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  • 1
    Publication Date: 2015-05-12
    Description: Motivation: Sequence-variation analysis is conventionally performed on mapping results that are highly redundant and occasionally contain undesirable heuristic biases. A straightforward approach to single-nucleotide polymorphism (SNP) analysis, using the Burrows–Wheeler transform (BWT) of short-read data, is proposed. Results: The BWT makes it possible to simultaneously process collections of read fragments of the same sequences; accordingly, SNPs were found from the BWT much faster than from the mapping results. It took only a few minutes to find SNPs from the BWT (with a supplementary data, fragment depth of coverage [FDC]) using a desktop workstation in the case of human exome or transcriptome sequencing data and 20 min using a dual-CPU server in the case of human genome sequencing data. The SNPs found with the proposed method almost agreed with those found by a time-consuming state-of-the-art tool, except for the cases in which the use of fragments of reads led to sensitivity loss or sequencing depth was not sufficient. These exceptions were predictable in advance on the basis of minimum length for uniqueness (MLU) and FDC defined on the reference genome. Moreover, BWT and FDC were computed in less time than it took to get the mapping results, provided that the data were large enough. Availability and implementation: A proof-of-concept binary code for a Linux platform is available on request to the corresponding author. Contact: kouichi.kimura.hh@hitachi.com Supplementary information: Supplementary data are available at Bioinformatics online.
    Print ISSN: 1367-4803
    Electronic ISSN: 1460-2059
    Topics: Biology , Computer Science , Medicine
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