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首页> 外文期刊>Journal of bacteriology >Vp1659 Is a Vibrio parahaemolyticus Type III Secretion System 1 Protein That Contributes to Translocation of Effector Proteins Needed To Induce Cytolysis, Autophagy, and Disruption of Actin Structure in HeLa Cells
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Vp1659 Is a Vibrio parahaemolyticus Type III Secretion System 1 Protein That Contributes to Translocation of Effector Proteins Needed To Induce Cytolysis, Autophagy, and Disruption of Actin Structure in HeLa Cells

机译:Vp1659是一种副溶血性弧菌III型分泌系统1蛋白,可促进效应蛋白易位,以诱导HeLa细胞中肌动蛋白结构的细胞分解,自噬和破坏。

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摘要

Vibrio parahaemolyticus harbors two type III secretion systems (T3SSs; T3SS1 and T3SS2), of which T3SS1 is involved in host cell cytotoxicity. T3SS1 expression is positively regulated by ExsA, and it is negatively regulated by ExsD. We compared the secretion profiles of a wild-type strain (NY-4) of V. parahaemolyticus with those of an ExsD deletion mutant (ΔexsD) and with a strain of NY-4 that overexpresses T3SS1 (NY-4:pexsA). From this comparison, we detected a previously uncharacterized protein, Vp1659, which shares some sequence homology with LcrV from Yersinia. We show that vp1659 expression is positively regulated by ExsA and is negatively regulated by ExsD. Vp1659 is specifically secreted by T3SS1 of V. parahaemolyticus, and Vp1659 is not required for the successful extracellular secretion of another T3SS1 protein, Vp1656. Mechanical fractionation showed that Vp1659 is translocated into HeLa cells in a T3SS1-dependent manner and that deletion of Vp1659 does not prevent VopS from being translocated into HeLa cells during infection. Deletion of vp1659 significantly reduces cytotoxicity when HeLa cells are infected by V. parahaemolyticus, while complementation of the Δvp1659 strain restores cytotoxicity. Differential staining showed that Vp1659 is required to induce membrane permeability in HeLa cells. We also show evidence that Vp1659 is required for actin rearrangement and the induction of autophagy. On the basis of these data, we conclude that Vp1659 is a T3SS1-associated protein that is a component of the secretion apparatus and that it is necessary for the efficient translocation of effector proteins into epithelial cells.
机译:副溶血性弧菌具有两个III型分泌系统(T3SS; T3SS1和T3SS2),其中T3SS1参与宿主细胞的细胞毒性作用。 T3SS1表达受到ExsA的正调控,而受到ExsD的负调控。我们比较了 V的野生株(NY-4)的分泌情况。 parahaemolyticus 与一个ExsD缺失突变体(Δ exsD )和一株过表达T3SS1的NY-4菌株(NY-4:p exsA )。通过此比较,我们检测到了以前未鉴定的蛋白Vp1659,该蛋白与耶尔森氏菌的LcrV具有某些序列同源性。我们显示 vp1659 表达受到ExsA的正调控,而受到ExsD的负调控。 Vp1659由 V的T3SS1专门分泌。 parahaemolyticus ,而成功地胞外分泌另一种T3SS1蛋白Vp1656则不需要Vp1659。机械分馏显示,Vp1659以T3SS1依赖的方式转移到HeLa细胞中,而删除Vp1659并不能防止VopS在感染过程中转移到HeLa细胞中。当 V感染HeLa细胞时, vp1659 的删除会大大降低细胞毒性。副溶血性,而Δ vp1659 菌株的互补可恢复细胞毒性。差异染色表明,Vp1659是诱导HeLa细胞膜通透性所必需的。我们还显示了肌动蛋白重排和自噬诱导需要Vp1659的证据。根据这些数据,我们得出结论,Vp1659是T3SS1相关蛋白,是分泌设备的组成部分,对于将效应蛋白有效转运到上皮细胞是必需的。

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