Significance
Group 3 innate lymphoid cells (ILC3s) play decisive roles in mammalian physiology including tissue repair, lymphoid tissue development, and immune regulation. So far, the functions of ILC3s in the adult immune system have been mainly linked to their capacity to release cytokines in response to microbial or inflammatory signals. The results presented here show that activated ILC3s can alter the outcome of adaptive immune responses by directly stimulating CD4
+
T cells. Indeed, IL-1β–activated ILC3s express costimulatory molecules and induce cognate CD4
+
T-cell responses. More importantly, antigen-driven T- and B-cell responses are impaired in vivo when this cellular interaction is disrupted. Overall, our data show that peripheral ILC3s play a yet unappreciated role in T-cell–mediated immunity.
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