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Computationally identifying novel essential genes, including non-coding RNAs, in intergenic sequences in bacterial genomes

机译:通过计算鉴定细菌基因组中基因间序列中的新必需基因,包括非编码RNA

摘要

The increasing availability of bacterial genome sequences and genome-wide laboratory analyses has opened the door for high-throughput bioinformatic approaches to accelerate the discovery of antimicrobial drug targets. To expand the list of such possible drug targets, I have developed an approach to identify novel essential genes encoded in unusually large intergenic regions between previously annotated genes. Applying this approach to the analysis of the intrinsically antibiotic resistant pathogen P. aeruginosa PAO1, I computationally predicted at least 5 novel protein-coding genes that were also confirmed to be transcribed by RT-PCR. In addition, at least 5 novel non-coding RNAs were predicted. I used the same computational pipeline to predict such novel putative genes in Mycobacterium tuberculosis H37Rv, reflecting the general applicability of the method. Finally, I analyzed the phylogenetic distribution of the essential genes, providing insight into their evolutionary origins.
机译:细菌基因组序列和全基因组实验室分析的可用性不断提高,为高通量生物信息学方法打开了大门,以加速发现抗菌药物靶标。为了扩大此类可能的药物靶标的范围,我开发了一种方法来鉴定在先前注释的基因之间的异常大的基因间区域编码的新颖必需基因。将这种方法应用于对内在抗生素耐药性病原体铜绿假单胞菌PAO1的分析中,我计算了至少5个新的蛋白质编码基因,这些基因也已被RT-PCR确认转录。另外,预测了至少5个新的非编码RNA。我使用相同的计算流程预测了结核分枝杆菌H37Rv中的此类新推定基因,反映了该方法的普遍适用性。最后,我分析了必需基因的系统发育分布,从而洞悉了它们的进化起源。

著录项

  • 作者

    Ho Chi Kin;

  • 作者单位
  • 年度 2008
  • 总页数
  • 原文格式 PDF
  • 正文语种 English
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