The development of inflammatory bowel disease (IBD) is driven by the interaction among host genetics, microbiota, and the immune system of the entire digestive tract. Atg16L1T300A polymorphism is a genetic factor that confers increased risk for the pathogenesis of Crohn's disease. However, the exact contributions of Atg16L1T300A to intestinal mucosal homeostasis are not well understood. Here we show that Atg16L1T300A polymorphism impacts commensal bacterial flora in the intestine under a steady state. Analysis of intestinal bacteria from Atg16L1 mice showed that they harbored an altered microbiota in both the terminal ileum and colon compared to cohoused WT mice. Interestingly, Atg16L1 mice harbored a significant increase in the abundance of , , , and which were known associated with IBD. Moreover, , a bacterium that is mucin-associated, was reduced greatly in Atg16L1 mice. Further analysis indicated that goblet cells of Atg16L1 mice had diminished mucin secretion that resulted from defective autophagy. Finally, Atg16L1 mice developed more severe inflammation in the DSS colitis model than in WT mice. These results indicate that the altered microbiota in Atg16L1 mice might be an important factor that contributed to the risk of Atg16L1T300A carriers to Crohn's disease and supports a multi-hit disease model involving specific gene-microbe interactions.
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| http://dx.doi.org/10.3389/fimmu.2021.772189 | DOI Listing |
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