pylori-positive than -negative subjects.21 In various human and in animal model systems, RAS components are expressed by different gastric mucosal cell types, such as endocrine, glandular epithelial, Y-27632 price mesenchymal, lamina propria and vascular endothelial.21,24 Inflammatory cell migration and activation
enhances mucosal inflammation in response to the locally produced proinflammatory cytokines.25 In a gerbil model, levels of gastric mucosal AT1R show a particular correlation with those of gastric mucosal interleukin (IL)-17 mRNA, but not with levels of IL-1β, IL-11, IL-18 or tumor necrosis factor (TNF)-α. It is this association with IL-17 mRNA which ultimately influences the outcome of H. pylori-associated disease (Fig. 3b).23 In humans, the infection initially presents as an antral-predominant gastritis, followed by the extension of inflammation into the corpus gastritis and eventually leading to atrophic gastritis with metaplasia, gastric ulcers and, rarely, even gastric cancer.6 It is therefore important to clarify the molecule profile of RAS components in the acute and chronic phases of H. pylori infection. Differential expression pattern may play different roles in gastric mucosal pathogenesis
and in the development of atrophic gastritis, peptic ulcers and gastric cancer. In a Mongolian gerbil model, AT1R and AT2R mRNA levels gradually increase with time after H. pylori infection (Figs 2,4),23 and antral AT1R mRNA Cabozantinib datasheet level dominated over that in the body mucosa in the acute phase (Fig. 4)23 but were significantly higher
than those in the antrum in the chronic phase. The fact that AT1R levels in the body are significantly higher in the chronic phase of H. pylori infection may mean that AT1R expression plays a role in gastric mucosal inflammatory cell infiltration and the development of atrophy, with greater potential for the development of gastric cancer. However, only one report has described these time course findings selleckchem after H. pylori infection,23 and further research using animal models is required. The presence and differential activities of H. pylori virulence factors correlate with the severity of gastric mucosal injury and inflammation, and thus with the risk of developing different gastroduodenal diseases.26–28 Among putative H. pylori virulence genes, the outer inflammatory protein (OipA) functions as an adhesion which is involved in inducing the pro-inflammatory response27 and is associated with high H. pylori cell density and severe inflammatory cell infiltrations.29 In Mongolian gerbils, oipA-negative H. pylori strains exhibit diminished ability to induce gastric inflammation and disease relative to decreased H. pylori density.30 The status of oipA needs to be functional for it to enhance gastric ATR levels.