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多基因信号表明人类的性选择存在性别差异,该研究来自英国生物库。

Polygenic signals of sex differences in selection in humans from the UK Biobank.

机构信息

School of Biological Sciences, Monash University, Clayton, Victoria, Australia.

School of BioSciences, University of Melbourne, Parkville, Victoria, Australia.

出版信息

PLoS Biol. 2022 Sep 6;20(9):e3001768. doi: 10.1371/journal.pbio.3001768. eCollection 2022 Sep.

Abstract

Sex differences in the fitness effects of genetic variants can influence the rate of adaptation and the maintenance of genetic variation. For example, "sexually antagonistic" (SA) variants, which are beneficial for one sex and harmful for the other, can both constrain adaptation and increase genetic variability for fitness components such as survival, fertility, and disease susceptibility. However, detecting variants with sex-differential fitness effects is difficult, requiring genome sequences and fitness measurements from large numbers of individuals. Here, we develop new theory for studying sex-differential selection across a complete life cycle and test our models with genotypic and reproductive success data from approximately 250,000 UK Biobank individuals. We uncover polygenic signals of sex-differential selection affecting survival, reproductive success, and overall fitness, with signals of sex-differential reproductive selection reflecting a combination of SA polymorphisms and sexually concordant polymorphisms in which the strength of selection differs between the sexes. Moreover, these signals hold up to rigorous controls that minimise the contributions of potential confounders, including sequence mapping errors, population structure, and ascertainment bias. Functional analyses reveal that sex-differentiated sites are enriched in phenotype-altering genomic regions, including coding regions and loci affecting a range of quantitative traits. Population genetic analyses show that sex-differentiated sites exhibit evolutionary histories dominated by genetic drift and/or transient balancing selection, but not long-term balancing selection, which is consistent with theoretical predictions of effectively weak SA balancing selection in historically small populations. Overall, our results are consistent with polygenic sex-differential-including SA-selection in humans. Evidence for sex-differential selection is particularly strong for variants affecting reproductive success, in which the potential contributions of nonrandom sampling to signals of sex differentiation can be excluded.

摘要

性别间遗传变异对适合度的影响差异可能会影响适应速度和遗传变异的维持。例如,对一种性别有利而对另一种性别有害的“性拮抗”(SA)变异既可以限制适应,又可以增加生存、繁殖力和疾病易感性等适应成分的遗传变异性。然而,检测具有性别差异的适合度效应的变异是困难的,需要大量个体的基因组序列和适合度测量。在这里,我们开发了一种新的理论来研究整个生命周期中的性别差异选择,并使用来自大约 25 万英国生物库个体的基因型和繁殖成功数据来测试我们的模型。我们发现了影响生存、繁殖成功和整体适合度的性别差异选择的多基因信号,反映了性别差异的生殖选择信号,包括 SA 多态性和性一致的多态性,在性一致的多态性中,性别之间的选择强度不同。此外,这些信号经得起严格的控制,最大限度地减少了潜在混杂因素的影响,包括序列映射错误、群体结构和选择偏差。功能分析表明,性别差异的位点在改变表型的基因组区域中富集,包括编码区域和影响一系列数量性状的位点。群体遗传分析表明,性别差异的位点表现出由遗传漂变和/或瞬时平衡选择主导的进化历史,但没有长期平衡选择,这与历史上小群体中有效弱 SA 平衡选择的理论预测一致。总的来说,我们的结果与人类多基因性别差异(包括 SA)选择一致。对于影响繁殖成功的变异,性别差异选择的证据尤其强烈,在这种情况下,可以排除非随机抽样对性别分化信号的潜在贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cbbd/9481184/2676dc6ccf6a/pbio.3001768.g001.jpg

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