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人类持续性沙门氏菌感染与 BarA/SirA 调节途径中的突变有关。

Persistent Salmonella infections in humans are associated with mutations in the BarA/SirA regulatory pathway.

机构信息

Infectious Disease and Microbiome Program, Broad Institute of MIT and Harvard, Cambridge, MA 02142, USA.

Infectious Diseases Research Laboratory, Sheba Medical Center, Tel-Hashomer, Israel; Department of Clinical Microbiology and Immunology, Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel.

出版信息

Cell Host Microbe. 2024 Jan 10;32(1):79-92.e7. doi: 10.1016/j.chom.2023.12.001.

Abstract

Several bacterial pathogens, including Salmonella enterica, can cause persistent infections in humans by mechanisms that are poorly understood. By comparing genomes of isolates longitudinally collected from 256 prolonged salmonellosis patients, we identified repeated mutations in global regulators, including the barA/sirA two-component regulatory system, across multiple patients and Salmonella serovars. Comparative RNA-seq analysis revealed that distinct mutations in barA/sirA led to diminished expression of Salmonella pathogenicity islands 1 and 4 genes, which are required for Salmonella invasion and enteritis. Moreover, barA/sirA mutants were attenuated in an acute salmonellosis mouse model and induced weaker transcription of host immune responses. In contrast, in a persistent infection mouse model, these mutants exhibited long-term colonization and prolonged shedding. Taken together, these findings suggest that selection of mutations in global virulence regulators facilitates persistent Salmonella infection in humans, by attenuating Salmonella virulence and inducing a weaker host inflammatory response.

摘要

几种细菌病原体,包括沙门氏菌,通过机制在人类中引起持续感染,这些机制尚未得到很好的理解。通过比较从 256 例持续性沙门氏菌病患者中纵向收集的分离株的基因组,我们在多个患者和沙门氏菌血清型中发现了全局调节剂(包括 barA/sirA 双组分调节系统)的重复突变。比较 RNA-seq 分析表明,barA/sirA 中的不同突变导致沙门氏菌致病性岛 1 和 4 基因的表达减少,这些基因是沙门氏菌侵袭和肠炎所必需的。此外,barA/sirA 突变体在急性沙门氏菌病小鼠模型中减毒,诱导宿主免疫反应的转录减弱。相比之下,在持续性感染小鼠模型中,这些突变体表现出长期定植和延长的脱落。总之,这些发现表明,选择全局毒力调节剂中的突变有助于人类持续性沙门氏菌感染,通过减弱沙门氏菌的毒力并诱导较弱的宿主炎症反应。

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