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鼠伤寒沙门氏菌的侵袭相关III型分泌系统将Sip蛋白转运到宿主细胞中。

The invasion-associated type III system of Salmonella typhimurium directs the translocation of Sip proteins into the host cell.

作者信息

Collazo C M, Galán J E

机构信息

Department of Molecular Genetics and Microbiology, School of Medicine, State University of New York at Stony Brook, 11794-5222, USA.

出版信息

Mol Microbiol. 1997 May;24(4):747-56. doi: 10.1046/j.1365-2958.1997.3781740.x.

Abstract

The ability of Salmonella typhimurium to interact with host cells is largely dependent on the function of a type III protein-secretion system encoded at centisome 63 of its chromosome. We have shown here that two targets of this protein-secretion system, SipB and SipC, are translocated into cultured intestinal Henle-407 cells. Translocation required the function of the type III secretion apparatus, as an S. typhimurium strain carrying a mutation in invA, which encodes an essential component of this system, failed to translocate the Sip proteins. Null mutations in the genes encoding SipB, SipC or SipD, prevented protein translocation, indicating that these proteins are involved in the translocation process. In contrast, mutations in sipA and sptP, which also encode secreted proteins, did not interfere with the translocation of SipC, indicating that only a subset of targets of the type III secretion system act as translocases. Externally or internally localized bacteria could direct protein translocation into Henle-407 cells as this process occurred in the presence of cytochalasin D at a concentration that prevented bacterial entry, or in the presence of gentamicin added shortly after bacterial internalization at a concentration that killed extracellular Salmonella. These results indicate that protein translocation into host cells may be a universal function of all type III secretion systems.

摘要

鼠伤寒沙门氏菌与宿主细胞相互作用的能力在很大程度上取决于其染色体63分摩处编码的III型蛋白质分泌系统的功能。我们在此表明,该蛋白质分泌系统的两个靶标SipB和SipC被转运到培养的肠道亨勒-407细胞中。转运需要III型分泌装置的功能,因为携带invA突变的鼠伤寒沙门氏菌菌株未能转运Sip蛋白,invA编码该系统的一个必需组分。编码SipB、SipC或SipD的基因中的无效突变阻止了蛋白质转运,表明这些蛋白质参与了转运过程。相比之下,同样编码分泌蛋白的sipA和sptP中的突变并不干扰SipC的转运,表明III型分泌系统的靶标中只有一部分充当转运酶。外部或内部定位的细菌均可将蛋白质转运到亨勒-407细胞中,因为此过程发生在存在细胞松弛素D(其浓度可阻止细菌进入)的情况下,或在细菌内化后不久添加庆大霉素(其浓度可杀死细胞外沙门氏菌)的情况下。这些结果表明,蛋白质转运到宿主细胞中可能是所有III型分泌系统的普遍功能。

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