| Literature DB >> 29887373 |
Christoph Schneider1, Claire E O'Leary1, Jakob von Moltke1, Hong-Erh Liang1, Qi Yan Ang2, Peter J Turnbaugh2, Sridhar Radhakrishnan3, Michael Pellizzon3, Averil Ma1, Richard M Locksley4.
Abstract
The small intestinal tuft cell-ILC2 circuit mediates epithelial responses to intestinal helminths and protists by tuft cell chemosensory-like sensing and IL-25-mediated activation of lamina propria ILC2s. Small intestine ILC2s constitutively express the IL-25 receptor, which is negatively regulated by A20 (Tnfaip3). A20 deficiency in ILC2s spontaneously triggers the circuit and, unexpectedly, promotes adaptive small-intestinal lengthening and remodeling. Circuit activation occurs upon weaning and is enabled by dietary polysaccharides that render mice permissive for Tritrichomonas colonization, resulting in luminal accumulation of acetate and succinate, metabolites of the protist hydrogenosome. Tuft cells express GPR91, the succinate receptor, and dietary succinate, but not acetate, activates ILC2s via a tuft-, TRPM5-, and IL-25-dependent pathway. Also induced by parasitic helminths, circuit activation and small intestinal remodeling impairs infestation by new helminths, consistent with the phenomenon of concomitant immunity. We describe a metabolic sensing circuit that may have evolved to facilitate mutualistic responses to luminal pathosymbionts.Entities:
Keywords: A20; IL-25; ILC2s; TRPM5; Tritrichomonas; concomitant immunity; helminths; succinate; succinate receptor; tuft cells
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Year: 2018 PMID: 29887373 PMCID: PMC6046262 DOI: 10.1016/j.cell.2018.05.014
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582