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全局调节因子CodY中的突变赋予对种间氧化还原活性抗菌剂的耐受性。

Mutations in the Global Regulator CodY Confer Tolerance to an Interspecies Redox-Active Antimicrobial.

作者信息

Martini Anthony M, Alexander Sara A, Khare Anupama

机构信息

Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.

出版信息

bioRxiv. 2024 Jul 3:2024.07.02.601769. doi: 10.1101/2024.07.02.601769.

Abstract

Bacteria often exist in multispecies communities where interactions among different species can modify individual fitness and behavior. Although many competitive interactions have been characterized, molecular adaptations that can counter this antagonism and preserve or increase fitness remain underexplored. Here, we characterize the adaptation of to pyocyanin, a redox-active interspecies antimicrobial produced by , a co-infecting pathogen frequently isolated from wound and chronic lung infections with . Using experimental evolution, we identified mutations in a conserved global transcriptional regulator, CodY, that confer tolerance to pyocyanin and thereby enhance survival of . The transcriptional response of a pyocyanin tolerant CodY mutant to pyocyanin indicated a two-pronged defensive response compared to the wild type. Firstly, the CodY mutant strongly suppressed metabolism, by downregulating pathways associated with core metabolism, especially translation-associated genes, upon exposure to pyocyanin. Metabolic suppression via ATP depletion was sufficient to provide comparable protection against pyocyanin to the wild-type strain. Secondly, while both the wild-type and CodY mutant strains upregulated oxidative stress response pathways, the CodY mutant overexpressed multiple stress response genes compared to the wild type. We determined that catalase overexpression was critical to pyocyanin tolerance as its absence eliminated tolerance in the CodY mutant and overexpression of catalase was sufficient to impart tolerance to the wild-type strain. Together, these results suggest that both transcriptional responses likely contribute to pyocyanin tolerance in the CodY mutant. Our data thus provide new mechanistic insight into adaptation toward interbacterial antagonism via altered regulation that facilitates multifaceted protective cellular responses.

摘要

细菌通常存在于多物种群落中,不同物种之间的相互作用会改变个体的适应性和行为。尽管已经描述了许多竞争性相互作用,但能够对抗这种拮抗作用并维持或提高适应性的分子适应机制仍未得到充分探索。在这里,我们描述了[细菌名称]对绿脓菌素的适应性,绿脓菌素是由[另一种细菌名称]产生的一种具有氧化还原活性的种间抗菌物质,[另一种细菌名称]是一种经常从伤口和慢性肺部感染中分离出来的共感染病原体,与[细菌名称]共同感染。通过实验进化,我们在一个保守的全局转录调节因子CodY中鉴定出突变,这些突变赋予了对绿脓菌素的耐受性,从而提高了[细菌名称]的存活率。与野生型相比,耐绿脓菌素的CodY突变体对绿脓菌素的转录反应表明其具有双管齐下的防御反应。首先,CodY突变体通过在暴露于绿脓菌素时下调与核心代谢相关的途径,特别是与翻译相关的基因,强烈抑制了新陈代谢。通过ATP消耗进行的代谢抑制足以提供与野生型菌株相当的抗绿脓菌素保护作用。其次,虽然野生型和CodY突变体菌株都上调了氧化应激反应途径,但与野生型相比,CodY突变体过表达了多个应激反应基因。我们确定过氧化氢酶的过表达对绿脓菌素耐受性至关重要,因为它的缺失消除了CodY突变体中的耐受性,而过氧化氢酶的过表达足以赋予野生型菌株耐受性。总之,这些结果表明这两种转录反应可能都有助于CodY突变体对绿脓菌素的耐受性。因此,我们的数据通过改变调节促进多方面的保护性细胞反应,为细菌间拮抗作用的适应提供了新的机制见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/28e7/11261909/45afe26c54d2/nihpp-2024.07.02.601769v1-f0003.jpg

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