利用eBWT检测突变

N. Prezza, N. Pisanti, M. Sciortino, Giovanna Rosone
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引用次数: 11

摘要

在本文中,我们发展了一种理论,描述了DNA片段集合的扩展Burrows-Wheeler变换(eBWT)如何倾向于将基因组g测序的核苷酸拷贝聚集在一起。我们的理论准确地预测了每个这样的簇中预期的任何核苷酸的拷贝数,以及基于LCP阵列的优雅和精确的程序如何在eBWT中定位这些簇。我们的发现非常普遍,可以应用于各种不同的问题。在本文中,我们考虑了在多个reads集合中发现无比对和无参考的snp的情况。我们注意到,根据我们的理论结果,snp聚集在reads集合的eBWT中,并且我们开发了一个工具,通过简单扫描eBWT和LCP阵列来查找snp。初步结果表明,我们的方法比最先进的工具需要的覆盖范围小得多,同时大大提高了精度和灵敏度。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Detecting Mutations by eBWT
In this paper we develop a theory describing how the extended Burrows-Wheeler Transform (eBWT) of a collection of DNA fragments tends to cluster together the copies of nucleotides sequenced from a genome G. Our theory accurately predicts how many copies of any nucleotide are expected inside each such cluster, and how an elegant and precise LCP array based procedure can locate these clusters in the eBWT. Our findings are very general and can be applied to a wide range of different problems. In this paper, we consider the case of alignment-free and reference-free SNPs discovery in multiple collections of reads. We note that, in accordance with our theoretical results, SNPs are clustered in the eBWT of the reads collection, and we develop a tool finding SNPs with a simple scan of the eBWT and LCP arrays. Preliminary results show that our method requires much less coverage than state-of-the-art tools while drastically improving precision and sensitivity.
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