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Genomic analysis identifies targets of convergent positive selection in drug-resistant Mycobacterium tuberculosis

机译:基因组分析确定耐药结核分枝杆菌会聚阳性选择的靶标

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摘要

M. tuberculosis is evolving antibiotic resistance, threatening attempts at tuberculosis epidemic control. Mechanisms of resistance, including genetic changes favored by selection in resistant isolates, are incompletely understood. Using 116 newly sequenced and 7 previously sequenced M. tuberculosis whole genomes, we identified genome-wide signatures of positive selection specific to the 47 drug-resistant strains. By searching for convergent evolution - the independent fixation of mutations in the same nucleotide position or gene - we recovered 100% of a set of known resistance markers. We also found evidence of positive selection in an additional 39 genomic regions in resistant isolates. These regions encode components in cell wall biosynthesis, transcriptional regulation and DNA repair pathways. Mutations in these regions could directly confer resistance or compensate for fitness costs associated with resistance. Functional genetic analysis of mutations in one gene, ponA1, demonstrated an in vitro growth advantage in the presence of the drug rifampicin.
机译:结核分枝杆菌正在发展对抗生素的耐药性,威胁着结核病流行控制的尝试。尚不完全了解抗药性的机制,包括通过选择抗药性菌株而促进的遗传变化。使用116个新测序的结核分枝杆菌全基因组和7个先前测序的结核分枝杆菌全基因组,我们鉴定了47种耐药菌株特有的阳性选择的全基因组范围的特征。通过寻找趋同进化-在相同核苷酸位置或基因中突变的独立固定-我们回收了100%的已知抗性标记。我们还在抗性分离株的另外39个基因组区域中发现了阳性选择的证据。这些区域编码细胞壁生物合成,转录调控和DNA修复途径中的成分。这些区域的突变可直接赋予抵抗力或补偿与抵抗力有关的适应性成本。对一个基因ponA1中的突变进行功能遗传分析表明,在存在利福平药物的情况下具有体外生长优势。

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