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李斯特菌 monocytogenes timABR 抗性操纵子感知和解毒 Tartrolon。

Tartrolon sensing and detoxification by the Listeria monocytogenes timABR resistance operon.

机构信息

FG11 Division of Enteropathogenic Bacteria and Legionella, Robert Koch Institute, Wernigerode, Germany.

Department of Microbial Natural Products, Helmholtz Centre for Infection Research, Saarland University, Saarbrücken, Germany.

出版信息

Mol Microbiol. 2023 Nov;120(5):629-644. doi: 10.1111/mmi.15178. Epub 2023 Oct 7.

Abstract

Listeria monocytogenes is a foodborne bacterium that naturally occurs in the soil. Originating from there, it contaminates crops and infects farm animals and their consumption by humans may lead to listeriosis, a systemic life-threatening infectious disease. The adaptation of L. monocytogenes to such contrastive habitats is reflected by the presence of virulence genes for host infection and other genes for survival under environmental conditions. Among the latter are ABC transporters for excretion of antibiotics produced by environmental competitors; however, most of these transporters have not been characterized. Here, we generated a collection of promoter-lacZ fusions for genes encoding ABC-type drug transporters of L. monocytogenes and screened this reporter strain collection for induction using a library of natural compounds produced by various environmental microorganisms. We found that the timABR locus (lmo1964-lmo1962) was induced by the macrodiolide antibiotic tartrolon B, which is synthesized by the soil myxobacterium Sorangium cellulosum. Tartrolon B resistance of L. monocytogenes was dependent on timAB, encoding the ATPase and the permease component of a novel ABC transporter. Moreover, transplantation of timAB was sufficient to confer tartrolon B resistance to Bacillus subtilis. Expression of the timABR locus was found to be auto-repressed by the TimR repressor, whose repressing activity was lost in the presence of tartrolon B. We also demonstrate that tartrolon sensitivity was suppressed by high external potassium concentrations, suggesting that tartrolon acts as potassium ionophore. Our results help to map the ecological interactions of an important human pathogen with its co-residing species within their joint natural reservoir.

摘要

李斯特菌是一种食源性病原体,天然存在于土壤中。它从土壤中污染农作物,并感染农场动物,人类食用这些动物可能会导致李斯特菌病,这是一种全身性的、危及生命的传染病。李斯特菌适应这种对比鲜明的栖息地的方式,反映在其宿主感染的毒力基因和在环境条件下生存的其他基因上。后者包括 ABC 转运体,用于排出环境竞争者产生的抗生素;然而,这些转运体中的大多数尚未被描述。在这里,我们生成了李斯特菌 ABC 型药物转运体基因的启动子 -lacZ 融合物集合,并使用各种环境微生物产生的天然化合物文库筛选了该报告菌株集合,以寻找诱导物。我们发现 timABR 基因座(lmo1964-lmo1962)被土曲霉属放线菌产生的大环内酯类抗生素塔鲁隆 B 诱导,塔鲁隆 B 是由土壤粘细菌放线菌属细胞体合成的。李斯特菌对塔鲁隆 B 的抗性依赖于 timAB,它编码一种新型 ABC 转运体的 ATP 酶和渗透酶成分。此外,移植 timAB 足以赋予枯草芽孢杆菌对塔鲁隆 B 的抗性。发现 timABR 基因座的表达受到 TimR 抑制剂的自动抑制,而在塔鲁隆 B 的存在下,TimR 抑制剂的抑制活性丧失。我们还证明,塔鲁隆敏感性被高钾浓度抑制,这表明塔鲁隆是钾离子载体。我们的结果有助于描绘一种重要的人类病原体与其共同居住的物种在其共同的自然库中相互作用的生态关系。

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