1. Calcineurin-mediated IL-2 production by CD11chighMHCII+ myeloid cells is crucial for intestinal immune homeostasis.
- Author
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Mencarelli, Andrea, Khameneh, Hanif Javanmard, Fric, Jan, Vacca, Maurizio, Daker, Sary El, Janela, Baptiste, Jing Ping Tang, Nabti, Sabrina, Balachander, Akhila, Tong Seng Lim, Ginhoux, Florent, Ricciardi-Castagnoli, Paola, and Mortellaro, Alessandra
- Subjects
INFLAMMATORY bowel diseases ,HOMEOSTASIS ,B cells ,IMMUNOLOGICAL tolerance ,CELL populations ,CELLS - Abstract
The intestinal immune system can respond to invading pathogens yet maintain immune tolerance to self-antigens and microbiota. Myeloid cells are central to these processes, but the signaling pathways that underlie tolerance versus inflammation are unclear. Here we show that mice lacking Calcineurin B in CD11c
high MHCII+ cells (Cnb1CD11c mice) spontaneously develop intestinal inflammation and are susceptible to induced colitis. In these mice, colitis is associated with expansion of T helper type 1 (Th1) and Th17 cell populations and a decrease in the number of FoxP3+ regulatory T (Treg) cells, and the pathology is linked to the inability of intestinal Cnb1-deficient CD11chigh MHCII+ cells to express IL-2. Deleting IL-2 in CD11chigh MHCII+ cells induces spontaneous colitis resembling human inflammatory bowel disease. Our findings identify that the calcineurin–NFAT–IL-2 pathway in myeloid cells is a critical regulator of intestinal homeostasis by influencing the balance of inflammatory and regulatory responses in the mouse intestine. [ABSTRACT FROM AUTHOR]- Published
- 2018
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