Affiliation:
1. Australian Infectious Diseases Research Centre, School of Chemistry and Molecular Biosciences, University of Queensland, Brisbane, Australia
2. Département de Microbiologie, Unité de Génétique des Biofilms, Institut Pasteur, Paris, France
Abstract
ABSTRACT
Uropathogenic
Escherichia coli
(UPEC) is responsible for the majority of urinary tract infections (UTI). To cause a UTI, UPEC must adhere to the epithelial cells of the urinary tract and overcome the shear flow forces of urine. This function is mediated primarily by fimbrial adhesins, which mediate specific attachment to host cell receptors. Another group of adhesins that contributes to UPEC-mediated UTI is autotransporter (AT) proteins. AT proteins possess a range of virulence properties, such as adherence, aggregation, invasion, and biofilm formation. One recently characterized AT protein of UPEC is UpaH, a large adhesin-involved-in-diffuse-adherence (AIDA-I)-type AT protein that contributes to biofilm formation and bladder colonization. In this study we characterized a series of naturally occurring variants of UpaH. We demonstrate that extensive sequence variation exists within the passenger-encoding domain of UpaH variants from different UPEC strains. This sequence variation is associated with functional heterogeneity with respect to the ability of UpaH to mediate biofilm formation. In contrast, all of the UpaH variants examined retained a conserved ability to mediate binding to extracellular matrix (ECM) proteins. Bioinformatic analysis of the UpaH passenger domain identified a conserved region (UpaH
CR
) and a hydrophobic region (UpaH
HR
). Deletion of these domains reduced biofilm formation but not the binding to ECM proteins. Despite variation in the
upaH
sequence, the transcription of
upaH
was repressed by a conserved mechanism involving the global regulator H-NS, and mutation of the
hns
gene relieved this repression. Overall, our findings shed new light on the regulation and functions of the UpaH AT protein.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
30 articles.
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