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分泌型侵袭蛋白IpaB和IpaC及其胞质伴侣蛋白IpgC是弗氏志贺菌细胞间传播所必需的。

The secreted IpaB and IpaC invasins and their cytoplasmic chaperone IpgC are required for intercellular dissemination of Shigella flexneri.

作者信息

Page A L, Ohayon H, Sansonetti P J, Parsot C

机构信息

Unité de Pathogénie Microbienne Moléculaire, INSERM U389, Paris, France.

出版信息

Cell Microbiol. 1999 Sep;1(2):183-93. doi: 10.1046/j.1462-5822.1999.00019.x.

Abstract

Invasion of epithelial cells by Shigella flexneri involves entry and dissemination. The main effectors of entry, IpaB and IpaC, are also required for contact haemolytic activity and escape from the phagosome in infected macrophages. These proteins are stored in the cytoplasm in association with the chaperone IpgC, before their secretion by a type III secretion apparatus is activated by host cells. We used a His-tagged IpgC protein to purify IpgC-containing complexes and showed that only IpaB and IpaC are associated with IpgC. Plasmids expressing His6-IpgC either alone or together with IpaB or IpaC under the control of an IPTG-inducible lac promoter were introduced into ipgC, ipaB or ipaC mutants. Induction of expression of the recombinant plasmid-encoded proteins by IPTG allowed bacteria to enter epithelial cells, and the role of these proteins in dissemination was investigated by incubating infected cells in either the absence or the presence of IPTG. The size of plaques produced by recombinant strains on cell monolayers was regulated by IPTG, indicating that IpgC, IpaB and IpaC were each required for efficient dissemination. Electron microscopy analysis of infected cells indicated that these proteins were necessary for lysis of the membrane of the protrusions during cell-to-cell spread.

摘要

福氏志贺菌对上皮细胞的侵袭涉及进入和扩散。进入过程的主要效应蛋白IpaB和IpaC,对于感染巨噬细胞中的接触溶血活性和从吞噬体逃逸也是必需的。这些蛋白质在与伴侣蛋白IpgC结合的情况下储存在细胞质中,直到它们被宿主细胞激活III型分泌装置进行分泌。我们使用带有His标签的IpgC蛋白来纯化含有IpgC的复合物,并表明只有IpaB和IpaC与IpgC相关联。将在IPTG诱导的lac启动子控制下单独表达His6-IpgC或与IpaB或IpaC一起表达的质粒导入ipgC、ipaB或ipaC突变体中。通过IPTG诱导重组质粒编码蛋白的表达,使细菌能够进入上皮细胞,并通过在有无IPTG的情况下培养感染细胞来研究这些蛋白在扩散中的作用。重组菌株在细胞单层上产生的噬斑大小受IPTG调节,表明IpgC、IpaB和IpaC各自对于有效扩散都是必需的。对感染细胞的电子显微镜分析表明,这些蛋白质对于细胞间传播过程中突起膜的裂解是必需的。

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