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Design and application of a target capture sequencing of exons and conserved non-coding sequences for the rat

机译:大鼠外显子和保守非编码序列目标捕获序列的设计和应用

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Background Target capture sequencing is an efficient approach to directly identify the causative mutations of genetic disorders. To apply this strategy to laboratory rats exhibiting various phenotypes, we developed a novel target capture probe set, TargetEC (target capture for exons and conserved non-coding sequences), which can identify mutations not only in exonic regions but also in conserved non-coding sequences and thus can detect regulatory mutations. Results TargetEC covers 1,078,129 regions spanning 146.8?Mb of the genome. We applied TargetEC to four inbred rat strains (WTC/Kyo, WTC- swh /Kyo, PVG/Seac, and KFRS4/Kyo) maintained by the National BioResource Project for the Rat in Japan, and successfully identified mutations associated with these phenotypes, including one mutation detected in a conserved non-coding sequence. Conclusions The method developed in this study can be used to efficiently identify regulatory mutations, which cannot be detected using conventional exome sequencing, and will help to deepen our understanding of the relationships between regulatory mutations and associated phenotypes.
机译:背景技术靶标捕获测序是一种直接鉴定遗传疾病致病突变的有效方法。为了将这种策略应用于表现出各种表型的实验大鼠,我们开发了一种新型的靶标捕获探针集,TargetEC(外显子和保守的非编码序列的靶标捕获),不仅可以识别外显子区域的突变,而且还可以识别保守的非编码序列序列,因此可以检测调控突变。结果TargetEC覆盖了基因组146.8?Mb的1,078,129个区域。我们将TargetEC应用于日本国家老鼠的国家生物资源计划(National BioResource Project)所维护的四种近交大鼠品系(WTC / Kyo,WTC-swh / Kyo,PVG / Seac和KFRS4 / Kyo),并成功鉴定了与这些表型相关的突变,包括在保守的非编码序列中检测到一个突变。结论本研究开发的方法可用于有效鉴定常规突变,不能用常规外显子组测序检测到,这将有助于加深我们对调节突变与相关表型之间关系的理解。

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