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小分子 GTP 酶与布鲁氏菌进入内质网。

Small GTPases and Brucella entry into the endoplasmic reticulum.

机构信息

URBM, NARILIS, University of Namur (FUNDP), Namur, Belgium.

出版信息

Biochem Soc Trans. 2012 Dec 1;40(6):1348-52. doi: 10.1042/BST20120156.

Abstract

A key determinant for intracellular pathogenic bacteria to ensure their virulence within host cells is their ability to bypass the endocytic pathway and to reach a safe niche of replication. In the case of Brucella, the bacterium targets the ER (endoplasmic reticulum) to create a replicating niche called the BCV (Brucella-containing vacuole). The ER is a suitable strategic place for pathogenic Brucella. Indeed, bacteria can be hidden from host cell defences to persist within the host, and they can take advantage of the membrane reservoir delivered by the ER to replicate. Interaction with the ER leads to the presence on the BCV of the GAPDH (glyceraldehyde-3-phosphate dehydrogenase) and the small GTPase Rab2 known to be located on secretory vesicles that traffic between the ER and the Golgi apparatus. GAPDH and the small GTPase Rab2 controls Brucella replication at late times post-infection. A specific interaction between the human small GTPase Rab2 and a Brucella spp. protein named RicA was identified. Altered kinetics of intracellular trafficking and faster proliferation of the Brucella abortus ΔricA mutant was observed compared with the wild-type strain. RicA is the first reported effector with a proposed function for B. abortus.

摘要

对于细胞内致病性细菌来说,确保其在宿主细胞内的毒力的一个关键决定因素是它们绕过内吞作用途径并到达安全复制位置的能力。对于布鲁氏菌而言,细菌将内质网(ER)作为目标,以创建一个称为 BCV(布鲁氏菌包含的空泡)的复制位置。ER 是致病性布鲁氏菌的合适战略位置。实际上,细菌可以躲避宿主细胞防御,在宿主体内持续存在,并且可以利用 ER 提供的膜储备来进行复制。与 ER 的相互作用导致 GAPDH(甘油醛-3-磷酸脱氢酶)和小 GTPase Rab2 出现在 BCV 上,已知它们位于在 ER 和高尔基体之间运输的分泌小泡上。GAPDH 和小 GTPase Rab2 控制感染后晚期的布鲁氏菌复制。鉴定了人类小 GTPase Rab2 与一种名为 RicA 的布鲁氏菌属蛋白之间的特定相互作用。与野生型菌株相比,观察到布鲁氏菌 abortusΔricA 突变体的细胞内运输动力学改变和更快的增殖。RicA 是第一个报道的具有 B. abortus 功能的效应物。

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