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单倍型特异性连锁不平衡模式定义了人类主要组织相容性复合体的遗传图谱。

Haplotype-specific linkage disequilibrium patterns define the genetic topography of the human MHC.

作者信息

Ahmad Tariq, Neville Matt, Marshall Sara E, Armuzzi Alessandro, Mulcahy-Hawes Kim, Crawshaw Jonathan, Sato Hiroe, Ling Khoon-Lin, Barnardo Martin, Goldthorpe Sue, Walton Robert, Bunce Mike, Jewell Derek P, Welsh Ken I

机构信息

Gastroenterology Unit, University of Oxford, Gibson Laboratories, Radcliffe Infirmary, Woodstock Road, Oxford, OX2 6HE, UK.

出版信息

Hum Mol Genet. 2003 Mar 15;12(6):647-56.

Abstract

Detailed knowledge of linkage disequilibrium (LD) is regarded as a prerequisite for population-based disease gene mapping. Variable patterns across the human genome are now recognized, both between regions and populations. Here, we demonstrate that LD may also vary within a genomic region in a haplotype-specific manner. In 864 Caucasian unrelated individuals, we describe haplotype-specific LD patterns across the human MHC by the construction of gene-specific allelic haplotypes at 25 loci between HLA-A and Tapasin. Strong and extensive LD is found across both common and rare haplotypes, suggesting that haplotype structure is influenced by factors other than genetic drift, including both selection and differential haplotype recombination. Knowledge of haplotype-specific LD in the HLA may explain the apparent discrepant data from previous studies of global LD, help delineate key areas in mapping HLA-associated diseases and, together with recombination data, provide valuable information about a population's demographic history and the selective pressures operating on it.

摘要

连锁不平衡(LD)的详细知识被视为基于人群的疾病基因定位的先决条件。现在人们认识到,人类基因组中存在着跨区域和人群的可变模式。在这里,我们证明LD在基因组区域内也可能以单倍型特异性方式发生变化。在864名无亲缘关系的白种人中,我们通过构建HLA-A和TAPASIN之间25个位点的基因特异性等位基因单倍型,描述了人类MHC上的单倍型特异性LD模式。在常见和罕见单倍型中均发现了强烈而广泛的LD,这表明单倍型结构受到遗传漂变以外的因素影响,包括选择和差异单倍型重组。了解HLA中特定单倍型的LD可能解释先前全球LD研究中明显矛盾的数据,有助于划定HLA相关疾病定位的关键区域,并与重组数据一起提供有关人群人口历史和作用于其上的选择压力的有价值信息。

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