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首页> 外文期刊>Molecular biology and evolution >Excess of Deleterious Mutations around HLA Genes Reveals Evolutionary Cost of Balancing Selection
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Excess of Deleterious Mutations around HLA Genes Reveals Evolutionary Cost of Balancing Selection

机译:HLA基因周围有害突变的过量揭示了平衡选择的进化成本。

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摘要

Deleterious mutations are expected to evolve under negative selection and are usually purged from the population. However, deleterious alleles segregate in the human population and some disease-associated variants are maintained at considerable frequencies. Here, we test the hypothesis that balancing selection may counteract purifying selection in neighboring regions and thus maintain deleterious variants at higher frequency than expected from their detrimental fitness effect. We first show in realistic simulations that balancing selection reduces the density of polymorphic sites surrounding a locus under balancing selection, but at the same time markedly increases the population frequency of the remaining variants, including even substantially deleterious alleles. To test the predictions of our simulations empirically, we then use whole-exome sequencing data from 6,500 human individuals and focus on the most established example for balancing selection in the human genome, the major histocompatibility complex (MHC). Our analysis shows an elevated frequency of putatively deleterious coding variants in nonhuman leukocyte antigen (non-HLA) genes localized in the MHC region. The mean frequency of these variants declined with physical distance from the classical HLA genes, indicating dependency on genetic linkage. These results reveal an indirect cost of the genetic diversity maintained by balancing selection, which has hitherto been perceived as mostly advantageous, and have implications both for the evolution of recombination and also for the epidemiology of various MHC-associated diseases.
机译:有害突变有望在阴性选择下进化,通常会从种群中清除。然而,有害的等位基因在人群中隔离,并且一些与疾病相关的变异以相当高的频率维持。在这里,我们测试了以下假设:平衡选择可能会抵消邻近区域的纯化选择,从而使有害变体的出现频率高于其有害适应性效果所预期的频率。我们首先在现实的模拟中表明,平衡选择降低了平衡选择下基因座周围多态位点的密度,但同时显着增加了其余变体(甚至包括有害等位基因)的种群频率。为了凭经验检验模拟的预测,我们然后使用来自6,500个人类个体的全外显子组测序数据,并着眼于建立平衡人类基因组选择的最成熟示例,即主要组织相容性复合体(MHC)。我们的分析表明,位于MHC区域的非人类白细胞抗原(non-HLA)基因中推定有害的编码变体的频率升高。这些变体的平均频率随与经典HLA基因的物理距离而降低,表明对遗传连锁的依赖性。这些结果揭示了通过平衡选择维持的遗传多样性的间接成本,这迄今为止被认为是最有利的,并且对重组的进化以及与各种MHC相关疾病的流行病学都有影响。

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