Lamina propria T cells of LPSWT-treated EndohiRag1−/− mice showed significantly higher expression of interferon gamma and IL-17a as compared with LPSMUT-treated EndohiRag1−/− mice. However, no significant differences
in FoxP3 expression of lp T cells was observed ( Figure 4E). In summary, these data show that changes in the lipid A structure can convert a pro-inflammatory E coli strain into an anti-inflammatory E coli strain, and that the proportion of LPS with different lipid A structures within the intestinal microbiota might have a critical influence on development of colitis in a genetically predisposed host in the context of a specific microbiota. Recent studies cAMP inhibitor have examined the function of the intestinal microbiota in the pathogenesis of inflammatory intestinal diseases in genetically predisposed hosts and the prospects of preventing inflammation by selective alteration of the intestinal microbiota.26, 27, 28 and 29 We identified LPS as a microbial factor that, according to its composition/structure, can either promote or prevent the development of bowel inflammation in the CD4+ T-cell transfer model of colitis in Rag1−/− mice. We demonstrated that probably by structural changes in the lipid A, the colitogenic potential of a commensal E coli strain BTK inhibitor in vivo can not only be abolished,
but also converted into a protective commensal strain that prevents development of T-cell−induced colitis. Several animal studies demonstrated that the intestinal microbiota shapes homeostasis of the intestinal mucosal immune system,29, 30, 31, 32, 33 and 34 and that a distinct composition of the intestinal microbiota is associated with promotion Tenofovir cell line of bowel inflammation.29, 30, 31 and 35 However, it
is not yet clear whether a specific microbiota composition or a specific microbial compound might initiate the inflammatory process or perpetuate the chronic inflammation. To clarify this, we used Rag1−/− mice transferred with T cells that develop colitis in the presence of a specific complex microbiota or specific pathobionts (eg, Helicobacter hepaticus 36), but remain healthy under germ-free conditions. In our model, we observed that an intestinal microbiota exhibiting low endotoxicity and harboring a high proportion of Bacteroidetes (Endolo) was associated with prevention of T-cell−induced colitis, supporting the idea that low endotoxic microbiota or bacteria of the Bacteroidetes group might inhibit mucosal pro-inflammatory host responses. In contrast, the high endotoxicity and high proportion of Enterobacteriaceae in EndohiRag1−/− mice was clearly associated with development of intestinal inflammation.