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首页> 外文期刊>Journal of Clinical Microbiology >Polymorphisms in the Intermediate Region of VacA Impact Helicobacter pylori-Induced Disease Development
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Polymorphisms in the Intermediate Region of VacA Impact Helicobacter pylori-Induced Disease Development

机译:VacA中间区域的多态性影响幽门螺杆菌诱发的疾病发展

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摘要

Helicobacter pylori is the etiological agent of diseases such as gastritis, gastric and duodenal ulcers, and two types of gastric cancers. While some insight has been gained into the etiology of these diverse manifestations, by and large, the reason that some individuals develop more severe disease remains elusive. Recent studies have focused on the roles of H. pylori toxins CagA and VacA on the disease process and have suggested that both toxins are intimately involved. Moreover, CagA and VacA are polymorphic within different H. pylori strains, and particular polymorphisms seem to show a correlation with the development of particular disease states. Among VacA polymorphisms, the intermediate region has recently been proposed to play a major role in disease outcome. In this article, we describe a detailed sequence analysis of the polymorphic intermediate region of vacA from strains obtained from a large South Korean population. We show that polymorphisms found at amino acid position 196 are associated with more severe disease manifestations. Additionally, polymorphisms found at amino acid position 231 are linked to disease in strains that carry the non-EPIYA-ABD allele of CagA. Collectively, these data help explain the impact of the VacA intermediate region on disease and lead to the hypothesis that there are allele-driven interactions between VacA and CagA.
机译:幽门螺杆菌是胃炎,胃和十二指肠溃疡以及两种类型的胃癌等疾病的病因。尽管已经获得了对这些多样表现的病因学的一些见解,但总的来说,某些个体患上更严重疾病的原因仍然难以捉摸。最近的研究集中在 H的作用上。幽门螺杆菌毒素CagA和VacA与疾病进程有关,并表明这两种毒素都密切相关。此外,CagA和VacA在不同的H中是多态的。幽门螺杆菌菌株和特定的多态性似乎与特定疾病状态的发展有关。在VacA多态性中,最近提出了在疾病结果中起主要作用的中间区域。在本文中,我们描述了 vacA 的多态性中间区域的详细序列分析,该区域来自大量韩国人群。我们显示在氨基酸196位发现的多态性与更严重的疾病表现有关。另外,在氨基酸位置231发现的多态性与携带CagA的非EPIYA-ABD等位基因的菌株中的疾病有关。总而言之,这些数据有助于解释VacA中间区域对疾病的影响,并导致以下假设:VacA和CagA之间存在等位基因驱动的相互作用。

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