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减数分裂驱动影响连锁基因座上性对抗性选择的结果。

Meiotic drive influences the outcome of sexually antagonistic selection at a linked locus.

作者信息

Patten M M

机构信息

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

出版信息

J Evol Biol. 2014 Nov;27(11):2360-70. doi: 10.1111/jeb.12493. Epub 2014 Oct 8.

Abstract

Most meiotic drivers, such as the t-haplotype in Mus and the segregation distorter (SD) in Drosophila, act in a sex-specific manner, gaining a transmission advantage through one sex although suffering only the fitness costs associated with the driver in the other. Their inheritance is thus more likely through one of the two sexes, a property they share with sexually antagonistic alleles. Previous theory has shown that pairs of linked loci segregating for sexually antagonistic alleles are more likely to remain polymorphic and that linkage disequilibrium accrues between them. I probe this similarity between drive and sexual antagonism and examine the evolution of chromosomes experiencing these selection pressures simultaneously. Reminiscent of previous theory, I find that: the opportunity for polymorphism increases for a sexually antagonistic locus that is physically linked to a driving locus; the opportunity for polymorphism at a driving locus also increases when linked to a sexually antagonistic locus; and stable linkage disequilibrium accompanies any polymorphic equilibrium. Additionally, I find that drive at a linked locus favours the fixation of sexually antagonistic alleles that benefit the sex in which drive occurs. Further, I show that under certain conditions reduced recombination between these two loci is selectively favoured. These theoretical results provide clear, testable predictions about the nature of sexually antagonistic variation on driving chromosomes and have implications for the evolution of genomic architecture.

摘要

大多数减数分裂驱动因子,如小家鼠中的t单倍型和果蝇中的分离畸变因子(SD),以性别特异性方式起作用,通过一种性别获得传递优势,尽管在另一种性别中仅承受与驱动因子相关的适合度代价。因此,它们更有可能通过两种性别之一遗传,这一特性与性拮抗等位基因相同。先前的理论表明,为性拮抗等位基因分离的连锁基因座对更有可能保持多态性,并且它们之间会积累连锁不平衡。我探究了驱动与性拮抗之间的这种相似性,并研究了同时经历这些选择压力的染色体的进化。与先前的理论类似,我发现:与驱动基因座物理连锁的性拮抗基因座的多态性机会增加;当与性拮抗基因座连锁时,驱动基因座的多态性机会也会增加;任何多态平衡都伴随着稳定的连锁不平衡。此外,我发现连锁基因座上的驱动有利于那些使驱动发生的性别受益的性拮抗等位基因的固定。此外,我表明在某些条件下,这两个基因座之间重组的减少受到选择青睐。这些理论结果为驱动染色体上性拮抗变异的性质提供了清晰、可检验的预测,并对基因组结构的进化具有启示意义。

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