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弗氏志贺菌Ipa侵袭素的分泌由上皮细胞激活,并受IpaB和IpaD调控。

The secretion of the Shigella flexneri Ipa invasins is activated by epithelial cells and controlled by IpaB and IpaD.

作者信息

Ménard R, Sansonetti P, Parsot C

机构信息

Unité de Pathogénie Microbienne Moléculaire, Institut Pasteur, Paris, France.

出版信息

EMBO J. 1994 Nov 15;13(22):5293-302. doi: 10.1002/j.1460-2075.1994.tb06863.x.

Abstract

Shigella species are enteropathogens that invade epithelial cells of the human colon. Entry into epithelial cells is triggered by the IpaB, IpaC and IpaD proteins which are translocated into the medium through the specific Mxi-Spa machinery. In vitro, Shigella cells secrete only a small fraction of the Ipa proteins, the majority of which remains in the cytoplasm. We show here that upon interaction with cultured epithelial cells or in the presence of fetal bovine serum, S.flexneri release pre-synthesized Ipa molecules from the cytoplasm into the environment. Evidence is presented that IpaB and IpaD are essential for both blocking secretion through the Mxi-Spa translocon in the absence of a secretion-inducing signal and controlling secretion of the Ipa proteins in the presence of a signal. Subcellular localization and analysis of the molecular interactions of the Ipa proteins indicate that IpaB and IpaD associate transiently in the bacterial envelope. We propose that IpaB and IpaD, by interacting in the secretion apparatus, modulate secretion.

摘要

志贺氏菌属是侵入人类结肠上皮细胞的肠道病原体。IpaB、IpaC和IpaD蛋白通过特定的Mxi-Spa机制转运到培养基中,从而触发其进入上皮细胞。在体外,志贺氏菌细胞仅分泌一小部分Ipa蛋白,其中大部分仍留在细胞质中。我们在此表明,在与培养的上皮细胞相互作用时或在胎牛血清存在的情况下,福氏志贺氏菌会将预先合成的Ipa分子从细胞质释放到环境中。有证据表明,IpaB和IpaD对于在没有分泌诱导信号的情况下阻断通过Mxi-Spa转运体的分泌以及在有信号存在时控制Ipa蛋白的分泌都是必不可少的。Ipa蛋白的亚细胞定位和分子相互作用分析表明,IpaB和IpaD在细菌包膜中短暂结合。我们提出,IpaB和IpaD通过在分泌装置中相互作用来调节分泌。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6007/395485/e3d76e6624ec/emboj00070-0052-a.jpg

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