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产肠毒素大肠杆菌的EtpA外蛋白促进肠道定植,并且在小鼠感染实验模型中是一种保护性抗原。

The EtpA exoprotein of enterotoxigenic Escherichia coli promotes intestinal colonization and is a protective antigen in an experimental model of murine infection.

作者信息

Roy Koushik, Hamilton David, Allen Kenneth P, Randolph Mildred P, Fleckenstein James M

机构信息

Department of Medicine, University of Tennessee Health Science Center, Memphis, Tennessee 38104, USA.

出版信息

Infect Immun. 2008 May;76(5):2106-12. doi: 10.1128/IAI.01304-07. Epub 2008 Feb 19.

Abstract

The enterotoxigenic Escherichia coli (ETEC) strains are major causes of morbidity and mortality due to diarrheal illness in developing countries. At present, there is no broadly protective vaccine for this diverse group of pathogens. The EtpA protein, identified in ETEC H10407 in a recent search for candidate immunogens, is a large glycosylated exoprotein secreted via two-partner secretion (TPS). Similar to structurally related molecules, EtpA functions in vitro as an adhesin. The studies reported here use a recently developed murine model of ETEC intestinal colonization to examine the immunogenicity and protective efficacy of EtpA. We report that mice repeatedly exposed to ETEC are protected from subsequent colonization and that they mount immune responses to both EtpA and its presumed two-partner secretion transporter (EtpB) during the course of experimental infection. Furthermore, isogenic etpA deletion mutants were impaired in the colonization of mice, and intranasal immunization of mice with recombinant EtpA conferred protection against ETEC H10407 in this model. Together, these data suggest that EtpA is required for optimal colonization of the intestine, findings paralleling those of previous in vitro studies demonstrating its role in adherence. EtpA and other TPS proteins may be viable targets for ETEC vaccine development.

摘要

产肠毒素大肠杆菌(ETEC)菌株是发展中国家因腹泻病导致发病和死亡的主要原因。目前,针对这类多样病原体尚无广泛有效的保护性疫苗。近期在ETEC H10407中寻找候选免疫原时鉴定出的EtpA蛋白,是一种通过双组分分泌(TPS)分泌的大型糖基化外蛋白。与结构相关分子类似,EtpA在体外作为黏附素发挥作用。本文报道的研究使用了最近开发的ETEC肠道定植小鼠模型,以检验EtpA的免疫原性和保护效力。我们报告称,反复接触ETEC的小鼠可免受后续定植,并且在实验感染过程中它们对EtpA及其假定的双组分分泌转运体(EtpB)产生免疫反应。此外,同基因的etpA缺失突变体在小鼠定植方面受损,在该模型中用重组EtpA对小鼠进行鼻内免疫可提供针对ETEC H10407的保护。这些数据共同表明,EtpA是肠道最佳定植所必需的,这一发现与先前体外研究证明其在黏附中的作用一致。EtpA和其他TPS蛋白可能是ETEC疫苗开发的可行靶点。

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