首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Signatures of strong population differentiation shape extended haplotypes across the human CD28, CTLA4, and ICOS costimulatory genes
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Signatures of strong population differentiation shape extended haplotypes across the human CD28, CTLA4, and ICOS costimulatory genes

机译:强烈的群体分化形状的特征在人类CD28,CTLA4和ICOS共刺激基因中扩展了单倍型

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摘要

The three members of the costimulatory receptor family, CD28, CTLA-4, and ICOS, have complementary effects on T cell activation, and their balance controls the overall outcome of immune and autoimmune responses. They are encoded in a short genomic interval, and overall activity may result from interplay between allelic variants at each locus. With multiethnic DNA panels that represent a wide spectrum of human populations, we demonstrate long-range linkage disequilibrium among the three genes. A large fraction of the variation found in the locus can be explained by the presence of extended haplotypes encompassing variants at CD28, CTLA4, and the ICOS promoter. There are unusual differences in the distribution of some variants and haplotypes between geographic regions. The differences may reflect demographic events and/or the adaptation to diverse environmental and microbial challenges encountered in the course of human migrations and will be important to consider when interpreting association to immune/ autoimmune responsiveness.
机译:共刺激受体家族的三个成员CD28,CTLA-4和ICOS对T细胞活化具有互补作用,它们的平衡控制着免疫和自身免疫反应的总体结果。它们以短的基因组间隔进行编码,并且总体活性可能来自每个位点的等位基因变体之间的相互作用。利用代表着广泛人群的多种族DNA面板,我们证明了这三个基因之间的长期连锁不平衡。在基因座中发现的很大一部分变异可以解释为存在延伸的单倍型,其中包括CD28,CTLA4和ICOS启动子的变异。地理区域之间某些变体和单倍型的分布存在不同寻常的差异。这些差异可能反映了人口事件和/或对人类迁移过程中遇到的各种环境和微生物挑战的适应性,在解释与免疫/自身免疫应答的关联时,必须考虑这些差异。

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