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Retrotransposition of gene transcripts leads to structural variation in mammalian genomes

机译:基因转录物的逆转座导致哺乳动物基因组的结构变异

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Background Retroposed processed gene transcripts are an important source of material for new gene formation on evolutionary timescales. Most prior work on gene retrocopy discovery compared copies in reference genome assemblies to their source genes. Here, we explore gene retrocopy insertion polymorphisms (GRIPs) that are present in the germlines of individual humans, mice, and chimpanzees, and we identify novel gene retrocopy insertions in cancerous somatic tissues that are absent from patient-matched non-cancer genomes.Results Through analysis of whole-genome sequence data, we found evidence for 48 GRIPs in the genomes of one or more humans sequenced as part of the 1,000 Genomes Project and The Cancer Genome Atlas, but which were not in the human reference assembly. Similarly, we found evidence for 755 GRIPs at distinct locations in one or more of 17 inbred mouse strains but which were not in the mouse reference assembly, and 19 GRIPs across a cohort of 10 chimpanzee genomes, which were not in the chimpanzee referencegenome assembly. Many of these insertions are new members of existing gene families whose source genes are highly and widely expressed, and the majority have detectable hallmarks of processed gene retrocopy formation. We estimate the rate of novel generetrocopy insertions in humans and chimps at roughly one new gene retrocopy insertion for every 6,000 individuals. Conclusions We find that gene retrocopy polymorphisms are a widespread phenomenon, present a multi-species analysis of these events, and provide a method for their ascertainment.
机译:背景技术加工后的基因转录本是进化时标上新基因形成的重要物质来源。关于基因逆转录发现的大多数先前工作将参考基因组装配体中的拷贝与其源基因进行了比较。在这里,我们探索了在人类,小鼠和黑猩猩的种系中存在的基因逆转录插入多态性(GRIP),并鉴定了在患者匹配的非癌症基因组中缺少的癌性体组织中的新基因逆转录插入。通过对全基因组序列数据的分析,我们发现了一个或多个人类基因组中有48个GRIP的证据,这些基因已作为1,000个基因组计划和《癌症基因组图集》的一部分进行了测序,但并未纳入人类参考文献中。同样,我们在17个近交小鼠品系中的一个或多个中的不同位置发现了755个GRIP,但这些证据不在小鼠参考装配中,而在10个黑猩猩基因组队列中的19个GRIP却不在黑猩猩参考基因组装配中。这些插入物中的许多是现有基因家族的新成员,其原始基因高度且广泛表达,并且大多数具有加工过的基因逆转录形成的可检测特征。我们估计人类和黑猩猩的新基因逆转录插入率约为每6,000个个体一个新基因逆转录插入。结论我们发现基因逆转录多态性是一种普遍现象,对这些事件进行了多物种分析,并提供了确定它们的方法。

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