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首页> 外文期刊>Journal of Clinical Microbiology >Microevolution of Helicobacter pylori Type IV Secretion Systems in an Ulcer Disease Patient over a Ten-Year Period
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Microevolution of Helicobacter pylori Type IV Secretion Systems in an Ulcer Disease Patient over a Ten-Year Period

机译:溃疡病患者十年中幽门螺杆菌IV型分泌系统的微进化

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Helicobacter pylori cagA and vacA genotypes have been used for almost a decade as stable entities to link the severity of gastritis and ulcer disease. We describe here microevolution of the two genomic islands, cag pathogenicity island (cagPAI; 40 kb) and tfs3 (16 kb) from isolates obtained at inclusion (one subclone) and after a 10-year period (two subclones) from a duodenal ulcer patient. Our results indicate microevolution in cagA, cagE, and cag7 genes of the cagPAI and open reading frames G, P, and L in tfs3, which possibly leads to inactivation or pseudogenization of these genes. Interestingly, no significant reduction in the severity of gastroduodenal pathology was found. These results point to an obvious difficulty in correlating the continuously evolving virulence factors such as the cagPAI genes with disease characteristics that appear to remain stable.
机译:幽门螺杆菌cagA vacA 基因型已被用作将胃炎和溃疡病的严重程度联系起来的稳定实体已有近十年的历史。我们在这里描述了从获得的分离物中分离到的两个基因组岛 cag 致病性岛( cag PAI; 40 kb)和 tfs3 (16 kb)的微进化。十二指肠溃疡患者入选时(一个亚克隆)和十年期后(两个亚克隆)。我们的结果表明 cag PAI的 cagA cagE cag7 基因和开放阅读框G的微进化, tfs3 中的P和L,可能导致这些基因失活或假基因化。有趣的是,没有发现胃十二指肠病理的严重程度明显降低。这些结果指出了将持续发展的毒力因子(例如 cag PAI基因)与似乎保持稳定的疾病特征联系起来的明显困难。

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