Acquired Haemolytic Anaemias
Can be divided into immune or non-immune
Immune Haemolytic Anaemias
· These can be subdivided into:
· Autoimmune
· Alloimmune
· Drug-induced
Autoimmune Haemolytic Anaemias (AIHA)
· Caused by antibodies produced by patient’s own immune system
· Classified according to thermal properties of antibodies:
· warm antibodies bind to RBC most avidly at 370C
· cold antibodies bind best below 320C
Warm AIHA:
· Antibody usually IgG, but may be IgM or IgA
· Usually facilitate sequestration of sensitized RBCs in spleen
· May be primary or secondary - autoimmune disorders, HIV, chronic lymphocytic leukaemia (CLL), non-Hodgkin's lymphoma (NHL)
· Most common type
Incidence:
· Occurs in either sec but female preponderance reported esp. primary
· Occurs in all ages
Higher incidence of secondary noted in patients > 45 years
Clinical Features:
· Haemolytic anaemia of varying severity
· Tends to remit and relapse
· Symptoms of anaemia
· Jaundice
· Splenomegaly
· Symptoms of underlying disorder (if 20)
Laboratory Features:
· Variable anaemia
· Blood film: polychromasia, microspherocytes
· Severe cases: nucleated RBCs, RBC fragments
· Mild neutrophilia, normal platelet count
· Evan’s syndrome: association with ITP
· Bone marrow: erythroid hyperplasia; underlying lymphoproliferative disorder
· Unconjugated hyperbilirubinaemia
· Haptoglobin levels low
· Urinary urobilinogen usually increased; haemoglobinuria uncommon
Serological Features:
· Direct antiglobulin test (DAT; Coomb's test) usually positive
· DAT: rabbit antiserum to human IgG or complement (Coomb's reagent) added to suspensions of washed RBCs. Agglutination signifies presence of surface IgG or complement
· RBC may be coated with
· IgG alone
· IgG and complement
· complement only
· Rarely anti-IgA and anti-IgM encountered
Treatment:
· Remove/treat underlying cause
· Corticosteroids - high doses then tapering when PCV stabilizes
· Splenectomy:
· patients who fail to respond to steroids
· unacceptably high doses of steroids to maintain adequate PCV
· unacceptable side-effects
· Transfusion
· Immunosuppressive Drugs:
· Azathioprine
· Cyclophosphamide (CTX)
· Others:
· plasmapheresis
· Intravenous immunoglobulin (IVIG)
· Androgens e.g. danazol
Cold AIHA:
· Two major types of cold antibody: cold agglutinins and Donath-Landsteiner antibodies
· Causes either immediate intravascular destruction of sensitized RBCs by complement-mediated mechanisms or sequestration by liver (C3 coated RBCs preferentially removed here)
Cold Agglutinins:
· IgM autoantibodies that agglutinate RBCs optimally between 0 to 50C. Complement fixation occurs at higher temperatures
· Primary - Cold Haemagglutinin Disease (CHAD) or secondary (usually due to infections)
· Peak incidence for CHAD > 50 years
· Primary usually monoclonal; secondary usually polyclonal
Pathogenesis:
· Specificity usually against I/i antigens
· Varying severity depending on:
· titre of antibody in serum
· affinity for RBCs
· ability to bind complement
· thermal amplitude
· Bind red cells in peripheral circulation impeding capillary flow, producing acrocyanosis
Clinical Features:
· Chronic haemolysis; episodes of acute haemolysis can occur on chilling
· Acrocyanosis frequent; skin ulceration and necrosis uncommon
· Mild jaundice and splenomegaly
· Secondary cases e.g. Mycoplasma, self-limited
Laboratory Features:
· Anaemia- mild to moderate
· Blood film: agglutination, spherocytosis less marked than warm AIHA
· DAT +ve: complement only
· Anti-I: idiopathic disease, mycoplasma, some lymphomas
· Anti-i: infectious mono, lymphomas
Treatment:
· Keep patient warm
· Treat underlying cause
· Alkylating agents: chlorambucil, CTX
· Splenectomy and steroids generally not helpful
· Plasmapheresis- temporary relief
· Transfusion- washed packed cells
Paroxysmal Cold Haemoglobinuria
· Rare form of haemolytic anaemia
· Characterized by recurrent haemolysis following exposure to cold
· Formerly, more common due to association with syphilis
· Self-limited form occurs in children following viral infections
· Antibodies usually IgG with specificity for P antigen
· Biphasic: binds to red cells at low temperatures, lysis with complement occurs at 37C
Drug-induced Haemolytic Anaemia
· May cause immune haemolytic anaemia by three different mechanisms:
1) Drug adsorption mechanism e.g. Penicillin
2) Neoantigen type e.g. Quinidine
3) Autoimmune mechanism e.g. a - Methyldopa
Drug adsorption mechanism
· Also known as hapten mechanism
· Drug binds tightly to red cell membrane
· Antibody attaches to drug without direct interaction with RBC
· Usually seen in patients receiving high doses of penicillin – substantial coating of RBC with drug
· Small proportion develop anti-penicillin antibody Ô binds to drug on RBC
· DAT +ve and haemolysis may ensue
· Occurs after 7-10 days of treatment
· Ceases few days to 2 weeks after drug stopped
Neoantigen type
- Formerly known as immune complex / innocent bystander
- Old theory suggested drug formed immune complex with anti-drug antibody Ô attached non-specifically to red cell Ô destruction by complement
- However where complex displays rare specificity for a particular antigen on RBC e.g. I, antibody does not bind to cells lacking that antibody, even in presence of drug
- Suggests that interaction required component of red cell membrane to bind to antigen recognition site on antibody
Autoimmune mechanism
· Truly autoimmune in nature
· Antibody binds to red cell membrane antigens in a manner indistinguishable from sporadic AIHA
· Alpha-methyldopa responsible for most cases
· DAT becomes +ve in 8-36% of patients taking drug
· However, only 0.8% of patients develop clinical haemolysis
· Induces auotimmune red cell antibodies by unknown mechanisms
Alloimmune Haemolytic Anaemias
· Two important situations:
· ABO incompatibility
· Haemolytic disease of the newborn
ACQUIRED HAEMOLYTIC ANAEMIA (2)
Non-immune haemolytic anaemias:
· Paroxysmal nocturnal haemoglobinuria (PNH)
· Red cell fragmentation syndromes
· Infections
· Chemical and physical agents
· Secondary haemolytic anaemia
Paroxysmal nocturnal haemoglobinuria (PNH)
· Acquired haemopoietic stem cell disorder
· Characterized by increased sensitivity of red cells to haemolysis by complement
Pathogenesis:
· Arise as a clonal abnormality of stem cells
· Disorder a consequence of somatic mutations Ô error in synthesis of the glycosylphosphatidylinositol (GPI) anchor
· Results in deficiencies of several GPI-anchored membrane proteins – decay accelerating factor (DAF), membrane inhibitor of reactive lysis (MIRL), acetylcholine esterase, leukocyte alkaline phosphatase (LAP)
· Some of these proteins involved in complement degradation
· Absence of MIRL plays most critical role
Clinical Features:
· Haemoglobinuria occurs intermittently precipitated by a variety of events
· Nocturnal haemoglobinuria uncommon
· Chronic haemolytic anaemia which may be severe
· Iron deficiency due to loss in urine
· Bleeding may occur secondary to thrombocytopenia
· Thrombosis a prominent feature
Laboratory Features:
· Pancytopenia
· Anaemia may be severe
· Macrocytosis may be present due to mild reticulocytosis
· Hypochromic, microcytic due to iron deficiency
· Marrow: erythroid hyperplasia; may be aplastic
· Urine: haemosiderinuria constant feature; haemoglobin sometimes present
· Ham’s (acidified serum lysis) test positive
Treatment:
· Transfusion of washed packed red cells
· Oral iron
· Folate supplements
· Steroids may be of benefit
· Anticoagulation for thrombotic complications
Course:
· Variable
· May transform to acute leukaemia or aplastic anaemia
Red Cell Fragmentation Syndromes
1. Microangiopathic haemolytic anaemia (MAHA)
· Intravascular haemolysis due to fragmentation of normal red cells passing through aneh arterioles
· Deposition of platelets and fibrin most common cause of microvascular lesions
· Red cells adhere to fibrin and are fragmented by force of blood flow
· Underlying disorders:
· Mucin-producing adenocarcinomas
· Complications of pregnancy: Preeclampsia, eclampsia, Haemolysis, Elevated Liver enzymes, Low Platelets (HELLP)
· Disseminated Intravascular Coagulation (DIC)
· Thrombotic Thrombocytopenic Purpura (TTP)/ Haemolytic Uraemic Syndrome (HUS)
· Malignant hypertension
· Drugs: mitomycin, bleomycin, cisplatin
Laboratory Findings:
· Blood film: schistocytes prominent, spherocytes, reticulocytes, normoblasts
· Thrombocytopenia
· Coagulopathy in DIC
Treatment:
· Treat underlying cause
2. Traumatic cardiac haemolytic anaemia
· Seen in patients with prosthetic heart valves, cardiac valvular disorders esp. severe aortic stenosis
· Due to physical damage of red cells from turbulence and high shear
stresses
· Haemolytic anaemia usually mild and well compensated
March Haemoglobinuria
· Due to damage to red cells between small bones of feet
· Usually during prolonged marching or running
· Blood film does not show fragments
Infections
· Cause haemolysis in a variety of ways
· Ppt acute haemolytic crisis in G6PD deficiency
· Cause MAHA e.g. meningococcus
· Direct invasion of red cells by infective organisms e.g. malaria
· Elaboration of haemolytic toxins e.g. clostridium
· Production of red cell autoantibodies e.g. viral infections
Chemical and physical agents
· Certain drugs cause oxidative damage in high doses e.g. dapsone
· Acute haemolytic anaemia due to high levels of Cu e.g. Wilson’s disease
· Chemical poisoning e.g. Pb, chlorate or arsine may cause severe haemolysis
· Severe burns
· Snake / spider bites
· Hypophosphataemia
Secondary haemolytic anaemias
· Red survival shortened in many systemic disorders
· Renal failure – ‘burr’ cells
· Liver disease – acanthocytes, sasaran cells
· Zieve’s syndrome – acute haemolytic anaemia with intravascular haemolysis, hyperlipidaemia and abdominal pain in alcoholics
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