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首页> 外文期刊>BMC Bioinformatics >RISCI - Repeat Induced Sequence Changes Identifier: a comprehensive, comparative genomics-based, in silico subtractive hybridization pipeline to identify repeat induced sequence changes in closely related genomes
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RISCI - Repeat Induced Sequence Changes Identifier: a comprehensive, comparative genomics-based, in silico subtractive hybridization pipeline to identify repeat induced sequence changes in closely related genomes

机译:RISCI-重复诱导序列变化标识符:基于基因组的全面,基于比较的计算机模拟消减杂交流程,可识别密切相关的基因组中的重复诱导序列变化

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Background - The availability of multiple whole genome sequences has facilitated in silico identification of fixed and polymorphic transposable elements (TE). Whereas polymorphic loci serve as makers for phylogenetic and forensic analysis, fixed species-specific transposon insertions, when compared to orthologous loci in other closely related species, may give insights into their evolutionary significance. Besides, TE insertions are not isolated events and are frequently associated with subtle sequence changes concurrent with insertion or post insertion. These include duplication of target site, 3' and 5' flank transduction, deletion of the target locus, 5' truncation or partial deletion and inversion of the transposon, and post insertion changes like inter or intra element recombination, disruption etc. Although such changes have been studied independently, no automated platform to identify differential transposon insertions and the associated array of sequence changes in genomes of the same or closely related species is available till date. To this end, we have designed RISCI - 'Repeat Induced Sequence Changes Identifier' - a comprehensive, comparative genomics-based, in silico subtractive hybridization pipeline to identify differential transposon insertions and associated sequence changes using specific alignment signatures, which may then be examined for their downstream effects. Results - We showcase the utility of RISCI by comparing full length and truncated L1HS and AluYa5 retrotransposons in the reference human genome with the chimpanzee genome and the alternate human assemblies (Celera and HuRef). Comparison of the reference human genome with alternate human assemblies using RISCI predicts 14 novel polymorphisms in full length L1HS, 24 in truncated L1HS and 140 novel polymorphisms in AluYa5 insertions, besides several insertion and post insertion changes. We present comparison with two previous studies to show that RISCI predictions are broadly in agreement with earlier reports. We also demonstrate its versatility by comparing various strains of Mycobacterium tuberculosis for IS 6100 insertion polymorphism. Conclusions - RISCI combines comparative genomics with subtractive hybridization, inferring changes only when exclusive to one of the two genomes being compared. The pipeline is generic and may be applied to most transposons and to any two or more genomes sharing high sequence similarity. Such comparisons, when performed on a larger scale, may pull out a few critical events, which may have seeded the divergence between the two species under comparison.
机译:背景-多个完整基因组序列的可用性促进了计算机方法识别固定和多态转座因子(TE)。尽管多态性位点可作为系统发育和法医分析的工具,但与其他紧密相关物种的直向同源位点相比,固定物种特异的转座子插入可提供其进化意义的见解。此外,TE插入不是孤立的事件,通常与插入或插入后并发的细微序列变化相关。这些包括靶位点的重复,3'和5'侧翼转导,靶基因座的缺失,转座子的5'截短或部分缺失和倒置以及插入后的变化,如元件间或元件内重组,破坏等。迄今为止,已经独立研究了没有自动平台来鉴定差异转座子插入以及相同或紧密相关物种的基因组中序列变化的相关阵列。为此,我们设计了RISCI-“重复诱导的序列变化标识符”-一种全面的,基于基因组的,基于比较的计算机模拟消减杂交流水线,可使用特定的比对标记识别差异的转座子插入和相关的序列变化,然后可以对其进行检查。他们的下游影响。结果-我们通过比较黑猩猩基因组和其他人类组件(Celera和HuRef)在参考人类基因组中的全长和截短的L1HS和AluYa5逆转座子来展示RISCI的实用性。使用RISCI将参考人类基因组与其他人类装配体进行比较,可以预测全长L1HS中有14种新的多态性,截短的L1HS中有24种新的多态性,AluYa5插入中有140种新的多态性,此外还有一些插入和插入后的变化。我们将与之前的两项研究进行比较,以表明RISCI的预测与先前的报告大体一致。我们还通过比较各种结核分枝杆菌IS 6100插入多态性菌株来证明其多功能性。结论-RISCI将比较基因组学与减性杂交相结合,仅在两个比较基因组之一互斥时才推断出变化。流水线是通用的,可以应用于大多数转座子以及共享高序列相似性的任何两个或多个基因组。当进行较大规模的比较时,这样的比较可能会导致一些关键事件的发生,这些关键事件可能会播种正在比较的两个物种之间的差异。

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