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表达失调作为抗生素耐药性中适应代价的中介。

Expression Dysregulation as a Mediator of Fitness Costs in Antibiotic Resistance.

机构信息

Swiss Tropical and Public Health Institutegrid.416786.a, Basel, Switzerland.

University of Basel, Basel, Switzerland.

出版信息

Antimicrob Agents Chemother. 2021 Aug 17;65(9):e0050421. doi: 10.1128/AAC.00504-21.

Abstract

Antimicrobial resistance (AMR) poses a threat to global health and the economy. Rifampicin-resistant Mycobacterium tuberculosis accounts for a third of the global AMR burden. Gaining the upper hand on AMR requires a deeper understanding of the physiology of resistance. AMR often results in a fitness cost in the absence of drug. Identifying the molecular mechanisms underpinning this cost could help strengthen future treatment regimens. Here, we used a collection of M. tuberculosis strains that provide an evolutionary and phylogenetic snapshot of rifampicin resistance and subjected them to genome-wide transcriptomic and proteomic profiling to identify key perturbations of normal physiology. We found that the clinically most common rifampicin resistance-conferring mutation, RpoB Ser450Leu, imparts considerable gene expression changes, many of which are mitigated by the compensatory mutation in RpoC Leu516Pro. However, our data also provide evidence for pervasive epistasis-the same resistance mutation imposed a different fitness cost and functionally distinct changes to gene expression in genetically unrelated clinical strains. Finally, we report a likely posttranscriptional modulation of gene expression that is shared in most of the tested strains carrying RpoB Ser450Leu, resulting in an increased abundance of proteins involved in central carbon metabolism. These changes contribute to a more general trend in which the disruption of the composition of the proteome correlates with the fitness cost of the RpoB Ser450Leu mutation in different strains.

摘要

抗微生物药物耐药性(AMR)对全球健康和经济构成威胁。耐 rifampicin 的结核分枝杆菌占全球 AMR 负担的三分之一。要想在 AMR 方面取得优势,就需要更深入地了解耐药性的生理学。在没有药物的情况下,AMR 通常会导致适应性成本。确定支撑这种成本的分子机制可能有助于加强未来的治疗方案。在这里,我们使用了一组结核分枝杆菌菌株,这些菌株提供了 rifampicin 耐药性的进化和系统发育快照,并对其进行了全基因组转录组和蛋白质组谱分析,以确定正常生理学的关键扰动。我们发现,临床上最常见的 rifampicin 耐药性赋予突变 RpoB Ser450Leu 导致相当大的基因表达变化,其中许多变化被 RpoC Leu516Pro 的补偿性突变所减轻。然而,我们的数据也提供了广泛的上位性证据-相同的耐药性突变对遗传上无关的临床菌株中的基因表达施加了不同的适应性成本和功能上不同的变化。最后,我们报告了一种可能的转录后基因表达调控,这种调控在携带 RpoB Ser450Leu 的大多数测试菌株中都存在,导致参与中心碳代谢的蛋白质丰度增加。这些变化导致了一种更普遍的趋势,即蛋白质组组成的破坏与不同菌株中 RpoB Ser450Leu 突变的适应性成本相关。

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