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携带CD38前噬菌体的艰难梭菌的全局转录反应。

Global transcriptional response of Clostridium difficile carrying the CD38 prophage.

作者信息

Sekulovic Ognjen, Fortier Louis-Charles

出版信息

Appl Environ Microbiol. 2015 Feb;81(4):1364-74. doi: 10.1128/AEM.03656-14.

DOI:10.1128/AEM.03656-14
PMID:25501487
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4309704/
Abstract

Clostridium difficile is one of the most dangerous pathogens in hospital settings. Most strains of C. difficile carry one or more prophages, and some of them, like CD38-2 and CD119, can influence the expression of toxin genes. However, little is known about the global host response in the presence of a given prophage. In order to fill this knowledge gap, we used high-throughput RNA sequencing (RNA-seq) to conduct a genome-wide transcriptomic analysis of the epidemic C. difficile strain R20291 carrying the CD38-2 prophage. A total of 39 bacterial genes were differentially expressed in the R20291 lysogen, 26 of them being downregulated. Several of the regulated genes encode transcriptional regulators and phosphotransferase system (PTS) subunits involved in glucose, fructose, and glucitol/sorbitol uptake and metabolism. CD38-2 also upregulated the expression of a group of regulatory genes located in phi-027, a resident prophage common to most ribotype 027 isolates. The most differentially expressed gene was that encoding the conserved phase-variable cell wall protein CwpV, which was upregulated 20-fold in the lysogen. Quantitative PCR and immunofluorescence showed that the increased cwpV expression results from a greater proportion of cells actively transcribing the gene. Indeed, 95% of f lysogenic cells express cwpV, as opposed to only 5% of wild-type cells. Furthermore, the higher proportion of cells expressing cwpV results from a higher frequency of recombination of the genetic switch controlling phase variation, which we confirmed to be dependent on the host-encoded recombinase RecV. In summary, CD38-2 interferes with phase variation of the surface protein CwpV and the expression of metabolic genes.

摘要

艰难梭菌是医院环境中最危险的病原体之一。大多数艰难梭菌菌株携带一个或多个前噬菌体,其中一些,如CD38 - 2和CD119,可影响毒素基因的表达。然而,对于在特定前噬菌体存在下的整体宿主反应知之甚少。为了填补这一知识空白,我们使用高通量RNA测序(RNA-seq)对携带CD38 - 2前噬菌体的流行艰难梭菌菌株R20291进行全基因组转录组分析。在R20291溶原菌中共有39个细菌基因差异表达,其中26个基因表达下调。一些受调控的基因编码参与葡萄糖、果糖以及葡糖醇/山梨醇摄取和代谢的转录调节因子和磷酸转移酶系统(PTS)亚基。CD38 - 2还上调了位于phi - 027中的一组调控基因的表达,phi - 027是大多数核糖体分型027分离株共有的常驻前噬菌体。差异表达最显著的基因是编码保守的相变细胞壁蛋白CwpV的基因,其在溶原菌中的表达上调了20倍。定量PCR和免疫荧光显示,cwpV表达增加是由于更多比例的细胞积极转录该基因。实际上,95%的溶原菌细胞表达cwpV,而野生型细胞中只有5%表达。此外,表达cwpV的细胞比例较高是由于控制相变的遗传开关的重组频率较高,我们证实这依赖于宿主编码的重组酶RecV。总之,CD38 - 2干扰表面蛋白CwpV的相变和代谢基因的表达。

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