Sideroblastic anemia

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Synonyms and keywords: Sideroblastic anaemia

Overview

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

Sideroblastic anemia is diverse type of anemia with both congenital and acquired underlying causative factors. The resulting anemia varies in severity. Ring sideroblasts in the bone marrow are the pathognomic feature of both congenital and acquired sideroblastic anemias. Ringed sideroblasts are the erythroblasts in bone marrow with iron loaded mitochondria and are visualized with prussian blue staining. The underlying cause for these iron deposits is defect in incorporation of iron in to heme resulting in accumulation of iron in mitochondria. The main acquired factors in etiology of sideroblastic anemia are alcohol and drugs, which responds well to removing the underlying agent and pyridoxine therapy. The common forms of congenital sideroblastic anemias are X-linked sideroblastic anemia due to an ALAS2 mutation and the autosomal recessive pattern with mutations in SLC25A38 genes. Overall, XLSA is a benign disorder and mostly responds to pyridoxine. The congenital autosomal recessive sideroblastic anemia due to SLC25A38 mutations is considered to be more severe. It does not respond to pyridoxine. The patients are usually of young age and stem cell transplantation is the only treatment of these patients.

Ring sideroblasts

Ring sideroblasts are erythroblasts with iron-loaded mitochondria visualized by Prussian blue staining (Perls’ reaction) as a perinuclear ring of blue granules

Historical Perspective

X-linked sideroblastic anemia was first described by Cooley (1945), a Detroit pediatrician-hematologist. He considered possible X-linkage in a family in which 19 males in 5 generations were affected, with transmission through unaffected females. In 1946 Rundles and Falls reported 2 families. Slightly enlarged spleens and minor red cell abnormalities without anemia were observed in female carriers. Pyridoxine responsiveness was observed in at least 2 affected members of Rundles and Falls’ family In 1961 Byrd and Cooper named the disorder as hereditary iron-loading anemia. In 1983 Peto et al concentrated on iron overload in mild sideroblastic anemia after the death from cardiac siderosis of a middle-aged woman with a very mild form of familial sideroblastic anemia. Cotter et al. (1995) described a previously healthy 81-year-old woman with microcytic sideroblastic anemia. The diagnosis of the X-linked congenital sideroblastic anemia resulted in successful treatment with pyridoxine. She was diagnosed to be heterozygous for a point mutation of the ALAS2 gene. Aivado et al. (2006) reported a family in which a mother and her 2 daughters had sideroblastic anemia that was unresponsive to pyridoxine. It was confirmed by genetic analysis. The disorder was variable in severity and X-chromosome inactivation studies were done. In 1971 Hines found decreased levels of pyridoxal phosphokinase in red cells and livers of patients with pyridoxine-dependent refractory sideroblastic anemia. In 1973A oki et al found deficiency of delta-aminolevulinic acid synthetase in the red cells of patients with sideroblastic anemia. In 2001 Levi et al discovered that iron accumulates in the mitochondria.

Classification

sideroblastic anemia may be classified according to its etiology into two groups, congenital and acquired. Congenital catagory include X-linked, autosomal and mitochondrial DNA defects. Acquired sideroblastic anemias is divided in to 2 catogries, acquired reversible and acquired clonal. Sideroblastic anemias secondry to alcohol ingestion,drugs like isoniazid and chloramphenicol, comes under the catagory of acquired reversible sideroblastic anemia. Copper and vitamin B6 deficiency also causes acquired reversible sideroblastic anemias. Acquired clonal sideroblastic anemias include refractory anaemia with ring sideroblasts (RARS) refractory anaemia with multilineage dysplasia and ring sideroblasts (RCMD) and refractory anaemia with ring sideroblasts and thrombocytosis (RARS-T). sideroblastic anemia can be divided according to MCV mean corpuscular volume in to two catogries, MCV decreased and MCV normal or increased. X linked sideroblastic anemia in males, X linked sideroblastic anemia with ataxia, and autosomal recessive congenital sideroblastic anemia (ARCSA) present with low MCV. Isoniazid also causes low MCV. Alcoholism, copper defeciency, X linked sideroblastic anemia in females and pearson marrow-pancreas syndrome will show either high or normal MCV

Pathophysiology

It is understood that sideroblastic anemia is the result of defects in the steps of heme biosynthesis that occur within the mitochondrion. Sideroblasts are the pathognomic feature of sideroblastic anemia. There is deffect in incorporation of iron in to heme. As a result the iron accumulates in mitochondria of red cell precursors. Ring sideroblasts are erythroblasts that have iron-loaded mitochondria. The iron granules are arranged around the nucleus in a ring form. They can be seen with prussian blue staining as blue granules around the nucleus.The pathophysiology of sideroblastic anemia depends on the underlying cause. Impaired hemoglobin production, results in reduced number of mature erythrocytes. Resulting anemia is usually microcytic and hypochromic. The iron overload in sideroblastic anemia is due to abnormalities in iron utilization. There is increased iron transport to erythroblasts. Since the body sense anemia intestinal iron absorption increases. There is increased iron content in mitochondria of erythroblasts and systemic iron accumulation. Systemic iron overload occurs only in some forms of sideroblastic anemia, usually when the defects in iron metabolisms involve earlier stages of erythroid pathways. The development of congenital sideroblastic anemia is the result of multiple genetic mutations in several genes involved in heme synthesis resulting in autosomal recessive congenital sideroblastic anemia. Out of many genes SLC25A38 mutations is the most common.

Causes

There are no life-threatening causes of sideroblastic anemia, however complications resulting from untreated sideroblastic anemia are common. Common causes of sideroblastic anemia include, alcoholism, chloramphenicol, isoniazid, copper deficiency (nutritional, zinc-induced, copper chelation), vit B-6 deficiency, X-linked sideroblastic anemia. Less common causes of sideroblastic anemia include those associated with myelodysplastic syndrome, autosomal recessive disorders, X-linked sideroblastic anemia, defect in ALAS2 autosomal recessive sideroblastic anemia with mutations in the SLC25A38 gene and genetic syndromes.

Differentiating Sideroblastic anemia overview from Other Diseases

Epidemiology and Demographics

Patients of all age groups may develop sideroblastic anemia. The incidence of acquired sideroblastic anemia increases with age; the median age at diagnosis is 74 years. Chronic sideroblastic anemia is usually first diagnosed among middle and older age group. There is no racial predilection to sideroblastic anemia. Males are more commonly affected than females in X-linked recessive types of sideroblastic anemia.

Risk Factors

Common risk factors in the development of sideroblastic anemia are male gender (X-linked SA) family history of hreditary SA. chronic alcohol abuse.Less common risk factors in the development of sideroblastic anemia are drugs, isoniazid, pyrazinamide, chloramphenicol, cycloserine, and azathioprine, copper deficiency and pyridoxine deficiency. Hypothermia causes sideroblastic anemia by affecting mitochondrial functions.

Screening

According to The National Center for Biotechnology Information NCBI, screening for sideroblastic anemia by using one of the tests, mitochondrial focused nuclear gene panel, congenital sideroblastic anemia panel and PUS1 gene sequencing is available for, molecular confirmation of genetic sideroblastic anemia, testing of patients with positive family history of sideroblastic anemia and prenatal diagnosis for gene mutation in at-risk pregnancies.

Natural History, Complications, and Prognosis

Natural History

Majority of patients of sideroblastic anemia at the time of diagnosis shows erythroid abnormalities and ineffective erythropoiesis. Granulocytic and megakaryocytic cell lines involvement is also common. In the initial stages bone marrow reveal erythroid expansion with ineffective erythropoiesis. Progression to bone marrow failure occurs in the course of the disease. The next phase in natural history of sideroblastic anemia is iron overload and evolution to nonlymphocytic leukemia. The most common causes of death are related to complications of iron overload and evolution into acute nonlymphocytic leukemia ANLL.

Complications

Common complications of sideroblastic anemia include secondry hemochromatosis , thrombocytopenia, growth retardation, blindness, deafness, Ineffective erythropoiesis. myocardial siderosis, liver cirrhosis and malabsorption.

Prognosis

Depending on the type of sideroblastic anemia the prognosis may vary. However, the prognosis is generally regarded as good. Sideroblastic anemia secondry to drugs or alcohol as underlying cause is associated with the most favorable prognosis. (5-10%) of Severe refractory sideroblastic anemias associated with MDS undergo leukemic transformation. and acute myeloid leukemia markedly reduce life expectancy. Patients who do not need blood transfusions are likely to be long-term survivors. The transfusion dependent are at risk of death from the complications of secondary hemochromatosis.

Diagnosis

Diagnostic Criteria

Sideroblastic anemia may be diagnosed at any time if one or more of the following criteria are met, microcytic hypochromic anemia and ring sideroblasts.

History and Symptoms

The hallmark of sideroblastic is fatigue, decreased tolerence to physical activity and dizziness. A positive history of toxin or drug exposure, family history of unexplained anemia, and alcoholism is suggestive of sideroblastic anemia. The most common symptoms of sideroblastic anemia include malaise, irritibility, fatigue, dyspnea on exertion, and palpiataion. Less common symptoms are diarrhea, polyuria, deafness, blindness, and abdominal pain.

Physical Examination

Patients usually presents with signs of anemia with pale skin, dyspnea, tachycardia. Growth retardation is seen in children. Other signs include hypothermia, lead line on teeth margins, photosensitivity, petechiae, optic atrophy, ataxia, incoordination. Hepatosplenomegaly is common patients with iron overload.

Laboratory Findings

Laboratory findings consistent with the diagnosis of sideroblastic anemia include decreased MCV, low reticulocyte count, increased ferritin levels, decreased total iron binding capacity. Hematocrit falls to 20-30%. Serum iron levels are high so as transferrin saturation. In sideroblastic anemia associated with lead toxicity, basophilic stippling of red blood cells on peripheral smear is common. Prussian Blue stain of RBC in marrow, shows ringed sideroblasts. sideroblastic anemia that is associated with myelodysplastic syndrome (MDS), may show leukopenia, and thrombocytopenia,

Imaging Findings

No imaging studies are usually done for sideroblastic anemia.

Other Diagnostic Studies

Genetic testing is done to diagnose the type of mutations and diagnose the disease in high risk patients with positive family history of sideroblastic anemia.

Treatment

Medical Therapy

The medical therapy for sideroblastic anemia include pyridoxine, thiamine and follic acid. For iron overload iron chelators are used. In severe cases, bone marrow transplant is also an option with limited information about the success rate.

Surgery

there is no surgical treatment for sideroblastic anemia.

Prevention

Effective measures for the prevention of acquired sideroblastic anemia include refraining from alcohol, avoiding excessive intake of zinc, nutritional supplements, pyridoxine prophylaxis in patients recieving isoniazid.

References

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Historical Perspective

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

X-linked sideroblastic anemia was first described by Cooley (1945), a Detroit pediatrician–hematologist. He considered possible X-linkage in a family in which 19 males in 5 generations were affected, with transmission through unaffected females. In 1946 Rundles and Falls reported 2 families. Slightly enlarged spleens and minor red cell abnormalities without anemia were observed in female carriers. Pyridoxine responsiveness was observed in at least 2 affected members of Rundles and Falls’ family In 1961 Byrd and Cooper named the disorder as hereditary iron-loading anemia. In 1983 Peto et al concentrated on iron overload in mild sideroblastic anemia after the death from cardiac siderosis of a middle-aged woman with a very mild form of familial sideroblastic anemia. Cotter et al. (1995) described a previously healthy 81-year-old woman with microcytic sideroblastic anemia. The diagnosis of the X-linked congenital sideroblastic anemia resulted in successful treatment with pyridoxine. She was diagnosed to be heterozygous for a point mutation of the ALAS2 gene. Aivado (2006) reported a family in which a mother and her 2 daughters had sideroblastic anemia that was unresponsive to pyridoxine. It was confirmed by genetic analysis. The disorder was variable in severity and X-chromosome inactivation studies were done. In 1971 Hines found decreased levels of pyridoxal phosphokinase in red cells and livers of patients with pyridoxine-dependent refractory sideroblastic anemia. In 1973A Oki found deficiency of delta-aminolevulinic acid synthetase in the red cells of patients with sideroblastic anemia. In 2001 Levi discovered that iron accumulates in the mitochondria of red cell precursors.

Historical Perspective

X-linked sideroblastic anemia was first described by Cooley (1945), a Detroit pediatrician-hematologist.
He considered possible X-linkage in a family in which 19 males in 5 generations were affected, with transmission through unaffected females.
In 1946 Rundles and Falls reported 2 families.
Slightly enlarged spleens and minor red cell abnormalities without anemia were observed in female carriers.
Pyridoxine responsiveness was observed in at least 2 affected members of Rundles and Falls’ family
In 1961 Byrd and Cooper named the disorder as hereditary iron-loading anemia
In 1983 Peto et al concentrated on iron overload in mild sideroblastic anemia after the death from cardiac siderosis of a middle-aged woman with a very mild form of familial sideroblastic anemia.
Cotter Pd. (1995) described a previously healthy 81-year-old woman with microcytic sideroblastic anemia.
The diagnosis of the X-linked congenital sideroblastic anemia resulted in successful treatment with pyridoxine.
She was diagnosed to be heterozygous for a point mutation of the ALAS2 gene.
Aivado (2006) reported a family in which a mother and her 2 daughters had sideroblastic anemia that was unresponsive to pyridoxine.
It was confirmed by genetic analysis.
The disorder was variable in severity and X-chromosome inactivation studies were done.
In 1971 Hines found decreased levels of pyridoxal phosphokinase in red cells and livers of patients with pyridoxine-dependent refractory sideroblastic anemia.
In 1973A oki found deficiency of delta-aminolevulinic acid synthetase in the red cells of patients with sideroblastic anemia.
Cotter in 1994 identified mutation in the ALAS2 gene.
In 2001 Levi discovered that iron accumulates in the mitochondria.^[1]

References

↑ Aivado M, Gattermann N, Rong A, Giagounidis AA, Prall WC, Czibere A, Hildebrandt B, Haas R, Bottomley SS (2006). “X-linked sideroblastic anemia associated with a novel ALAS2 mutation and unfortunate skewed X-chromosome inactivation patterns”. Blood Cells Mol. Dis. 37 (1): 40–5. doi:10.1016/j.bcmd.2006.04.003. PMID 16735131.

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Classification

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

sideroblastic anemia may be classified according to its etiology into two groups, congenital and acquired. Congenital catagory include X-linked, autosomal and mitochondrialDNA defects. Acquired sideroblastic anemias is divided in to 2 catogries, acquired reversible and acquired clonal. Sideroblastic anemias secondry to alcohol ingestion,drugs like isoniazid and chloramphenicol, comes under the catagory of acquired reversible sideroblastic anemia. Copper and vitamin B6 deficiency also causes acquired reversible sideroblastic anemias. Acquired clonal sideroblastic anemias include refractory anaemia with ring sideroblasts (RARS) refractory anaemia with multilineage dysplasia and ring sideroblasts (RCMD) and refractory anaemia with ring sideroblasts and thrombocytosis (RARS-T). sideroblastic anemia can be divided according to MCV mean corpuscular volume in to two catogries, MCV decreased and MCV normal or increased. X linked sideroblastic anemia in males, X linked sideroblastic anemia with ataxia, and autosomal recessive congenital sideroblastic anemia (ARCSA) present with low MCV. Isoniazid also causes low MCV. Alcoholism, copper defeciency, X linked sideroblastic anemia in females and pearson marrow-pancreas syndrome will show either high or normal MCV.

Classification

Sideroblastic anemia may be classified according to its etiology into two groups:^[1]^[2]

Congenital
Acquired


Congenital sideroblastic anaemias
X-linked	X-linked sideroblastic anaemia (XLSA) X-linked sideroblastic anemia with ataxia (XLSA/A)
Autosomal	Glutaredoxin-5 deficiency Thiamine-responsive megaloblastic anaemia (TRMA) Associated with erythropoietic protoporphyria (EPP) Myopathy lactic acidosis and sideroblastic anaemia (MLASA)
Mitochondrial DNA	Pearson syndrome


Acquired sideroblastic anaemias
Acquired reversible SA	Alcoholism Drugs (chloramphenicol, isoniazid) Copper deficiency (nutritional, zinc-induced, copper chelation) Vit B-6 deficiency
Acquired clonal SA	Refractory anaemia with ring sideroblasts (RARS) Refractory anaemia with multilineage dysplasia and ring sideroblasts (RCMD) Refractory anaemia with ring sideroblasts and thrombocytosis (RARS-T)

sideroblastic anemias can be subdivided according to red blood cell size (microcytic or normocytic-to-macrocytic)


MCV decreased	MCV normal or increased
Isoniazid	Alcoholism
X-linked sideroblastic anemia (XLSA) in males	Copper deficiency
Autosomal recessive congenital sideroblastic anemia (ARCSA)	X-linked sideroblastic anemia (XLSA) in females
SIFD (ARCSA with immunodeficiency)	X-linked MLASA varian
Erythropoietic protoporphyria (EPP)	Pearson marrow-pancreas syndrome
X-linked sideroblastic anemia with ataxia	TRMA
	MDS-RS-SLD
	MDS-RS-MLD
	MDS/MPN-RS-T

MCV: mean corpuscular volume; XLSA: X-linked sideroblastic anemia; ARCSA: autosomal recessive congenital sideroblastic anemia; SIFD: sideroblastic anemia with B cell immunodeficiency, periodic fevers, and developmental delay; MLASA: myopathy, lactic acidosis, and sideroblastic anemia; TRMA: thiamine-responsive megaloblastic anemia; MDS-RS-SLD: myelodysplastic syndrome with ring sideroblasts and single lineage dysplasia; MDS-RS-MLD: myelodysplastic syndrome with ring sideroblasts and multilineage dysplasia; MDS/MPN-RS-T: myelodysplastic/myeloproliferative neoplasm with ring sideroblasts and thrombocytosis

References

↑ Fujiwara T, Harigae H (December 2013). “Pathophysiology and genetic mutations in congenital sideroblastic anemia”. Pediatr Int. 55 (6): 675–9. doi:10.1111/ped.12217. PMID 24003969.
↑ Cazzola M, Invernizzi R (June 2011). “Ring sideroblasts and sideroblastic anemias”. Haematologica. 96 (6): 789–92. doi:10.3324/haematol.2011.044628. PMC 3105636. PMID 21632840.

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Pathophysiology

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

It is understood that sideroblastic anemia is the result of defects in the steps of heme biosynthesis that occur within the mitochondrion. Sideroblasts are the pathognomic feature of sideroblastic anemia. There is deffect in incorporation of iron in to heme. As a result the iron accumulates in mitochondria of red cell precursors. Ring sideroblasts are erythroblasts that have iron-loaded mitochondria. The iron granules are arranged around the nucleus in a ring form. They can be seen with prussian blue staining as blue granules around the nucleus.The pathophysiology of sideroblastic anemia depends on the underlying cause. Impaired hemoglobin production, results in reduced number of mature erythrocytes. Resulting anemia is usually microcytic and hypochromic. The iron overload in sideroblastic anemia is due to abnormalities in iron utilization. There is increased iron transport to erythroblasts. Since the body sense anemia intestinal iron absorption increases. There is increased iron content in mitochondria of erythroblasts and systemic iron accumulation. Systemic iron overload occurs only in some forms of sideroblastic anemia, usually when the defects in iron metabolisms involve earlier stages of erythroid pathways. The development of heriditory sideroblastic anemia is the result of multiple genetic mutations in several genes involved in heme synthesis resulting in autosomal recessive congenital sideroblastic anemia. Out of many genes SLC25A38 mutations is the most common.

Pathophysiology

Physiology

Image showing Heme structuresource:By SubDural12 [Public domain, from Wikimedia Commons]

Heme is porphyrin containing compound, with an Fe iron ion in the centre,surrounded by heterocyclic organic ring of porphyrin.

The normal physiology of heme synthesis can be understood as follows:^[1]

Mitochondria in the developing erythroid cells are the cellular site of heme production and iron utilization.
Glycine combines with succinylcoA to form aminolenolinic acid(ALA)
This reaction is catalyzed by ALA sunthetase enzyme (ALAS2) in mitochondria
ALA synthetase requires vit B-6 as a cofactor
Two molecules of aminolenolinic acid condense in cytosol to form porphobilinogen(PBG)
This reaction is catalyzed by zinc containing enzyme called ALA dehydratase.
Multiple enzymatic transformations in cytoplasm produce coproporphyrinogen III (CPG).
Coproporphyrinogen III (CPG) enters the mitochondrion.
Additional modifications of CPG in mitochondrion produces protoporphyrin IX.
The final step is the insertion of iron into the protoporphyrin IX ring producing heme.
This final reaction is catalyzed by enzyme ferrochelatase.

Pathogenesis

Image showing Heme synthesis source:By Wmheric [CC BY-SA 3.0 (https://creativecommons.org/licenses/by-sa/3.0) [Public domain], from Wikimedia Commons]

It is understood that sideroblastic anemia is the result of defects in the steps of heme biosynthesis that occur within the mitochondrion.^[2]
Sideroblasts are the pathognomic feature of sideroblastic anemia.
- There is deffect in incorporation of iron in to heme.
- As a result the iron accumulates in mitochondria of red cell precursors
  - Ring sideroblasts are erythroblasts that have iron-loaded mitochondria.
  - The iron granules are arranged around the nucleus in a ring form
  - They can be seen with prussian blue staining as blue granules around the nucleus.^[3]

The pathophysiology of sideroblastic anemia depends on the underlying cause.^[4]

The X-linked hereditary sideroblastic anemias result from mutations in the gene encoding ALAS2.

Isoniazide, produces sideroblastic anemia in people who dont use pyridoxine prophylaxis,
- Pyridoxine is a cofactor for ALAS2 enzyme.
- Its deficiency directly impairs ALAS2 function

Mitochondrial cytopathies
- Result from deletions of portions of the mitochondrial genome .
- The consequent marked mitochondrial dysfunction causes sideroblastic anemia in these disorders.
Ethanol is the most common cause of toxin-induced sideroblastic anemia.
Ethanol causes sideroblastic anemia by two mechanisms
- Direct antagonism to pyridoxal phosphate
- Dietary deficiency of this compound.
- The bone marrow shows sideroblasts and vacuoles in the normoblasts in ethanol toxicity.
Lead intoxication causes sideroblastic anemia by inhibiting two enzymes in heme pathway:
- ALA dehaydratase
- Ferrochelatase
Penicillamine or triethylene tetramine dihydrochloride (Trientene or TTH) used in treatment of Wilsons disease can produce sideroblastic anemia.
- Excessive chelation produces copper deficiency.
- Copper catalyzes the last step in heme biosynthesis, insertion of iron into protoporphyrin IX.
Zinc intoxication causes sideroblastic anemia in patients using large amount of zinc supplements.
Excessive zinc reduces serum copper levels.

Mechanism of iron overload

Abnormalities in iron utilization in sideroblastic anemia
There is increased iron transport to erythroblasts since the body senses anemia.
Intestinal iron absorption increases.
There is increased iron content in mitochondria of erythroblasts and systemic iron accumulation.
Systemic iron overload occurs only in some forms of sideroblastic anemia, usually when the defects in iron metabolisms involve earlier stages of erythroid pathways.

Genetics

The development of sideroblastic anemia is the result of multiple genetic mutations in several genes involved in heme synthesis resulting in autosomal recessive congenital sideroblastic anemia (ARCSA)^[2]^[4]

SLC25A38 –SLC25A38 mutations is the most common. SLC25A38 encodes an erythroid-specific mitochondrial amino acid carrier that transports glycine into mitochondria for the first step in heme synthesis.

GLRX5 – GLRX5 encodes protein used in the synthesis of iron-sulfur (Fe-S) clusters.

HSPA9 – HSPA9 encodes the mitochondrial HSP70 homologue HSPA9, which is also involved in Fe-S cluster formation.

FECH – FECH encodes ferrochelatase, the final enzyme in the heme synthesis pathway, which inserts an iron atom into protoporphyrin IX

X-linked sideroblastic anemia with ataxia (ABCB7 mutation)
Pearson syndrome ( mitochondrial DNA deletion)
- Pearson syndrome is a congenital condition
- It affects multiple systems,
- Results in severe sideroblastic anemia, thrombocytopenia and neutropenia.
- Pancreatic insufficiency, lactic acidosis, and growth retardation are other common features.

References

↑ Layer G, Reichelt J, Jahn D, Heinz DW (June 2010). “Structure and function of enzymes in heme biosynthesis”. Protein Sci. 19 (6): 1137–61. doi:10.1002/pro.405. PMC 2895239. PMID 20506125.
↑ ^2.0 ^2.1 Fleming MD (2011). “Congenital sideroblastic anemias: iron and heme lost in mitochondrial translation”. Hematology Am Soc Hematol Educ Program. 2011: 525–31. doi:10.1182/asheducation-2011.1.525. PMID 22160084.
↑ Cazzola M, Invernizzi R (June 2011). “Ring sideroblasts and sideroblastic anemias”. Haematologica. 96 (6): 789–92. doi:10.3324/haematol.2011.044628. PMC 3105636. PMID 21632840.
↑ ^4.0 ^4.1 Fujiwara T, Harigae H (December 2013). “Pathophysiology and genetic mutations in congenital sideroblastic anemia”. Pediatr Int. 55 (6): 675–9. doi:10.1111/ped.12217. PMID 24003969.

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Causes

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

There are no life-threatening causes of sideroblastic anemia, however complications resulting from untreated sideroblastic anemia is common.Common causes of sideroblastic anemia may include, alcoholism, chloramphenicol, isoniazid, copper deficiency (nutritional, zinc-induced, copper chelation), vit B-6 deficiency, X-linked sideroblastic anemia. Less common causes of sideroblastic anemia include myelodysplastic syndrome, autosomal recessive disorders, X-linked sideroblastic anemia. defect in ALAS2, autosomal recessive sideroblastic anemia with mutations in the SLC25A38 gene and genetic syndromes.

Causes

Life-threatening Causes

There are no life-threatening causes of sideroblastic anemia, however complications resulting from untreated sideroblastic anemia are common.

Common Causes

Common causes of sideroblastic anemia may include:^[1]^[2]

Alcoholism
Chloramphenicol
Isoniazid
Copper deficiency (nutritional, zinc-induced, copper chelation)
Vit B-6 deficiency
X-linked sideroblastic anemia

Less Common Causes

Less common causes of sideroblastic anemia include:

Genetic Causes

X-linked sideroblastic anemia. defect in ALAS2.^[3]
Autosomal recessive sideroblastic anemia with mutations in the SLC25A38 gene.
Genetic syndromes

Causes by Organ System

Cardiovascular	No underlying causes
Chemical/Poisoning	Lead poisoning, zinc
Dental	No underlying causes
Dermatologic	No underlying causes
Drug Side Effect	Chloramphenicol,Isoniazid cycloserine, linezolid,
Ear Nose Throat	No underlying causes
Endocrine	No underlying causes
Environmental	No underlying causes
Gastroenterologic	No underlying causes
Genetic	X-linked sideroblastic anemia. Autosomal recessive sideroblastic . Genetic syndromes
Hematologic	Myelodysplastic syndrome
Iatrogenic	No underlying causes
Infectious Disease	No underlying causes
Musculoskeletal/Orthopedic	No underlying causes
Neurologic	No underlying causes
Nutritional/Metabolic	Vit B-6 deficiency
Obstetric/Gynecologic	No underlying causes
Oncologic	No underlying causes
Ophthalmologic	No underlying causes
Overdose/Toxicity	Alcohol
Psychiatric	No underlying causes
Pulmonary	No underlying causes
Renal/Electrolyte	No underlying causes
Rheumatology/Immunology/Allergy	No underlying causes
Sexual	No underlying causes
Trauma	No underlying causes
Urologic	No underlying causes
Miscellaneous	No underlying causes

Causes in Alphabetical Order

List the causes of the disease in alphabetical order:

Alcohol
Vit B-6 def
Chloromphenicol
Copper deficiency
Cause 5
Cause 6
Cause 7
Cause 8
isoniazid
Cause 10

Toxins: lead or zinc poisoning

Drug-induced: Cycloserine, ethanol, isoniazid, chloramphenicol, cycloserine, Penicillamine

Nutritional: pyridoxine or copper deficiency

Genetic: ALA synthase deficiency (X-linked)

References

↑ Cazzola M, Invernizzi R (June 2011). “Ring sideroblasts and sideroblastic anemias”. Haematologica. 96 (6): 789–92. doi:10.3324/haematol.2011.044628. PMC 3105636. PMID 21632840.
↑ Bottomley SS, Fleming MD (August 2014). “Sideroblastic anemia: diagnosis and management”. Hematol. Oncol. Clin. North Am. 28 (4): 653–70, v. doi:10.1016/j.hoc.2014.04.008. PMID 25064706.
↑ Long Z, Li H, Du Y, Han B (August 2018). “Congenital sideroblastic anemia: Advances in gene mutations and pathophysiology”. Gene. 668: 182–189. doi:10.1016/j.gene.2018.05.074. PMID 29787825.

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Differentiating Sideroblastic Anemia from other Diseases

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

Sideroblastic anemia must be differentiated from other causes of microcytic hypochromic anemia: iron deficiency anemia, thalassemia, anemia of chronic disease, lead poisoning, and blood loss.

Differential Diagnosis

Sideroblastic anemia must be differentiated from other causes of microcytic hypochromic anemia: iron deficiency anemia, thalassemia, anemia of chronic disease, lead poisoning, and blood loss.^[1]^[2]

Anemia must be differentiated based on different laboratory findings including mean cell volume (MCV), reticulocytosis, and hemolysis.

To review the differential diagnosis of anemia, see below table.

To review the differential diagnosis of microcytic anemia, click here.

To review the differential diagnosis of normocytic anemia, click here.

To review the differential diagnosis of macrocytic anemia, click here.

To review the differential diagnosis of hypochromic anemia, click here.

To review the differential diagnosis of normochromic anemia, click here.

To review the differential diagnosis of anisochromic anemia, click here.

To review the differential diagnosis of hemolytic anemia, click here.

To review the differential diagnosis of anemia with intrinsic hemolysis, click here.

To review the differential diagnosis of anemia with extrinsic hemolysis, click here.

To review the differential diagnosis of anemia with low reticulocytosis, click here.

To review the differential diagnosis of anemia with normal reticulocytosis, click here.

To review the differential diagnosis of anemia with high reticulocytosis, click here.

Disease	Genetics	Clinical manifestation					Lab findings
		History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Iron studies					Specific finding on blood smear
		History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	Transferrin or TIBC	Ferritin	Transferrin saturation	Specific finding on blood smear
Iron deficiency anemia^[3]	−	Menorrhagia GI loss GI surgery Pregnancy	Koilonychia Pica	Glossitis Cheilosis Dysphagia	−	−	Hypochromic	Microcytic	↑	Nl or ↓	Nl	Nl	↓	↑	↑	↓	↓↓↓	Central pallor
Iron deficiency anemia (early phase)^[4]	−	Pica Glossitis Cheilosis	Fatigue Headache	Koilonychia Conjunctival pallor Dry skin	−	−	Normochromic	Normocytic	↑	↓	Nl	Nl	↓	↑	↑	↓	↓	Pencil cells Elliptocytosis Hypochromasia
Lead poisoning^[5]	−	House painted with chipped paint	Burtonian lines Basophilic stippling Wrist drop Foot drop	Wrist drop Foot drop Burtonian lines	−	−	Hypochromic	Microcytic	Nl	Nl or ↓	Nl	Nl	Nl to ↓	Nl	Nl	Nl to ↓	−	RBCs retain aggregates of rRNA Basophilic stippling
Sideroblastic anemia^[6]	Defect in ALA synthase gene Autosomal dominant Autosomal recessive X-linked	Alcohol abuse Isoniazid use Chloramphenicol use Idiopathic	Seborrheic dermatitis Glossy Tongue Tingling	Patient present with symptoms of Vitamin B6, copper deficiency symptoms	−	−	Hypochromic	Microcytic	Nl	Nl or ↓	Nl	Nl	↑	Nl	Nl to ↓	↑	−	Ringed sideroblasts
Disease	Genetics	History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	IBC	Ferritin	Transferrin saturation	Specific finding on blood smear
Anemia of chronic disease^[7]	−	Rheumatoid arthritis SLE Neoplasm Chronic kidney disease	Headache Shortness of breath	−	−	−	Hypochromic	Microcytic	Nl	Nl or ↓	Nl	↑	↓	Nl	↓	↑	−	NA
Thalassemia^[8]	α-thalassemia α– globin gene deletions Cis deletions Trans deletions β-thalassemia Point mutation in splice sites and promoter sequences	Associated with parvovirus B19	α-thalassemia Hydrops fetalis β-thalassemia Skeletal deformities Chipmunk facies	Hepatomegaly Splenomegaly	−	−	Hypochromic	Microcytic	Nl	Thalassemia trait: Nl or ↓ Thalassemia Syndromes: ↑	Nl	Nl	Nl to ↑	Nl	Nl	↑	Nl to ↑	Target cells Anisopoikilocytosis
G6pd deficiency^[9]	Defect in G6PD enzyme X-Linked recessive	History of using Sulfa drugs Antimalarials Fava Beans Infections	Back pain Hemoglobinuria	Back pain	+	Intrinsic	Normochromic	Normocytic	↑	↑ but usually causes resolution within 4-7 days	↓	↓	Nl to ↑	Nl	↑	↑	↑	RBC with Heinz bodies Bite cells Blister cells
Pyruvate kinase deficiency^[10]	Mutation in the PKLR and PKM gene Autosomal recessive	Gallstones	Hydrops fetalis Neonatal hyperbilirubinemia Iron overload Perinatal complications	Skin ulcers Splenomegaly	+	Intrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	↑	Nl	Nl	↑	−	Prickle cells Polychromatophilic erythrocytes
Disease	Genetics	History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	IBC	Ferritin	Transferrin saturation	Specific finding on blood smear
Sickle cell anemia^[11]	Hbs point mutation causes a single amino acid replacement in β chain	High altitude Low Oxygen Acidosis African-American race Parvovirus B19 infection	Painful crisis Dactylitis Priapism Acute chest syndrome Avascular Necrosis Stroke Autosplenectomy Salmonella osteomyelitis	Dactylitis Priapism	+	Intrinsic	Normochromic	Normocytic	↑	↑	↓	Nl or moderately ↑	Nl	Nl	Nl or moderately ↑	↓	Nl	Increased erythropoiesis Howell-Jolly bodies Anisocytosis
HbC disease^[12]	Glutamic acid–to-lysine mutation in β-globin	Gallstone	Joint pains Increased risk of infections	Splenomegaly Cholelithiasis Avascular necrosis of the femoral head	+	Intrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	Nl	Nl	Nl	↓	−	Hemoglobin crystals inside RBCs Target cells
Paroxysmal nocturnal hemoglobinuria^[13]^[14]	PIGA gene mutations Impaired synthesis of GPI anchor for decay-accelerating factor	Associated with aplastic anemia Thrombosis	Fatigue Chest pain Dyspnea on exertion Headache	Chronic hemolysis Hepatomegaly Ascites Papilledema Skin nodules	+	Intrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	↓	Nl	↑	↓	−	NA
Hereditary spherocytosis^[15]	Mutations in Ankyrin, Band 3, Protein 4.2, and spectrin	Associated with parvovirus B19 Cholelithiasis Megaloblastic crisis	Aplastic crisis	Splenomegaly	+	Intrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	↓	Nl	↑	Nl	−	Small, round RBCs with less surface area and no central pallor
Disease	Genetics	History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	IBC	Ferritin	Transferrin saturation	Specific finding on blood smear
Microangiopathic hemolytic anemia^[16]^[17]	−	Associated with DIC TTP HUS SLE HELLP syndrome Hypertensive emergency	Purpura Confusion Aphasia Diplopia	Numbness of an arm or hand Jaundice Pale conjunctiva	+	Extrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	↓	Nl	−	↑	−	Helmet cells
Macroangiopathic hemolytic anemia^[18]	Autoimmune	Associated with Prosthetic heart valves Aortic stenosis	Pallor Fatigue	Signs of anemia Complications of hemolysis Decreased vascular volume	+	Extrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	↓	Nl	−	−	−	Spherocytes or schistocytes
Autoimmune hemolytic anemia^[19]	−	Associated with: SLE CLL Mycoplasma pneumonia	Painful blue fingers and toes on exposure to cold temperature Chest pain Chills Dizziness Tachycardia Headache Fatigue	Painful, blue fingers and toes with cold weather	+	Extrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	↓	Nl	−	−	−	RBC agglutination
Aplastic anemia^[20]	Constitutive expression of Tbet Mutations in the perforin gene Mutations in SAP gene	Exposure to Radiation Drugs like Benzene, chloramphenicol, alkylating agents Viral infections like EBV, HIV, Hepatitis Fanconi anemia Idiopathic like Immune mediated, primary stem cell defect	Symptoms based on underlying condition	Short stature Cafe-au-lait spots Thumb defects Radial defects	−	−	Normochromic	Normocytic	↑	↓	Nl	Nl	↓	↓	Nl	↑	↓	Pancytopenia Fatty infiltration
Disease	Genetics	History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	IBC	Ferritin	Transferrin saturation	Specific finding on blood smear
Folate deficiency^[21]	Impaired DNA synthesis	Alcohol consumption History of using drugs like methotrexate, trimethoprim, and phenytoin Low socioeconomic groups with poor nutrition Older people Pregnant and lactating women	No neurological symptoms vs B12 deficiency Odynophagia Angular stomatitis	Glossitis Signs of heart failure Anencephaly and spina bifida	−	−	Anisochromic	Macrocytic	↑	↓	Nl	Nl	↑	↑	↓	↑	↑	RBC macrocytosis Hypersegmented neutrophils Pancytopenia in severe cases
Vitamin B12 deficiency^[22]	Impaired DNA synthesis	Pernicious anemia Crohn’s disease Gastrectomy Veganism Diphyllobothrium latum infection	Psychosis Insomnia Depression Cognitive slowing Restless leg syndrome	Neurological deficit Myelopathy Memory loss with reduced attention span Nystagmus Positive romberg sign Positive Lhermitte’s sign	−	−	Anisochromic	Macrocytic	↑	↓	Nl	Nl	↑	↑	↓	↑	↑	Senile neutrophil Anisocytosis Ovalocytes
Orotic aciduria^[23]	Autosomal recessive Deficiency of enzyme UMPS	Episodic vomiting Rhabdomyolysis	Coma Gastrointestinal manifestation	Neurological manifestation	−	−	Anisochromic	Macrocytic	↑	↓	Nl	Nl	↑	↑	↓	↑	↑	NA
Fanconi anemia^[24]	Autosomal recessive X-linked recessive	History of anemia at age 16	Hypopigmentation Cafe-au-lait patches Radial ray anomaly	Significant for bilateral short thumbs	−	−	Anisochromic	Macrocytic	↑	↓	Nl	Nl	↑	↑	↓	↑	↑	Nl appearing WBC, RBC and Platelets But the number is greatly reduced
Disease	Genetics	History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	IBC	Ferritin	Transferrin saturation	Specific finding on blood smear
Diamond-Blackfan anemia^[25]	Mutations in: RPL5 RPL11 RPL35A RPS7 RPS10 RPS17 RPS19 RPS24 RPS26	Associated with myelodysplastic syndrome Increased risk of AML	Pale skin Sleepiness Heart murmurs	Triphalangeal thumbs Short stature Microcephaly Hypertelorism Ptosis Micrognathia	−	−	Anisochromic	Macrocytic	Nl	↓	Nl	Nl	↑	↑	↓	↑	↑	NA
Infections^[26]	−	Associated with Malaria Babesia	Fever	Fever Signs of shock Headache	+	Extrinsic	Normochromic	Normocytic	↑	↑	↓	Nl	Nl	Nl	−	−	−	Trophozoite Maltese crosses
Chronic kidney disease^[27]	−	Pericarditis Encephalopathy Rectal incontinence Decreased libido Restless leg syndrome	Polyuria Hematuria Edema	Hypertension	−	−	Normochromic	Normocytic	↑	Nl/↑	Nl	↑	↓	−	↓	↑	↓	Nl
Liver disease^[28]	−	Hepatitis Binge drinking Gall bladder disease	Jaundice Abdominal pain Itchy skin	Ascites Right upper quadrant pain Hepatomegaly Swelling in the legs Ankle swelling	−	−	Anisochromic	Macrocytic	↑	↑	Nl	Nl	↑	↑	↓	↑	↑	Round macrocytes Target macrocytes
Alcoholism^[29]	−	History of increased alcohol intake Folic acid deficiency	Memory impairment Nausea Sweating	Truncal obesity Asterixis Encephalopathy Spider angiomas Hematemesis Gynecomastia	−	−	Anisochromic	Macrocytic	↑	↑	Nl	Nl	↑	↑	↓	↑	↑	Oval macrocytes Hypersegmented neutrophils
Disease	Genetics	History	Symptoms	Signs	Hemolysis	Intrinsic/ Extrinsic	Hb concentration	MCV	RDW	Reticulocytosis	Haptoglobin levels	Hepcidin	Serum iron	Serum Tfr level	IBC	Ferritin	Transferrin saturation	Specific finding on blood smear

References

↑ Bottomley SS, Muller-Eberhard U (October 1988). “Pathophysiology of heme synthesis”. Semin. Hematol. 25 (4): 282–302. PMID 3064310.
↑ Cattivelli K, Campagna DR, Schmitz-Abe K, Heeney MM, Yaish HM, Caruso Brown AE, Kearney S, Walkovich K, Markianos K, Fleming MD, Neufeld EJ (May 2017). “Ringed sideroblasts in β-thalassemia”. Pediatr Blood Cancer. 64 (5). doi:10.1002/pbc.26324. PMC 5697724. PMID 27808451.
↑ Camaschella C (May 2015). “Iron-deficiency anemia”. N. Engl. J. Med. 372 (19): 1832–43. doi:10.1056/NEJMra1401038. PMID 25946282.
↑ De Andrade Cairo RC, Rodrigues Silva L, Carneiro Bustani N, Ferreira Marques CD (June 2014). “Iron deficiency anemia in adolescents; a literature review”. Nutr Hosp. 29 (6): 1240–9. doi:10.3305/nh.2014.29.6.7245. PMID 24972460.
↑ Bain BJ (December 2014). “Lead poisoning”. Am. J. Hematol. 89 (12): 1141. doi:10.1002/ajh.23852. PMID 25220013.
↑ Bottomley SS, Fleming MD (August 2014). “Sideroblastic anemia: diagnosis and management”. Hematol. Oncol. Clin. North Am. 28 (4): 653–70, v. doi:10.1016/j.hoc.2014.04.008. PMID 25064706.
↑ Roy CN (2010). “Anemia of inflammation”. Hematology Am Soc Hematol Educ Program. 2010: 276–80. doi:10.1182/asheducation-2010.1.276. PMID 21239806.
↑ Zainal NZ, Alauddin H, Ahmad S, Hussin NH (December 2014). “α-Thalassemia with Haemoglobin Adana mutation: prenatal diagnosis”. Malays J Pathol. 36 (3): 207–11. PMID 25500521.
↑ Luzzatto L, Seneca E (February 2014). “G6PD deficiency: a classic example of pharmacogenetics with on-going clinical implications”. Br. J. Haematol. 164 (4): 469–80. doi:10.1111/bjh.12665. PMC 4153881. PMID 24372186.
↑ Grace RF, Zanella A, Neufeld EJ, Morton DH, Eber S, Yaish H, Glader B (September 2015). “Erythrocyte pyruvate kinase deficiency: 2015 status report”. Am. J. Hematol. 90 (9): 825–30. doi:10.1002/ajh.24088. PMC 5053227. PMID 26087744.
↑ Singh PC, Ballas SK (March 2015). “Emerging drugs for sickle cell anemia”. Expert Opin Emerg Drugs. 20 (1): 47–61. doi:10.1517/14728214.2015.985587. PMID 25431087.
↑ Lemonne N, Billaud M, Waltz X, Romana M, Hierso R, Etienne-Julan M, Connes P (2016). “Rheology of red blood cells in patients with HbC disease”. Clin. Hemorheol. Microcirc. 61 (4): 571–7. doi:10.3233/CH-141906. PMID 25335812.
↑ Bunyaratvej A, Butthep P (January 1992). “Cytometric analysis of paroxysmal nocturnal hemoglobinuria erythrocytes”. J Med Assoc Thai. 75 Suppl 1: 237–42. PMID 1402472.
↑ Kahng J, Kim Y, Kim JO, Koh K, Lee JW, Han K (January 2015). “A novel marker for screening paroxysmal nocturnal hemoglobinuria using routine complete blood count and cell population data”. Ann Lab Med. 35 (1): 35–40. doi:10.3343/alm.2015.35.1.35. PMC 4272963. PMID 25553278.
↑ Da Costa L, Galimand J, Fenneteau O, Mohandas N (July 2013). “Hereditary spherocytosis, elliptocytosis, and other red cell membrane disorders”. Blood Rev. 27 (4): 167–78. doi:10.1016/j.blre.2013.04.003. PMID 23664421.
↑ Morishita E (July 2015). “[Diagnosis and treatment of microangiopathic hemolytic anemia]”. Rinsho Ketsueki (in Japanese). 56 (7): 795–806. doi:10.11406/rinketsu.56.795. PMID 26251142.
↑ George JN, Charania RS (March 2013). “Evaluation of patients with microangiopathic hemolytic anemia and thrombocytopenia”. Semin. Thromb. Hemost. 39 (2): 153–60. doi:10.1055/s-0032-1333538. PMID 23390027.
↑ Westphal RG, Azen EA (May 1971). “Macroangiopathic hemolytic anemia due to congenital cardiovascular anomalies”. JAMA. 216 (9): 1477–8. PMID 5108522.
↑ Hill QA (October 2015). “Autoimmune hemolytic anemia”. Hematology. 20 (9): 553–4. doi:10.1179/1024533215Z.000000000401. PMID 26447931.
↑ Dolberg OJ, Levy Y (2014). “Idiopathic aplastic anemia: diagnosis and classification”. Autoimmun Rev. 13 (4–5): 569–73. doi:10.1016/j.autrev.2014.01.014. PMID 24424170.
↑ Koike H, Takahashi M, Ohyama K, Hashimoto R, Kawagashira Y, Iijima M, Katsuno M, Doi H, Tanaka F, Sobue G (March 2015). “Clinicopathologic features of folate-deficiency neuropathy”. Neurology. 84 (10): 1026–33. doi:10.1212/WNL.0000000000001343. PMID 25663227.
↑ Hunt A, Harrington D, Robinson S (September 2014). “Vitamin B12 deficiency”. BMJ. 349: g5226. PMID 25189324.
↑ Grohmann K, Lauffer H, Lauenstein P, Hoffmann GF, Seidlitz G (April 2015). “Hereditary orotic aciduria with epilepsy and without megaloblastic anemia”. Neuropediatrics. 46 (2): 123–5. doi:10.1055/s-0035-1547341. PMID 25757096.
↑ Alter BP (2014). “Fanconi anemia and the development of leukemia”. Best Pract Res Clin Haematol. 27 (3–4): 214–21. doi:10.1016/j.beha.2014.10.002. PMC 4254647. PMID 25455269.
↑ Vlachos A, Blanc L, Lipton JM (June 2014). “Diamond Blackfan anemia: a model for the translational approach to understanding human disease”. Expert Rev Hematol. 7 (3): 359–72. doi:10.1586/17474086.2014.897923. PMID 24665981.
↑ Bustinduy AL, Parraga IM, Thomas CL, Mungai PL, Mutuku F, Muchiri EM, Kitron U, King CH (March 2013). “Impact of polyparasitic infections on anemia and undernutrition among Kenyan children living in a Schistosoma haematobium-endemic area”. Am. J. Trop. Med. Hyg. 88 (3): 433–40. doi:10.4269/ajtmh.12-0552. PMC 3592521. PMID 23324217.
↑ Drawz P, Rahman M (June 2015). “Chronic kidney disease”. Ann. Intern. Med. 162 (11): ITC1–16. doi:10.7326/AITC201506020. PMID 26030647.
↑ Marks PW (July 2013). “Hematologic manifestations of liver disease”. Semin. Hematol. 50 (3): 216–21. doi:10.1053/j.seminhematol.2013.06.003. PMID 23953338.
↑ Yokoyama A, Yokoyama T, Brooks PJ, Mizukami T, Matsui T, Kimura M, Matsushita S, Higuchi S, Maruyama K (May 2014). “Macrocytosis, macrocytic anemia, and genetic polymorphisms of alcohol dehydrogenase-1B and aldehyde dehydrogenase-2 in Japanese alcoholic men”. Alcohol. Clin. Exp. Res. 38 (5): 1237–46. doi:10.1111/acer.12372. PMID 24588059.

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Epidemiology and Demographics

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

Patients of all age groups may develop sideroblastic anemia. The incidence of acquired sideroblastic anemia increases with age; the median age at diagnosis is 74 years. Chronic sideroblastic anemia is usually first diagnosed among middle and older age group. There is no racial predilection to sideroblastic anemia. Males are more commonly affected than females in X-linked recessive types of sideroblastic anemia.

Epidemiology and Demographics

Age

Patients of all age groups may develop sideroblastic anemia.
Congenital X-linked sideroblastic anemia due to ALAS mutation can remain undiagnosed and then present late in the fourth to eighth decades of life.
The incidence of acquired sideroblastic anemia increases with age; the median age at diagnosis is 74 years.
Chronic sideroblastic anemia is usually first diagnosed among middle and older age group.^[1]

Race

There is no racial predilection to sideroblastic anemia.

Gender

Males are more commonly affected than females in X-linked recessive types of sideroblastic anemia.
A female would have to inherit 1 abnormal chromosome from each parent to acquire the sideroblastic anemia.
Primary acquired sideroblastic anemia was found in 60.4% male and 39.6% female.^[1]

Region

Sideroblastic anemia is more prevalent in European countries,in peadiatric population.

References

↑ ^1.0 ^1.1 Hadnagy C (1991). “Primary acquired sideroblastic anemia and myelodysplastic syndrome from a geriatric point of view”. Z Gerontol. 24 (2): 105–9. PMID 1877285.

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Risk Factors

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

Common risk factors in the development of sideroblastic anemia are male gender (X-linked SA), family history of hreditary SA, chronic alcohol abuse. Less common risk factors in the development of sideroblastic anemia are drugs, isoniazid, pyrazinamide, chloramphenicol, cycloserine, and azathioprine, copper deficiency and pyridoxine deficiency. Hypothermia causes sideroblastic anemia by affecting mitochondrial functions.

Risk Factors

Common Risk Factors

Common risk factors in the development of sideroblastic anemia are ^[1]
- Male gender (X-linked SA)
- Family history of hereditary SA
- Chronic alcohol abuse
- Lead toxicity

Less Common Risk Factors

Less common risk factors in the development of sideroblastic anemia are^[1]
- Drugs
- Copper deficiency
- Pyridoxine deficiency
- Hypothermia affecting mitochondrial functions
- High dose zinc supplements

References

↑ ^1.0 ^1.1 Cazzola M, Invernizzi R (June 2011). “Ring sideroblasts and sideroblastic anemias”. Haematologica. 96 (6): 789–92. doi:10.3324/haematol.2011.044628. PMC 3105636. PMID 21632840.

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Screening

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

According to The National Center for Biotechnology Information NCBI, screening for sideroblastic anemia by using one of the tests, mitochondrial focused nuclear gene panel, congenital sideroblastic anemia panel and PUS1 gene sequencing is available for, molecular confirmation of genetic sideroblastic anemia, testing of patients with positive family history of sideroblastic anemia and prenatal diagnosis for gene mutation in at-risk pregnancies.

Screening

Tests name

According to the National Center for Biotechnology Information center, the following tests are available for screening sideroblastic anemia:^[1]^[2]

Mitochondrial focused nuclear gene panel
Congenital sideroblastic anemia panel
PUS1 gene sequencing

Clinical utility

Molecular confirmation of genetic sideroblastic anemia
Testing of patients with positive family history of sideroblastic anemia
Prenatal diagnosis for gene mutation in at-risk pregnancies.

References

↑ Koenig MK (May 2008). “Presentation and diagnosis of mitochondrial disorders in children”. Pediatr. Neurol. 38 (5): 305–13. doi:10.1016/j.pediatrneurol.2007.12.001. PMC 3099432. PMID 18410845.
↑ Taylor RW, Pyle A, Griffin H, Blakely EL, Duff J, He L, Smertenko T, Alston CL, Neeve VC, Best A, Yarham JW, Kirschner J, Schara U, Talim B, Topaloglu H, Baric I, Holinski-Feder E, Abicht A, Czermin B, Kleinle S, Morris AA, Vassallo G, Gorman GS, Ramesh V, Turnbull DM, Santibanez-Koref M, McFarland R, Horvath R, Chinnery PF (July 2014). “Use of whole-exome sequencing to determine the genetic basis of multiple mitochondrial respiratory chain complex deficiencies”. JAMA. 312 (1): 68–77. doi:10.1001/jama.2014.7184. PMID 25058219.

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Natural History, Complications and Prognosis

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Nazia Fuad M.D.

Overview

Majority of patients of sideroblastic anemia at the time of diagnosis shows erythroid abnormalities and ineffective erythropoiesis. Granulocytic and megakaryocytic cell lines involvement is also common. In the initial stages bone marrow reveal erythroid expansion with ineffective erythropoiesis. Progression to bone marrow failure occurs in the course of the disease. The next phase in natural history of sideroblastic anemia is iron overload and evolution to nonlymphocytic leukemia. complications of sideroblastic anemia include secondry hemochromatosis, thrombocytopenia, Growth retardation, Blindness, Ineffective erythropoiesis, myocardial siderosis, liver cirrhosis and malabsorption. Prognosis depends on the type and cause of sideroblastic anemia. Sideroblastic anemia secondry to drugs or alcohol as underlying cause is associated with the most favorable prognosis. Sideroblastic anemias associated with MDS undergo leukemic transformation in 5-10% cases. The transfusion dependent are at risk of death from the complications of secondary hemochromatosis.

Natural History

Majority of patients of sideroblastic anemia at the time of diagnosis shows erythroid abnormalities and ineffective erythropoiesis.
Granulocytic and megakaryocytic cell lines involvement is also common.
In the initial stages bone marrow reveal erythroid expansion with ineffective erythropoiesis.
Progression to bone marrow failure occurs in the course of the disease.
The next phase in natural history of sideroblastic anemia is iron overload and evolution to nonlymphocytic leukemia.
The most common causes of death are related to complications of iron overload and evolution into ANLL.^[1]

Complications

Common complications of sideroblastic anemia include

Secondry hemochromatosis
Thrombocytopenia
Growth retardation
Blindness
Deafness
Ineffective erythropoiesis
Myocardial siderosis
Liver cirrhosis
Malabsorption

Prognosis

Depending on the type of sideroblastic anemia the prognosis may vary. However, the prognosis is generally regarded as good^[1].
Sideroblastic anemia secondry to drugs or alcohol as underlying cause is associated with the most favorable prognosis.
(5-10%) of Severe refractory sideroblastic anemias associated with MDS undergo leukemic transformation.
AML markedly reduce life expectancy
Patients who do not need blood transfusions are likely to be long-term survivors.
The transfusion dependent are at risk of death from the complications of secondary hemochromatosis.

References

↑ ^1.0 ^1.1 Cazzola M, Barosi G, Gobbi PG, Invernizzi R, Riccardi A, Ascari E (February 1988). “Natural history of idiopathic refractory sideroblastic anemia”. Blood. 71 (2): 305–12. PMID 3337899.

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Diagnosis

Treatment

Case Studies

Case #1

Related Chapters

Template:Hematology

Template:WikiDoc Sources

[pmid16735131-1] Aivado M, Gattermann N, Rong A, Giagounidis AA, Prall WC, Czibere A, Hildebrandt B, Haas R, Bottomley SS (2006). “X-linked sideroblastic anemia associated with a novel ALAS2 mutation and unfortunate skewed X-chromosome inactivation patterns”. Blood Cells Mol. Dis. 37 (1): 40–5. doi:10.1016/j.bcmd.2006.04.003. PMID 16735131.

[pmid24003969-1] Fujiwara T, Harigae H (December 2013). “Pathophysiology and genetic mutations in congenital sideroblastic anemia”. Pediatr Int. 55 (6): 675–9. doi:10.1111/ped.12217. PMID 24003969.

[pmid21632840-2] Cazzola M, Invernizzi R (June 2011). “Ring sideroblasts and sideroblastic anemias”. Haematologica. 96 (6): 789–92. doi:10.3324/haematol.2011.044628. PMC 3105636. PMID 21632840.

[pmid20506125-1] Layer G, Reichelt J, Jahn D, Heinz DW (June 2010). “Structure and function of enzymes in heme biosynthesis”. Protein Sci. 19 (6): 1137–61. doi:10.1002/pro.405. PMC 2895239. PMID 20506125.

[pmid22160084-2] 2.0 ^2.1 Fleming MD (2011). “Congenital sideroblastic anemias: iron and heme lost in mitochondrial translation”. Hematology Am Soc Hematol Educ Program. 2011: 525–31. doi:10.1182/asheducation-2011.1.525. PMID 22160084.

[pmid21632840-3] Cazzola M, Invernizzi R (June 2011). “Ring sideroblasts and sideroblastic anemias”. Haematologica. 96 (6): 789–92. doi:10.3324/haematol.2011.044628. PMC 3105636. PMID 21632840.

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Sideroblastic anemia

Overview

Ring sideroblasts

Historical Perspective

Classification

Pathophysiology

Causes

Differentiating Sideroblastic anemia overview from Other Diseases

Epidemiology and Demographics

Risk Factors

Screening

Natural History, Complications, and Prognosis

Natural History

Complications

Prognosis

Diagnosis

Diagnostic Criteria

History and Symptoms

Physical Examination

Laboratory Findings

Imaging Findings

Other Diagnostic Studies

Treatment

Medical Therapy

Surgery

Prevention

References

Overview

Historical Perspective

References

Overview

Classification

References

Overview

Pathophysiology

Physiology

Pathogenesis

Genetics

References

Overview

Causes

Life-threatening Causes

Common Causes

Less Common Causes

Genetic Causes

Causes by Organ System

Causes in Alphabetical Order

References

Overview

Differential Diagnosis

References

Overview

Epidemiology and Demographics

Age

Race

Gender

Region

References

Overview

Risk Factors

Common Risk Factors

Less Common Risk Factors

References

Overview

Screening

Tests name

Clinical utility

References

Overview

Natural History

Complications

Prognosis

References

Diagnosis

Treatment

Case Studies

Related Chapters

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