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西部低地大猩猩(Pan troglodytes verus)和人类的遗传多样性和连锁不平衡具有相似模式,表明 MHC 分子进化的高度保守机制。

Similar patterns of genetic diversity and linkage disequilibrium in Western chimpanzees (Pan troglodytes verus) and humans indicate highly conserved mechanisms of MHC molecular evolution.

机构信息

Laboratory of Anthropology, Genetics and Peopling History, Department of Genetics and Evolution, Anthropology Unit, University of Geneva, Geneva, Switzerland.

Institute of Genetics and Genomics in Geneva (iGE3), University of Geneva, Geneva, Switzerland.

出版信息

BMC Evol Biol. 2020 Sep 15;20(1):119. doi: 10.1186/s12862-020-01669-6.

Abstract

BACKGROUND

Many species are threatened with extinction as their population sizes decrease with changing environments or face novel pathogenic threats. A reduction of genetic diversity at major histocompatibility complex (MHC) genes may have dramatic effects on populations' survival, as these genes play a key role in adaptive immunity. This might be the case for chimpanzees, the MHC genes of which reveal signatures of an ancient selective sweep likely due to a viral epidemic that reduced their population size a few million years ago. To better assess how this past event affected MHC variation in chimpanzees compared to humans, we analysed several indexes of genetic diversity and linkage disequilibrium across seven MHC genes on four cohorts of chimpanzees and we compared them to those estimated at orthologous HLA genes in a large set of human populations.

RESULTS

Interestingly, the analyses uncovered similar patterns of both molecular diversity and linkage disequilibrium across the seven MHC genes in chimpanzees and humans. Indeed, in both species the greatest allelic richness and heterozygosity were found at loci A, B, C and DRB1, the greatest nucleotide diversity at loci DRB1, DQA1 and DQB1, and both significant global linkage disequilibrium and the greatest proportions of haplotypes in linkage disequilibrium were observed at pairs DQA1 ~ DQB1, DQA1 ~ DRB1, DQB1 ~ DRB1 and B ~ C. Our results also showed that, despite some differences among loci, the levels of genetic diversity and linkage disequilibrium observed in contemporary chimpanzees were globally similar to those estimated in small isolated human populations, in contrast to significant differences compared to large populations.

CONCLUSIONS

We conclude, first, that highly conserved mechanisms shaped the diversity of orthologous MHC genes in chimpanzees and humans. Furthermore, our findings support the hypothesis that an ancient demographic decline affecting the chimpanzee populations - like that ascribed to a viral epidemic - exerted a substantial effect on the molecular diversity of their MHC genes, albeit not more pronounced than that experienced by HLA genes in human populations that underwent rapid genetic drift during humans' peopling history. We thus propose a model where chimpanzees' MHC genes regenerated molecular variation through recombination/gene conversion and/or balancing selection after the selective sweep.

摘要

背景

随着环境的变化或面临新的致病威胁,许多物种的种群数量减少,面临灭绝的威胁。主要组织相容性复合体 (MHC) 基因的遗传多样性减少可能对种群的生存产生巨大影响,因为这些基因在适应性免疫中发挥关键作用。这种情况可能发生在黑猩猩身上,它们的 MHC 基因显示出古老的选择清除的特征,这可能是由于几百万年前的一场病毒流行导致其种群数量减少。为了更好地评估过去的事件如何影响黑猩猩和人类的 MHC 变异,我们分析了四个黑猩猩群体的七个 MHC 基因上的几个遗传多样性和连锁不平衡指标,并将它们与大量人类群体中的同源 HLA 基因进行了比较。

结果

有趣的是,分析结果揭示了黑猩猩和人类七个 MHC 基因的分子多样性和连锁不平衡的相似模式。事实上,在这两个物种中,A、B、C 和 DRB1 位点的等位基因丰富度和杂合度最大,DRB1、DQA1 和 DQB1 位点的核苷酸多样性最大,DQA1DQB1、DQA1DRB1、DQB1DRB1 和 BC 对的全局连锁不平衡和最大比例的连锁不平衡单倍型都很明显。我们的结果还表明,尽管各基因座之间存在一些差异,但当代黑猩猩中观察到的遗传多样性和连锁不平衡水平与小而孤立的人类群体中估计的水平总体上相似,与大群体相比则存在显著差异。

结论

首先,我们得出结论,高度保守的机制塑造了黑猩猩和人类同源 MHC 基因的多样性。此外,我们的研究结果支持这样一种假设,即影响黑猩猩种群的古老人口下降——如归因于病毒流行——对其 MHC 基因的分子多样性产生了巨大影响,尽管不如人类群体中的 HLA 基因在人类迁徙历史中经历的快速遗传漂变更为明显。因此,我们提出了一个模型,即黑猩猩的 MHC 基因在选择清除后通过重组/基因转换和/或平衡选择产生了分子变异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d82/7491122/c04a6ec45c44/12862_2020_1669_Fig1_HTML.jpg

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