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HLA-DQβ序列多态性与胰岛素依赖型糖尿病的遗传易感性

HLA-DQ beta sequence polymorphism and genetic susceptibility to IDDM.

作者信息

Erlich H A, Bugawan T L, Scharf S, Nepom G T, Tait B, Griffith R L

机构信息

Cetus Corporation, Department of Human Genetics Emeryville, California 94608.

出版信息

Diabetes. 1990 Jan;39(1):96-103. doi: 10.2337/diacare.39.1.96.

DOI:10.2337/diacare.39.1.96
PMID:2210066
Abstract

The analysis of HLA-DQ beta nucleotide sequence polymorphism in insulin-dependent diabetes mellitus (IDDM) patients and control subjects suggests a role for the DQ beta-chain in genetic susceptibility. Sequence determination and oligonucleotide hybridization was carried out on enzymatically amplified DNA from various HLA-DR-typed individuals, including the rare class of DR2+ patients. In the analysis of DQ beta variation in DR4, DRw6, and DR2 haplotypes, a correlation was observed between the presence of the negatively charged residue Asp at position 57 and low susceptibility and the presence of an Ala (DR4), Val (DRw6), or Ser (DR2) and higher susceptibility. However, important exceptions to this pattern have been identified in the analysis of heterozygous DR1/4 IDDM patients. In these individuals, susceptibility appears to correlate with specific DR beta l alleles (Dw4) on the DR4 haplotype, rather than with the DQ beta allele (DQB3.2) that contains Ala at position 57. The DQ beta alleles found in some Chinese IDDM patients also proved discordant with the position-57 correlations. Thus, although there is a general correlation between the residue at position 57 of the DQ beta-chain and IDDM susceptibility, these data do not support the notion that Asp 57 confers complete resistance or protection to IDDM. In general, these results suggest that IDDM susceptibility is conferred by specific combinations of DQ beta and DR beta sequences.

摘要

对胰岛素依赖型糖尿病(IDDM)患者和对照受试者的HLA-DQβ核苷酸序列多态性分析表明,DQβ链在遗传易感性中起作用。对来自各种HLA-DR分型个体(包括罕见的DR2 +患者类别)的酶促扩增DNA进行了序列测定和寡核苷酸杂交。在对DR4、DRw6和DR2单倍型的DQβ变异分析中,观察到57位带负电荷的残基天冬氨酸(Asp)的存在与低易感性之间存在相关性,而丙氨酸(Ala,DR4)、缬氨酸(Val,DRw6)或丝氨酸(Ser,DR2)的存在与较高易感性之间存在相关性。然而,在对杂合DR1/4 IDDM患者的分析中发现了这种模式的重要例外情况。在这些个体中,易感性似乎与DR4单倍型上的特定DRβ1等位基因(Dw4)相关,而不是与57位含有丙氨酸的DQβ等位基因(DQB3.2)相关。在一些中国IDDM患者中发现的DQβ等位基因也与57位的相关性不一致。因此,尽管DQβ链57位的残基与IDDM易感性之间存在普遍相关性,但这些数据并不支持天冬氨酸57赋予对IDDM完全抗性或保护的观点。总体而言,这些结果表明,IDDM易感性是由DQβ和DRβ序列的特定组合赋予的。

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HLA-DQ beta sequence polymorphism and genetic susceptibility to IDDM.HLA-DQβ序列多态性与胰岛素依赖型糖尿病的遗传易感性
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引用本文的文献

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HLA DR-DQ haplotypes and genotypes and type 1 diabetes risk: analysis of the type 1 diabetes genetics consortium families.人类白细胞抗原DR-DQ单倍型和基因型与1型糖尿病风险:1型糖尿病遗传学联盟家族分析
Diabetes. 2008 Apr;57(4):1084-92. doi: 10.2337/db07-1331. Epub 2008 Feb 5.
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Genetic predisposition to IDDM.
胰岛素依赖型糖尿病的遗传易感性。
Clin Rev Allergy Immunol. 2000 Dec;19(3):227-46. doi: 10.1385/CRIAI:19:3:227.
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The role of HLA class II genes in insulin-dependent diabetes mellitus: molecular analysis of 180 Caucasian, multiplex families.人类白细胞抗原II类基因在胰岛素依赖型糖尿病中的作用:对180个高加索多重家庭的分子分析
Am J Hum Genet. 1996 Nov;59(5):1134-48.
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Newborn screening for HLA markers associated with IDDM: diabetes autoimmunity study in the young (DAISY).新生儿筛查与胰岛素依赖型糖尿病相关的人类白细胞抗原标志物:青少年糖尿病自身免疫研究(DAISY)。
Diabetologia. 1996 Jul;39(7):807-12. doi: 10.1007/s001250050514.
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Critical contribution of beta chain residue 57 in peptide binding ability of both HLA-DR and -DQ molecules.β链57位残基对HLA-DR和-DQ分子肽结合能力的关键作用。
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Polymorphic structural features of modelled HLA-DQ molecules segregate according to susceptibility or resistance to IDDM.模拟的HLA-DQ分子的多态性结构特征根据对胰岛素依赖型糖尿病的易感性或抗性而分离。
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Diabetologia. 1993 Nov;36(11):1210-1. doi: 10.1007/BF00401069.
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