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免疫球蛋白重链基因座:遗传变异、缺失数据及其对人类疾病的影响。

The immunoglobulin heavy chain locus: genetic variation, missing data, and implications for human disease.

机构信息

Department of Biological Sciences, Simon Fraser University, Burnaby, BC, Canada.

出版信息

Genes Immun. 2012 Jul;13(5):363-73. doi: 10.1038/gene.2012.12. Epub 2012 May 3.

DOI:10.1038/gene.2012.12
PMID:22551722
Abstract

The immunoglobulin (IG) loci consist of repeated and highly homologous sets of genes of different types, variable (V), diversity (D) and junction (J), that rearrange in developing B cells to produce an individual's highly variable repertoire of expressed antibodies, designed to bind to a vast array of pathogens. This repeated structure makes these loci susceptible to a high frequency of insertion and deletion events through evolutionary time, and also makes them difficult to characterize at the genomic level or assay with high-throughput techniques. Given the central role of antibodies in the adaptive immune system, it is not surprising that early candidate gene approaches showed that germline polymorphisms in these regions correlated with susceptibility to both infectious and autoimmune diseases. However, more recent studies, particularly those using high-throughput genome-wide arrays, have failed to implicate these loci in disease. In this review of the IG heavy chain variable gene cluster (IGHV), we examine how poorly we understand the distribution of haplotype variation in this genomic region, and we argue that this lack of information may mask candidate loci in the IGHV gene cluster as causative factors for infectious and autoimmune diseases.

摘要

免疫球蛋白(IG)基因座由不同类型的可变(V)、多样性(D)和连接(J)基因的重复和高度同源序列组成,这些基因在发育中的 B 细胞中重排,产生个体高度可变的表达抗体库,旨在与大量病原体结合。这种重复结构使这些基因座在进化过程中容易发生高频插入和缺失事件,并且也使它们难以在基因组水平上进行特征描述或使用高通量技术进行检测。鉴于抗体在适应性免疫系统中的核心作用,早期候选基因方法表明这些区域的种系多态性与感染性和自身免疫性疾病的易感性相关,这并不奇怪。然而,最近的研究,特别是使用高通量全基因组芯片的研究,未能表明这些基因座与疾病有关。在对 IG 重链可变基因簇(IGHV)的综述中,我们研究了我们对该基因组区域单倍型变异分布的理解程度很差,并且我们认为这种信息的缺乏可能掩盖了 IGHV 基因簇中作为感染性和自身免疫性疾病致病因素的候选基因座。

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