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多效性中的遗传变异:差异上位性作为长骨长度与体重之间异速生长关系变异的一个来源。

Genetic variation in pleiotropy: differential epistasis as a source of variation in the allometric relationship between long bone lengths and body weight.

作者信息

Pavlicev Mihaela, Kenney-Hunt Jane P, Norgard Elizabeth A, Roseman Charles C, Wolf Jason B, Cheverud James M

机构信息

Department of Anatomy and Neurobiology, Washington University, St Louis, MO 63110, USA.

出版信息

Evolution. 2008 Jan;62(1):199-213. doi: 10.1111/j.1558-5646.2007.00255.x. Epub 2007 Nov 12.

DOI:10.1111/j.1558-5646.2007.00255.x
PMID:18005158
Abstract

Pleiotropy is an aspect of genetic architecture underlying the phenotypic covariance structure. The presence of genetic variation in pleiotropy is necessary for natural selection to shape patterns of covariation between traits. We examined the contribution of differential epistasis to variation in the intertrait relationship and the nature of this variation. Genetic variation in pleiotropy was revealed by mapping quantitative trait loci (QTLs) affecting the allometry of mouse limb and tail length relative to body weight in the mouse-inbred strain LG/J by SM/J intercross. These relationship QTLs (rQTLs) modify relationships between the traits affected by a common pleiotropic locus. We detected 11 rQTLs, mostly affecting allometry of multiple bones. We further identified epistatic interactions responsible for the observed allometric variation. Forty loci that interact epistatically with the detected rQTLs were identified. We demonstrate how these epistatic interactions differentially affect the body size variance and the covariance of traits with body size. We conclude that epistasis, by differentially affecting both the canalization and mean values of the traits of a pleiotropic domain, causes variation in the covariance structure. Variation in pleiotropy maintains evolvability of the genetic architecture, in particular the evolvability of its modular organization.

摘要

多效性是表型协方差结构背后遗传结构的一个方面。多效性中遗传变异的存在对于自然选择塑造性状间协变模式是必要的。我们研究了差异上位性对性状间关系变异的贡献以及这种变异的本质。通过对小鼠近交系LG/J与SM/J杂交后代中影响小鼠肢体和尾巴长度相对于体重的异速生长的数量性状位点(QTL)进行定位,揭示了多效性中的遗传变异。这些关系QTL(rQTL)改变了受共同多效性位点影响的性状之间的关系。我们检测到11个rQTL,大多影响多块骨骼的异速生长。我们进一步确定了导致观察到的异速生长变异的上位性相互作用。确定了40个与检测到的rQTL发生上位性相互作用的位点。我们展示了这些上位性相互作用如何不同地影响体型方差以及性状与体型的协方差。我们得出结论,上位性通过不同地影响多效性领域性状的稳态化和平均值,导致协方差结构发生变异。多效性的变异维持了遗传结构的进化能力,特别是其模块化组织的进化能力。

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