World Library  
Flag as Inappropriate
Email this Article


Article Id: WHEBN0004210617
Reproduction Date:

Title: Alpha-thalassemia  
Author: World Heritage Encyclopedia
Language: English
Subject: Heinz body, Nutritional anemia, Delta-thalassemia, Hexokinase deficiency, Congenital amegakaryocytic thrombocytopenia
Publisher: World Heritage Encyclopedia


Classification and external resources
ICD-10 D56.0
ICD-9 282.43
OMIM 141800 141850 142310 604131 141800 141850 142310 604131
DiseasesDB 448 33334, 33678
eMedicine article/955496
MeSH D017085
  • Alpha-Thalassemia

Alpha-thalassemia (α-thalassemia, α-thalassaemia) is a form of thalassemia involving the genes HBA1[1] and HBA2.[2] Alpha-thalassemia is due to impaired production of 1,2,3, or 4 alpha globin chains, leading to a relative excess of beta globin chains. The degree of impairment is based on which clinical phenotype is present (how many chains are affected).


The worldwide distribution of inherited alpha-thalassemia corresponds to areas of malaria exposure,[3] suggesting a protective role for alpha-thalassemia against the more severe manifestations of malaria. Thus, alpha-thalassemia is common in sub-Saharan Africa, the Mediterranean Basin, the Middle East, South Asia, and Southeast Asia, and different genetic subtypes have variable frequencies in each of these areas.[4] The epidemiology of alpha-thalassemia in the US reflects this global distribution pattern. The most common form of alpha(+) thalassemia seen in the US is due to the -alpha(3.7) deletion, a single alpha-globin gene deletion, and is present in approximately 30% of African Americans.[5] However, even in the homozygous state this disorder will result only in a mild microcytic anemia. The more serious clinical disorders of Hb H and Hb Bart hydrops fetalis syndrome, although found throughout the US today, are more common in the Western US and have dramatically increased in prevalence in the past 2 decades due to increased Asian immigration.[6]


It is most commonly inherited in a Mendelian recessive fashion. It is also connected to the deletion of the 16p chromosome.

It can also be acquired, under rare circumstances.[7] Due to the low occurrence of alpha-thalassemia, the disease can be mistaken for iron deficiency anemia.[8]


α thalassemias result in decreased alpha-globin production, therefore fewer alpha-globin chains are produced, resulting in an excess of β chains in adults and excess γ chains in newborns. The excess β chains form unstable tetramers (called Hemoglobin H or HbH of 4 beta chains) which have abnormal oxygen dissociation curves. The excess γ chains form tetramers which are poor carriers of O2 since their affinity for O2 is too high so it is not dissociated in the periphery. Homozygote α0 thalassaemias, where there is lots of γ4 but no α-globins at all (referred to as Hb Barts), often result in still birth.


There are two genetic loci for α globin, and thus four genes in diploid cells. Two genes are maternal in origin and two genes are paternal in origin. The severity of the α thalassemias is correlated with the number of affected α globin genes: the greater, the more severe will be the manifestations of the disease.

When noting the genotype, a "-" indicates an absence of function, and a "α" indications a functional alpha chain. (In contrast to the "βo" and "β+" notation used in beta-thalassemia, in alpha-thalassemia a distinction between absent and reduced function is not usually noted.)

Alleles affected Description Genotype
One This is known as alpha thalassemia minima and with this type there is minimal effect on hemoglobin synthesis. Three α-globin genes are enough to permit normal hemoglobin production, and there are no clinical symptoms. They have been called silent carriers. They may have a slightly reduced mean corpuscular volume and mean corpuscular hemoglobin. -/α α/α
Two The condition is called alpha thalassemia minor. Two α genes permit nearly normal production of red blood cells, but there is a mild microcytic hypochromic anemia. The disease in this form can be mistaken for iron deficiency anemia and treated inappropriately with iron.

Alpha thalassemia minor can exist in two forms:

  • alpha-thal-1 (αα/--), associated with Asians, involves cis deletion of both alpha genes on the same chromosome;
  • alpha-thal-2 (α-/α-), associated with Africans, involves trans deletion of alpha genes on different (homologous) chromosomes.[9]
-/- α/α or
-/α -/α
Three The condition is called Hemoglobin H disease. Two unstable hemoglobins are present in the blood: Hemoglobin Barts (tetrameric γ chains) and Hemoglobin H (tetrameric β chains). Both of these unstable hemoglobins have a higher affinity for oxygen than normal hemoglobin, resulting in poor oxygen delivery to tissues. There is a microcytic hypochromic anemia with target cells and Heinz bodies (precipitated HbH) on the peripheral blood smear, as well as hepatosplenomegaly. The disease may first be noticed in childhood or in early adult life, when the anemia and hepatosplenomegaly are noted. -/- -/α
Four The fetus cannot live once outside the uterus and may not survive gestation: most such infants are stillborn with hydrops fetalis, and those who are born alive die shortly after birth. They are edematous and have little circulating hemoglobin, and the hemoglobin that is present is all tetrameric γ chains (hemoglobin Barts). -/- -/-


  1. ^ Online 'Mendelian Inheritance in Man' (OMIM) Hemoglobin—Alpha locus 1; HBA1 -141800
  2. ^ Online 'Mendelian Inheritance in Man' (OMIM) Hemoglobin—Alpha locus 2; HBA2 -141850
  3. ^ Flint J, Hill AV, Bowden DK, et al. (1986). "High frequencies of alpha-thalassaemia are the result of natural selection by malaria". Nature 321 (6072): 744–50.  
  4. ^ Bernini LF. Geographic distribution of alpha thalassemia. In: Steinberg M, Forget B, Higgs D, et al., eds. Disorders of hemoglobin. New York, NY: Cambridge University Press; 2001:878-894.
  5. ^ Beutler E, West C (July 2005). "Hematologic differences between African-Americans and whites: the roles of iron deficiency and alpha-thalassemia on hemoglobin levels and mean corpuscular volume". Blood 106 (2): 740–5.  
  6. ^ Vichinsky EP, MacKlin EA, Waye JS, Lorey F, Olivieri NF (December 2005). "Changes in the epidemiology of thalassemia in North America: a new minority disease". Pediatrics 116 (6): e818–25.  
  7. ^ Steensma DP, Gibbons RJ, Higgs DR (January 2005). "Acquired alpha-thalassemia in association with myelodysplastic syndrome and other hematologic malignancies". Blood 105 (2): 443–52.  
  8. ^
  9. ^ "Alpha Thalassemia Trait". St. Jude Children's Research Hospital. Retrieved 15 January 2014. 
This article was sourced from Creative Commons Attribution-ShareAlike License; additional terms may apply. World Heritage Encyclopedia content is assembled from numerous content providers, Open Access Publishing, and in compliance with The Fair Access to Science and Technology Research Act (FASTR), Wikimedia Foundation, Inc., Public Library of Science, The Encyclopedia of Life, Open Book Publishers (OBP), PubMed, U.S. National Library of Medicine, National Center for Biotechnology Information, U.S. National Library of Medicine, National Institutes of Health (NIH), U.S. Department of Health & Human Services, and, which sources content from all federal, state, local, tribal, and territorial government publication portals (.gov, .mil, .edu). Funding for and content contributors is made possible from the U.S. Congress, E-Government Act of 2002.
Crowd sourced content that is contributed to World Heritage Encyclopedia is peer reviewed and edited by our editorial staff to ensure quality scholarly research articles.
By using this site, you agree to the Terms of Use and Privacy Policy. World Heritage Encyclopedia™ is a registered trademark of the World Public Library Association, a non-profit organization.

Copyright © World Library Foundation. All rights reserved. eBooks from Project Gutenberg are sponsored by the World Library Foundation,
a 501c(4) Member's Support Non-Profit Organization, and is NOT affiliated with any governmental agency or department.