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志贺氏菌的IpaC和沙门氏菌的SipC具有相似的生化特性,但功能不同。

IpaC from Shigella and SipC from Salmonella possess similar biochemical properties but are functionally distinct.

作者信息

Osiecki J C, Barker J, Picking W L, Serfis A B, Berring E, Shah S, Harrington A, Picking W D

机构信息

Department of Molecular Biosciences, University of Kansas, Lawrence, KS 66045, USA.

出版信息

Mol Microbiol. 2001 Oct;42(2):469-81. doi: 10.1046/j.1365-2958.2001.02654.x.

Abstract

Invasion plasmid antigen C (IpaC) is secreted via the type III secretion system (TTSS) of Shigella flexneri and serves as an essential effector molecule for epithelial cell invasion. The only homologue of IpaC identified thus far is Salmonella invasion protein C (SipC/SspC), which is essential for enterocyte invasion by Salmonella typhimurium. To explore the biochemical and functional relatedness of IpaC and SipC, recombinant derivatives of both proteins were purified so that their in vitro biochemical properties could be compared. Both proteins were found to: (i) enhance the entry of wild-type S. flexneri and S. typhimurium into cultured cells; (ii) interact with phospholipid membranes; and (iii) oligomerize in solution; however, IpaC appeared to be more efficient in carrying out several of the biochemical properties examined. Overall, the data indicate that purified IpaC and SipC are biochemically similar, although not identical with respect to their in vitro activities. To extend these observations, complementation analyses were conducted using S. flexneri SF621 and S. typhimurium SB220, neither of which is capable of invading epithelial cells because of non-polar null mutations in ipaC and sipC respectively. Interestingly, both ipaC and sipC restored invasiveness to SB220 whereas only ipaC restored invasiveness to SF621, suggesting that SipC lacks an activity possessed by IpaC. This functional difference is not at the level of secretion because IpaC and SipC are both secreted by SF621 and it does not appear to be because of SipC dependency on this native chaperone as coexpression of sipC and sicA in SF621 still failed to restore detectable invasiveness. Taken together, the data suggest that IpaC and SipC differ in either their ability to be translocated into host cells or in their function as effectors of host cell invasion. Because IpaB shares significant sequence homology with the YopB translocator of Yersinia species, the ability for IpaC and SipC to associate with this protein was explored as a potential indicator of translocation function. Both proteins were found to bind to purified IpaB with an apparent dissociation constant in the nanomolar range, suggesting that they may differ with respect to effector function. Interestingly, whereas SB220 expressing sipC behaved like wild-type Salmonella, in that it remained within its membrane-bound vacuole following entry into host cells, SB220 expressing ipaC was found in the cytoplasm of host cells. This observation indicates that IpaC and SipC are responsible for a major difference in the invasion strategies of Shigella and Salmonella, that is, they escape into the host cell cytoplasm. The implications of the role of each protein's biochemistry relative to its in vivo function is discussed.

摘要

侵袭质粒抗原C(IpaC)通过福氏志贺菌的III型分泌系统(TTSS)分泌,是上皮细胞侵袭所必需的效应分子。迄今为止鉴定出的IpaC唯一同源物是鼠伤寒沙门氏菌侵袭蛋白C(SipC/SspC),它对鼠伤寒沙门氏菌侵入肠上皮细胞至关重要。为了探究IpaC和SipC的生化及功能相关性,纯化了这两种蛋白的重组衍生物,以便比较它们的体外生化特性。发现这两种蛋白均:(i)增强野生型福氏志贺菌和鼠伤寒沙门氏菌进入培养细胞的能力;(ii)与磷脂膜相互作用;(iii)在溶液中寡聚化;然而,IpaC在执行所检测的几种生化特性方面似乎更有效。总体而言,数据表明纯化的IpaC和SipC在生化方面相似,尽管它们的体外活性并不相同。为了扩展这些观察结果,使用福氏志贺菌SF621和鼠伤寒沙门氏菌SB220进行了互补分析,这两种菌株分别由于ipaC和sipC中的非极性无效突变而无法侵袭上皮细胞。有趣的是,ipaC和sipC均恢复了SB220的侵袭性,而只有ipaC恢复了SF621的侵袭性,这表明SipC缺乏IpaC所具有的一种活性。这种功能差异不在分泌水平,因为IpaC和SipC均由SF621分泌,而且似乎也不是因为SipC依赖这种天然伴侣蛋白,因为在SF621中共表达sipC和sicA仍未能恢复可检测到的侵袭性。综上所述,数据表明IpaC和SipC在转运到宿主细胞的能力或作为宿主细胞侵袭效应分子的功能方面存在差异。由于IpaB与耶尔森菌属的YopB转运蛋白具有显著的序列同源性,因此探究了IpaC和SipC与该蛋白结合的能力,作为转运功能的潜在指标。发现这两种蛋白均以纳摩尔范围内的表观解离常数与纯化的IpaB结合,这表明它们在效应分子功能方面可能存在差异。有趣的是,表达sipC的SB220表现得像野生型沙门氏菌,即进入宿主细胞后它仍保留在膜结合的液泡内,而表达ipaC的SB220则存在于宿主细胞的细胞质中。这一观察结果表明,IpaC和SipC是志贺菌和沙门氏菌侵袭策略的主要差异所在,即它们逃入宿主细胞细胞质中。讨论了每种蛋白的生物化学作用与其体内功能的关系。

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