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大肠杆菌通过外膜囊泡释放I型分泌性α-溶血素。

Release of the type I secreted alpha-haemolysin via outer membrane vesicles from Escherichia coli.

作者信息

Balsalobre Carlos, Silván Jose Manuel, Berglund Stina, Mizunoe Yoshimitsu, Uhlin Bernt Eric, Wai Sun Nyunt

机构信息

Department of Molecular Biology, Umeå University, S-90187 Umeå, Sweden.

出版信息

Mol Microbiol. 2006 Jan;59(1):99-112. doi: 10.1111/j.1365-2958.2005.04938.x.

Abstract

The alpha-haemolysin is an important virulence factor commonly expressed by extraintestinal pathogenic Escherichia coli. The secretion of the alpha-haemolysin is mediated by the type I secretion system and the toxin reaches the extracellular space without the formation of periplasmic intermediates presumably in a soluble form. Surprisingly, we found that a fraction of this type I secreted protein is located within outer membrane vesicles (OMVs) that are released by the bacteria. The alpha-haemolysin appeared very tightly associated with the OMVs as judged by dissociation assays and proteinase susceptibility tests. The alpha-haemolysin in OMVs was cytotoxically active and caused lysis of red blood cells. The OMVs containing the alpha-haemolysin were distinct from the OMVs not containing alpha-haemolysin, showing a lower density. Furthermore, they differed in protein composition and one component of the type I secretion system, the TolC protein, was found in the lower density vesicles. Studies of natural isolates of E. coli demonstrated that the localization of alpha-haemolysin in OMVs is a common feature among haemolytic strains. We propose an alternative pathway for the transport of the type I secreted alpha-haemolysin from the bacteria to the host cells during bacterial infections.

摘要

α-溶血素是肠道外致病性大肠杆菌普遍表达的一种重要毒力因子。α-溶血素的分泌由I型分泌系统介导,毒素无需形成周质中间体可能以可溶性形式到达细胞外空间。令人惊讶的是,我们发现这种I型分泌蛋白的一部分位于细菌释放的外膜囊泡(OMV)内。通过解离试验和蛋白酶敏感性试验判断,α-溶血素似乎与OMV紧密结合。OMV中的α-溶血素具有细胞毒性活性,可导致红细胞裂解。含有α-溶血素的OMV与不含α-溶血素的OMV不同,密度较低。此外,它们的蛋白质组成也不同,并且在低密度囊泡中发现了I型分泌系统的一个组分,即TolC蛋白。对大肠杆菌自然分离株的研究表明,α-溶血素在OMV中的定位是溶血菌株的一个共同特征。我们提出了一种在细菌感染期间将I型分泌的α-溶血素从细菌转运到宿主细胞的替代途径。

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