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Comparative analysis of mycobacterium and related actinomycetes yields insight into the evolution of mycobacterium tuberculosis pathogenesis

机译:对分枝杆菌和相关放线菌的比较分析可深入了解结核分枝杆菌发病机理的演变

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Background The sequence of the pathogen Mycobacterium tuberculosis (Mtb) strain H37Rv has been available for over a decade, but the biology of the pathogen remains poorly understood. Genome sequences from other Mtb strains and closely related bacteria present an opportunity to apply the power of comparative genomics to understand the evolution of Mtb pathogenesis. We conducted a comparative analysis using 31 genomes from the Tuberculosis Database (TBDB.org), including 8 strains of Mtb and M. bovis, 11 additional Mycobacteria, 4 Corynebacteria, 2 Streptomyces, Rhodococcus jostii RHA1, Nocardia farcinia, Acidothermus cellulolyticus, Rhodobacter sphaeroides, Propionibacterium acnes, and Bifidobacterium longum. Results Our results highlight the functional importance of lipid metabolism and its regulation, and reveal variation between the evolutionary profiles of genes implicated in saturated and unsaturated fatty acid metabolism. It also suggests that DNA repair and molybdopterin cofactors are important in pathogenic Mycobacteria. By analyzing sequence conservation and gene expression data, we identify nearly 400 conserved noncoding regions. These include 37 predicted promoter regulatory motifs, of which 14 correspond to previously validated motifs, as well as 50 potential noncoding RNAs, of which we experimentally confirm the expression of four. Conclusions Our analysis of protein evolution highlights gene families that are associated with the adaptation of environmental Mycobacteria to obligate pathogenesis. These families include fatty acid metabolism, DNA repair, and molybdopterin biosynthesis. Our analysis reinforces recent findings suggesting that small noncoding RNAs are more common in Mycobacteria than previously expected. Our data provide a foundation for understanding the genome and biology of Mtb in a comparative context, and are available online and through TBDB.org.
机译:背景病原体结核分枝杆菌(Mtb)菌株H37Rv的序列已有十多年的历史了,但对病原体的生物学知之甚少。来自其他Mtb菌株和密切相关细菌的基因组序列为利用比较基因组学的力量了解Mtb发病机理的发展提供了机会。我们使用来自结核病数据库(TBDB.org)的31个基因组进行了比较分析,包括8株Mtb和牛分枝杆菌,11个其他分枝杆菌,4个棒杆菌,2个链霉菌,何氏红球菌RHA1,诺卡氏菌,粉红色嗜酸菌,解酸嗜热菌,球形红细菌,痤疮丙酸杆菌和长双歧杆菌。结果我们的结果突出了脂质代谢及其调控的功能重要性,并揭示了涉及饱和和不饱和脂肪酸代谢的基因的进化谱之间的差异。这也表明DNA修复和钼蝶呤辅助因子在致病性分枝杆菌中很重要。通过分析序列保守和基因表达数据,我们确定了近400个保守的非编码区。这些包括37个预测的启动子调控基序,其中14个对应于先前验证的基序,以及50个潜在的非编码RNA,我们通过实验确定了其中的4个表达。结论我们对蛋白质进化的分析突出了与环境分枝杆菌适应专性发病有关的基因家族。这些家族包括脂肪酸代谢,DNA修复和钼蝶呤的生物合成。我们的分析进一步证实了最近的发现,表明分枝杆菌中较小的非编码RNA比以前预期的更为普遍。我们的数据为在比较背景下了解Mtb的基因组和生物学提供了基础,可以在线或通过TBDB.org获得。

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