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Hotspots for copy number variation in chimpanzees and humans

机译:黑猩猩和人类中拷贝数变异的热点

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摘要

Copy number variation is surprisingly common among humans and can be involved in phenotypic diversity and variable susceptibility to complex diseases, but little is known of the extent of copy number variation in nonhuman primates. We have used two array-based comparative genomic hybridization platforms to identify a total of 355 copy number variants (CNVs) in the genomes of 20 wild-born chimpanzees (Pan troglodytes) and have compared the identified chimpanzee CNVs to known human CNVs from previous studies. Many CNVs were observed in the corresponding regions in both chimpanzees and humans; especially those CNVs of higher frequency. Strikingly, these loci are enriched 20-fold for ancestral segmental duplications, which may facilitate CNV formation through nonallelic homologous recombination mechanisms. Therefore, some of these regions may be unstable "hotspots" for the genesis of copy number variation, with recurrent duplications and deletions occurring across and within species.
机译:拷贝数变异令人惊讶地在人类中普遍存在,并且可能涉及表型多样性和对复杂疾病的易感性,但是对于非人类灵长类动物的拷贝数变异程度知之甚少。我们使用了两个基于阵列的比较基因组杂交平台,在20个野生黑猩猩(Pan troglodytes)的基因组中鉴定出总共355个拷贝数变异(CNV),并将已鉴定的黑猩猩CNV与先前研究中的已知人类CNV进行了比较。在黑猩猩和人类的相应区域都观察到许多CNV。特别是那些频率较高的CNV。令人惊讶的是,这些基因座富集了20倍的祖先节段重复,可通过非等位基因同源重组机制促进CNV的形成。因此,这些区域中的某些区域对于拷贝数变异的起源可能是不稳定的“热点”,在物种内部和内部发生重复的复制和缺失。

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