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Divergence patterns of genic copy number variation in natural populations of the house mouse (Mus musculus domesticus) reveal three conserved genes with major population-specific expansions

机译:家鼠(mus musculus domesticus)自然群体中基因拷贝数变异的分歧模式揭示了具有主要种群特异性扩增的三个保守基因。

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摘要

Copy number variation represents a major source of genetic divergence, yet the evolutionary dynamics of genic copy number variation in natural populations during differentiation and adaptation remain unclear. We applied a read depth approach to genome resequencing data to detect copy number variants (CNVs) ≥1 kb in wild-caught mice belonging to four populations of Mus musculus domesticus. We complemented the bioinformatics analyses with experimental validation using droplet digital PCR. The specific focus of our analysis is CNVs that include complete genes, as these CNVs could be expected to contribute most directly to evolutionary divergence. In total, 1863 transcription units appear to be completely encompassed within CNVs in at least one individual when compared to the reference assembly. Further, 179 of these CNVs show population-specific copy number differences, and 325 are subject to complete deletion in multiple individuals. Among the most copy-number variable genes are three highly conserved genes that encode the splicing factor CWC22, the spindle protein SFI1, and the Holliday junction recognition protein HJURP. These genes exhibit population-specific expansion patterns that suggest involvement in local adaptations. We found that genes that overlap with large segmental duplications are generally more copy-number variable. These genes encode proteins that are relevant for environmental and behavioral interactions, such as vomeronasal and olfactory receptors, as well as major urinary proteins and several proteins of unknown function. The overall analysis shows that genic CNVs contribute more to population differentiation in mice than in humans and may promote and speed up population divergence.
机译:拷贝数变异代表了遗传差异的主要来源,但尚不清楚在分化和适应过程中自然种群中基因拷贝数变异的进化动力学。我们对基因组重测序数据应用了读取深度方法,以检测属于四个家蝇种群的野外捕获小鼠中的拷贝数变异(CNV)≥1 kb。我们通过使用液滴数字PCR的实验验证对生物信息学分析进行了补充。我们分析的重点是包含完整基因的CNV,因为可以预期这些CNV对进化差异的贡献最大。与参考组件相比,至少有1个个体的CNV共有1863个转录单位。此外,这些CNV中有179个显示出特定群体的拷贝数差异,而325个在多个个体中完全缺失。在拷贝数最多的可变基因中,有三个高度保守的基因,它们编码剪接因子CWC22,纺锤体蛋白SFI1和霍利迪连接识别蛋白HJURP。这些基因表现出特定于种群的扩展模式,表明参与局部适应。我们发现与大的节段重复重叠的基因通常具有更多的拷贝数变量。这些基因编码与环境和行为相互作用有关的蛋白质,例如犁鼻和嗅觉受体,以及主要的尿液蛋白质和功能未知的几种蛋白质。总体分析表明,与小鼠相比,基因CNV对小鼠的种群分化贡献更大,并且可以促进和加速种群分化。

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