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志贺氏菌 IpaD 具有双重作用:从 III 型分泌系统针尖端进行信号转导和细胞内分泌调节。

Shigella IpaD has a dual role: signal transduction from the type III secretion system needle tip and intracellular secretion regulation.

机构信息

School of Cellular & Molecular Medicine, University of Bristol, University Walk, Bristol BS8 1TD, UK.

出版信息

Mol Microbiol. 2013 Feb;87(3):690-706. doi: 10.1111/mmi.12124. Epub 2013 Jan 11.

Abstract

Type III secretion systems (T3SSs) are protein injection devices essential for the interaction of many Gram-negative bacteria with eukaryotic cells. While Shigella assembles its T3SS when the environmental conditions are appropriate for invasion, secretion is only activated after physical contact with a host cell. First, the translocators are secreted to form a pore in the host cell membrane, followed by effectors which manipulate the host cell. Secretion activation is tightly controlled by conserved T3SS components: the needle tip proteins IpaD and IpaB, the needle itself and the intracellular gatekeeper protein MxiC. To further characterize the role of IpaD during activation, we combined random mutagenesis with a genetic screen to identify ipaD mutant strains unable to respond to host cell contact. Class II mutants have an overall defect in secretion induction. They map to IpaD's C-terminal helix and likely affect activation signal generation or transmission. The Class I mutant secretes translocators prematurely and is specifically defective in IpaD secretion upon activation. A phenotypically equivalent mutant was found in mxiC. We show that IpaD and MxiC act in the same intracellular pathway. In summary, we demonstrate that IpaD has a dual role and acts at two distinct locations during secretion activation.

摘要

III 型分泌系统(T3SS)是许多革兰氏阴性细菌与真核细胞相互作用所必需的蛋白质注射装置。志贺氏菌在适合入侵的环境条件下组装其 T3SS,但只有在与宿主细胞物理接触后才会激活分泌。首先,转运器被分泌以在宿主细胞膜上形成孔,然后效应子操纵宿主细胞。分泌的激活受到保守的 T3SS 成分的严格控制:针尖端蛋白 IpaD 和 IpaB、针本身和细胞内守门员蛋白 MxiC。为了进一步表征 IpaD 在激活过程中的作用,我们将随机诱变与遗传筛选相结合,以鉴定无法响应宿主细胞接触的 ipaD 突变株。II 类突变体在分泌诱导方面存在整体缺陷。它们映射到 IpaD 的 C 末端螺旋上,可能会影响激活信号的产生或传递。I 类突变体过早分泌转运器,并且在激活时特异性地缺乏 IpaD 分泌。在 mxiC 中发现了一个表型等效的突变体。我们表明 IpaD 和 MxiC 在相同的细胞内途径中起作用。总之,我们证明了 IpaD 具有双重作用,并在分泌激活过程中在两个不同的位置起作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/17bb/3575693/39be3ee2b58b/mmi0087-0690-f1.jpg

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