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Molecular mechanisms of gastric epithelial cell adhesion and injection of CagA by Helicobacter pylori

机译:幽门螺杆菌与胃黏膜上皮细胞黏附及注射CagA的分子机制

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摘要

Helicobacter pylori is a highly successful pathogen uniquely adapted to colonize humans. Gastric infections with this bacterium can induce pathology ranging from chronic gastritis and peptic ulcers to gastric cancer. More virulent H. pylori isolates harbour numerous well-known adhesins (BabA/B, SabA, AlpA/B, OipA and HopZ) and the cag (cytotoxin-associated genes) pathogenicity island encoding a type IV secretion system (T4SS). The adhesins establish tight bacterial contact with host target cells and the T4SS represents a needle-like pilus device for the delivery of effector proteins into host target cells such as CagA. BabA and SabA bind to blood group antigen and sialylated proteins respectively, and a series of T4SS components including CagI, CagL, CagY and CagA have been shown to target the integrin β1 receptor followed by injection of CagA across the host cell membrane. The interaction of CagA with membrane-anchored phosphatidylserine may also play a role in the delivery process. While substantial progress has been made in our current understanding of many of the above factors, the host cell receptors for OipA, HopZ and AlpA/B during infection are still unknown. Here we review the recent progress in characterizing the interactions of the various adhesins and structural T4SS proteins with host cell factors. The contribution of these interactions to H. pylori colonization and pathogenesis is discussed.
机译:幽门螺杆菌是一种非常成功的病原体,独特地适应了人类的定殖。这种细菌的胃感染可诱发从慢性胃炎和消化性溃疡到胃癌的各种病理。更具毒性的幽门螺杆菌分离株具有许多众所周知的粘附素(BabA / B,SabA,AlpA / B,OipA和HopZ)和cag(与细胞毒素相关的基因)致病性岛,其编码IV型分泌系统(T4SS)。粘附素建立与宿主靶细胞的紧密细菌接触,而T4SS代表一种针状菌毛装置,用于将效应蛋白递送到宿主靶细胞(如CagA)中。 BabA和SabA分别与血型抗原和唾液酸化蛋白结合,并且已显示一系列T4SS组分(包括CagI,CagL,CagY和CagA)靶向整联蛋白β1受体,然后跨宿主细胞膜注射CagA。 CagA与膜锚定的磷脂酰丝氨酸的相互作用也可能在传递过程中起作用。尽管我们目前对上述许多因素的了解已取得实质性进展,但感染期间OipA,HopZ和AlpA / B的宿主细胞受体仍然未知。在这里,我们回顾了表征各种粘附素和结构性T4SS蛋白与宿主细胞因子相互作用的最新进展。讨论了这些相互作用对幽门螺杆菌定植和发病机理的贡献。

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