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一种分泌型抗激活因子OspD1及其伴侣蛋白Spa15参与了福氏志贺菌中III型分泌系统活性对转录的调控。

A secreted anti-activator, OspD1, and its chaperone, Spa15, are involved in the control of transcription by the type III secretion apparatus activity in Shigella flexneri.

作者信息

Parsot Claude, Ageron Elisabeth, Penno Christophe, Mavris Maria, Jamoussi Kais, d'Hauteville Hélène, Sansonetti Philippe, Demers Brigitte

机构信息

Unité de Pathogénie Microbienne Moléculaire, INSERM U389, Institut Pasteur, 25 rue du Dr Roux, 75724 Paris Cedex 15, France.

出版信息

Mol Microbiol. 2005 Jun;56(6):1627-35. doi: 10.1111/j.1365-2958.2005.04645.x.

Abstract

Bacteria of Shigella spp. are responsible for shigellosis in humans and use a type III secretion (TTS) system to enter epithelial cells and trigger apoptosis in macrophages. Transit of translocator and effector proteins through the TTS apparatus is activated upon contact of bacteria with host cells. Transcription of approximately 15 genes encoding effectors is regulated by the TTS apparatus activity and controlled by MxiE, an AraC family activator, and its coactivator IpgC, the chaperone of IpaB and IpaC translocators. Using a genetic screen, we identified ospD1 as a gene whose product negatively controls expression of genes regulated by secretion activity. OspD1 associates with the chaperone Spa15 and the activator MxiE and acts as an anti-activator until it is secreted. The mechanism regulating transcription in response to secretion activity involves an activator (MxiE), an anti-activator (OspD1), a co-anti-activator (Spa15), a coactivator (IpgC) and two anti-coactivators (IpaB and IpaC) whose alternative and mutually exclusive interactions are controlled by the duration of the TTS apparatus activity.

摘要

志贺氏菌属细菌可导致人类患志贺氏菌病,并利用III型分泌(TTS)系统进入上皮细胞并引发巨噬细胞凋亡。当细菌与宿主细胞接触时,转运蛋白和效应蛋白通过TTS装置的转运被激活。大约15个编码效应蛋白的基因的转录受TTS装置活性调节,并由AraC家族激活剂MxiE及其共激活剂IpgC(IpaB和IpaC转运蛋白的伴侣蛋白)控制。通过遗传筛选,我们鉴定出ospD1是一个基因,其产物负向控制受分泌活性调节的基因的表达。OspD1与伴侣蛋白Spa15和激活剂MxiE结合,并作为一种抗激活剂,直到它被分泌。响应分泌活性调节转录的机制涉及一种激活剂(MxiE)、一种抗激活剂(OspD1)、一种共抗激活剂(Spa15)、一种共激活剂(IpgC)和两种抗共激活剂(IpaB和IpaC),它们的交替和互斥相互作用受TTS装置活性持续时间的控制。

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