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性别差异选择对细胞核质多态性和不平衡的影响。

Effects of differential selection in the sexes on cytonuclear polymorphism and disequilibria.

作者信息

Babcock C S, Asmussen M A

机构信息

Department of Genetics, University of Georgia, Athens 30502, USA.

出版信息

Genetics. 1996 Oct;144(2):839-53. doi: 10.1093/genetics/144.2.839.

Abstract

We develop a series of models that examine the effects of differential selection between the sexes on cytonuclear polymorphism and disequilibria. A detailed analysis is provided for populations under constant fertility or viability selection censused at life stages without frequency differences in the sexes. We show analytically that cytonuclear disequilibria can be generated de novo if the cytoplasmic and nuclear loci each affect female fitness and there is no nonmultiplicative fitness interaction between them. While computer simulations demonstrate that the majority of disequilibria produced by random selection are transient and small in magnitude, measurable permanent disequilibria can result from selective differences both within and between the two sexes. We derive analytic conditions for a protected cytonuclear polymorphism and use numerical simulations to quantitate the likelihood of obtaining permanent nuclear, cytoplasmic, and cytonuclear variation under various patterns of selection. The numerical analysis identifies special selection regimes more likely to generate disequilibria and maintain cytonuclear polymorphism and reveals a direct correlation to the strength of selection. As a byproduct, our models also provide the first decomposition of the different parental contributions to cytonuclear dynamics and the analytic conditions under which selection can cause cytoplasmic frequency changes or a cytonuclear hitchhiking effect.

摘要

我们开发了一系列模型,用于研究两性间差异选择对细胞核质多态性和不平衡的影响。针对在生命阶段进行普查且两性频率无差异的恒定生育力或生存力选择下的种群,提供了详细分析。我们通过分析表明,如果细胞质和细胞核基因座均影响雌性适合度且它们之间不存在非乘法适合度相互作用,那么细胞核质不平衡可以重新产生。虽然计算机模拟表明随机选择产生的大多数不平衡是短暂的且幅度较小,但两性内部和之间的选择差异可能导致可测量的永久性不平衡。我们推导了受保护的细胞核质多态性的分析条件,并使用数值模拟来量化在各种选择模式下获得永久性核、细胞质和细胞核质变异的可能性。数值分析确定了更有可能产生不平衡并维持细胞核质多态性的特殊选择机制,并揭示了与选择强度的直接相关性。作为一个副产品,我们的模型还首次分解了不同亲本对细胞核质动态的贡献以及选择可导致细胞质频率变化或细胞核质搭便车效应的分析条件。

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