0327 - Red Cell Disorders I Flashcards
What is anaemia?
A reduction in haemoglobin due to quantitative or qualitative impairment in red cell production (including those causing premature cell lysis).
What are the clinical features of haemolytic anaemia?
Pallor
Jaundice
Splenomegaly
Gallstones (bilirubin)
What are some DDX’s for haemolytic anaemia?
Thalassaemia
Sickle Cell Anaemia
Hereditary Spherocytosis
What are the laboratory features of haemolytic anaemia?
RBC/Film, WBC, Platelets, Bilirubin, LDH, Haptoglobin
RBC changes - could be spherocytes, poikilocytes, polychromasia, reticulocytosis
WBC and platelets often normal
Raised bilirubin
Raised LDH (released by lysis)
Low haptoglobin (binds free Hb, so all taken up)
What is the difference between a thalassaemia and a haemoglobinopathy?
Thalassaemia - imbalance in globin chains (e.g. beta thalassaemia)
Haemoglobinopathy - structural abnormality in the globin molecule due to point mutations (e.g. Sickle cell disease)
What is the difference between foetal and adult Hb?
Foetal - alpha and gamma strands (2 of each)
Adult - Alpha and Beta strands (2 of each), with around 3% A2 (alpha and delta strands - 2 of each), which is increased in beta thalassaemia.
Which chromosomes code for alpha and beta haemoglobins?
Alpha - Chromosome 16 (2 places, 4 sites total)
Beta - Chromosome 11 (1 place, 2 sites total)
How does Hb change over foetal gestation?
Hb ramps up to 6 weeks, where around 50% will be alpha, most of rest gamma.
Gamma drops off rapidly at birth, with beta rising significantly from 36 weeks.
How can you test for Haemoglobin qualities and haemoglobinopathies?
High Pressure Liquid Chromatography. Formerly used electrophoresis.
Can also do a DNA study if you know the change you’re looking for.
Provide a brief overview of the pathophysiology of beta thalassaemia major.
Autosomal Recessive - Decreased or no synthesis of beta chain prevents formation of normal Hb tetramere.
Free alpha chains form unstable aggregates, leading to cell membrane damage, loss of K+, and impaired DNA synthesis.
This causes destruction of RBC precursors within marrow, and haemolysis in spleen, leading to anaemia.
Severe enough anaemia leads to extramedullary erythropoiesis (compensation), and skeletal abnormalities in children.
Also leads to excess absorption of iron, which, together with repeated blood transfusions, causes severe iron overload (can now be treated with chelation).
What are the three main problems associated with beta thalassaemia major?
Ineffective erythropoisis
Anaemia
Iron overload leading to organ damage.
What are the clinical features of beta thalassaemia major?
Severe anaemia
Ineffective and extramedullary erythro/haemopoisis
Enlarged liver and spleen
Expansion of flat bones, with spontaneous fractures
Iron overload (biggest problem, now treated with chelation)
Reduced growth, endocrinopathy, delayed puberty
What are the laboratory features of beta thalassaemia major?
Blood film, Marrow, Hb HPLC
Anaemia
Hypochromic cells, target cells, Nucleated RBCs
Marrow - red cell hyperplasia, increased iron
Most Hb is HbF
What is alpha thalassaemia? How can it vary in severity?
Genetic disease characterised by the deletion of any or all of the four normally present alpha-globin chains.
Defect in 1-2 genes - Hypochromic, microcytic blood film, no clinical significance except for genetic counselling.
Defect in 3 genes - HbH disease (tetramers of B-Hb), Thalassaemia intermedia
Defect in 4 genes - Hydrops foetalis.
What is sickle cell anaemia?
Commonest severe structural Hb variant. A disease in which abnormal HbS polymerises when deoxygenated. This forms sickle-shaped cells, which live around 20 days, cannot easily travel through capillaries, and adhere to endothelium, causing infarctions (the main problem). Particularly get trapped in spleen.
