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Targeted enrichment beyond the consensus coding DNA sequence exome reveals exons with higher variant densities

机译:超出共识编码DNA序列外显子组的靶向富集揭示了具有更高变异密度的外显子

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摘要

BackgroundEnrichment of loci by DNA hybridization-capture, followed by high-throughput sequencing, is an important tool in modern genetics. Currently, the most common targets for enrichment are the protein coding exons represented by the consensus coding DNA sequence (CCDS). The CCDS, however, excludes many actual or computationally predicted coding exons present in other databases, such as RefSeq and Vega, and non-coding functional elements such as untranslated and regulatory regions. The number of variants per base pair (variant density) and our ability to interrogate regions outside of the CCDS regions is consequently less well understood.
机译:背景技术通过DNA杂交捕获富集基因座,然后进行高通量测序,是现代遗传学中的重要工具。当前,最常见的富集靶标是由共有编码DNA序列(CCDS)代表的蛋白质编码外显子。但是,CCDS排除了其他数据库(例如RefSeq和Vega)中存在的许多实际或计算预测的编码外显子,以及诸如非翻译和调控区之类的非编码功能元件。因此,对每个碱基对的变体数量(变异密度)以及我们询问CCDS区域以外区域的能力的了解较少。

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