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在爱尔兰西部各郡进行的一项针对易患乳糜泻基因的常染色体筛查。

An autosomal screen for genes that predispose to celiac disease in the western counties of Ireland.

作者信息

Zhong F, McCombs C C, Olson J M, Elston R C, Stevens F M, McCarthy C F, Michalski J P

机构信息

Department of Internal Medicine, University of South Alabama, Mobile 36688, USA.

出版信息

Nat Genet. 1996 Nov;14(3):329-33. doi: 10.1038/ng1196-329.

Abstract

Celiac disease is a strongly heritable gastrointestinal illness that is an especially important model of the genetically complex multifactorial immune mediated diseases. The HLA component of celiac disease (a specific HLA-DQ heterodimer)is largely established and is relatively uncomplicated, and the environmental component (gluten and related grain storage proteins in the diet) is remarkably well understood. Previous family studies of celiac disease suggested that there is at least one important non-HLA locus. This locus may be a stronger genetic factor than HLA, and it apparently has a recessive mode of inheritance. We used a three step genome screening protocol to identify loci that contribute to celiac disease in the western counties of ireland, a region with the highest prevalence of celiac disease in the world. The most significant of several possible non-HLA loci that we found was on chromosome 6p about 30 cM telomeric from HLA. It has a multipoint maximum lod score of 4.66 (compared with 4.44 for HLA-DQ) and appears to have a recessive mode of inheritance. Our study localizes and provides strong evidence for linkage of at least one non-HLA locus to celiac disease and may serve as a prototype for an efficient approach to screening the human genome for loci that contribute to complex diseases.

摘要

乳糜泻是一种具有高度遗传性的胃肠道疾病,是遗传复杂的多因素免疫介导疾病的一个特别重要的模型。乳糜泻的HLA成分(一种特定的HLA-DQ异二聚体)在很大程度上已明确,且相对不复杂,其环境成分(饮食中的麸质及相关谷物储存蛋白)也已被充分了解。先前关于乳糜泻的家族研究表明,至少存在一个重要的非HLA基因座。该基因座可能是比HLA更强的遗传因素,且显然具有隐性遗传模式。我们采用三步基因组筛选方案,在爱尔兰西部各县识别与乳糜泻相关的基因座,该地区是世界上乳糜泻患病率最高的地区。我们发现的几个可能的非HLA基因座中,最显著的位于6号染色体上,距HLA约30厘摩端粒处。其多点最大对数优势得分为4.66(相比之下,HLA-DQ为4.44),且似乎具有隐性遗传模式。我们的研究定位了至少一个非HLA基因座与乳糜泻的连锁关系,并提供了有力证据,可为在人类基因组中筛选与复杂疾病相关基因座的有效方法提供范例。

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