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Back-Translation for Discovering Distant Protein Homologies

机译:反向翻译发现远距离蛋白质同源性

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摘要

Frameshift mutations in protein-coding DNA sequences produce a drastic change in the resulting protein sequence, which prevents classic protein alignment methods from revealing the proteins' common origin. Moreover, when a large number of substitutions are additionally involved in the divergence, the homology detection becomes difficult even at the DNA level. To cope with this situation, we propose a novel method to infer distant homology relations of two proteins, that accounts for frameshift and point mutations that may have affected the coding sequences. We design a dynamic programming alignment algorithm over memory-efficient graph representations of the complete set of putative DNA sequences of each protein, with the goal of determining the two putative DNA sequences which have the best scoring alignment under a powerful scoring system designed to reflect the most probable evolutionary process. This allows us to uncover evolutionary information that is not captured by traditional alignment methods, which is confirmed by biologically significant examples.
机译:蛋白质编码DNA序列中的移码突变会在最终的蛋白质序列中产生巨大变化,从而阻止了经典的蛋白质比对方法揭示蛋白质的共同来源。此外,当分歧中另外涉及大量取代时,即使在DNA水平,同源性检测也变得困难。为了应对这种情况,我们提出了一种新颖的方法来推断两种蛋白质的远距离同源性,该方法考虑了可能影响编码序列的移码和点突变。我们针对每种蛋白质的完整推定DNA序列的完整存储效率的图形表示设计了一种动态编程比对算法,目的是在一个功能强大的计分系统下确定两个具有最佳得分比对的推定DNA序列,这些序列旨在反映最可能的进化过程。这使我们能够发现传统比对方法无法捕获的进化信息,这一点已被生物学上重要的例子所证实。

著录项

  • 来源
    《Algorithms in bioinformatics》|2009年|108-120|共13页
  • 会议地点 Philadelphia PA(US);Philadelphia PA(US)
  • 作者单位

    INRIA Lille - Nord Europe, LIFL/CNRS, Universite Lille 1, 59655 Villeneuve d'Ascq, France;

    INRIA Lille - Nord Europe, LIFL/CNRS, Universite Lille 1, 59655 Villeneuve d'Ascq, France;

    INRIA Lille - Nord Europe, LIFL/CNRS, Universite Lille 1, 59655 Villeneuve d'Ascq, France;

  • 会议组织
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物工程学(生物技术);
  • 关键词

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