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来自秘鲁亚马逊地区美洲印第安人的幽门螺杆菌中减弱的 CagA 癌蛋白。

Attenuated CagA oncoprotein in Helicobacter pylori from Amerindians in Peruvian Amazon.

机构信息

Department of Microbiology and Immunology, Institute of Medical Science, University of Tokyo, Tokyo, Japan.

出版信息

J Biol Chem. 2011 Aug 26;286(34):29964-72. doi: 10.1074/jbc.M111.263715. Epub 2011 Jul 8.

Abstract

Population genetic analyses of bacterial genes whose products interact with host tissues can give new understanding of infection and disease processes. Here we show that strains of the genetically diverse gastric pathogen Helicobacter pylori from Amerindians from the remote Peruvian Amazon contain novel alleles of cagA, a major virulence gene, and reveal distinctive properties of their encoded CagA proteins. CagA is injected into the gastric epithelium where it hijacks pleiotropic signaling pathways, helps Hp exploit its special gastric mucosal niche, and affects the risk that infection will result in overt gastroduodenal diseases including gastric cancer. The Amerindian CagA proteins contain unusual but functional tyrosine phosphorylation motifs and attenuated CRPIA motifs, which affect gastric epithelial proliferation, inflammation, and bacterial pathogenesis. Amerindian CagA proteins induced less production of IL-8 and cancer-associated Mucin 2 than did those of prototype Western or East Asian strains and behaved as dominant negative inhibitors of action of prototype CagA during mixed infection of Mongolian gerbils. We suggest that Amerindian cagA is of relatively low virulence, that this may have been selected in ancestral strains during infection of the people who migrated from Asia into the Americas many thousands of years ago, and that such attenuated CagA proteins could be useful therapeutically.

摘要

对与宿主组织相互作用的细菌基因进行群体遗传学分析,可以深入了解感染和疾病的发生过程。在这里,我们展示了来自秘鲁偏远亚马逊地区的美洲原住民的遗传多样性很大的胃病原体幽门螺杆菌菌株含有 cagA 这一主要毒力基因的新型等位基因,并揭示了其编码的 CagA 蛋白的独特特性。CagA 被注入胃上皮细胞,在那里它劫持了多效信号通路,帮助 Hp 利用其特殊的胃黏膜小生境,并影响感染导致显性胃十二指肠疾病(包括胃癌)的风险。美洲原住民的 CagA 蛋白含有不寻常但功能正常的酪氨酸磷酸化基序和减弱的 CRPIA 基序,这会影响胃上皮细胞的增殖、炎症和细菌发病机制。与原型西方或东亚菌株相比,美洲原住民 CagA 蛋白诱导的 IL-8 和与癌症相关的 Mucin 2 产生较少,并且在蒙古沙鼠的混合感染中作为原型 CagA 作用的显性负抑制剂。我们认为,美洲原住民的 cagA 相对毒性较低,这可能是几千年前从亚洲迁徙到美洲的人群感染过程中祖先菌株的选择结果,而这种减弱的 CagA 蛋白可能具有治疗用途。

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