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性拮抗导致 X 染色体与常染色体冲突的镶嵌现象。

Sexual antagonism leads to a mosaic of X-autosome conflict.

机构信息

Department of Ecology and Evolutionary Biology, University of California, Irvine, California, 92697.

Department of Biology, Georgetown University, Washington, DC, 20057.

出版信息

Evolution. 2020 Feb;74(2):495-498. doi: 10.1111/evo.13918. Epub 2020 Jan 11.

DOI:10.1111/evo.13918
PMID:31885085
Abstract

Males and females have different optimal values for some traits, such as body size. When the same genes control these traits in both sexes, selection pushes in opposite directions in males and females. Alleles at autosomal loci spend equal amounts of time in males and females, suggesting that the sexually antagonistic selective forces may approximately balance between the opposing optima. Frank and Crespi noted that alleles on the X chromosome spend twice as much time in diploid females as in haploid males. That distinction between the sexes may tend to favor X-linked genes that push more strongly toward the female optimum than the male optimum. The female bias of X-linked genes opposes the intermediate optimum of autosomal genes, potentially creating a difference between the direction of selection on traits favored by X chromosomes and autosomes. Patten has recently argued that explicit genetic assumptions about dominance and the relative magnitude of allelic effects may lead X-linked genes to favor the male rather than the female optimum, contradicting Frank and Crespi. This article combines the insights of those prior analyses into a new, more general theory. We find some parameter combinations for X-linked loci that favor a female bias and other parameter combinations that favor a male bias. We conclude that the X likely contains a mosaic pattern of loci that differ with autosomes over sexually antagonistic traits. The overall tendency for a female or male bias on the X depends on prior assumptions about the distribution of key parameters across X-linked loci. Those parameters include the dominance coefficient and the way in which ploidy influences the magnitude of allelic effects.

摘要

男性和女性在某些特征(如体型)上有不同的最佳值。当相同的基因控制两性的这些特征时,选择在男性和女性身上朝着相反的方向推动。常染色体座位上的等位基因在男性和女性中花费相同的时间,这表明性拮抗选择力可能在相反的最佳值之间大致平衡。Frank 和 Crespi 注意到,X 染色体上的等位基因在二倍体雌性中花费的时间是在单体雄性中的两倍。这种性别的区别可能倾向于支持那些比雄性最佳值更强烈地推向雌性最佳值的 X 连锁基因。X 连锁基因的雌性偏性与常染色体基因的中间最佳值相悖,这可能导致 X 染色体和常染色体所支持的特征选择方向之间存在差异。Patten 最近认为,关于显性和等位基因效应相对大小的明确遗传假设可能导致 X 连锁基因偏向于雄性而不是雌性最佳值,这与 Frank 和 Crespi 的观点相矛盾。本文将这些先前分析的见解结合到一个新的、更普遍的理论中。我们发现了一些有利于雌性偏性的 X 连锁基因的参数组合,以及一些有利于雄性偏性的参数组合。我们的结论是,X 染色体可能包含一个不同的基因座模式,这些基因座在性拮抗特征上与常染色体不同。X 染色体上的整体雌性或雄性偏性趋势取决于 X 连锁基因上位点的关键参数分布的先验假设。这些参数包括显性系数以及ploidy 影响等位基因效应大小的方式。

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