Overview of Hemolytic Anemia - Overview of Hemolytic Anemia - MSD Manual Professional Edition (2024)

At the end of their normal life span (approximately 120 days), senescent red blood cells (RBCs) are removed from the circulation. Hemolysis is defined as premature destruction and hence a shortened RBC life span (< 120 days). Anemia results when bone marrow production can no longer compensate for the shortened RBC survival; this condition is termed uncompensated hemolytic anemia. If the marrow can compensate, the condition is termed compensated hemolytic anemia.

Etiology of Hemolytic Anemia

Hemolysis can be classified according to whether the hemolysis is

  • Extrinsic: From a source outside the red cell; disorders extrinsic to the RBC are usually acquired

  • Intrinsic: Due to an defect within the red cell; intrinsic RBC abnormalities (see table Hemolytic Anemias) are usually inherited

Disorders extrinsic to the red blood cell

Causes of disorders extrinsic to the RBC include

  • trimethoprim/sulfamethoxazole

  • Immunologic abnormalities (eg, autoimmune hemolytic anemia, acquired thrombotic thrombocytopenic purpura, transfusion reactions)

  • Infections

  • Mechanical intravascular hemolysis (microangiopathic hemolytic anemia, including thrombotic microangiopathies, prosthetic heart valve, march hemoglobinuria)

  • Hypersplenism

  • Toxins (eg, lead, copper, insect bites/venom)

  • Thermal injury

Infectious organisms may cause hemolytic anemia through the following mechanisms:

  • Direct action of toxins (eg, Clostridium perfringens)

  • Invasion and destruction of the RBC by the organism (eg, Plasmodium species, Bartonella species, Babesia species)

  • Antibody production (eg, Epstein-Barr virus, mycoplasma)

  • Hemolytic uremic syndrome (caused by Shiga toxin–producing Escherichia coli)

Intrinsic red blood cell abnormalities

Defects intrinsic to the RBC that can cause hemolysis involve abnormalities of the following:

  • RBC membrane

  • Cell metabolism

  • Hemoglobin structure

Abnormalities include

  • Hereditary cell membrane disorders (eg, hereditary spherocytosis)

  • Acquired cell membrane disorders (eg, paroxysmal nocturnal hemoglobinuria)

  • Disorders of RBC metabolism (eg, glucose-6-phosphate dehydrogenase (G6PD) deficiency)

  • Hemoglobinopathies (eg, sickle cell disease, thalassemias, unstable hemoglobins --ie, rare, inherited variants affecting globin genes that decrease stability and solubility of hemoglobin)

Quantitative and functional abnormalities of certain RBC membrane proteins (alpha- and beta-spectrin, protein 4.1, F-actin, ankyrin) cause hemolytic anemias.

Table

Table

Hemolytic Anemias

Mechanism

Disorder or Agent

Disorders extrinsic to the red blood cell

Immunologic abnormalities

Autoimmune hemolytic anemias:

  • Cold antibody

  • Drug-induced

  • Epstein-Barr virus

  • Mycoplasma

  • Paroxysmal cold hemoglobinuria

  • Warm antibody

Transfusion reactions (alloantibody-mediated)

Infectious organisms (direct invasion)

Babesia

Bartonella bacilliformis

Plasmodium falciparum

P. malariae

P. vivax

Mechanical trauma

Disseminated intravascular coagulation (DIC)

Extracorporeal membrane oxygenation (ECMO)

March hemoglobinuria

Valvular heart disorders and mechanical valves

Ventricular assist devices

Primary thrombotic microangiopathies (TMA) including thrombotic thrombocytopenic purpura, atypical or complement-mediated hemolytic uremic syndrome, hemolytic uremic syndrome (shiga toxin-mediated)

Disorders with microangiopathic hemolytic anemia and thrombocytopenia, often considered secondary TMAs, including transplant-associated TMA, HELLP (Hemolysis, Elevated Liver Enzymes, and Low Platelets) syndrome, autoimmune TMA (eg, associated with SLE, catastrophic antiphospholipid syndrome, scleroderma renal crisis), drug-Induced TMA, or related to severe hypertension, infection, or malignancy

Reticuloendothelial hyperactivity

Hypersplenism

Toxin production by infectious organisms

Clostridium perfringens

Shiga toxin

Toxins

Copper (Wilson disease)

Lead

Insect venom

Snake venom

Thermal injury

Associated with burns

Intrinsic red blood cell abnormalities

Acquired red blood cell membrane disorders

Severe hypophosphatemia (depletion of adenosine triphosphate [ATP])

Paroxysmal nocturnal hemoglobinuria

Stomatocytosis

Spur cell anemia (acanthocytosis)

Congenital red blood cell membrane disorders

Hereditary elliptocytosis

Hereditary spherocytosis

Hereditary stomatocytosis

Disorders of hemoglobin synthesis

Hemoglobin C disease

Hemoglobin E disease

Sickle cell disease

Thalassemias

Unstable hemoglobins

Disorders of red blood cell metabolism

Glycolytic pathway defects (eg, pyruvate kinase deficiency)

Hexose monophosphate shunt defects (eg, glucose-6-phosphate dehydrogenase [G6PD] deficiency)

Pathophysiology of Hemolytic Anemia

Hemolysis may be

  • Acute

  • Chronic

  • Episodic

Hemolysis may also be

  • Extravascular

  • Intravascular

  • Both

Normal red blood cell processing

Senescent RBCs lose membrane and are cleared from the circulation by the phagocytic cells of the reticuloendothelial system in the spleen, liver, and bone marrow. Hemoglobin is broken down in these cells primarily by the heme oxygenase system. The iron is conserved and reutilized, and heme is degraded to bilirubin, which is conjugated in the liver to bilirubin glucuronide and excreted in the bile.

Extravascular hemolysis

Most pathologic hemolysis is extravascular and occurs when damaged or abnormal RBCs are cleared from the circulation by the spleen and liver. The spleen contributes to hemolysis by destroying mildly abnormal RBCs or cells coated with warm antibodies. An enlarged spleen may sequester even normal RBCs. Severely abnormal RBCs or RBCs coated with IgG antibodies or complement (C3) are destroyed within the spleen and liver, which (because of its large blood flow) can remove damaged cells efficiently. In extravascular hemolysis, the peripheral smear may show spherocytes or with cold agglutinins, erythrocyte agglutination if the blood is not warmed upon collection.

Intravascular hemolysis

Intravascular hemolysis is an important reason for premature RBC destruction and occurs when the cell membrane has been severely damaged by any of a number of different mechanisms, including

  • Immune phenomena

  • Direct trauma (eg, march hemoglobinuria)

  • Shear stress (eg, defective mechanical heart valves, TMA)

  • Disseminated intravascular coagulation (DIC)

  • Toxins (eg, clostridial toxins, venomous snake bite)

Intravascular hemolysis results in hemoglobinemia when the amount of hemoglobin released into plasma exceeds the hemoglobin-binding capacity of the plasma-binding protein haptoglobin, a protein normally present in concentrations of approximately 100 mg/dL (1.0 g/L) in plasma. Thus, intravascular hemolysis reduces unbound plasma haptoglobin. With hemoglobinemia, unbound hemoglobin dimers are filtered into the urine and reabsorbed by renal tubular cells; hemoglobinuria results when reabsorptive capacity is exceeded. Iron is released from catabolized hemoglobin and embedded in hemosiderin within the tubular cells; some of the iron is assimilated for reutilization and some reaches the urine when the tubular cells slough.

Consequences of hemolysis

Unconjugated (indirect) hyperbilirubinemia and jaundice occur when the conversion of hemoglobin to bilirubin exceeds the liver’s capacity to conjugate and excrete bilirubin. Bilirubin catabolism causes increased stercobilin in the stool and urobilinogen in the urine and sometimes cholelithiasis.

Increased production of erythropoietin by the kidneys in response to the ensuing anemia causes the bone marrow to accelerate production and release of RBCs, resulting in reticulocytosis.

Symptoms and Signs of Hemolytic Anemia

Systemic manifestations of hemolytic anemias resemble those of other anemias and include pallor, fatigue, dizziness, and weakness. Scleral icterus and/or jaundice may occur, and the spleen may enlarge. Thrombosis increases with many forms of hemolytic anemia.

Hemolytic crisis (acute, severe hemolysis) is uncommon; it may be accompanied by chills, fever, back and abdominal pain, and shock. Hemoglobinuria causes red or reddish-brown urine.

Diagnosis of Hemolytic Anemia

  • Peripheral smear and reticulocyte count

  • Serum bilirubin (indirect), lactic dehydrogenase (LDH), and haptoglobin

  • Sometimes antiglobulin (Coombs) test and/or hemoglobinopathy screen

  • Urinalysis

Hemolysis is suspected in patients with anemia and reticulocytosis. If hemolysis is suspected, a peripheral smear is examined and serum bilirubin, LDH, and haptoglobin are measured. The peripheral smear and reticulocyte count are the most important tests to diagnose hemolysis. Antiglobulin testing or hemoglobinopathy screening (eg, high-performance liquid chromatography [HPLC]) can help identify the cause of hemolysis based on the results of the above laboratory investigations. However, in some patients with a hemolytic anemia, the reticulocyte count fails to increase due to factors such as renal insufficiency, infection, or bone marrow failure, creating a hematologic emergency. This lack of the expected compensation (reticulocytopenia) necessitates prompt transfusion therapy.

Abnormalities of RBC morphology often suggest the presence and cause of hemolysis (see table Red Blood Cell Morphologic Changes in Hemolytic Anemias). The presence of spherocytes on the peripheral smear suggests an extravascular cause of hemolysis such as autoimmune hemolytic anemia or hereditary spherocytosis, while the presence of schistocytes or other fragmented red cells suggests an intravascular cause such as microangiopathic hemolytic anemia (eg, thrombotic thrombocytopenic purpura, hemolytic-uremic syndrome, or valvular hemolysis). Other suggestive findings include increased levels of serum LDH and indirect bilirubin, decreased haptoglobin, and the presence of urinary urobilinogen.

Haptoglobin levels can decrease because of hepatocellular dysfunction and can increase because of systemic inflammation. Intravascular hemolysis is suggested by urinary hemosiderin. Urinary hemoglobin, like hematuria and myoglobinuria, produces a positive benzidine reaction on dipstick testing; it can be differentiated from hematuria by the absence of RBCs on microscopic urine examination. Free hemoglobin may make plasma reddish brown, noticeable often in centrifuged blood; myoglobin does not.

Once hemolysis has been identified, the etiology is sought. To narrow the differential diagnosis in hemolytic anemias

  • Consider risk factors (eg, geographic location, genetics, underlying disorder)

  • Examine the patient for splenomegaly

  • Do a direct antiglobulin (direct Coombs) test if cause is not suggested by initial laboratory investigations

Most hemolytic anemias cause abnormalities in one of these variables, and so test results can direct further testing.

Other laboratory tests that can help discern the causes of hemolysis include the following:

  • Quantitative hemoglobin electrophoresis and HPLC

  • RBC enzyme assays

  • Flow cytometry

  • Cold agglutinins

  • Osmotic fragility

  • Genetic testing for membranopathies and enzymopathies

  • If thrombotic microangiopathies are being considered, ADAMTS13 activity, shiga toxin testing if diarrhea, and if negative, consider sequencing of complement regulatory genes and factor H autoantibody testing

Direct Antiglobulin (Direct Coombs) Test

The direct Coombs test is used to determine whether red blood cell (RBC)-binding antibody (IgG) or complement (C3) is present on RBC membranes. The patient's RBCs are incubated with antibodies to human IgG and C3. If IgG or C3 is bound to RBC membranes, agglutination occurs–a positive result. A positive result suggests the presence of autoantibodies to the patient's RBCs. If the patient has received a transfusion in the last 3 months, a positive result could also represent alloantibodies to transfused RBCs (usually occurring in acute or delayed hemolytic reaction).

Indirect Antiglobulin (Indirect Coombs) Test

The indirect Coombs test is used to detect IgG antibodies against red blood cells (RBCs) in a patient's serum. The patient's serum is incubated with reagent RBCs; then Coombs serum (antibodies to human IgG, or human anti-IgG) is added. If agglutination occurs, IgG antibodies (autoantibodies or alloantibodies) against RBCs are present. This test is also used to determine the specificity of an alloantibody.

Table

Table

Red Blood Cell Morphologic Changes in Hemolytic Anemias

RBC Morphology

Causes

Acanthocytes (spur cells)

Abetalipoproteinemia

Anorexia

Hypothyroidism

Liver disease

Neuroacanthocytosis

Agglutinated cells

Cold agglutinin disease

Echinocytes

Glycolytic pathway defects

Liver dysfunction

Renal dysfunction

Heinz bodies (bite or blister cells)

Glucose-6-phosphate dehydrogenase (G6PD) deficiency

Oxidant stress

Unstable hemoglobin

Nucleated erythroblasts and basophilic stippling

Thalassemia major

Schistocytes

Microangiopathic hemolytic anemia (MAHA), including disseminated intravascular coagulation (DIC) and thrombotic microangiopathy (TMA)

Valve hemolysis, Intravascular prostheses, and extracorporeal devices

Vitamin B12 deficiency (pseudo-thrombotic thrombocytopenic purpura [pseudo-TTP])

Sickle cells

Sickle cell disease

Spherocytes

Hereditary spherocytosis

Transfused blood

Warm antibody hemolytic anemia

Target cells

Hemoglobinopathies (eg, sickle cell disease, hemoglobin C disease, thalassemias)

Liver dysfunction

Post-splenectomy

Treatment of Hemolytic Anemia

Treatment depends on the specific mechanism of hemolysis.

Corticosteroids are helpful in the initial treatment of warm antibody autoimmune hemolysis. Transfusions are used in patients with symptomatic anemia or when there is reticulocytopenia.

Splenectomy is beneficial in some situations, particularly when splenic sequestration is the major cause of RBC destruction. If possible, splenectomy is delayed until 2 weeks after vaccination with the following:

  • Haemophilus influenzae vaccine

  • Meningococcal vaccine

In cold agglutinin disease, avoidance of cold is recommended, and blood will need to be warmed before transfusion. Folate replacement is needed for patients with ongoing long-term hemolysis.

Overview of Hemolytic Anemia - Overview of Hemolytic Anemia - MSD Manual Professional Edition (2024)

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