Title of article
Disparate phenotypic expression of ALAS2 R452H (nt 1407 G → A) in two brothers, one with severe sideroblastic anemia and iron overload, hepatic cirrhosis, and hepatocellular carcinoma
Author/Authors
James C. Barton، نويسنده , , Pauline L. Lee، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2006
Pages
5
From page
342
To page
346
Abstract
We report the case of a man with severe X-linked sideroblastic anemia, severe iron overload, and hepatic cirrhosis who died of hepatocellular carcinoma. Evaluation of family members using DNA sequencing revealed that he was hemizygous for the novel ALAS2 mutation R452H (exon 9; nt 1407 G → A). The probandʹs brother, an ALAS2 R452H hemizygote, had mild anemia and mild iron overload. Four female relatives were ALAS2 R452H heterozygotes, but they had mild or no anemia and no iron overload. Sequencing of TFR2, HFE, FPN1 (SLC40A1), HAMP, HJV, and the erythrocyte pyruvate kinase genes of family members was also performed. We thus detected the novel TFR2 missense mutation I449V (exon 10; nt 1345 A → G) in the probandʹs wife and daughter, neither of whom had anemia or iron overload. Possible explanations for the disparate red blood cell and iron phenotypes of the proband and his family members are discussed.
Keywords
Missense mutation , skewed X-inactivation , Penetrance , TFR2 I449V , X chromosome
Journal title
Blood Cells, Molecules and Diseases
Serial Year
2006
Journal title
Blood Cells, Molecules and Diseases
Record number
498953
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