Effect of HFE Gene Mutations on Iron Metabolism of Beta-Thalassemia Carriers
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Monaco, Maria E.
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Alvarez Asensio, Natalia S.
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Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, ArgentinaUniv Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
Alvarez Asensio, Natalia S.
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Haro, Cecilia
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Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, ArgentinaUniv Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
Haro, Cecilia
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Teran, Magdalena M.
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Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, ArgentinaUniv Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
Teran, Magdalena M.
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Ledesma Achem, Miryam E.
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Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, ArgentinaUniv Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
Ledesma Achem, Miryam E.
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Isse, Blanca A.
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Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, ArgentinaUniv Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
Isse, Blanca A.
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Lazarte, Sandra S.
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Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, ArgentinaUniv Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
Lazarte, Sandra S.
[2
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[1] Univ Nacl Tucuman, Fac Bioquim, Inst Biol, Quim & Farm, Chacabuco 461,4000, San Miguel De Tucuman, Argentina
[2] Univ Nacl Tucuman, Fac Bioquim, Inst Bioquim Aplicada, Quim & Farm, Balcarce 747,4000, San Miguel De Tucuman, Argentina
The human hemochromatosis protein HFE is encoded by the HFE gene and participates in iron regulation. The aim of this study was to detect the most frequent HFE gene mutations in a control population and in beta-thalassemia trait (BTT) carriers, and to study their relationship with iron metabolism. Total blood count, hemoglobin electrophoresis at alkaline pH, HbA(2) quantification, iron (Fe), total Fe binding capacity and ferritin were assayed. HFE gene mutations were analyzed by real-time PCR. A total of 119 individuals (69 normal and 50 BTT) were examined. In the control group, 9% (6/69) presented a codon 282 heterozygous mutation (C282Y), and 19% a codon 63 mutation (H63D) (13/69, 11 heterozygotes and 2 homozygotes). In the BTT group, 3 carriers (6%) were heterozygous for C282Y, 14 (28%) for H63D, 1 (2%) for a codon 65 mutation and 1 (2%) was H63D and C282Y double heterozygous. Control group Fe metabolism did not show significant differences (p > 0.05) according to whether or not they carried an HFE gene mutation; while the BTT group with and without HFE mutation showed higher Fe and ferritin than the control group (p < 0.05). However, no increases in iron parameters were detected in BTT carriers that simultaneously exhibited an H63D mutation compared to BTT subjects without a mutation. Therefore, the iron metabolism alterations observed in BTT carriers could not be attributed to the presence of HFE gene mutations. It is likely that BTT individuals have other genetic modifiers that affect their iron balance.
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Department of Biology,Faculty of Science,Chiang Mai UniversityDepartment of Clinical Microscopy,Faculty of Allied Health Sciences,Chulalongkorn University
Pathrapol Lithanatudom
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Wannapa Sornjai
Duncan R.Smith
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Molecular Pathology Laboratory.Institute of Molecular Biosciences,Mahidol UniversityDepartment of Clinical Microscopy,Faculty of Allied Health Sciences,Chulalongkorn University