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Mutation discovery in mice by whole exome sequencing.

机译:通过全外显子组测序在小鼠中发现突变。

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摘要

We report the development and optimization of reagents for in-solution, hybridization-based capture of the mouse exome. By validating this approach in a multiple inbred strains and in novel mutant strains, we show that whole exome sequencing is a robust approach for discovery of putative mutations, irrespective of strain background. We found strong candidate mutations for the majority of mutant exomes sequenced, including new models of orofacial clefting, urogenital dysmorphology, kyphosis and autoimmune hepatitis.
机译:我们报告了小鼠外显子的溶液中,基于杂交的捕获试剂的开发和优化。通过在多种近交系和新型突变体中验证该方法,我们表明,整个外显子组测序是发现假定突变的可靠方法,而与菌株背景无关。我们发现大多数已测序的突变外显子组都具有很强的候选突变,包括口面部裂痕,泌尿生殖器畸形,驼背和自体免疫性肝炎的新模型。

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