Gastric Microenvironment Enables Persistence of Helicobacter pylori: a Physician's Combat Towards Eradication and Directions for the Future

Ebinesh Arulnathan, Bharath N. Lakshminarasimmaiah, Harshitha J Naik
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Abstract

lymphoid tissue (MALT) lymphoma, and gastric carcinoma (Malfertheiner et al., 2009; Kuipers, 1997; IARC monograph, 1994) as being associated with H. pylori infection. Efforts were also focused on instituting modalities to counter these pathologies in the form of reinforcing the gastric wall and killing the causative bacteria. Deep insight into the microbial structure, virulence factors, pathogenesis, and associated pathological states has directed scientists and clinical researchers to design compactly constituted drug regimens comprising antibiotics (amoxicillin, clarithromycin, metronidazole, levofloxacin, etc.), anti-secretory agents (PPIs and H2 blockers), and topical medications (colloidal bismuth preparations) for the eradication of H. pylori. These endeavours should simplify and expedite the process of the absolute eradication of H. pylori from the stomach. However, it proves to be a significant challenge. This bacterial endurance has been attributed to phenotypic and genotypic variations such as the development of drug resistance (Ebinesh and Kailash, 2016; Broutet et al., 2003) and the impotency of antimicrobial agents in the stomach (Vakil and Megraud, 2007; Bloom and Polak, 1980). The role of the stomach and its microenvironment in eradication failure (Table 1) and future prospects for successful eradication will be discussed.
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胃微环境使幽门螺杆菌持续存在:医生的根除战斗和未来的方向
淋巴组织(MALT)淋巴瘤和胃癌(Malferthener等人,2009;Kuipers,1997;IARC专著,1994)与幽门螺杆菌感染有关。还致力于制定以加强胃壁和杀死致病细菌的形式对抗这些病理的方法。对微生物结构、毒力因子、发病机制和相关病理状态的深入了解指导科学家和临床研究人员设计紧凑的药物方案,包括抗生素(阿莫西林、克拉霉素、甲硝唑、左氧氟沙星等)、抗分泌剂(PPIs和H2阻滞剂),以及根除幽门螺杆菌的局部药物(胶体铋制剂)。这些努力应该简化并加快从胃中彻底根除幽门螺杆菌的过程。然而,事实证明这是一个重大挑战。这种细菌耐受性归因于表型和基因型变异,如耐药性的发展(Ebinesh和Kailash,2016;Broutet等人,2003)和胃中抗菌剂的缺乏(Vakil和Megraud,2007;Bloom和Polak,1980)。将讨论胃及其微环境在根除失败中的作用(表1)以及成功根除的未来前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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