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The Thalassaemia Syndromes Ahmad Sh. Silmi Msc Haematology, FIBMS
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The Thalassaemia Syndromes The thalassaemia are heterogeneous group of inherited disorders, which are characterized by reduced or absent synthesis of one or more globin chain type. The imbalance of globin chain synthesis, which result leads to ineffective erythropoiesis and a shortened red cell lifespan. In contrast to the structural haemoglobinopathies, the affected globin chain is structurally normal; it is only the rate at which it is synthesized which is affected.
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Incidence and Distribution
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The thalassaemia are most common in part of the world where malaria is, or was recently, endemic: the result of positive selection for a gene, which affords some protection against malaria. The distribution of the different forms of thalassaemia is not uniform: each is most commonly found in certain populations. β Thalassaemia is most common in people from the Mediterranean, Africa, India, SE Asia and Indonesia. The incidence of mutations, which lead to β thalassaemia, reaches almost 10% in some parts of Greece. The disorder is relatively rare in Northern and Western Europeans and in native Americans. The clinically mild forms of α thalassaemia (α + thalassaemia) are most common in American blacks, Indonesia, SE Asia, the Middle East, India, and the Mediterranean. 30% of American blacks are silent carriers of α + heterozygous, while 3% are homozygous. Homozygous express minimal symptoms of disease. The clinically sever a thalassaemia (α 0 thalassaemia) are common in people from the Philippines, SE Asia and S China. The population incidence of deletions, which leads to this form, reaches 25% in some parts of Thailand.
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Classification The thalassaemias are classified according to three criteria: 1- The affected globin gene(s) e.g. α, β, dδ, etc. 2- Whether the reduction in synthesis in the affected gene is partial ( β + ) or absolute ( β 0 ). 3- The genotype e.g. homozygous β 0.
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α -Thalassaemia More than 95% of a thalassaemias result from the deletion of one or both of a globin genes located on chromosome 16. This gives rise to five possible genotypes:
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β-Thalassaemia
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Pathophysiology The myriad manifestation of this complex group of disorders result from the imbalanced synthesis of α-like and non- α -like globin chains. Under normal circumstances, the rate of synthesis of α globin must be more or less matched by the total synthesis of β, δ and γ globin chains.
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Pathophysiology Impaired synthesis of α globin results in the accumulation of unpaired non- α globins within the developing erythroblasts and vice versa.
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Pathophysiology Unpaired globin chains are unstable: they form aggregates and precipitate within the cell, causing decreased deformability, membrane damage and selective removal of the damaged cell by reticuloendothelial system.
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Pathophysiology Unpaired α globin chains are extremely insoluble and causes sever damage to the developing erythroblasts. Unpaired β globin chains, on the other hand, form haemoglobin H, which is relatively stable and only precipitate as the red cell ages. Thus moderate impairment of β globin synthesis is associated with a greater degree of ineffective erythropoiesis and haemolysis than an equivalent impairment of α globin synthesis.
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α Thalassaemia The affected individuals in this disease are belonging to one of four groups according to the increasing severity of their symptoms: 1- "silent" carriers 2- α thalassaemia trait 3- haemoglobin H disease 4- haemoglobin Barts hydrops foetalis The groups correspond approximately to the functional equivalent of the deletion of 1, 2, 3 or 4 a globin genes respectively.
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1- "Silent" carriers Deletion of a single a globin gene has no significant effect on the affected individual. As adults, no haematological abnormality can be demonstrated using standard laboratory techniques (excluding DNA analysis). Umbilical cord blood of newborns may contain 1% of haemoglobin Barts (γ 4 ). Such individuals can only be defined with complete reliability by DNA analysis.
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2- α Thalassaemia Trait Individuals with deletion of two α globin genes may be: α + homozygous (α-/α-) or α 0 heterozygous (- -/ α α). It's important to know to which group a given individual belong to give accurate genetic counseling. The two groups are clinically indistinguishable and present identical laboratory results.
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Laboratory findings of Thalassaemia Trait Affected individuals typically show: 1- Mild microcytic hypochromic anaemia with no significant symptoms. 2- Precipitated haemoglobin H (- - /α -) can be demonstrated by supravital stain in small minority of red cells. 3- Umbilical cord blood contains up to 10% of haemoglobin Barts.
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3- Haemoglobin H Disease It's arises from the deletion of three α globin genes. The severity of Hb H is highly variable. It's characterized by a moderately sever anaemia and hepatosplenomegally. Typically, the haemoglobin level is maintained around 8 g/dl, and transfusion support is unnecessary. Extramedullary haemopoiesis and skeletal abnormalities are uncommon.
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Laboratory Findings The Peripheral blood film includes: Microcytosis, hypochromasia, fragmented red cells, poikilocytosis, and polychromasia and target cells. Multiple haemoglobin H inclusions are seen in most of the cells; these bodies cause haemolytic anaemia, which characterizes the condition. Umbilical cord blood contains up to 40% haemoglobin Barts. Adult's blood contains between 5-35% of haemoglobin H.
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4- Haemoglobin Barts Hydrops Foetalis The most sever form of a thalassaemia results from the deletion of all four a globin genes and so is associated with a complete absence of a globin synthesis.
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4- Haemoglobin Barts Hydrops Foetalis Because of the absence of a globin synthesis, no functionally normal haemoglobins are formed after the cessation of ζ globin synthesis at about 10 weeks gestation. Instead, functionally useless tetrameric molecules such as haemoglobin Barts (γ 4 ) and haemoglobin H (β 4 ) are synthesized. Thus, although the haemoglobin concentration at delivery typically is about 6 g/dl, functional anaemia is much more sever. The severity of anaemia causes gross oedema secondary to congestive cardiac failure and massive hepatosplenomegally. Pregnancy usually terminates in a third trimester stillbirth, often after a difficult delivery.
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Laboratory Findings The peripheral blood smear shows marked microcytosis, hypochromasia, poikilocytosis, fragmentation and numerous nucleated red cells. Haemoglobin electrophoresis confirms this abnormality.
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β Thalassaemia β Thalassaemia usually results from point mutations within the β globin gene cluster, β thalassaemia can be classified according to the severity of their symptoms into three groups: 1- β thalassaemia minor (or trait) 2- β thalassaemia major 3- β thalassaemia intermediate
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1- β Thalassaemia minor It's the mildest form, which arises from the inheritance of a single abnormal β globin gene. Typically, the affected individual exhibits no significant signs of the disease, and may be unaware of the condition, and generally live a normal lifespan.
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Laboratory findings Microcytic hypochromic anaemia, with target cells a prominent feature in the peripheral blood film. Red blood cell count is high to compensate for the generated anaemia. Haemoglobin level is around 10-11 g/dl. Reticulocyte is slightly increased. White blood cells is normal
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Bone marrow : Generally shows some degree of erythroid hyperplasia and mild ineffective erythropoiesis. Iron storage is slightly increased. Haemoglobin Electrophoresis: Hb F(2 - 6 % ) Hb A 2 ( 3 - 7 %) Hb A (87 - 95 %)
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Beta thalassemia - heterozygous (minor or trait)
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2- β Thalassaemia major β Thalassaemia major results from the inheritance of two b thalassaemia genes. Affected individuals are either homozygous or double heterozygous for two distinct mutations. In the absence of treatment, the condition is characterized by : 1- sever anaemia 2- gross splenomegally 3- Frequently hepatomegally 4- Retarted growth 5- Facial mongoloid appearance 6- Rarely live beyond the second decay.
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Laboratory findings 1.peripheral blood Sever haemolytic anaemia with Hb< 7.0 g/dl Microcytic hypochromic due to decrease globin synthesis. Marked anisocytosis and poikilocytosis. Increased polychromatophilia. Numerous target cells. Howell-jolly bodies and sedrocyte are common. Increased NRBC's ( 200 or more / 100 WBC's) Increased reticulocyte. WBC is slightly increased with occasional immature granulocyte. Platelets are slightly increased
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2- Bone Marrow: The bone marrow shows erythroid hyperplasia, and excess blood transfusion & haemolysis will lead to precipitation of iron in spleen and liver. 3- Biochemical tests: Haptoglobin is decreased. Bilirubin is increased.
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4- Haemoglobin Electrophoresis Analysis of the haemoglobins present reveals a marked increase in Hb F, the precise value of which is dependent on the genetic defect(s) present. for example: In homozygous β 0 thalassaemia: Hb F accounts for up to 98 % of the total. In double heterozygous β + thalassaemia: Hb F accounts for 40-60 % Hb A2 is increased in both defects. The increase in d and g chains is a compensatory mechanism due to the decrease in the production of β chain.
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Beta thalassemia major
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Beta thalassemia major treatment Transfusion Iron chelation stem cell transplant
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3- β Thalassaemia intermedia Typically, thalassaemia intermedia arise from one of three circumstances: Inheritance of mild β thalassaemia mutations. Co-inheritance of a gene which increases the rate of γ globin synthesis. Co-inheritance of α thalassaemia. Reduction in a globin synthesis reduces the imbalance in α: non-α globin synthetic ratio.
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3- β Thalassaemia intermedia Thalassaemia intermedia encompass all cases of β thalassaemia with significant symptoms of disease which do not require regular transfusion to maintain their haemoglobin level above 7 g/dl. The laboratory and clinical features of this condition mirror those of the more sever phenotype. The major cause of morbidity is due to iron overload as a result of increase gastrointestinal absorption of dietary iron in anaemic patients; these results in increase total body iron. The bone marrow is massively imposed by erythroid hyperplasia, this leads to increase demand of iron, which exceeds the supply capacity of the reticuloendothelial system. Thus functional iron deficiency is present, despite raised in iron stores.
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Stepwise approach to the diagnosis of thalassemia
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