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MODERATOR PRESENTER
DR. K. K. GUPTA VIVEK KUMAR
HISTORICAL PERSPECTIVE AND PREVALENCE : The Thalassemias are a
group of congenital anemia that have in common deficient synthesis of one or more of the globin
subunits of the normal human hemoglobin , particularly common in the Mediterranean region and south
east Asia .Over 180 million people in the world and 20 million in India carry the gene for β-thalassemia.
There is very little evidence that it was recognized as a specific clinical entity before its first clinical
description in 1925 . But by the start of the 20th century clinician were becoming aware of the syndrome
of splenic anemia of infancy, which was first described by Rudolf Von Jaksch – Warterhorst and it
became a common practice to describe any unusual anemia in infancy as “Von Jaksch’s anemia” ,
particularly if the spleen was enlarged. The credit for the first clinical description of the condition which
later became known as thalassemia is given to the American pediatrician Thomas B. Cooley , in 1925.
The term ‘thalassemia’ was introduced by Whipple and Bradford in 1932.The word is taken from the
Greek word ‘thalassa’, meaning the sea , indicating its Mediterranean connection.
• α-Thalassemia
Hemoglobin H disease(--/-α)
Hydrops fetalis(--/--)
• β-Thalassemia
Major
Intermedia
Minor
• β-Thalassemia hemoglobinopathies
δ-thalassemia
δβ-thalassemia
γδβ-thalassemia
Hb Lepore
Hyperunstable globins
Transcription Mutation :
Promoter mutation: several mutations have been described in or around the conserved motifs in the 5’ –
flanking sequence of β– globin genes ( TATA box and the proximal and distal CACCC box) . This
reduce binding of RNA polymerase, there by reduce the rate of mRNA transcription to 20 – 30 % of
normal . Hence result in a mild phenotype.
5’ Untranslated region mutation : several mutations also have been reported in this 50- nucleotide
region ; all have a mild effect on gene transcription. Heterozygote have a normal or borderline red cell
indices and HbA2, and compound heterozygotes , with severe β-thalassemia alleles ,usually have mild
phenotype.
Splice junction and consensus sequence mutation : Mutations of the invariants 5’ –GT- and 3’ –AG-
dinuleotide completely abolish normal splicing and result in βo–thalassemia. The efficiency of normal
splicing may be decreased by mutations within the consensus sequences immediately adjacent to the
splice junction . The reduction of beta globin production is quite variable and the resulting phenotypes
range from mild to severe.
Cryptic site mutations in Introns and Exons : Along introns and exons there are sequences simlar to
those found at the intron/exon boundaries, which normally are not used for splicing (“cryptic” splice
sites) . A number of nucleotide substitutions involving these sequences transform a cryptic site into a
legitimate one , resulting in a severe βo– or β+– thalassemia phenotyope.
Poly (A) and other 3’ untranslated region mutation : Downstream of the mRNA terminal codon , there is
highly conserved AAUAAA sequences , which represent a signal for the cleavage and polyadenylation
reaction , as a part of the RNA transcript processing . Because polyadenylation is important in
determing the stability of mRNA, mutations at the AAUAAA sequences affect the efficiency of
translation ,resulting in β+– thalassemia of variable , but usually mild severity . Other mutations in 3’
UTR also produce β silent thalassemia.
Nonsense mutation : Single nucleotide substitution may change a codon for a given amino acid to one of
the three possible chain termination codons :TAA,TAG or TGA .The result is a premature interruption of
mRNA translation with absence of β-globin production (βo - thalassemia ).
Frameshift mutation : Insertion or deletion of one or a few nucleotides (other than three or multiples of
three ) alters the reading frame of the encoded mRNA starting at the site of the mutation . The new
reading frame usually results in a novel abnormal amino acid sequence and in a premature termination
further downstream . The mutant globin chain is rapidly degraded , and the final result is a βo-
thalassemia .
In addition to above mentioned mutations , several deletions , affecting only the β- globin gene and
ranging size from 290 bp to approximately 67 kb , have been reported .
β – Thalassemia Hemoglibinopathies
This group includes some structurally abnormal hemoglobin with a thalassemia phenotype , they can be
classified according to the molecular mechanism .
δβ- Hybrid Gene : Unequal crossing over between the homologous δ- and β- globin genes results in
the formation of hybrid δβ and βδ genes ,referred to as Lepore and anti-Lepore genes. The Lepore
hemoglobin contain the N- terminal sequence of the normal δ – chain and C- terminal sequences of the
normal β- chain. The pathophysiology is similar to that of β- thalassemia .This abnormal hybrid globin
chains are relatively instable and are also in-effectively synthesized , leading to an excess of α- chains ,
leading to ineffective erythropoiesis and anemia . The homozygous and the heterozygous states of Hb –
Lepore are clinically similar to those of β- thalassemia .
Hyper unstable Globins : This is singular group of β- globin gene mutants that are characterized by
amino acid substitution , additions or deletions in the β- globin chain associated with a thalassemia
phenotype in heteroygous state . For this reason , these forms are also referred to as dominantly inherited
β- thalassemia . In contrast to the typical recessively inherited forms of β- thalassemia , which lead to a
reduced synthesis of normal β-globin chain. This group of mutations results in the production of β –
globin variants that are extremely unstable. These hyperunstable globins fail to form functional
tetramers and precipitate in the erythroid precursors , leading to ineffective erythropoiesis, which is
exacerbated by the concomitant relative excess of α – chain . Most patients present with clinical
phenotype of thalassemia intermedia.
δ- Thalassemia : Several mutations of the δ- globin gene results in reduced (δ+- thalassemia ) or
absent ( δ0- thalassemia ) production of δ- globin chains . These conditions do not have clinical
relevance but the co-inheritance with β-thalassemia mutations may create problems in β-carrier
identification ,because the HbA2 may be normal or borderline.
δβ – Thalassemia : This includes a group of disorders characterized by reduced or absent production
of both δ- and β – globin chains and by a variable increase in γ-chain synthesis that only partially
balances the δ- and β-chain deficiency . The most common molecular mechanism consists of deletion of
variable extent of β-globin gene cluster , which involve the δ- and β-genes . The thalassemia due to
homozygous mutation is frequently confused with HPFH because both disorders have 100 % HbF
.However, unlike HPFH , increased γ- chain production fails to fully compensate for the loss of β- chain
production . It appears that in δβ-thalassemia , there is less compensation by γ –chain synthesis than in
HPFH but more than in homozygous β-thalassemia . Thus most patients with δβ-thalassemia have a mild
anemia with slight hepatoslenomegaly and some bone changes associated with chronic erythroid
hyperplasia . The heterozygous form of δβ-thalassemia is not identified with any specific clinical
finding .
γδβ- thalassemia : This rare form of thalassemia has several variants and is characterized by deletion
or inactivation of the entire β- gene complex . Only the heterozygous state has been encountered ,
although neonates have severe hemolytic anemia but as the child grows , the disease evolves to a mild
form of β-thalassemia .
PATHOPHYSIOLOGY :
Normally equal quantities of α- and β- chains are synthesized by the maturing erythrocytes resulting in a
β- to α- chain ratio of 1.0 . the basic defect in β- thalassemia is a reduced or absent production of β-
globin chains with relative excess of α- chain . The direct consequences is a net decrease in the
hemoglobin production and an imbalance of globin chain sythesis . In heterozygous thalassemia , the β-
to α- chain ratio is decreased to 0.5 – 0.7 , where as in homozygous thalassemia the ratio is less than
0.25 . This imbalance has a dramatic effects on the red cell precursors , resulting in their premature
destruction in the bone marrow and extramdullary sites . This process is referred to as ineffective
erythropiesis and is the hallmark of β- thalassemia . Using ferrokinetic analysis , it has been shown that
in β- thalassemia patients only 15 % of Fe59 is incorporated in circulating erythrocytes , indicating that
ineffective eryhtropoiesis could account for as much as 60 to 75 % of the erythropoiesis . Hemolysis of
the erythrocytes containing inclusion that reach peripheral blood is a minor cause of anemia ,
particularly in thalassemia major . The excess α- chain lies at the center in the pathophysiology of β-
thalassemia and thus the main determinant of the clinical severity is the degree of α/non-α gene
imbalance.
The free excess α-chains are unstable and precipitate within the cell. There is further oxidation of
excess α-chains which result in the formation of hemichromes . Irreversible hemichromes and denatured
α-chains precipitate as inclusionbodies early during differentiation and throughout erythroid maturation .
α- chain precipitation in the red cell membrane causes structural and functional alterations with changes
in deformability , stability and red cell hydration . A further consequence of the membrane bound
hemichromes is their association with the cytoplasmic domain protein band 3 , creating a neoantigen that
is subjected to opsonization with autologous immunoglobulin G and compliments , and later removal of
the cell by macrophages . Besides oxidation , free α – chain are subjected to degradation resulting in the
formation of denatured α- globin protein , heme and free iron . These degradation products play a role in
damaging erythroid precursors and red cell membranes. Free iron via the “Fenton reaction” generates
reactive oxygen species , which cause lipid and protein peroxidation with consequent damage to red cell
membrane and intracellular organelles . Also heme and its oxidized form hemin produce oxidative
damage to the different components of the red cell membrane with consequent structural and fuctional
alterations.These alterations of erythroid precursors result in an enhanced rate of apoptosis . Apoptosis
contributes significantly to ineffective erythropoiesis and occurs primarily at the polychromatophilic
erythroblast stage. However it is not clear how α-globin precipitation causes apoptosis .
Ineffective erythropoiesis and anemia have several consequences . The first response to anemia is an
increased production of erythropoietin , causing marked erythroid hyperplasia , which may range
between 10 to 30 times normal . Anemia may produce cardiac enlargement and may contribute to
cardiac failure .Erythroid expansion produces skeletal deformities , osteoporosis and occasionally ,
extramedullary masses . Untreated and undertreated individuals with thalassemia major have retarted
growth as a result of anemia and an excessive metabolic burden imposed by erythroid expansion .
Ineffective erythropoiesis is associated with increased iron absorption that further contributes to the iron
burden imposed by blood transfusions. Iron overload damages several organs , including the
myocardium , liver and endocrine glands . Removal of the abnormal RBCs by the reticuloendothelial
elements of the sleen results in splenomegaly and hypersplenism . A further consequence of the RBC
membrane damage is the increased surface exposure of the procoagulants , negatively charged
phospholipids phosphatidyl serine and phosphatidylethanolamine , the anionic phospholipids increases
thrombin generation.
The most severe form is defined β-thalassemia major and is characterized by transfusion dependent
anemia . Thalassemia intermedia is the term used to designate a form of anemia, independent of the
genotype , that does not require transfusions. Thalassemia minor indicates the heterozygous state that is
usually asymptomatic.
Thalassemia major presents in early infancy ( 6 – 18 months ) with progressive pallor,
hepatosplenomegaly and bony changes ,and if left untreated , is invariably fatal during the first few
years of life . At the other end of the spectra is a heterogenous form ( thalassemia minor ) in which
patient can lead practically normal life except for a mild persistent anemia and have a normal life span .
In between these two extremes is a form with varying degrees of clinical manifestations of anemia ,
splenohepatomegaly and bony changes and who maintain their life fairly comfortably, and are usually
not dependent on regular blood transfusion .
• Peripheral blood smears are diagnostic with microcytic , hypochromic , poikilocytic and
polychromatic red cells . There is also moderate basophilic stippling with fragmented erythrocytes ,
target cells and large numbers of normoblasts . Reticulocyte count is low usually below 1 % in
thalassemia major , but it is generally increased to twice than normal in thalassemia minor and have
been found to correlate with Hb level .
• Bone marrow examination shows normoblastic erythroid hyperplasia with increased stained iron .
• Red cell survival measured by Cr51 shows ineffective erythropoiesis rather than peripheral
hemolysis .
• Hb electrophoresis is diagnostic . HbF is increased , HbA2 is usually over 3.5 % , but may be normal
. HbA is reduced to absent depending upon the genotype .
2. IRON CHELATION
3. SPLENECTOMY
4. VITAMIN SUPPLEMENTATION
5. MANAGEMENT OF COMPLICATIONS
ENDORINOPATHIES
HEART FAILURE
Transfusion may also be required for those children with thalassemia intermedia who cannot maintain
Hb above 7 g/dl or for those who show evidence of growth retardation , severe bony changes or
hypersplenism.
Transfusion regimen may be (1) low transfusion regimen where Hb is maintained around 6 – 10 g/dl ,
(2) hypertransfusion : Hb level 10 – 12 g/dl and (3) supertransfusion, where Hb is maintained at 12 –
14 g/dl or PCV maintained above 35 % .The most widely accepted regimen of today is a
hypertransfusion regimen . To reduce the volume transfused and to avoid the administration of foreign
protein packed RBC must be transfused and to avoid transfusion reaction the blood product should be
rendered WBC free. This can be achieved by using frozen blood but it is expensive . At present
leucocyte depletion is achieved by filtering donor blood.Transfusion of neocytes obtained by
centrifugation has been proposed in the attempt to reduce the blood requirement , but the results were
not cost effective .
In general , the amount transfused should not exceed 15 to 20 ml/kg/day at a maximum rate of 5ml/kg/hr
to avoid rapid increase of blood volume . The recommended interval between transfusion is usually 2 to
3 weeks.
Complication of transfusions :
1.Febrile reactions : it is seen in 3 – 20 % of patients and may be due to leucocyte or platelet antibodies,
antibodies against RBC antigens, allergic reactions to other plasma or due to pyrogens present in
transfused blood . Febrile reactions usually respond to antipyretic and antihistaminic .
2. Hemolytic transfusion reactions : it occurs in 5 – 15 % of cases. These are due to major or minor
blood group mismatch and are characterized by fever
, chills, tachycardia, restlessness, flushing of face ,chest pain, dyspnoea ,cynosis and collapse. Most
feared complications are acute renal failure, DIC and anaphylactic shock .
3. Transfusion transmitted diseases like malaria , syphilis, hepatitis B, hepatitis C, CMV and
HIV infection can occur. All thalassemics who are negative for the hepatitis B surface antigen
should receive hepatitis B vaccine.
4. Iron overload : Two factors contribute to iron overload in a thalassemic child :
a) Enhanced gastrointestinal absorption of iron ,
b) Transfusional siderosis .
In normal individual 1 mg of iron/day is absorbed from the gut , while in a thalassemic child it may be
as high as 10 mg/day .Each unit of blood contains approximately 200mg of iron (1 mg/ml) ,a patient
who receives 25 to 30 units of blood /year, in the absence of chelation, accumulates more than 70 g of
iron by the third decad of life . The accumulation of iron in tissues causes cellular damage presumably
by accelerating the generation of reactive oxygen species (ROS), which then overwhelm the cell’s
protective ability to reduce them . These uncontained ROS then attack and oxidatively alter cellular
proteins and lipids. Some authors believe that the level of nontransferrin bound iron (NTBI) in the
blood is a major cause of oxidative damage . Iron accumulates in those tissues that have the highest
levels of transferrin receptor , which are primarily the liver , heart , and endocrine organs . Iron
accumulation is documented by measuring levels of ferritn, serum iron, transferrin and calculating the
percent of iron saturation.Though helpful , neither the ferritin level nor the percent iron saturation
provides sufficient definitive information to guide therapy . The gold standard for assessing
accumulation of iron stores is an adequate liver biopsy , followed by measurement of the liver iron
content by histochemical staining or more accurately by atomic absorption spectrometry . An accurate
and noninvasive method for measuring liver iron is SQUID (superconducting quantum interference
device). Unfortunately none of the methods listed above accurately records the extent of cardiac iron
loading and there is a poor correlation between ferritin, liver iron content, and cardiac iron .Even studies
using endomyocardial biopsies have yielded variable results .The traditional diagnostic tools ( i.e. ECG,
holter tracing , echocardiography , nuclear studies ) ,although routinely used , are not predictive of
subsequent cardiac dysfunction. The prognosis for patients with heart failure has always been poor.
CHELATION THERAPY :
To prevent hemosiderosis , iron administered as blood must be chelated and excreted . Two main sources
of chelatable iron are (a) the intracellular pool derived from lysosomal catabolism of ferritin and from
transferrin and NTBI and (b) the iron derived from red cell catabolism in macrophages . The first
contributes to the hepatocellular load and is excreted as fecal iron , where as the second is the ,major
source of urinary iron. Ferric iron has six coordination sites , which need to be chelated completely to
prevent free radical generation .The iron chelators are :
Desferrioxamine (DFO)
Deferiprone :
Deferiprone is an orally effective bidentate iron chelator .Three molecules of deferiprone are required to
effectively chelate one iron molecule and prevent it from generating ROS. Deferiprone can enter cells
and bind iron there , and the iron thus chelated is primarily excreted in the urine . Deferiprone in
customary doses is less effective than DFO in preventing liver iron accumulation . In addition , it causes
arthralgia and leucopenia in 2 % of patients and neutropenia in 0.5 % .Deferiprone may be able to
remove iron from from the heart , as measured by the T2*method and there seems to be parallel
improvement in clinical measures of cardiac disease. Defepriprone being able to pass through
membranes , could ‘shuttle’ tissue iron to DFO in the blood and then be removed .Based on this
investigators are testing a ‘shuttle’ method to treat cardiac hemochromatosis . An initial dose of
deferiprone is given orally presumbly to enter cardiac cells , bind iron there, and then transfer the
chelated iron to the blood. After precisely timed interval , parenteral DFO is given to bind this iron in the
blood and exrete this iron in urine and stool.
ICL670 (EXJADE)
ICL670 is an orally active tridentate chelator that has shown good pharmacokinetics in trials in several
sites . It seems to be relatively nontoxic and removes iron from the liver about as well as DFO , but no
data on its ability to enter cells or remove cardiac iron. This drug has recently been approved by FDA.
SPLENECTOMY
The introduction of regular transfusion has significantly delayed appearance of splenomegaly The
splenectomy should be performed when transfusion requirements exceeds 50 % above that of the
average of the splenectomized population, this occurs when more than 200 – 250 ml/kg/yr of pure RBC
are required to maintain a pretransfusional Hb of 9.0 -9.5 g/dl.Patient undergoing slplenectomy should
receive pneumococcal vaccine , H. influenza vaccine and meningococcalvaccine 4 weeks prior to
surgery . Prophylactic penicillin therapy must be continued life-long
Endocrinopathies :
Iron deposition can damagethe endocrineglands,either ditrectly or throughthe hypothalamic-pituitary
axis. Endocrinopathies are quite common in thalassemic patients . One study found hypogonadism in
22.9% of boys and 12.2% of girls , hypoparathyroidism in 7.6%, short stature in 39.3%. Fertility is
impaired in the more severe forms of thalassemia.
Cardiac Problems :
Cardiac complications are the major cause of death in well-transfused patients with β-thalassemia major.
The more important complications include congestive heart failure and arrhythmias. The underlying
causes are chronic anemia , iron overload , myositis. Cardiomyopathy and pulmonary hypertension.
Monitoring of left ventricular ejection fraction (LVEF) is the most sensitive method for detecting
evolving problems. Recent data indicate that in case of a drop in LVEF to < 45% ,instituting a very
aggressive chelation program can markedly improve cardiac function and survival. Pulmonary
hypertension is now recognized as a major issue, particularly in splenectomized patients. Anecdotal
studies suggest the sildanfil may be beneficial in reducing pulmonary hypertension.
Role of VITAMIN C
Hemosiderotic parients are often found to be vit C deficient .At one hand Vit C enhances DFO induced
iron excretion by helping in conversion of homosiderin to ferritin , but on the other hand it may
potentiate cardiotoxicity .So vitamin C supplementation is therefore recommended only in patients not
affected by myocardiopathy,unsatisfactory iron excretion and demonstrated vitamin C deficiency in
usual dose of 50 – 100 mg/day.
So far only curative therapy in β-thalassemia available is allogeneic haemopoitic stem cell
transplantation but this is successful in only 65-70% of cases and is not available to most patients.
Therefore the mainstay treatment for the majority remains life long blood transfusion in combination
with a rigorous regime of iron chelation . Improved understanding of the pathophysiology and molecular
basis of the disease has provided clues for more effective strategies that aim to correct the defect in β-
globin chain synthesis at the primary level or redress the α/β-globin chain imbalance at the secondary
level. Improved understanding of the , molecular basis of the disease complications, such as iron
overloading, has also provided clues for potential molecular targets at the tertiary level.
Targeting the primary causes of reduced β-globin production involves several strategies including
haemopoietic stem cell transplantation (HSCT), gene therapy using viral vectors and antisense mRNA .
HSCT
Haemopoietic stem cell transplantation is conceptually the simplest and the only approach so far , that
may lead to a definitive cure for β-thalassemia. Patients who stand to derive most benefit from such
treatment are those with early but severe transfusion dependent disease and have few co-morbities. But
the major limitations of HSCT are-
1. Shortage of suitable donors
2. Transplant related mortality (TRM)
3. Graft failure
4. Graft versus host disease (GVHT)
Recent evidence suggests that a cohort of patients who have stable Mixed Chimerism express
sufficient functional β–globin to be transfusion independent. This has led to trials with non-
myeloablative (Mini-) Bonemarrow translplantaion with some encouraging results
particularlly in high risk group (Andreani et al, 2000).
The use of related or non-related umbilical cord blood transplants has extended the donor
pool ,but cord blood transplantations have limited success because of the large numbers of
cells that are required to sustain haemopoiesis
GENE THERAPY
The genetic correction of autologous haematopoitic stem cell overcomes the dual dis- advantages of
donor shortage and GVHD in allogenic HSCT. Gene therapy in thalassemia has to meet following
criteria.
1. Safe and efficient viral / non-viral transfection
2. Erythroid lineage specificity and
3. Therapeutic levels of β-globin expression
Table : potential targets of molecular therapies in β-thalassemia.
TARGET LEVEL MOLECULR TARGETS POTENTIALTHERAPIES
Primary :
β-globin expression All genetic defects Haematopoietic stem cell transplant
gene therapy using lentivirus
Secondary :
Reducing α/β-globin Increased γ-globin expression Gene therapy using lentivirus vectors
Imbalance Synthetic transcription factors
Tertiary :
Promoting erythroid Supplementing inappropriately Human EPO
Survival low EPO
Decreasing iron overload supplementing inappropriately intraperitoneal injections of synthetic
Low hepcidin hepcidin
Antioxidants Reducing oxidative stress vitamins C and E
In recent studies HIV based lentiviral (LV) vectors were shown to stably transmit the human β-globin
gene and a large LCR element , resulting in correction of beta thalassemia intermedia in mice , with
similar reports by several other groups , however the level of expression were insufficient to fully
correct the anemia in thalassemia major mouse model .Insertion of chicken hypersensitive site -4,
chicken insulator element (cHS4) in self in activating (SIN) LV vector resulted in higher and less
variable expression of human β-globin . The levels of β-globin expression achieved from insulated SIN
– LV vector were sufficient phenotypically to correct the thalassemia phenotype in vitro study in four
patients and this correction persisted long term up to 4 month in xenotransplated mice in vivo . In
summary LV vectors have paved the way for clinical gene therapy trial.
HbF Augmentation :
The other object of therapy in the severe beta thalassemias is to increase the synthesis of gamma globin
chains, thereby compensating for the deficit of beta globin. These gamma chains combine with the
excess unmatched accumulating alpha globin chains. The combination produces a useful Hb, namely
HbF (fetal hemoglobin), but more importantly it reduces the burden of the alpha chains that produce
most of the pathophysiology.Apart from gene therapy using lentivirus vectors in murine models being
explored , several classes of agents have been tested, but none has been approved for regular clinical
use, like-
Hydroxyurea
Studies in sickle disease have shown that hydroxyurea, an inhibitor of ribonucleotide reductase, can
result in an increase in HbF. The mechanism is not entirely clear, but hydroxyurea has been given to
patients with beta thalassemia major and intermedia, and to patients with beta thalassemia/HbE disease,
with varying degrees of success . Some patients have become independent of RBC transfusion. In some
cases the Hb level has increased 1–3 g/dl, though in other reports there has been no increase in Hb. The
underlying reasons for this variability of results remain obscure. Hydroxyurea has potentially severe side
effects. It is myelosuppressive, and there is theoretical concern about the dangers of late-onset acute
leukemia or myelodysplastic disease although so far these have not occurred.
Hypomethylating Agents
Inhibitors of methyl-transferase can result in hypomethylation of DNA, a mechanism that overcomes the
normal downregulation of gamma globin synthesis. These inhibitors, 5 Azacytidine and its analog 5-aza-
2'-deoxycytidine (decitabine), have been given to beta thalassemic patients and have produced variable
increases in HbF along with variable increases in Hb levels. Again the lack of predictability has
remained puzzling. Both agents must be given parenterally and both cause myelosuppression.
Combinations of hydroxyurea, hypomethylating agents, and histone deacetylase inhibitors have been
tested in isolated case reports and may be more effective in combination in increasing HbF synthesis.
Conclusion
The β- thalassemias were among the first human diseases to be delineated at the molecular level. Many
clues toward molecular therapy have been derived from the extensive pathophysiological studies, and
treatment is evolving from the management of symptoms and complications to more effective curative
strategies that aim to correct the β-globin chain deficit, such as gene therapy using lentiviral vectors, or
redress the α/β-globin chain imbalance, such as induction of γ-globin chain synthesis by gene
transduction or pharmacological agents . These potential treatement options offer proof of principle of
the molecular mechanism underlying the disease but many are still in evolution.However,three treatment
options are nearing maturity : pharmacological induction of HbF , gene therapy using LV vectors and
mini-(or non-myeloablative -) bonemarrow transplantation.
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