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UpaH 是一种新鉴定的自转运蛋白,有助于尿路致病性大肠杆菌 CFT073 形成生物膜和膀胱定植。

UpaH is a newly identified autotransporter protein that contributes to biofilm formation and bladder colonization by uropathogenic Escherichia coli CFT073.

机构信息

School of Chemistry and Molecular Biosciences, Building 76, University of Queensland, Brisbane QLD 4072, Australia.

出版信息

Infect Immun. 2010 Apr;78(4):1659-69. doi: 10.1128/IAI.01010-09. Epub 2010 Feb 9.

Abstract

Escherichia coli is the primary cause of urinary tract infection (UTI) in the developed world. The major factors associated with virulence of uropathogenic E. coli (UPEC) are fimbrial adhesins, which mediate specific attachment to host receptors and trigger innate host responses. Another group of adhesins is represented by the autotransporter (AT) subgroup of proteins. In this study, we identified a new AT-encoding gene, termed upaH, present in a 6.5-kb unannotated intergenic region in the genome of the prototypic UPEC strain CFT073. Cloning and sequencing of the upaH gene from CFT073 revealed an intact 8.535-kb coding region, contrary to the published genome sequence. The upaH gene was widely distributed among a large collection of UPEC isolates as well as the E. coli Reference (ECOR) strain collection. Bioinformatic analyses suggest beta-helix as the predominant structure in the large N-terminal passenger (alpha) domain and a 12-strand beta-barrel for the C-terminal beta-domain of UpaH. We demonstrated that UpaH is expressed at the cell surface of CFT073 and promotes biofilm formation. In the mouse UTI model, deletion of the upaH gene in CFT073 and in two other UPEC strains did not significantly affect colonization of the bladder in single-challenge experiments. However, in competitive colonization experiments, CFT073 significantly outcompeted its upaH isogenic mutant strain in urine and the bladder.

摘要

大肠埃希菌是发达国家泌尿道感染(UTI)的主要病原体。与尿路致病性大肠埃希菌(UPEC)的毒力相关的主要因素是菌毛黏附素,它介导对宿主受体的特异性附着,并引发先天宿主反应。另一组黏附素由自主转运蛋白(AT)亚组蛋白代表。在这项研究中,我们在原型 UPEC 菌株 CFT073 的基因组中未注释的 6.5kb 基因间区发现了一个新的 AT 编码基因,命名为 upaH。从 CFT073 中克隆和测序 upaH 基因显示出完整的 8.535kb 编码区,与已发表的基因组序列相反。upaH 基因在大量 UPEC 分离株以及大肠杆菌参考(ECOR)菌株集中广泛分布。生物信息学分析表明,β-螺旋是大的 N 端乘客(α)结构域的主要结构,而 UpaH 的 C 端β-结构域则为 12 链β-桶。我们证明 UpaH 在 CFT073 的细胞表面表达并促进生物膜形成。在小鼠 UTI 模型中,CFT073 和另外两种 UPEC 菌株中 upaH 基因的缺失在单次挑战实验中对膀胱定植没有显著影响。然而,在竞争性定植实验中,CFT073 在尿液和膀胱中明显比其 upaH 同源突变株更具竞争力。

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