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OLFM4 modulates intestinal inflammation by promoting IL-22 + ILC3 in the gut.

Zhe XingXinyao LiJunyu HeYimin ChenLei ZhuXiaogang ZhangZhengcong HuangJian TangYuxiong GuoYumei He
Published in: Communications biology (2024)
Group 3 innate lymphoid cells (ILC3s) play key roles in intestinal inflammation. Olfactomedin 4 (OLFM4) is highly expressed in the colon and has a potential role in dextran sodium sulfate-induced colitis. However, the detailed mechanisms underlying the effects of OLFM4 on ILC3-mediated colitis remain unclear. In this study, we identify OLFM4 as a positive regulator of IL-22 + ILC3. OLFM4 expression in colonic ILC3s increases substantially during intestinal inflammation in humans and mice. Compared to littermate controls, OLFM4-deficient (OLFM4 -/- ) mice are more susceptible to bacterial infection and display greater resistance to anti-CD40 induced innate colitis, together with impaired IL-22 production by ILC3, and ILC3s from OLFM4 -/- mice are defective in pathogen resistance. Besides, mice with OLFM4 deficiency in the RORγt compartment exhibit the same trend as in OLFM4 -/- mice, including colonic inflammation and IL-22 production. Mechanistically, the decrease in IL-22 + ILC3 caused by OLFM4 deficiency involves the apoptosis signal-regulating kinase 1 (ASK1)- p38 MAPK signaling-dependent downregulation of RAR-related orphan receptor gamma (RORγt) protein. The OLFM4-metadherin (MTDH) complex upregulates p38/RORγt signaling, which is necessary for IL-22 + ILC3 activation. The findings indicate that OLFM4 is a novel regulator of IL-22 + ILC3 and essential for modulating intestinal inflammation and tissue homeostasis.
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