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Using Triplet Periodicity of Nucleotide Sequences for Finding Potential Reading Frame Shifts in Genes

机译:使用核苷酸序列的三重态周期性查找基因中潜在的阅读框位移

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摘要

We introduce a novel approach for the detection of possible mutations leading to a reading frame (RF) shift in a gene. Deletions and insertions of DNA coding regions are considerable events for genes because an RF shift results in modifications of the extensive region of amino acid sequence coded by a gene. The suggested method is based on the phenomenon of triplet periodicity (TP) in coding regions of genes and its relative resistance to substitutions in DNA sequence. We attempted to extend 326 933 regions of continuous TP found in genes from the KEGG databank by considering possible insertions and deletions. We revealed totally 824 genes where such extension was possible and statistically significant. Then we generated amino acid sequences according to active (KEGG's) and hypothetically ancient RFs in order to find confirmation of a shift at a protein level. Consequently, 64 sequences have protein similarities only for ancient RF, 176 only for active RF, 3 for both and 581 have no protein similarity at all. We aimed to have revealed lower bound for the number of genes in which a shift between RF and TP is possible. Further ways to increase the number of revealed RF shifts are discussed.
机译:我们介绍了一种新颖的方法来检测可能导致基因阅读框(RF)移位的突变。 DNA编码区的缺失和插入对于基因而言是相当大的事件,因为RF移位导致基因编码的氨基酸序列的广泛区域的修饰。所建议的方法是基于基因编码区中的三联体周期性(TP)现象及其对DNA序列取代的相对抗性。我们试图通过考虑可能的插入和缺失来扩展从KEGG数据库中的基因中发现的326 933个连续TP区域。我们揭示了总共824个基因,其中这种延伸是可能的,并且具有统计意义。然后,我们根据活性(KEGG's)和假设的古代RF生成了氨基酸序列,以便确定蛋白质水平上的偏移。因此,只有古老的RF有64个序列具有蛋白质相似性,活跃的RF只有176个序列,两者均为3个,而581个完全没有蛋白质相似性。我们旨在揭示在RF和TP之间可能发生转移的基因数量的下限。讨论了增加显示的RF移位数量的其他方法。

著录项

  • 作者

    Frenkel, F.E.; Korotkov, E.V.;

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  • 年度 2009
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  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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