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A strong signature of balancing selection in the 5′ cis-regulatory region of CCR5

机译:CCR5 5'顺式调节区域中平衡选择的有力标志

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摘要

CCR5 encodes a cell surface chemokine receptor molecule that serves as the principal coreceptor, with CD4, for HIV-type 1 (HIV-1). Varied HIV-1 susceptibility and time to progression to AIDS have been associated with polymorphisms in CCR5. Many of these polymorphisms are located in the 5′ cis-regulatory region of CCR5, suggesting that it may have been a target of natural selection. We characterized CCR5 sequence variation in this region in 400 chromosomes from worldwide populations and compared it to a genome-wide analysis of 100 Alu polymorphisms typed in the same populations. Variation was substantially higher than expected and characterized by an excess of intermediate-frequency alleles. A genealogy of CCR5 haplotypes had deep branch lengths despite markedly little differentiation among populations. This finding suggested a deviation from neutrality not accounted for by population structure, which was confirmed by tests for natural selection. These results are strong evidence that balancing selection has shaped the pattern of variation in CCR5 and suggest that HIV-1 resistance afforded by CCR5 5′ cis-regulatory region haplotypes may be the consequence of adaptive changes to older pathogens.
机译:CCR5编码一个细胞表面趋化因子受体分子,与CD4一起用作HIV 1型(HIV-1)的主要共受体。 HIV-1的易感性和发展为AIDS的时间与CCR5的多态性有关。这些多态性中的许多位于CCR5的5'顺式调控区域,表明它可能已经成为自然选择的目标。我们表征了来自全球人群的400条染色体中该区域的CCR5序列变异,并将其与同一人群中100种Alu多态性的全基因组分析进行了比较。变异显着高于预期,并以过量的中频等位基因为特征。 CCR5单倍体的谱系具有很深的分支长度,尽管在群体间差异很小。这一发现表明,人口结构并未解释与中立性的偏差,这一点已通过自然选择的测试得到证实。这些结果有力的证据表明,平衡选择已塑造了CCR5的变异模式,并表明CCR5 5'顺式调控区单倍型提供的HIV-1抗性可能是对较旧病原体适应性改变的结果。

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