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New Insights into VacA Intoxication Mediated through Its Cell Surface Receptors

机译:通过其细胞表面受体介导的VacA中毒的新见解

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摘要

Helicobacter pylori (H. pylori), a major cause of gastroduodenal diseases, produces VacA, a vacuolating cytotoxin associated with gastric inflammation and ulceration. The C-terminal domain of VacA plays a crucial role in receptor recognition on target cells. We have previously identified three proteins (i.e., RPTPα, RPTPβ, and LRP1) that serve as VacA receptors. These receptors contribute to the internalization of VacA into epithelial cells, activate signal transduction pathways, and contribute to cell death and gastric ulceration. In addition, other factors (e.g., CD18, sphingomyelin) have also been identified as cell-surface, VacA-binding proteins. Since we believe that, following interactions with its host cell receptors, VacA participates in events leading to disease, a better understanding of the cellular function of VacA receptors may provide valuable information regarding the mechanisms underlying the pleiotropic actions of VacA and the pathogenesis of H. pylori-mediated disease. In this review, we focus on VacA receptors and their role in events leading to cell damage.
机译:幽门螺杆菌(H. pylori)是胃十二指肠疾病的主要原因,可产生VacA,一种与胃炎症和溃疡相关的空泡细胞毒素。 VacA的C末端结构域在靶细胞的受体识别中起着至关重要的作用。我们先前已经确定了三种蛋白(即RPTPα,RPTPβ和LRP1)作为VacA受体。这些受体有助于VacA内化进入上皮细胞,激活信号转导途径,并有助于细胞死亡和胃溃疡。另外,还已经鉴定出其他因素(例如,CD18,鞘磷脂)是细胞表面的VacA结合蛋白。由于我们认为,VacA在与其宿主细胞受体相互作用后会参与导致疾病的事件,因此更好地了解VacA受体的细胞功能可能为VacA的多效作用机制和H的发病机理提供有价值的信息。幽门螺旋杆菌介导的疾病。在这篇综述中,我们集中于VacA受体及其在导致细胞损伤的事件中的作用。

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