant skull opposite the point of impact,
sedative medications and electrical artifacts are confounding. The most useful role of electroencephalography (EEG) in head can result in focal bleeding beneath the calvaria. Such bleeding can result in an intracerebral focal contusion or hemorrhage as
injuries may be to assist in the diagnosis of nonconvulsive status epilepticus. well as an extracerebral hemorrhage. Extracerebral hemorrhages are primarily subdural hemorrhages arising from tearing of
bridging veins, but epidural hemorrhages from tearing of the middle meningeal artery or the diploic veins are also common.
See Workup for more detail. Occasionally, subdural hemorrhages can result from disruption of cortical arteries. This type of subdural hemorrhage is rapidly
progressive and can occur after trivial head injury in elderly patients.[15]
Management
One study of CT images from 753 patients with severe head injury from the National Institute of Health Traumatic Coma Data
Intracranial pressure Bank in the United States found evidence of intracranial hemorrhagic lesions in 27%. Traumatic subarachnoid hemorrhage was
even more frequent and occurred in 39% of patients. Furthermore, diffuse cerebral edema also was present in 39%. Cerebral
If the intracranial pressure rises above 20-25 mm Hg, intravenous mannitol, cerebrospinal fluid drainage, and hyperventilation edema can be unilateral or diffuse and can occur even in the absence of intracranial bleeding. Severe brain edema probably
can be used. If the intracranial pressure does not respond to these conventional treatments, high-dose barbiturate therapy is occurs more commonly in children than in adults.[16]
permissible.[13]
Neuronal loss is also important. A recent pathological study found that quantitative loss of neurons from the dorsal thalamus
Another approach used by some clinicians is to focus primarily on improving cerebral perfusion pressure as opposed to correlated with severe disability and vegetative state outcomes in patients with closed head injuries.[17]
intracranial pressure in isolation.
Finally, axonal injury increasingly has been recognized as a structural sequela of brain injury. The use of amyloid precursor
Decompressive craniectomies are sometimes advocated for patients with increased intracranial pressure refractory to protein staining has resulted in increased recognition of this form of injury. Using this technique, researchers have readily
conventional medical treatment. identified axonal injury in patients with mild head injury. Interestingly, a prominent locus of axonal damage has been the fornices,
which are important for memory and cognition.[18] More severe and diffuse axonal injury has been found to correlate with
Hypertonicity vegetative states and the acute onset of coma following injury.[19]
Dantrolene, baclofen, diazepam, and tizanidine are current oral medication approaches to hypertonicity. Baclofen and tizanidine
are customarily preferred because of their more favorable side-effect profiles. Neurochemical changes
Subdural hematomas After traumatic brain injury, the brain is bathed with potentially toxic neurochemicals. Catecholamine surges have been
documented in the plasma (higher catecholamine levels correlated with worse clinical outcomes) and in the cerebrospinal fluid
Traditionally, the prompt surgical evacuation of subdural hematomas was believed to be a major determinant of an optimal (CSF) of patients with head injuries (higher CSF 5-hydroxyindole acetic acid (HIAA), the serotonin metabolite, correlated with
outcome. However, research indicates that the extent of the original intracranial injury and the generated intracranial pressures worse outcomes).[20] In addition, the excitotoxic amino acids (ie, glutamate, aspartate) initiate a cascade of processes
may be more important than the timing of surgery. culminating in an increase in intraneuronal calcium and cell death. Researchers using a microdialysis technique have correlated
high CSF levels of excitotoxic amino acids with poor outcomes in head injury.[21]
See Treatment and Medication for more detail.
Although neuroprotective strategies employing antiexcitotoxic pharmacotherapies were effective in diminishing the effects of
experimental brain injuries in laboratory animals, clinical trials in humans generally have been disappointing.[22] These failures
have prompted development of more complex models of neuronal injury and cell death. Recently, researchers have
demonstrated that although certain types of glutamate antagonists may protect against acute cell death, they potentiate slowly
progressive neuronal injury in experimental rodent models. Still others have found that low-dose glutamate administered before
Background brain injury is somehow neuroprotective. Such dose and timing effects are only beginning to be understood.[23]
Prostaglandins, inflammatory mediators produced by membrane lipid breakdown, are also elevated dramatically in the plasma
Head injury can be defined as any alteration in mental or physical functioning related to a blow to the head. Loss of of patients with moderate-to-severe head trauma during the first 2 weeks after injury. Patients with higher prostaglandin levels
consciousness does not need to occur. The severity of head injuries is most commonly classified by the initial postresuscitation had significantly worse outcomes than those with more modest elevations. Furthermore, levels of a thromboxane metabolite, a
Glasgow Coma Scale (GCS) score, which generates a numerical summed score for eye, motor, and verbal abilities. potent vasoconstricting prostaglandin, were elevated disproportionately.[24] Such a process may underlie posttraumatic
Traditionally, a score of 13–15 indicates mild injury, a score of 9-12 indicates moderate injury, and a score of 8 or less indicates vasospasm, which has been documented in some, but not all, transcranial Doppler studies of patients with closed head injuries,
severe injury. In the last few years, however, some studies have included those patients with scores of 13 in the moderate even in patients without traumatic subarachnoid bleeds.[25] Delayed clinical deterioration could represent ischemia from such
category, while only those patients with scores of 14 or 15 have been included as mild.[14] Concussion and mild head injury are vasospasm, particularly in younger patients.[26]
generally synonymous.
Head injury also causes the release of free radicals and the breakdown of membrane lipids. Panels of plasma metabolites
Research on head injury has advanced considerably in the last decade. As is typical of many endeavors, these efforts have related to fatty acid and lipid breakdown products have been found to be elevated in mildly concussed athletes compared to
exposed the complexity of this condition more deeply and have helped researchers and physicians to abandon crude controls.[27]
simplifications. This review concentrates primarily on current developments in the diagnosis and management of closed head
injuries in adults. Other inflammatory biomarkers have yielded complex and contradictory results. However, overall some initial inflammation may
promote recovery, but prolonged or high levels of inflammation could be detrimental.[28, 29] For example, in severely brain-
injured patients a group of CSF inflammatory mediators including intraleukin 6 and 8 discriminated between good versus poor 6-
month outcomes with higher levels of these inflammatory mediators occuring in those with poorer outcomes.[30]
In addition to structural and chemical changes, gene expression is altered following closed head injury. Genes involving growth
Pathophysiology factors, hormones, toxin-binders, apoptosis (programmed cell death), and inflammation have all been implicated in rodent
models. For example, in a mouse model of head injury, elevated levels of the transcription factor p53 were found. p53
translocates to the nucleus and initiates apoptosis or programmed cell death. Such a process could account for the delayed
Structural changes neuronal loss seen in head injuries.[31] Furthermore, in humans, differential activation of inflammatory regulatory genes has

been associated with the worse outcomes observed in elderly patients with closed head injuries compared to their younger A study of intentional head injury from Charlotte, North Carolina, found minority status was a major predictor of intentional head
counterparts.[32] injury, even after controlling for other demographic factors.[46] Furthermore, worse clinical outcomes have been described for
African American children with moderate-to-severe head injuries compared with their white counterparts.[47]
Secondary insults
Sex
Hypotension and hypoxia cause the most prominent secondary trauma-induced brain insults. Both hypoxia and hypotension had
adverse impacts on outcomes of 716 patients with severe head injuries from the Traumatic Coma Data Bank in the United Men in the United States are nearly twice as likely to be hospitalized with a brain injury than women. This male predominance is
States. Efforts to limit hypoxic injury with in-field intubation have been unsuccessful. Indeed, a multicenter study of 4098 patients found worldwide.
with severe traumatic brain injury found that in-field intubation was associated with a dramatic increase in death and poor long-
term neurologic outcome, even after controlling for injury severity.[33] More current epidemiologic research supports the lack of Age
benefit of early intubation.[34]
Approximately half of the patients admitted to a hospital for head injury are aged 24 years or younger. The rates of emergency
In the Trauma Coma Data Bank study, hypotension was even more significant than hypoxia and, by itself, was associated with a room visits for the head-injured elderly are more than 3 times higher for those over 84 years of age compared to those between
150% increase in mortality rate. Systemic hypotension is critical because brain perfusion diminishes with lower somatic blood 65 to 74 years of age.[48]
pressures. Brain perfusion (ie, cerebral perfusion pressure) is the difference between the mean arterial pressure and intracranial
pressure. The intracranial pressure is increased in head injury by intracranial bleeding, cell death, and secondary hypoxic and
ischemic injuries. Accordingly, another recent study reported that death and increased disability outcomes correlated with the
durations of both systemic hypotension and elevated intracranial pressures.[35]
Presentation
Severe anemia is often coexistent with head injuries, but blood transfusions have been associated with increased mortality and
complications among 1250 ICU-admitted patients with brain injuries. This relationship held even after controlling for the degree
of anemia.[36] Similarly, adverse thromboembolic events occured among 200 severely head-injured patients treated wtih
erythropoetin and transfusions.[37]
History
Finally, posttraumatic cerebral infarction occurs in up to 12% of patients with moderate and severe head injuries and is
associated with a decreased Glasgow Coma Scale, low blood pressure, and herniation syndromes.[38] History in most patients with head injury should be self-evident. However, consider trauma with intracerebral pathology in any
patient with a coma of unknown etiology.
In the acute setting, the patient may be comatose or confused, and witnesses to the accident or injury are of obvious and
crucial importance.
Elicit the type and mechanisms of the injury, as these may have prognostic value. Patients sustaining a head injury from
Epidemiology an assault or from being struck with a falling object have a markedly greater likelihood of poorer vocational outcomes
than patients sustaining the more common acceleration/deceleration injuries, presumably because the former injury
Frequency types entail greater axonal damage.[46]
United States Ascertain whether the patient lost consciousness. Even a questionable loss of consciousness can be a marker of severe
neurological injury.
In the United States, 2.8 million individuals per year incur a head injury. Of these injuries, 75% are classified as mild. Between
1998 and 2000, the incidence of mild traumatic brain injury was 503 cases per 100,000 persons, with a doubling of this The presence of prior head injuries, particularly prior concussive episodes in sports, can indicate the potential for more
incidence in Native Americans and children. Between 2007 and 2012, brain injury hospitalizations, death, and emergency severe long-term outcomes.
department visits increased from 640 to 890 cases per 100,000 persons in the United States.[1, 2]
Remote or active drug or alcohol use may raise the risk of intracranial bleeding and cloud the mental status assessment.
In 2003, elderly persons with head injuries exhibited a doubling in hospitalizations and deaths compared to the national average.
[39] This trend has persisted with Canadian, European, and US data demonstrating an increased frequency and severity of Present anticoagulant therapy is also worrisome.
traumatic brain injury in the elderly, primarily secondary to falls, while motor vehicular causes have decreased.[40, 41, 42, 2]
Among high school athletes with head injuries, on-field “dizziness,” but not objective balance impairments, at the time of
International concussion significantly correlated with prolonged return to play compared to athletes with head injuries who did not
experience this symptom.[49]
Head injury data are difficult to compare internationally for multiple reasons, including inconsistencies and complexities of
diagnostic coding and inclusion criteria, case definitions, ascertainment criteria (for example, hospital admissions versus door- Carefully consider past psychiatric disease and a premorbid history of headaches.
to-door surveys), transfers to multiple care facilities (for example, patient admissions may be counted more than once), and
regional medical practices, such as the recent development in the United States of more outpatient, as opposed to inpatient,
services for those with mild head injuries. Adding to this complexity is the finding that some individuals with cognitive and
emotional sequelae from mild head injury may not establish the casual connection between their injury and its consequences.
Such patients may not seek treatment and may not be expressed in official demographic data.[43, 44]
Physical
Despite such obstacles, a recent meta-analysis extrapolated head injury rates to total population estimates and found that
Southeast Asian and Western Pacific nations carried the heaviest global head injury burden.[45]
Elemental neurologic examination
Mortality/Morbidity See the list below:
According to the CDC, about 56,000 individuals die from traumatic brain injuries each year in the United States. Almost twice The Glasgow Coma Scale (GCS) is the mainstay for rapid neurologic assessment in acute head injury. Both initial and
that number suffer permanent disability.[2] worst GCS postresuscitation scores have correlated significantly with 1-year outcomes following severe head injury.
Race
Following ascertainment of the GCS score, focus the examination on signs of external trauma. Bruising or bleeding on In the long-term setting, bedside cognitive tests are employed to help distinguish damaged and spared realms of
the head and scalp and blood in the ear canal or behind the tympanic membranes may be clues to occult brain injuries. cognitive functioning.
Also consider coexistent cervical spine and other systemic injuries.
Even though most of these tests are not quantitative, they readily provide the examiner with immediate
Anosmia is common and probably is caused by the shearing of the olfactory nerves at the cribriform plate.[3] If information to help in diagnosis and therapy.
accompanied by rhinorrhea, a CSF leak with the attendant risk of ascending meningitis must be excluded.[50]
One standardized test that can be administered easily is the Mini-Mental State Examination. Although this test
Abnormal postresuscitation pupillary reactivity correlates with a poor 1-year outcome. In fact, a 2006 study reported no disproportionately emphasizes left hemisphere functioning, one study has documented that 23% of patients with
survivors among 173 head-injured patients who presented with bilaterally fixed and dilated pupils and a GCS score of mild head injuries score less than 24 out of 30 points when assessed with this instrument 1 year after injury.[57]
3[51] , while other researchers have demonstrated that only 9% of 92 such patients attained good outcomes[52] . A
unilaterally dilated pupil with or without evidence of ipsilateral cranial nerve (CN) III paralysis, such as ptosis or impaired Although all cognitive domains should be assessed, the investigation of frontal or executive systems assumes even
ocular motility, may indicate impending herniation. greater importance in the long-term setting. While examining mnemonic, visual spatial, and language functioning, the
quality of the patient's responses, whether perseverative or impulsive, socially sanctioned or grossly inappropriate, is also
Isolated internuclear ophthalmoplegia secondary to traumatic brainstem injuries has been described and has a relatively important to observe and document.
benign prognosis.[4]
Motor regulation can be assessed rapidly using the Luria "fist, chop, slap" sequencing task.
CN VI palsies may indicate raised intracranial pressure. CN VII palsy, particularly in association with decreased hearing,
may indicate a fracture of the temporal bone. An antisaccade task, in which the patient looks away from the offered visual stimulus, recently has been shown to be
impaired in patients with symptomatic brain injury compared to controls, although the sensitivity of this test in detecting
Hearing loss is also frequent with sensory neural loss occurring in 20-30% of patients with head injuries. Low-frequency brain injury has been questioned.[8]
loss typically improves after 1 year.[5]
Letter fluency, in which the patient names as many words as possible beginning with a specific letter in 1 minute, and
Dysphagia raises the risk of both aspiration and inadequate nutrition.[6] category fluency, in which the patient names as many items as possible in a certain category in 1 minute, provide further
information about self-generative frontal processes.
Focal motor findings may be manifestations of a localized contusion or, more ominously, an early herniation syndrome.
An untimed Trails B test, in which the patient alternates between number and letter sequences, allows further qualitative
Flexor or extensor posturing obviously implies extensive intracranial pathology or raised intracranial pressure. In testing of frontal functioning. Be cautious in overinterpreting this or any single test. Malingerers have been shown to fake
the chronic phase, motoric manifestations typically include spasticity or, more unusually, akinesia and rigidity. performance errors on the Trails B.[58]
Tremors and dystonia recede with time, but these still can affect as many as 12% of survivors of severe head
injury 2 years after the initial trauma.[53]
Although postural stability and balance depend on inputs from multiple components of the nervous system,
impairments in sitting balance alone have been demonstrated to be predictive of poor functional abilities upon
discharge from rehabilitation.[54] Causes
Primitive reflexes, despite their presence in some healthy elderly patients, are useful and when multiple can Road accidents involving motor vehicle drivers and occupants, cyclists, and pedestrians are the main risk factor for head
correlate with cognitive deficits. injuries. Assaults in economically depressed regions and during wartime are other major risk factors. Athletic participation,
especially football and soccer, is another important cause of these injuries.
Bedside cognitive testing
Falls cause head injuries in elderly patients and children, occasionally with catastrophic results. The incidence of fall-related
See the list below: traumatic brain injury has been increasing in the United States and in 2013 resulted in 12,015 deaths and 91,470
hospitalizations in the elderly.[2]
In the acute setting, measurements of the patient's level of consciousness, attention, and orientation are of primary
importance. Aphasia obviously implicates localized pathology. Blast injuries from incendiary devices can cause head trauma and primarily occur in soldiers, although even civilian tire
explosions have been implicated.[59] While the energy from the blast can directly impact the cranium and be transferred to the
Lucid intervals are not unusual. Of 838 patients with severe head injury in one study, 25% talked at some point between brain, some researchers have hypothesized that systemic blood vessels may actually transmit the shock waves.[60] Current
the trauma onset and their deterioration into coma. Although 81% of these patients had a focal lesion, 19% exhibited clinical studies, however, have failed to identify a unique pattern of neuropsychologic deficits in patients who have incurred such
diffuse brain swelling, and approximately one third of these patients demonstrated coexistent subarachnoid hemorrhage blast injuries.[61]
or other nonfocal intracranial bleeding. Such diffuse swelling was much more likely in children and adolescents than
adults.[55] Anticoagulants and antiplatelet medications, such as aspirin, raise the risk of intracranial bleeding with even trivial head injuries.
[62] For example, among elderly patients with head injuries, clopidogrel use has been associated with a 15 times greater
Some patients acutely recovering from head trauma demonstrate no ability to retain new information. mortality compared with patients not taking antithrombotics.[63] Head-injured warfarin users, compared to direct oral
anticoagulant users, exhibited a greater mortality and greater need for neurosurgical procedures.[64] Curiously, another study
This inability to lay down new memories after a head injury originally was labeled posttraumatic amnesia. documented counterintuitively that in patients with mild head injury, antiplatelet agent use more than doubled the risk of
intracranial bleeding compared to anticoagulant use.[65]
The patient's subjective estimate of his or her first recollection of events following the head injury defined the
termination of this period. Alcohol use raises the risks of incurring a head injury. Perhaps because it may impede excitotoxicity, alcohol use at the time of
injury may actually decrease the likelihood of a poor outcome.
These subjective estimates have yielded in recent years to prospective serial mental status assessments. These
mental status assessments have validated the prognostic value of the duration of posttraumatic amnesia; patients A newer study of intentional head injuries reported that patients consuming alcohol had higher initial GCS scores.[46] Another
with longer durations of posttraumatic amnesia have poorer outcomes.[7] study of patients with apparently trivial injuries (patients either were found down or fell from heights < 10 ft) found that outcomes
were better in patients who were severely intoxicated (blood alcohol levels >200 mg/dL). Methamphetamine use has also been
More recent work has suggested that posttraumatic amnesia is somewhat of a misnomer. Because severe shown to reduce mortality in severe head injury.[66] More recently, patients with severe brain injuries and high blood alcohol
inattention in the postinjury state primarily prevents retention of new information, "posttraumatic confusional state" levels (≥ 0.08 mg/L) exhibited a significantly lesser mortality compared with patients with lower levels or the absence of alcohol
may be a more accurate descriptor.[56] in their blood.[67]

The presence of even one of the alleles for the APOE4 genotype may increase the risk of a poor outcome. Laboratory Studies
An earlier study reported that patients who are homozygous or heterozygous for the APOE4 allele have an almost 14-
times greater likelihood of a poor outcome after head injury than those with other APOE genotypes.[68] See the list below:
Football players and boxers with an APOE4 allele are at greater risk for posttraumatic cognitive problems than APOE4 - Alterations in serum sodium levels are critical and occur in as many as 50% of comatose patients with head injuries.[9]
negative athletes.[69] Similarly, possesion of an APOE4 allele was associated with worse verbal memory after even mild
Hyponatremia may be due to the syndrome of inappropriate antidiuretic hormone (SIADH) or cerebral salt
head injuries compared to other APOE genotypes.[70]
wasting. Both syndromes involve decreased serum sodium level in the face of increased urinary sodium losses.
Other studies have called these APOE4 associations into question, but a 2008 meta-analysis as well as a 2015 one has
Unlike SIADH, in which the patient is euvolemic, cerebral salt wasting typically occurs with volume depletion and
supported these observations.[71, 72]
is caused by the release of a natriuretic hormone. Some researchers suggest that this natriuretic hormone can be
Genes regulating the interleukin, dopamine, and apoptotic systems as well as genes associated with angiotensin measured readily in the serum because it binds to digoxin antibodies and produces a false-positive test for digoxin
converting enzyme and calcium channel polymorphisms have all been implicated in head injury outcomes.[73] For in patients who are not receiving this medication.[76] The incidence of cerebral salt wasting ranges from 1% to
example, a polymorphism in the dopaminergic alpha-synuclein promoter gene has been correlated with poor memory in 35% of head-injured patients.[77]
mildly head-injured adults.[74] Furthermore, a polymorphism of the IL-6 receptor tripled the risk of concussions in
Elevated sodium levels in head injury indicate simple dehydration or diabetes insipidus.
athletes over those lacking this allelic variant.[75] Other genetic determinants of head injury will undoubtedly surface with
further research. Magnesium is depleted in the acute phases of both minor and severe head injuries.
Because this cation blocks the excitotoxic response and functions as an antioxidant, careful monitoring of
magnesium may improve outcomes.
DDx Early administration of magnesium has attenuated experimental brain injury in rats.[78]
Coagulation studies, including prothrombin times (PT), activated partial thromboplastin times (aPTT), and platelet counts,
Differential Diagnoses are important to exclude a coagulopathy. A limited trauma-induced coagulopathy as evidence by prolonged PT levels has
been found in patients hospitalized for head injury, but PT levels return to normal after 12 hours and the clinical
Acute Management of Stroke importance of this prolongation is currently unclear.[79]
Acute Subdural Hematoma in the ED Blood alcohol levels and drug screens are important because positive results may help explain subnormal levels of
consciousness and cognition in some patients with head trauma.
Alzheimer Disease Imaging
Obtain renal function tests and creatine kinase levels to help exclude rhabdomyolysis if a crush injury has occurred or
Anterior Circulation Stroke marked rigidity is present.
Brain Metastasis Older studies have demonstrated that elevated serum levels of neuron-specific enolase and protein S-100 B obtained
within 24 hours of head injury correlated with persistent cognitive impairment at 6 months in patients with severe or mild
Cerebral Aneurysms head injuries.[11] However, neuron-specific enolase and S-100 B elevations have even been correlated with frequent
"headings" of balls during soccer playing.[80] Unfortunately, even vigorous soccer training alone increases serum S-100
Confusional States and Acute Memory Disorders
B as much as playing and heading does, calling into question the specificity of S-100 B as a biomarker of head injury.[81]
Emergent Management of Subarachnoid Hemorrhage Furthermore, a 2018 review of neuron-specific enolase in mild head injuries found this marker to be poorly correlated
with both symptoms and measures of cognitive functioning.[82]
Epileptic and Epileptiform Encephalopathies
More recently, utilizing a unique serum immunoassay, elevation of neurofilament light (an axonal breakdown product)
Frontal Lobe Syndromes measured on day 6 post-injury identified those hockey players with perisistent post-concussive symptoms from those
who were able to return to play.[83]
Generalized Tonic-Clonic Seizures
Although other research on patients with mild closed head injuries has found that increased glial fibrillary acid protein
Hydrocephalus (GFAP) levels correlated with abnormal neuroimaging, both GFAP and S100B failed to significantly correlate with clinical
outcomes.[84] Nevertheless, combining serum elevations of GFAP along with heart fatty acid binding protein predicated
Prion-Related Diseases abnormal head CT findings in mildly head injured (GCS 15) patients,[85] and the FDA has recently approved a blood
test for head injury combining GFAP and a ubiquitin derivative.[12]
Psychiatric Disorders Associated With Epilepsy
Subdural Empyema
Temporal Lobe Epilepsy

Imaging Studies
Workup
CT scanning
Workup Computerized tomography (CT) is the main imaging modality used in the acute setting.
Controversy exists as to whether all patients with mild head injuries should have neuroimaging. In general, patients with any
loss of consciousness should undergo CT scanning.

Some researchers have established clinical criteria to identify those patients who are most likely to have abnormal scans. For
example, in a group of 909 consecutive patients who had experienced a mild head injury with a transient loss of consciousness,
yet scored a full 15 on their initial GCS, all 57 (6%) patients with abnormal CT scans were identified by the presence of any one
of the following clinical features: age older than 60 years, headaches, vomiting, alcohol or drug intoxication, trauma above the
clavicles, memory problems, or seizures.[86] More complicated criteria have been invoked to predict abnormal head CT scans
even without loss of consciousness; however, these rules are cumbersome.[87] Further validation of such imaging rules is
needed. In the specific case of the elderly with syncope and a subsequent fall, dramatically increased rates of CT abnormalities
have been observed.[88]
Repeat CT is needed, of course, when clinical deterioration occurs. The need for routine repeat head CT is unclear. A 2006
multistudy review found neurosurgical interventions resulting from a repeat CT scan occurred in 0-54% of patients.[89]
In addition, emergent brain imaging may be performed for nonmedical reasons. A 10-year study of elderly women with closed
head injuries revealed that in general, emergency department physicians who practice in states with tort reform laws ordered
significantly less neuroimaging studies than those physicians who practice in states without such legislation.[90]
See the images below.
This 40-year-old woman was anticoagulated with warfarin (Coumadin) and fell out of her hospital bed. She subsequently died.
Her CT scan shows an obvious right subdural hematoma with mass effect.
MRI
Magnetic resonance imaging (MRI) is typically reserved for patients who have mental status abnormalities unexplained by CT
scan findings. MRI has been demonstrated to be more sensitive than CT scanning, particularly at identifying nonhemorrhagic
diffuse axonal injury lesions.
MRI imaging has shown degeneration of the corpus callosum following severe head injuries with axonal damage in adults and
children.[91]
Furthermore, increased total lesion volume on fluid-attenuated inversion-recovery (FLAIR) MRI images has been demonstrated
to correlate with poor clinical outcomes as well.[92]
Remember that white matter hyperintensities in patients with head trauma may recede when initial MRI scans are compared
with those obtained in the months following the injury.
This 50-year-old woman with epilepsy seized and struck her head. Her initial Glasgow Coma Scale score was 12. Her scan
See the image below.
shows prominent right temporal bleeding. She recovered to baseline without surgery.

convulsive and nonconvulsive seizures in 22% of their subjects.[101] more recent investigations have found subclinical
seizures in only 3.8% of brain-injured patients monitored with continuous EEG.[102]
A 2012 study reported that severe slowing on continuous EEG monitoring related to delta waves or burst suppression
patterns is associated with poor outcomes at 3 and 6 months in patients with traumatic brain injuries.[103]
A meta-analysis of the prognostic ability of somatosensory evoked potentials in predicting outcomes in patients with
severe brain injuries examined 44 studies and found that if patients with focal lesions, recent decompressive
craniotomies, or subdural and extradural fluid collections were excluded, bilaterally absent somatosensory evoked
potentials correctly predicted unfavorable outcomes in 99.5% of patients.[104]
Histologic Findings
Although a comprehensive discussion of the histology of traumatic brain injury is beyond the scope of this article, several
important newer immunohistochemical techniques have further elucidated the pathophysiology of brain injury.
Beta-amyloid precursor protein is made in the neuron and transported to the axon. The shear forces incurred in head
injury damage the axon and beta-amyloid accumulates proximal to the injury. Special immunohistochemical stains for this
substance have detected beta-amyloid accumulation as early as 35 minutes after severe head injuries in humans.[105]
As mentioned previously, apoptosis (programmed cell death) is initiated in brain trauma and may account for delayed
loss of functioning. Using a combination of enzymatic and immunohistochemical marking, the DNA fragmentation
This 35-year-old man was in a motor vehicle accident. His initial Glasgow Coma Scale score was 7. He had left hemiparesis. accompanying apoptosis has been documented in human trauma patients and occurs from 2 hours to 12 days after the
He recovered orientation to temporal parameters after 1 week, but he remained disinhibited and hemiparetic (although able to initial injury.[106]
ambulate). His MRI shows a diffusion-weighted hyperintensity in the right posterior internal capsular limb. This was attributed
to an axonal injury. (An embolic workup for stroke was unremarkable, and no dissection was discerned on a carotid Doppler Chronic repetitive head injuries in athletes results in a tauopathy, which was previously known as dementia pugilistica (it
study.) is not confined to boxers alone). Tau reactive neurofibrillary tangles and astrocytic tangles accumulate primarily in the
frontal and temporal cortices in irregular patches, preferentially occupying the depths of sulci.[107] In afflicted patients,
initial psychiatric symptoms of depression and behavioral dyscontrol progress to a debilitating dementia.[108] This
Diffusion tensor imaging may document axonal pathologies in patients with head injury even when conventional MRI scans are syndrome is now known as Chronic Traumatic Encephalopathy (CTE). Indeed, fragments of tau have been identified in
unremarkable. For example, diffusion tensor imaging has identified impaired water diffusion indicating white matter tract the plasma of concussed hockey players, offering yet another serum biomarker of closed head injury.[109]
disruption in patients with mild head injuries whose MRI scans were normal. Cortical projection fibers were frequently abnormal,
and using an innovative fiber tracking methodology, actual disruption of cortical projection fibers could be visualized in 19% of
fiber groups studied.[93] Similarly, attention impairments in patients with mild head injuries have recently been correlated with
diffusion abnormalities in cortical projection fibers.[94] Furthermore, utilizing this methodology, aggresive behavior in mildly
head injured patients has been correlated with reduced white matter in the corpus callosum.[95] Finally, in severe head injuries, Treatment
reduced track length and reduced track number have correlated with a worse 6-month mortality.[96]
Functional imaging and MRI spectroscopy may have eventual clinical utility. At present, they are promising research tools.
Behavioral disorders, memory, and executive dysfunction correlated with abnormalities of cingulate gyrus metabolism in 13 Medical Care
patients with severe head injuries who underwent resting 18F-fluorodeoxyglucose positron emission tomographic (PET) imaging
and a battery of neuropsychological tests.[97] A more recent study found that while only 34% of CT results were abnormal in 92 Acute management
patients with mild head injury, 63% of SPECT results demonstrated regions of hypoperfusion within 72 hours of the trauma.
Frontal hypoperfusion predominated in adults.[98] In the setting of acute head injury, give priority to the immediate assessment and stabilization of the airway and circulation.
Despite the fact that prehospital intubation has become common, at least one study has reported a higher rate of mortality in
Proton magnetic resonance spectroscopy of frontal white matter that appears normal on MRI has shown a decrease in neuronal
patients intubated in the field than in those intubated in the hospital setting. In this study, however, more critically ill patients
N-acetylaspartate spectra and an increase in choline spectra in patients with head injuries indicating neuronal loss.[99, 100]
required in-field intubation.[33]
Following stabilization, direct attention to prevention of secondary injury. Keep mean arterial pressures above 90 mm Hg; arterial
saturations should be greater than 90%. Urgent CT scanning is a priority.
Next, focus attention on reducing intracranial pressure, since elevated intracranial pressure is an independent predictor of poor
Other Tests outcome. If the intracranial pressure rises above 20-25 mm Hg, intravenous mannitol, CSF drainage, and hyperventilation can
be used. Hypertonic saline has also been used in lieu of mannitol to lower intracranial pressure, but a recent meta-analysis
EEG is of limited usefulness in patients with head injuries. found no evidence of diminished mortality or improved ICP control with this treatment.[110] More definitive studies are obviously
needed.[111] If the intracranial pressure does not respond to these conventional treatments, high-dose barbiturate therapy is
Although certain EEG patterns may have prognostic significance, considerable interpretation is needed, and sedative permissible, despite the fact that no evidence currently suggests that barbiturate treatment actually improves outcomes. (Its
medications and electrical artifacts are confounding. blood pressure–lowering effects may be detrimental.)[13]
The most useful role of EEG in head injuries may be to assist in the diagnosis of nonconvulsive status epilepticus. Interestingly, a 2008 study utilizing the National Trauma Data Bank retrospectively uncovered a 45% reduction in survival in
Although a landmark study of continuous EEG monitoring in patients hospitalized with traumatic brain injury had found patients who underwent intracranial pressure monitoring.[112] These results had been called into question because of a dearth
of clinical and neuroimaging data, but a 2012 prospective study of 2134 patients with severe traumatic brain injury found Although promising in rodents, in a recent pair of randomized, controlled multicenter studies, the neurosteroid progesterone
improved 2-week survival in patients who underwent ICP monitoring compared to those who were not monitored. Nevertheless, showed no beneficial effect on functional outcomes in patients with acute traumatic brain injury.[132, 133, 134, 135]
the non-monitored patients may have had a more grave prognosis to start with because they were significantly older and more
likely to have had pupillary abnormalities, factors which could have impacted the treating physicians' decision to implement ICP The first trial, the double-blind PROTECT (Progesterone for the Traumatic Brain Injury, Experimental Clinical Treatment) III study
monitoring.[113] in patients with severe to moderate acute traumatic brain injury, found no significant difference in favorable outcomes between
treatment and placebo groups; the trial was halted after enrollment of 882 of 1140 planned participants.[132] Subjects in the
Another approach used by some clinicians is to focus primarily on improving cerebral perfusion pressure as opposed to progesterone group had higher rates of phlebitis or thrombophlebitis than those in the placebo group. In the second study,
intracranial pressure in isolation. One study reported that 80% of patients with severe head injuries experienced recoveries with SYNAPSE (the Study of a Neuroprotective Agent, Progesterone, in Severe Traumatic Brain Injury), 1195 patients with severe
no or little disability after volume expansion, mannitol, CSF drainage, and vasopressors were used to maintain a cerebral traumatic brain injury were assigned to receive either progesterone or placebo.[133] Similar rates of favorable outcomes and
perfusion pressure of at least 70 mm Hg.[114] Other studies have found higher perfusion pressures were associated with more mortality were observed in the two groups.
complications and have recommended maintaining a cerebral perfusion pressure of 50-70 mm Hg.[115]
Experimental brain injury creates permeability in mitochondrial membranes, which contributes to cell death by causing calcium
The question whether saline or albumin fluid resuscitation would maximize cerebral perfusion pressure and lead to improve effluxes and energy depletion. Cyclosporin inhibits mitochondrial permeability and has been used in a phase II study of patients
outcomes lead to a large, double-blind, randomized controlled study of 460 patients with Glasgow Coma Scale scores < 13 who with traumatic brain injuries. Further trials are planned.[136]
also had abnormal head CT scan results. A post-hoc 2-year follow-up demonstrated increased mortality in those receiving
albumin as opposed to saline.[116] More conventional agents have also included propranolol in a large, non-randomized prospective trial. When initiated within the
first 24 hours in patients with moderate to severe head injuries, propranolol significantly reduced mortality, presumable by
Although hypothermic therapy initially appeared promising, and despite the fact that hypothermia decreases intracranial blocking the catecholamine surge that accompanies the initial injury.[137] A recent randomized trial of erythropoetin also
pressure, a large randomized study of 392 patients with head injuries recently demonstrated that hypothermic therapy does not showed promising effects with 33% of treated severely head-injured patients exhibiting a good recovery compared to only 13%
improve outcomes. In addition, a post-hoc analysis found that the rewarming of patients with head injury who arrived in the of controls.[138]
emergency department already hypothermic was likely detrimental.[117] Furthermore, a current review of 23 randomized,
controlled trials concluded that this therapy was of no benefit.[118] Cannabinoids also protect against excitotoxicity, but disappointingly, in a recent phase 3 trial, dexanabinol, a weak N -methyl-D-
aspartic acid (NMDA) antagonist, showed no efficacy in outcome improvement when given within 6 hours to patients with severe
Although acute hypothermic treatment has been found to worsen outcomes in patients with diffuse head injuries, it may improve closed head injuries.[139] More encouraging but less rigorous was a retrospective analysis of traumatic brain-injured
outcomes in patients with surgically-evacuated hematomas. This indicates a potential benefit in this subgroup; however, further patients that found decreased mortality among those patients with THC in their urine compared to those without this substance.
prospective studies are needed.[119] Current opinion holds that therapeutic hypothermia administration should be reserved only [140]
for clinical trials.[120]
Rosuvastatin given in the acute phase of moderate head injury significantly reduced amnesia in a double-blind placebo-
Head injury induces a hypermetabolic state and early nutritional interventions may be as critical as cerebral perfusion pressure. controlled study of 34 patients.[141] Other research has retrospectively found that statin use was associated with a decreased
Parental or enteral feedings reduced mortality by at least 50% in one study when given early in the course of severe head injury. mortality in a large, 100,515 patient cohort of brain injured elderly.[142] Furthermore, a randomized prospective trial of
[121] atorvastatin demonstated improved functional outcomes at 3 months post-injury in patients with brain contusions who were
treated with a mere 10-day course.[143]
As mentioned previously, head injury may alter coagulation parameters, and this can raise the risk of deep venous thrombosis to
as much as 15% if no pharmacologic prophylaxis is given within the first 48 hours.[122] The risk of extension of intracranial Animal studies of some health food supplements may lead to new directions. The dietary supplement creatine, when fed to rats
bleeding needs to be balanced with the benefits of thromboembolic prevention. A retrospective review suggested that early for 4 weeks prior to an experimental brain injury, reduced cortical damage by 50%, primarily through stabilizing mitochondrial
prophylaxis is safe because there was no difference between intracranial hemorrhage progression in patients with head injury functioning.[144] Furthermore, an open-label study of children and adolescents with traumatic brain injuries reported not only a
who received enoxaparin or heparin within the first 3 days versus later in the course of their hospitalization.[123] Further studies, shortened duration of post-traumatic amnesia but also reduced subjective symptoms in those treated with oral creatine for 6
of course, are required. months compared to those not treated.[145] Melatonin is a free-radical scavenger, and when injected early in brain-injured rats,
it significantly reduced levels of lipid breakdown products.[146]
Steroids have demonstrated no benefit in the treatment of acute head injury. A 2004 multicenter European randomized trial of
steroids versus placebo found a higher mortality after only 2 weeks in the steroid-treated patients.[124] Steroid-induced Long-term management
hyperglycemia may have been detrimental as a recent meta-analysis found careful glucose regulation improved functional
outcomes in head-injured patients.[125] Hypertonicity from spasticity or dystonia with attendant muscle spasms is often disabling. Although dantrolene, baclofen,
diazepam, and tizanidine are current oral medication approaches to this problem, baclofen and tizanidine are customarily
Phenytoin has demonstrated efficacy in controlling early posttraumatic seizures, but mortality rates, surprisingly, were unaffected preferred because of their more favorable side effect profiles.
by this benefit. In 1 study, approximately 2.5% of patients treated with phenytoin had an allergic reaction to the drug during the
first 2 weeks of therapy.[126] A trial of valproate in early seizure prophylaxis showed a trend toward an increased mortality rate. When using these agents, careful evaluation of functional status and symptom relief is a priority since adverse effects such as
Because of its relatively benign side-effect profile, levetiracetam has been increasingly employed to prevent post-traumatic sedation may be pronounced.
seizures, but its efficacy has not been empirically validated.[127] Indeed, a retrospective review of 5551 acutely brain-injured
patients found no significant difference in seizure rates between the patients prophylaxed with levetiracetam and the patients Intrathecal baclofen is a newer approach with reported efficacy and minimal adverse effects. One study of 17 patients with
who were untreated, calling into question the routine practice of employing levetiracetam for seizure prophylaxis.[128] traumatic brain injuries showed improved motor tone and decreased muscle spasms with intrathecal baclofen, but whether
Anticonvulsant therapy, if used, should be discontinued after 1–2 weeks unless further seizures supervene.[129] these benefits will translate into improved functioning remains unknown.[147]
Finally, as stated previously, neuroprotective agents mostly have failed to improve the outcomes of patients with brain injury. Botulinum toxin also has shown promise in decreasing hypertonia in patients with head injuries, primarily by improving passive
However, the calcium channel blocker nimodipine was successful in reducing rates of death and severe disability when range of motion rather than by decreasing functional disability.[148, 149]
instituted acutely in patients with head injuries and traumatic subarachnoid hemorrhages, despite its failure to improve outcomes
in 2 large trials of patients with all types of traumatic intracranial injuries.[130] Solid data on cognitive enhancing medications for patients with head injury are lacking. Typically, only small numbers of subjects
have been used and demonstrable functional improvement has been only marginally convincing.
Although numerous synthetic neuroprotective agents are under development, several existing substances have shown promise,
but other agents have been disappointing. Despite these drawbacks, one double-blind, placebo-controlled study of methylphenidate demonstrated improved motor
outcomes and attention in patients with head injuries during active treatment, but only 6 patients completed each 30-day
Because of its excitotoxic blocking properties, magnesium chloride has been used to reduce cortical injury in experimentally treatment arm.[150] A 2006 double-blind, placebo-controlled study of 18 patients with closed head injuries treated with a single
brain-injured rats. Unfortunately, a human double-blind study of 499 patients with moderate or severe head injury failed to show dose of 20 mg of methylphenidate achieved significant improvement in reaction times on a working memory test, but no other
benefit; the magnesium-treated patients actually did worse. One potential confounder in this study was vigilance and aggressive cognitive tasks significantly benefited.[151]
repletion of hypomagnesemia in controls.[131]

Donepezil treatment significantly improved visual and verbal memory as well as attentional deployment in 18 patients with head Consultations
injuries of all levels of severity in a 2004 double-blind, placebo-controlled study.[152] Other less rigorous studies have also
reported cognitive improvements in donepezil-treated, head-injured patients.[153]
In the acute setting, a consultation with a neurosurgeon is critical for patients with moderate or severe head injuries, focal
Anecdotal reports exist of dramatic alerting responses to both levodopa and methylphenidate in patients with vegetative or neurological findings, or intracranial pathology identified on neuroimaging.
comatose states. Levodopa treatment has also resulted in improvement in patients with akinesia and rigidity secondary to
traumatic substantia nigral damage.[154] Furthermore, levodopa has even produced qualitative cognitive improvements in a
small number of head-injured patients.[155]
Emotional lability and the pathologic laughing and crying associated with pseudobulbar palsy reportedly have responded rapidly
and exquisitely to not only selective serotonin reuptake inhibitors but also possibly to dextromethorphan with quinidine.[156, Diet
157] Sertraline has shown efficacy in depression in mild head injury.[158] Treat other possible psychiatric complications of head
injury on a patient-by-patient basis, since no extensive pharmacologic trials of this dimension of head injury have been In the acute setting, nasogastric feedings may need to be initiated for patients with significant head injuries and depressed
conducted. levels of consciousness or dysphagia. Careful attention to protein stores and electrolyte balance is critical during this phase of
treatment.
Nonmedical therapy
Although a full review of nonmedical therapies is beyond the scope of this article, some promising new developments have
occurred in both physical and cognitive therapies.
Constraint-induced movement therapy is a form of physical therapy that emphasizes using the paralyzed arm and minimizes Activity
reliance on the unaffected extremity (patients commonly wear mittens on their unaffected arm for several hours a day). This
form of treatment has resulted in significantly improved function of the paralyzed arm when used in small numbers of brain-
injured patients 1-6 years after their injury.[159] Usually no general limitations are placed on activity. Patient-by-patient recommendations based on the individual's motoric and
cognitive recovery are necessary.
In a randomized trial in 120 military personnel with moderate-to-severe head injuries, in-hospital cognitive rehabilitation proved
unsuccessful compared to a limited in-home program, but a subgroup post hoc analysis indicated that patients with
unconsciousness lasting 1 hour or more had a greater functional recovery with in-hospital cognitive rehabilitation than those in
the control group.[160]
Guidelines
Guidelines Summary
Surgical Care
Guidelines for traumatic brain injury are undergoing constant revision with the incorporation of newly completed clinical studies
Traditionally, the prompt surgical evacuation of subdural hematomas in less than 4 hours was believed to be a major and research.
determinant of an optimal outcome. Indeed, a recent publication found a delay in surgery for acute subdural hematomas of over
5 hours was associated with increased mortality.[161] Nevertheless, other recent investigations have emphasized that the extent The American Association of Neurological Surgeons generally does not produce specific treatment guidelines. However, the
of the original intracranial injury and the generated intracranial pressures may be more important than the timing of surgery. Brain Trauma Foundation recently published revised guidelines for severe traumatic brain injury, and their recommendations
have been endorsed by neurosurgical professional organizations. These guidelines are based on high-to-moderate quality
For example, 70% of 83 patients with GCS scores of 11-15 who had subdural hematomas less than 1 cm in width and no evidence and are summarized below:[167]
cisternal effacement on neuroimaging or focal neurological deficits were successfully managed nonoperatively with only
6% eventually requiring surgery.[162] 1. If decompressive craniectomy is performed, a large frontal, temporal, and parietal one is preferred over smaller
craniectomies.
Subdural hematomas less than 5mm in thickness seldom require surgical attention.[163]
2. There is no evidence that hypothermia improves outcomes.
Another study of 462 patients with head injuries with CT-imaged intracranial hematomas who were treated
nonoperatively found that only approximately 10% progressed clinically and eventually required surgery. Frontal 3. There is insufficient evidence to support a specific hyperosmolar treatment (mannitol or hypertonic saline) for increased
parenchymal hematomas were more likely to require eventual surgery.[164] intracranial pressure.
Among 77 mild brain-injured patients with small subarachnoid bleeds, non-displaced skull fractures, and subdural 4. There is insufficient evidence to support CSF drainage.
hematomas less than 4mm, only 1.3% required a formal neurosurgical consult. The vast majority of patients were
5. There is insufficient evidence to support prophylactic hyperventilation.
managed by trauma surgeons alone with no untoward complications.[165]
6. There is insufficient evidence for sedatives, analgesics, or anesthetic agents.
Decompressive craniectomies are sometimes advocated for patients with increased intracranial pressure refractory to
conventional medical treatment. Although some studies have shown favorable long-term outcomes with this 7. Steroids are to be avoided as they increase mortality.
procedure[166]
8. Enteral feeding should be initiated within the first week.
The operative and nonoperative management of intracranial injuries is an ever-evolving area of study and, at present,
more a matter of neurosurgical judgment than hard and fast decision rules. 9. Early tracheostomy placement is recommended.
10. Povidone-iodine oral care should not be used as this may increase ARDS.
11. There is insufficient evidence to support specific DVT-prevention strategies.

In 2013, the American Academy of Neurology[168] introduced guidelines for concussion in sports. These guidelines endorsed
symptom checklists to be used by non-physician assesors to help diagnose concussions. An athlete with an identified
concussion is prohibited from returning to play until the signs and symptoms of the concussion have resolved. Athletes with Electrolytes
multiple concussions and objective neurologic or cognitive impairments are retired from play.
In 2008, the CDC recommended imaging guidelines for mild traumatic brain injury, which were re-affirmed in 2013. A CT of the Class Summary
head is indicated in patients with head injury and loss of consciousness or amnesia if the patient has also had any of the
following: headache, vomiting, age greater than 60 years, drug or alcohol intoxication, short-term memory loss, evidence of Magnesium is given in hypomagnesemic states to ensure that adequate stores are present during acute phase of head injuries.
trauma above the clavicles, a seizure, a focal neurologic deficit, a GCS less than 15, or a coagulopathy. Such complicated
decisions rules seem impractical and will hopefully be clarified with further research.[169]
Magnesium sulfate
Nutritional supplement in hyperalimentation; cofactor in enzyme systems involved in neurochemical transmission and muscular
excitability. In adults, 60-180 mEq of potassium, 10-30 mEq of magnesium, and 10-40 mmol of phosphate per day may be
Medication necessary for optimum metabolic response.
Medication Summary
Medications commonly are used in the acute setting to control early seizures, reduce intracranial pressure, and correct
electrolyte abnormalities. Nimodipine may be neuroprotective in the subset of patients with traumatic subarachnoid Barbiturates
hemorrhages.
In the long-term setting, cognitive and motoric augmentation as well as the control of spasticity and emotional incontinence may
require pharmacologic interventions.
Class Summary
These agents may help reduce intracranial pressure that is refractory to other conventional measures.
Pentobarbital (Nembutal)
Osmotic diuretics Short-acting barbiturate with sedative, hypnotic, and anticonvulsant properties. Can produce all levels of CNS depression.
Class Summary
These agents may help reduce intracranial pressure.
Calcium Channel Blocker
Mannitol (Osmitrol, Resectisol)
May reduce subarachnoid space pressure by creating osmotic gradient between CSF in arachnoid space and plasma. Not for
Class Summary
long-term use. Initially assess for adequate renal function in adults by administering test dose of 200 mg/kg, given IV over 3-5
min; should produce urine flow of at least 30-50 mL/h of urine over 2-3 h. Same test in children should produce urine flow of at Nimodipine has been demonstrated to improve outcomes of patients with traumatic subarachnoid hemorrhages.
least 1 mL/kg/h over 1-3 h.
Nimodipine (Nymalize)
Indicated for improvement of neurological impairments resulting from spasms following subarachnoid hemorrhage caused by
ruptured congenital intracranial aneurysm in patients who are in good neurological condition postictus.
Anticonvulsants While studies show benefit on severity of neurological deficits caused by cerebral vasospasm following subarachnoid
hemorrhage, no evidence that drug either prevents or relieves spasms of cerebral arteries. Thus, actual mechanism of action
unknown.
Class Summary
Therapy should start within 96 h of subarachnoid hemorrhage. If capsule cannot be swallowed because patient undergoing
These agents may help prevent early seizures in head injury. surgery or unconscious, a hole can be made at both ends of capsule with 18-gauge needle and contents extracted into a
syringe. Contents then can be emptied into patients' in situ nasogastric tube and washed down tube with 30 mL isotonic saline.
Phenytoin (Dilantin, Phenytek)

May act in motor cortex, where it may inhibit spread of seizure activity; activity of brainstem centers responsible for tonic phase
of grand mal seizures also may be inhibited.
Stimulants
Individualize dose. Administer larger dose in evening if dose cannot be divided equally.

Class Summary
These agents may help increase alertness and some aspects of cognitive functioning in patients with brain injury.
Antispasticity medications
Methylphenidate (Ritalin, Aptensio XR, Concerta, Daytrana, Methadate)
Blocks the reuptake of norepinephrine and dopamine into presynaptic neurons. May stimulate cerebral cortex and subcortical Class Summary
structures.
Antispasticity medications can be useful. These agents may reduce painful cramping and detrimental muscle tightening.
However, one of the drawbacks of using these agents is that some patients find that the stiffness of spasticity helps them to
overcome the muscle weakness. When patients are medicated to reduce stiffness, walking may become more difficult. Adverse
effects can also be a problem.
Dopamine agonist If the patient does well with the medications, however, discomfort associated with spasticity can generally be reduced, mobility
can be improved, and the effectiveness of physical therapy (PT) can be enhanced.
Class Summary Tizanidine hydrochloride (Zanaflex)

These agents may increase alertness in patients with brain injury; also may help in occasional patients with posttraumatic
Tizanidine is a centrally acting muscle relaxant that is metabolized in the liver and excreted in urine and feces. A single oral
parkinsonism.
dose of 8mg reduces muscle tone in patients with spasticity for several hours. Blood levels and the spasmolytic effect are
linearly correlated.
Levodopa (Dopar, Larodopa)
Baclofen (Lioresal)
Large neutral amino acid absorbed in proximal small intestine by saturable carrier-mediated transport system. Absorption
decreased by meals, which include other large neutral amino acids. Only patients with meaningful motor fluctuations need
May induce hyperpolarization of afferent terminals and inhibit both monosynaptic and polysynaptic reflexes at spinal level.
consider low-protein or protein-redistributed diet. Greater consistency of absorption achieved when levodopa taken 1 h or more
Baclofen presynaptically inhibits the nerve terminal. It is centrally acting and can be administered intrathecally or orally. Baclofen
after meals. Nausea often reduced if levodopa taken immediately following meals. Some patients with nausea benefit from
is the preferred drug for spasticity related to spinal cord injury (SCI). Tolerance can occur. Adverse effects are minimized if the
additional carbidopa in doses up to 200 mg/d. Half-life of levodopa/carbidopa approximately 2 h.
drug is given intrathecally.
When more carbidopa required, substitute 1 25/100 tab for each 10/100 tab; when more levodopa required, substitute 25/250
tab for 25/100 or 10/100 tab. Dantrolene (Dantrium)
Sustained release (SR) formulation of levodopa/carbidopa is absorbed more slowly and provides more sustained levodopa
levels than immediate release (IR) dosage form; SR as effective as IR formulation when levodopa initially required and may be This is a peripherally acting medication that prevents calcium release from the sarcoplasmic reticulum. It is particularly effective
more convenient when fewer intakes are desired. in cerebral-origin spasticity, such as that occurring in traumatic brain injury (TBI), stroke, or cerebral palsy. Stimulates muscle
relaxation by modulating skeletal muscle contractions at site beyond myoneural junction and acting directly on muscle.
Patients with dissipating motor fluctuations and no dyskinesia often benefit from prolongation of short-duration response when
switched from IR to SR; however, patients with meaningful fluctuations and dyskinesia often experience increase in dyskinesia
when switched to SR formulation.
Diazepam (Valium, Diazepam Intensol)
Doses and dosing intervals of SR form may be increased or decreased based on response; most patients have been treated Diazepam acts presynaptically and is a gamma-aminobutyric acid ̶ A (GABA-A) agonist. It is centrally acting. Tolerance and
adequately with 2-8 tab/d (divided doses) at intervals of 4-8 h while awake; higher doses (>12 tab/d) and intervals < 4 h have addiction can occur.Depresses all levels of CNS, possibly by increasing activity of GABA. Individualize dosage and increase
been used but usually are not recommended; if < 4-h interval used or if divided doses are not equal, give smaller doses at end cautiously to avoid adverse effects.
of day. Allow at least a 3-d interval between dosage adjustments. May administer as whole or half tab, which should not be
crushed or chewed.
N-Methyl-D-Aspartate Receptor Antagonists

Selective serotonin reuptake inhibitors
Class Summary
Class Summary Glutamate release inhibition and glutamate receptor blockade are alternatives to potentiating D2 receptors in the indirect pallidal
outflow pathway by reducing the glutamate-related excitatory circuit in the outflow pathway.
These agents have been of benefit in patients with head injuries and emotional incontinence.
Dextromethorphan/quinidine (Nuedexta)
Sertraline (Zoloft)
Dextromethorphan is a sigma-1 receptor agonist and an uncompetitive N-methyl-D-aspartate (NMDA) receptor antagonist.
SSRIs are antidepressant agents that are chemically unrelated to TCAs, tetracyclic antidepressants (TeCAs), or other available Quinidine increases plasma levels of dextromethorphan by competitively inhibiting cytochrome P4502D6, which catalyzes a
antidepressants. They inhibit central nervous system (CNS) neuronal uptake of serotonin and may have a weak effect on major biotransformation pathway for dextromethorphan. The mechanism by which dextromethorphan exerts therapeutic effects
neuronal reuptake of norepinephrine and dopamine. is unknown.
Mild head injury
Mild head injuries are those that generate GCS scores of 13-15. Such injuries usually are considered relatively benign, and the
Follow-up accompanying cognitive impairments typically resolve within 3 months of injury.
Patients with lingering complaints are often assumed to have either a psychological reaction to the injury or to be malingering.
Various standardized neuropsychologic instruments are available to help sort out legitimate from illegitimate cognitive
Further Outpatient Care impairments. About 25% of patients with mild head injury taking such tests yield invalid profiles.[176] Furthermore, coexisting
musculoskeletal injuries may impact cognitive testing. For example, collegiate athletes with musculoskeletal injuries performed
just as poorly on computerized neuropsychological tests as athletes with concussions.[177]
This also depends on the degree of the head injury and the individual patient's cognitive and motor abilities and pain complaints.
However, an initial grading of mild does not necessarily mean a mild outcome. As many as 3% of patients with an initial mild
injury may require a neurosurgical operation.[178] Some patients have died hours after sustaining trivial head injuries. Also, as
previously mentioned, axonal damage has been documented pathologically with mild head injuries.
Disability rates may be pronounced with putatively mild injuries as well. Recent studies have demonstrated that following mild
Further Inpatient Care head injury, only 54-79% of patients are able to return to full preinjury employment. One study of 148 patients with mild head
injury based on the GCS discovered that after 1 year, 26% had moderate disability and 3% had severe disability, but all these
This needs to be individualized. Certainly after a moderate or severe head injury, transfer to an inpatient rehabilitation unit is patients also had either radiological abnormalities or focal neurological signs, placing them in the more severe range of mild
recommended. head injuries.[179] A recent review sponsored by the National Institute of Medicine concluded that there is no clear evidence of
lasting cognitive impairments attributable to mild closed head injuries.[180]
Second impact syndrome
In the United States, athletic competitions account for 300,000 mild head injuries per year. The second impact syndrome occurs
Transfer when an athlete suffers a minor concussion and subsequently is re-injured in play. The repeated concussive events are
theorized to result in autoregulatory dysfunction and vascular congestion. Catastrophic brain edema, herniation, and sudden
death may ensue.
Patients with moderate or severe head injuries and head injuries with significant extracranial components are cared for best at a
specialized trauma center. At least 35 cases occurred among US football participants from 1980–1993, but the general incidence of this syndrome is
unknown. Concerns about athletes at risk returning to play too soon have generated formalized recommendations from the
American Academy of Neurology. Return to play is postponed for increasing lengths of time depending on the severity of the
concussion.[181, 182] In addition, return to play is contingent on the resolution of the initial concussion symptoms.[168]
Some researchers have questioned the existing literature's documentation of initial injuries, hypothesizing that the second
Deterrence/Prevention impact syndrome is more one of primary impact and that secondary prevention strategies are not justified empirically.[183] Other
researchers more recently have stressed the prolonged nature of recovery from athletic head injuries and the need for longer
Reducing morbidity and mortality rates associated with head injuries is likely to be difficult. Violence, automobiles, and drug and recuperation prior to return to play.[184] American football, male gender, and young age ranges are associated with this
alcohol use are prevalent. syndrome.[185]
A study of community-based programs reported modest success, primarily by employing increased police surveillance and law Posttraumatic epilepsy
enforcement to reduce overdrinking and alcohol-related injuries. Motor vehicle accidents in which the driver was intoxicated
declined 6%, and more significantly, overall assault cases seen in local emergency departments decreased 42%.[170] Posttraumatic seizures occur clinically in approximately 4% of patients with head injuries within the first week of the injury.
Continuous EEG monitoring may disclose a higher incidence (22%).[101, 102]
Another study has shown that patients who were screened for alcohol problems and provided with an organized intervention to
reduce their alcohol consumption exhibited a 47% decrease in emergency department–evaluated injuries compared to patients Seizures after the first week occur in 4-30% of patients. The severity of the head injury, early seizures, depressed skull fractures,
receiving no alcohol screening or intervention.[171] and temporal and frontal injuries identified on CT scans all have been associated with the development of late seizures.[186]
The use of protective devices also is promising. A meta-analysis of case-control studies of bicycle helmet use concluded that Although focal EEG findings traditionally have not been predictive of late seizures, one study reported that a focal EEG 1 month
helmets reduce the risk of severe head and brain injuries by 63–88%.[172] Indeed, a 2006 study of 160 cyclist injuries in after injury resulted in a 3.49-times higher risk of posttraumatic epilepsy.[187]
Singapore found that helmet users sustained head injuries only 5.9% of the time, compared with 40% of the time for nonusers.
[173] Similarly, a California law mandating the use of bicycle helmets for riders aged 17 years and younger reduced traumatic Recently, MRI-visualized hippocampal sclerosis has been associated with intractable epilepsy in patients who sustained
brain injuries by 18%. However, subgroup analysis revealed that this reduction failed to apply to urban, female, and African moderate-to-severe head injuries when aged 10-31 years.[188]
American riders.[174]
Posttraumatic headaches
Falls in the elderly are often multifactorial in origin and consequently, solutions are likely to be complex. Nevertheless, random
allocation of indepently living elderly patients to a fall-prevention regime of strength and balance training reduced both the Posttraumatic headaches are common and may occur in 30-90% of patients after a head injury.[189] The alterations in cations,
number of falls as well as their severity.[175] catecholamines, and excitatory amino acids are similar in both migraine and head injury.[190]
Posttraumatic headaches typically manifest with a vascular component, but chronic daily headaches are also common.
Although controversial, some authors have reported that most posttraumatic headaches are primarily rebound or analgesic-
overuse headaches. Nearly three fourths of such patients may benefit from cessation of pain medications.[191]
Complications Greater occipital neuralgia can occur following head and neck injuries. Greater occipital nerve pain occurs in the back of the
head and may be characterized by lancinating or aching sensations in this region.
Posttraumatic movement disorders vehicle accident victims demonstrated more than 3 times the mortality compared with their younger counterparts.[202,
203] Similar results were recently documented in a study of severely head-injured elders from Norway with 72%
Tremor, dystonia, parkinsonism, myoclonus, and hemiballism all can occur following head injuries. attaining an unfavorable outcome, defined as inability to be independent when out of their home environment.[204]
In a 2-year follow-up study of 398 patients with severe head injuries, 12% had persistent movement disorders. Disabling
dystonia and low-frequency kinetic tremors were present in 5.4%. Parkinsonism and myoclonus attributable to the injury
occurred in less than 1% of patients.[53]
Posttraumatic psychiatric disorders Patient Education

Disorders of emotional functioning have been documented repeatedly after head injuries. A case-control study of 91 patients The physician may be hesitant to suggest to patients that problems may arise from a mild head injury. Such information may
hospitalized with traumatic brain injury recorded a 33% incidence of major depression.[192] Depression has been associated induce the expectations of symptoms when no symptoms are present and arouse anxiety. However, at least one study has
with left frontal injuries. Using a questionnaire methodology, 56% of 774 head injured patients of all levels of severity exhibited shown that patients with head injury who were contacted by phone and offered education about their injury and follow-up care
depression 10 weeks after their injury.[193] Bipolar disorder is also more frequent in patients with head injuries than in the experienced significantly fewer postconcussive symptoms and less disruption of social activities.[205]
general population and is associated with seizures and right hemispheric lesions.
At present, most patients incurring a head injury probably should be informed that cognitive and emotional dysfunction as well
Additionally, impulsive and disinhibited behaviors are common in patients with frontal injuries, although even obsessive- as head pain and other somatic symptoms are not uncommon in the aftermath. At least in mild injuries, these symptoms
compulsive features have also been reported.[194] typically are self-limited, and most people return to normal functioning after a few weeks to months.
Head injury-related psychosis is controversial. A case-control study of 45 patients with psychosis following head injury found For excellent patient education resources, visit eMedicineHealth's First Aid and Injuries Center, Brain and Nervous System
that auditory hallucinations and paranoid delusions developed after a 54-month postinjury latent period. More widespread injury Center, and Eye and Vision Center. Also, see eMedicineHealth's patient education articles Concussion, Dementia in Head Injury,
on neuroimaging and decreased cognitive functioning characterized the psychotic patients with head injuries compared with and Black Eye.
nonpsychotic control patients with head injuries.[195]
Contributor Information and Disclosures
Author
Prognosis
David A Olson, MD Clinical Neurologist, Dekalb Neurology Group, Decatur, Georgia
This discussion has delineated a myriad of prognostic factors. Head injuries may result in death, a vegetative state, partial
recovery, or full return to work. Each patient presents with a unique baseline neurological make up, mechanisms of injury, David A Olson, MD is a member of the following medical societies: American Academy of Neurology
secondary complications, and postinjury adjustment and support system.
Disclosure: Nothing to disclose.
The most important prognostic factors are probably age, mechanism of injury, postresuscitation GCS score, postresuscitation
pupillary reactivity, postresuscitation blood pressures, intracranial pressures, duration of posttraumatic amnesia or confusion, Specialty Editor Board
sitting balance, and intracranial pathology identified on neuroimaging.
Francisco Talavera, PharmD, PhD Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy;
The mortality rate of severe head injuries ranges from 25-36% in adults within the first 6 months after injury. Most deaths occur Editor-in-Chief, Medscape Drug Reference
within the first 2 weeks.
Disclosure: Received salary from Medscape for employment. for: Medscape.
A study of 216 patients hospitalized during 2003-2005 in Ireland found 97% of patients with mild head injury attained a
good recovery as measured by the Glasgow Outcome Scale, while 82% of the patients with severe head injury were Florian P Thomas, MD, PhD, MA, MS Chair, Neuroscience Institute and Department of Neurology, Director, National MS
either vegetative or markedly disabled. After 1 year, 11% of the total patients were unable to work.[196] Society Multiple Sclerosis Center and Hereditary Neuropathy Foundation Center of Excellence, Hackensack University Medical
Center; Founding Chair and Professor, Department of Neurology, Hackensack Meridian School of Medicine at Seton Hall
Another contemporary study of 309 Italian patients with moderate head injury found that only 15% were vegetative or University; Professor Emeritus, Department of Neurology, St Louis University School of Medicine; Editor-in-Chief, Journal of
severely disabled after 6 months. Basal skull fractures, subarachnoid hemorrhages, coagulopathies, subdurals, and poor Spinal Cord Medicine
emergency room clinical status predicted these unfavorable outcomes.[68]
Florian P Thomas, MD, PhD, MA, MS is a member of the following medical societies: Academy of Spinal Cord Injury
Conversely, in Germany only 82% of 67 patients with mild or moderate head injury experienced a good 1-year outcome, Professionals, American Academy of Neurology, American Neurological Association, Consortium of Multiple Sclerosis Centers,
and only 73% were able to return to work. Subjective complaints persisted in a large minority, with more than one third of National Multiple Sclerosis Society, Sigma Xi
patients reporting drowsiness, fatigue, forgetfulness, poor concentration, and irritability.[197] Other studies have identified
dizziness along with analgesic and psychotropic medication use as predictors of failure to return to work after mild and Disclosure: Nothing to disclose.
moderate head injuries.[198]
Chief Editor
A five-year paid employment status study of 5683 moderate to severely head-injured patients found that not only did age
and injury severity adversely affect stable employment, but so did lack of transportation and elevated anxiety levels. Only Stephen A Berman, MD, PhD, MBA Professor of Neurology, University of Central Florida College of Medicine
27% attained stable 5-year employment.[199] Another study reported that 41% of 4927 moderate and severe head-
injured patients attained full or part-time paid employment at year 5.[200] Stephen A Berman, MD, PhD, MBA is a member of the following medical societies: Alpha Omega Alpha, American Academy of
Neurology, Phi Beta Kappa
Overall, patients with traumatic brain injury are 2.23 times more likely to die than their non-injured counterparts. Brain-
injured patients' life expectancies are reduced by about 9 years.[201] Disclosure: Nothing to disclose.
An Australian study of patients with head injuries incurred from 1984–1991 found that all 59 patients who were aged 65 Additional Contributors
years or older and scored less than 11 on the postresuscitation GCS either died or were left with severe disability.
Furthermore, even after controlling for injury severity and GCS scores, a current study of head-injured elderly motor

Tce - Medscape

Uploaded by

Document Information

Original Description:

Original Title

Copyright

Available Formats

Share this document

Share or Embed Document

Sharing Options

Did you find this document useful?

Is this content inappropriate?

Copyright:

Available Formats

Tce - Medscape

Uploaded by

Copyright:

Available Formats

21/1/2020 https://emedicine.medscape.com/article/1163653-print 21/1/2020 https://emedicine.medscape.

Cranial nerve (CN) VI palsy: May indicate raised intracranial pressure

Hearing loss: Occurs in 20–30% of patients with head injuries[5]

Dysphagia: Raises the risk of aspiration and inadequate nutrition[6]

Practice Essentials Bedside cognitive testing

Mini-Mental State Examination

Untimed Trails B test: Allows further qualitative testing of frontal functioning

https://emedicine.medscape.com/article/1163653-print 1/39 https://emedicine.medscape.com/article/1163653-print 2/39

https://emedicine.medscape.com/article/1163653-print 3/39 https://emedicine.medscape.com/article/1163653-print 4/39

https://emedicine.medscape.com/article/1163653-print 7/39 https://emedicine.medscape.com/article/1163653-print 8/39

Temporal Lobe Epilepsy

https://emedicine.medscape.com/article/1163653-print 9/39 https://emedicine.medscape.com/article/1163653-print 10/39

See the images below.

https://emedicine.medscape.com/article/1163653-print 11/39 https://emedicine.medscape.com/article/1163653-print 12/39

https://emedicine.medscape.com/article/1163653-print 15/39 https://emedicine.medscape.com/article/1163653-print 16/39

11. There is insufficient evidence to support specific DVT-prevention strategies.

https://emedicine.medscape.com/article/1163653-print 17/39 https://emedicine.medscape.com/article/1163653-print 18/39

Phenytoin (Dilantin, Phenytek)

https://emedicine.medscape.com/article/1163653-print 19/39 https://emedicine.medscape.com/article/1163653-print 20/39

Class Summary Tizanidine hydrochloride (Zanaflex)

N-Methyl-D-Aspartate Receptor Antagonists

Mild head injury

Second impact syndrome

Posttraumatic psychiatric disorders Patient Education

Contributor Information and Disclosures

You might also like