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Expanding whole exome resequencing into non-human primates

机译:将整个外显子组重排扩展为非人类灵长类动物

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Background: Complete exome resequencing has the power to greatly expand our understanding of non-human primate genomes. This includes both a better appreciation of the variation that exists in non-human primate model species, but also an improved annotation of their genomes. By developing an understanding of the variation between individuals, non-human primate models of human disease can be better developed. This effort is hindered largely by the lack of comprehensive information on specific non-human primate genetic variation and the costs of generating these data. If the tools that have been developed in humans for complete exome resequencing can be applied to closely related non-human primate species, then these difficulties can be circumvented. Results: Using a human whole exome enrichment technique, chimpanzee and rhesus macaque samples were captured alongside a human sample and sequenced using standard next-generation methodologies. The results from the three species were then compared for efficacy. The chimpanzee sample showed similar coverage levels and distributions following exome capture based on the human genome as the human sample. The rhesus macaque sample showed significant coverage in protein-coding sequence but significantly less in untranslated regions. Both chimpanzee and rhesus macaque showed significant numbers of frameshift mutations compared to self-genomes and suggest a need for further annotation. Conclusions: Current whole exome resequencing technologies can successfully be used to identify coding-region variation in non-human primates extending into old world monkeys. In addition to identifying variation, whole exome resequencing can aid in better annotation of non-human primate genomes.
机译:背景:完整的外显子组重新测序具有极大地扩展我们对非人类灵长类动物基因组的了解的能力。这不仅包括更好地了解非人类灵长类动物模型物种中存在的变异,还包括其基因组的改进注释。通过了解个体之间的变异,可以更好地开发人类疾病的非人类灵长类动物模型。由于缺乏有关特定非人类灵长类动物遗传变异的全面信息以及生成这些数据的成本,因此很大程度上阻碍了这项工作。如果已经为完全外显子组重测序在人类中开发的工具可以应用于紧密相关的非人类灵长类动物物种,那么就可以避免这些困难。结果:使用人类全外显子体富集技术,与人类样本一起捕获了黑猩猩和恒河猴,并使用标准的下一代方法进行了测序。然后比较这三个物种的结果的功效。在基于人类基因组的外显子组捕获后,黑猩猩样本显示出相似的覆盖水平和分布,与人类样本相似。猕猴样品在蛋白质编码序列中显示出显着的覆盖,但是在未翻译区域中显着较少。与自我基因组相比,黑猩猩和恒河猴都表现出大量的移码突变,这表明需要进一步注释。结论:当前的全外显子组重测序技术可以成功地用于鉴定延伸到旧世界猴子的非人类灵长类动物的编码区变异。除了识别变异之外,整个外显子组重测序还可以帮助更好地注释非人类灵长类动物基因组。

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