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在泰国人群中,一种血红蛋白E(HbE)变体与β-珠蛋白基因上游BP1结合位点处的(AT)9(T)5重复序列存在强连锁不平衡。

Strong linkage disequilibrium of a HbE variant with the (AT)9(T)5 repeat in the BP1 binding site upstream of the beta-globin gene in the Thai population.

作者信息

Ohashi Jun, Naka Izumi, Patarapotikul Jintana, Hananantachai Hathairad, Brittenham Gary, Looareesuwan Sornchai, Clark Andrew G, Tokunaga Katsushi

机构信息

Department of Human Genetics, Graduate School of Medicine, The University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, Tokyo, 113-0033, Japan.

Department of Molecular Biology and Genetics, Cornell University, Ithaca, NY, USA.

出版信息

J Hum Genet. 2005;50(1):7-11. doi: 10.1007/s10038-004-0210-z. Epub 2004 Nov 18.

Abstract

A binding site for the repressor protein BP1, which contains a tandem (AT)x(T)y repeat, is located approximately 530 bp 5' to the human beta-globin gene (HBB). There is accumulating evidence that BP1 binds to the (AT)9(T)5 allele more strongly than to other alleles, thereby reducing the expression of HBB. In this study, we investigated polymorphisms in the (AT)x(T)y repeat in 57 individuals living in Thailand, including three homozygotes for the hemoglobin E variant (HbE; beta26Glu-->Lys), 22 heterozygotes, and 32 normal homozygotes. We found that (AT)9(T)5 and (AT)7(T)7 alleles were predominant in the studied population and that the HbE variant is in strong linkage disequilibrium with the (AT)9(T)5 allele, which can explain why the betaE chain is inefficiently synthesized compared to the normal betaA chain. Moreover, the mildness of the HbE disease compared to other hemoglobinopathies in Thai may be due, in part, to the presence of the (AT)9(T)5 repeat on the HbE chromosome. In addition, a novel (AC)n polymorphism adjacent to the (AT)x(T)y repeat (i.e., (AC)3(AT)7(T)5) was found through the variation screening in this study.

摘要

阻遏蛋白BP1的结合位点位于人类β-珠蛋白基因(HBB)上游约530 bp处,该位点包含一个串联的(AT)x(T)y重复序列。越来越多的证据表明,BP1与(AT)9(T)5等位基因的结合比与其他等位基因的结合更强,从而降低了HBB的表达。在本研究中,我们调查了57名生活在泰国的个体中(AT)x(T)y重复序列的多态性,其中包括3名血红蛋白E变体(HbE;β26Glu→Lys)的纯合子、22名杂合子和32名正常纯合子。我们发现(AT)9(T)5和(AT)7(T)7等位基因在研究人群中占主导地位,并且HbE变体与(AT)9(T)5等位基因存在强连锁不平衡,这可以解释为什么与正常βA链相比,βE链的合成效率低下。此外,与泰国的其他血红蛋白病相比,HbE疾病的症状较轻可能部分归因于HbE染色体上存在(AT)9(T)5重复序列。此外,通过本研究中的变异筛选,我们发现了一个与(AT)x(T)y重复序列相邻的新型(AC)n多态性(即(AC)3(AT)7(T)5)。

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本文引用的文献

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