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Helicobacter hepaticus a new pathogenic species of the Helicobacter genus: Similarities and differences with H. pylori

机译:Helicobacter hepaticus一种新型的Helicobacter病原体:与幽门螺杆菌的异同

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摘要

Helicobacter hepaticus was discovered in 1992 as a cause of liver cancer in the A/JCr mouse model. In susceptible mice, infection by H. hepaticus causes chronic gastrointestinal inflammation leading to neoplasia. It can also cause morphological changes in breast-glands leading to neoplasm and adenocarcinoma in mouse models. Studies performed on humans have revealed that H. hepaticus may also be a human pathogen since infection by H. hepaticus can be associated with cholecystitis, cholelithiasis and gallbladder cancer. H. hepaticus is a close relative of H. pylori, but it lacks the major virulence factors of H. pylori including vacoulating cytotoxin A (VacA) and cytotoxin associated gene (cagA). Moreover, SabA, AlpA, and BabA, three important adhesin proteins of H. pylori, are absent in its genome. In contrast, the genome of H. hepaticus contains genes encoding some orthologus virulence factors of Campylobacter jejuni such as cytolethal distending toxin (CDT), and PebI adhesin factor. Other genes including 16S rRNA, 18 KDa immunogenic protein, and urease structural subunits are related to H. pylori. Its genome contains a small island consisting of 71 Kbp named HHGI1, which probably encodes a secretion system type IV (T4SS), and some other virulence factors. As far as the immunogenic antigens are concerned, the lipopolysaccharide (LPS) and flagellin of H. hepaticus are weak stimulants of the immune system, while pro-inflammatory responses are mainly induced by its lipoproteins and most likely by the peptidoglycan. Concerning the multidrug efflux pumps, a homologue of H. pylori TolC, HefA, has been observed in H. hepaticus which contributes to resistance to amoxicillin and bile acids.
机译:于1992年在A / JCr小鼠模型中发现肝杆菌是引起肝癌的原因。在易感小鼠中,被肝菌感染会引起慢性胃肠道炎症,从而导致肿瘤形成。它还可以引起小鼠腺体的形态变化,导致肿瘤和腺癌。对人类的研究表明,肝炎性肝炎也可能是人类的病原体,因为肝炎性肝炎的感染可能与胆囊炎,胆石症和胆囊癌有关。肝幽门螺杆菌是幽门螺杆菌的近亲,但它缺乏幽门螺杆菌的主要毒力因子,包括波动的细胞毒素A(VacA)和细胞毒素相关基因(cagA)。而且,幽门螺杆菌的三个重要粘附蛋白SabA,AlpA和BabA在其基因组中不存在。相比之下,H。hepaticus的基因组包含编码空肠弯曲菌某些直系同源毒力因子的基因,例如细胞致死性扩张毒素(CDT)和PebI粘附素因子。其他基因包括16S rRNA,18 KDa免疫原性蛋白和脲酶结构亚基,与幽门螺杆菌有关。它的基因组包含一个小岛,由71 Kbp的HHGI1组成,该岛可能编码IV型分泌系统(T4SS)和其他一些毒力因子。就免疫原性抗原而言,肝H.的脂多糖(LPS)和鞭毛蛋白是免疫系统的弱刺激物,而促炎反应主要由其脂蛋白诱导,最有可能由肽聚糖诱导。关于多药外排泵,已在肝菌中观察到幽门螺杆菌TolC的同系物HefA,这有助于抵抗阿莫西林和胆汁酸。

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