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细菌AfaD侵袭素对细胞β1链整合素的识别与表达afa的致病性大肠杆菌菌株的内化有关。

Recognition of the cellular beta1-chain integrin by the bacterial AfaD invasin is implicated in the internalization of afa-expressing pathogenic Escherichia coli strains.

作者信息

Plançon Laure, Du Merle Laurence, Le Friec Sandrine, Gounon Pierre, Jouve Mabel, Guignot Julie, Servin Alain, Le Bouguénec Chantal

机构信息

Unité de Pathogénie Bactérienne des Muqueuses, Institut Pasteur 28 rue du Dr Roux, F-75724 Paris, France.

出版信息

Cell Microbiol. 2003 Oct;5(10):681-93. doi: 10.1046/j.1462-5822.2003.00308.x.

DOI:10.1046/j.1462-5822.2003.00308.x
PMID:12969374
Abstract

The afa operons from Escherichia coli associated with extra-intestinal and intestinal infections have been characterized and the AfaD protein has been shown to be involved in the low internalization of laboratory strains expressing the afa-3 operon. The aim of this study was to determine the role of the AfaD invasin during the interaction of pathogenic E. coli with epithelial cells. We show that AfaD is implicated in the entry of a clinical isolate into both HeLa and undifferentiated Caco-2 cells. Once in the cytoplasm of these cells, the bacteria formed inclusions in which they were able to survive for at least 72 h. Internalization assays using polystyrene beads coated with His6-tagged purified AfaD (rAfaD) demonstrated that this invasin mediates entry into cells derived from various tissues (intestine and urothelium) that are targets for afa-positive strains. Consistent with the previous observation that an antibody blockade involving anti-alpha5beta1 integrin abolishes bacterial internalization, we show here that the entry of rAfaD-coated beads was dependent on the production and accessibility of beta1 integrins on the cells. The AfaD proteins belong to a family of invasins that are at least 45% identical. Despite their differences, the recombinant rAfaD-III and rAfaD-VIII proteins both bound to beta1 integrins. Our results suggest that beta1 integrin is a common receptor for AfaD invasins and that additional AfaD-type-specific receptors exist.

摘要

与肠外和肠道感染相关的大肠杆菌afa操纵子已被鉴定,并且已证明AfaD蛋白参与表达afa - 3操纵子的实验室菌株的低内化过程。本研究的目的是确定AfaD侵袭素在致病性大肠杆菌与上皮细胞相互作用中的作用。我们发现AfaD与一株临床分离株进入HeLa细胞和未分化的Caco - 2细胞有关。一旦进入这些细胞的细胞质中,细菌会形成包涵体,并能在其中存活至少72小时。使用包被有His6标签纯化AfaD(rAfaD)的聚苯乙烯珠子进行的内化试验表明,这种侵袭素介导afa阳性菌株的靶组织(肠道和尿道上皮)来源的细胞进入。与先前观察到的涉及抗α5β1整合素的抗体阻断可消除细菌内化一致,我们在此表明包被rAfaD的珠子进入细胞取决于细胞上β1整合素的产生和可及性。AfaD蛋白属于一类侵袭素家族,它们至少有45%的同源性。尽管存在差异,但重组的rAfaD - III和rAfaD - VIII蛋白均与β1整合素结合。我们的结果表明,β1整合素是AfaD侵袭素的共同受体,并且存在其他AfaD类型特异性受体。

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