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尿路致病性大肠杆菌中空泡自转运毒素的分子特征

Molecular Characterization of the Vacuolating Autotransporter Toxin in Uropathogenic Escherichia coli.

作者信息

Nichols Katie B, Totsika Makrina, Moriel Danilo G, Lo Alvin W, Yang Ji, Wurpel Daniël J, Rossiter Amanda E, Strugnell Richard A, Henderson Ian R, Ulett Glen C, Beatson Scott A, Schembri Mark A

机构信息

Australian Infectious Disease Research Centre, School of Chemistry and Molecular Biosciences, University of Queensland, Brisbane, Queensland, Australia.

Institute of Health and Biomedical Innovation, School of Biomedical Sciences, Queensland University of Technology, Brisbane, Queensland, Australia.

出版信息

J Bacteriol. 2016 Apr 28;198(10):1487-98. doi: 10.1128/JB.00791-15. Print 2016 May 15.

Abstract

UNLABELLED

The vacuolating autotransporter toxin (Vat) contributes to uropathogenic Escherichia coli (UPEC) fitness during systemic infection. Here, we characterized Vat and investigated its regulation in UPEC. We assessed the prevalence of vat in a collection of 45 UPEC urosepsis strains and showed that it was present in 31 (68%) of the isolates. The isolates containing the vat gene corresponded to three major E. coli sequence types (ST12, ST73, and ST95), and these strains secreted the Vat protein. Further analysis of the vat genomic locus identified a conserved gene located directly downstream of vat that encodes a putative MarR-like transcriptional regulator; we termed this gene vatX The vat-vatX genes were present in the UPEC reference strain CFT073, and reverse transcriptase PCR (RT-PCR) revealed that the two genes are cotranscribed. Overexpression of vatX in CFT073 led to a 3-fold increase in vat gene transcription. The vat promoter region contained three putative nucleation sites for the global transcriptional regulator histone-like nucleoid structuring protein (H-NS); thus, the hns gene was mutated in CFT073 (to generate CFT073 hns). Western blot analysis using a Vat-specific antibody revealed a significant increase in Vat expression in CFT073 hns compared to that in wild-type CFT073. Direct H-NS binding to the vat promoter region was demonstrated using purified H-NS in combination with electrophoresis mobility shift assays. Finally, Vat-specific antibodies were detected in plasma samples from urosepsis patients infected by vat-containing UPEC strains, demonstrating that Vat is expressed during infection. Overall, this study has demonstrated that Vat is a highly prevalent and tightly regulated immunogenic serine protease autotransporter protein of Enterobacteriaceae (SPATE) secreted by UPEC during infection.

IMPORTANCE

Uropathogenic Escherichia coli (UPEC) is the major cause of hospital- and community-acquired urinary tract infections. The vacuolating autotransporter toxin (Vat) is a cytotoxin known to contribute to UPEC fitness during murine sepsis infection. In this study, Vat was found to be highly conserved and prevalent among a collection of urosepsis clinical isolates and was expressed at human core body temperature. Regulation of vat was demonstrated to be directly repressed by the global transcriptional regulator H-NS and upregulated by the downstream gene vatX (encoding a new MarR-type transcriptional regulator). Additionally, increased Vat-specific IgG titers were detected in plasma from corresponding urosepsis patients infected with vat-positive isolates. Hence, Vat is a highly conserved and tightly regulated urosepsis-associated virulence factor.

摘要

未标记

空泡自转运毒素(Vat)在全身感染期间有助于尿路致病性大肠杆菌(UPEC)的适应性。在此,我们对Vat进行了表征并研究了其在UPEC中的调控。我们评估了45株UPEC脓毒症菌株中vat的流行情况,结果显示31株(68%)分离株中存在该基因。含有vat基因的分离株对应于三种主要的大肠杆菌序列类型(ST12、ST73和ST95),并且这些菌株分泌Vat蛋白。对vat基因组位点的进一步分析确定了一个位于vat直接下游的保守基因,该基因编码一种假定的MarR样转录调节因子;我们将此基因命名为vatX。vat-vatX基因存在于UPEC参考菌株CFT073中,逆转录聚合酶链反应(RT-PCR)显示这两个基因是共转录的。在CFT073中过表达vatX导致vat基因转录增加3倍。vat启动子区域包含全局转录调节因子组蛋白样核仁结构蛋白(H-NS)的三个假定成核位点;因此,在CFT073中对hns基因进行了突变(以产生CFT073 hns)。使用Vat特异性抗体的蛋白质印迹分析显示,与野生型CFT073相比,CFT073 hns中Vat表达显著增加。使用纯化的H-NS结合电泳迁移率变动分析证明了H-NS与vat启动子区域的直接结合。最后,在感染含vat的UPEC菌株的脓毒症患者的血浆样本中检测到Vat特异性抗体,表明Vat在感染期间表达。总体而言,本研究表明Vat是一种在感染期间由UPEC分泌的高度保守且受到严格调控的肠杆菌科免疫原性丝氨酸蛋白酶自转运蛋白(SPATE)。

重要性

尿路致病性大肠杆菌(UPEC)是医院获得性和社区获得性尿路感染的主要原因。空泡自转运毒素(Vat)是一种细胞毒素,已知在小鼠脓毒症感染期间有助于UPEC的适应性。在本研究中,发现Vat在一组脓毒症临床分离株中高度保守且普遍存在,并且在人体核心体温下表达。已证明vat的调控直接受到全局转录调节因子H-NS的抑制,并由下游基因vatX(编码一种新的MarR型转录调节因子)上调。此外,在感染vat阳性分离株的相应脓毒症患者的血浆中检测到Vat特异性IgG滴度增加。因此,Vat是一种高度保守且受到严格调控的与脓毒症相关的毒力因子。

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