AI Article Synopsis
- Group 2 innate lymphoid cells (ILC2s) play a significant role in type 2 inflammation, which is important for fighting parasites and allergic responses.
- Researchers identified the retinoid X receptor gamma (Rxrg) as a key factor in ILC2s, as it is highly expressed in small intestinal ILC2s and is quickly suppressed by inflammatory cytokines.
- Deleting Rxrg did not affect ILC2 development but enhanced their response to inflammatory stimuli, suggesting that RXRγ acts as a checkpoint to regulate ILC2 activation and proliferation through its influence on lipid metabolism.
Article Abstract
Group 2 innate lymphoid cells (ILC2s) are crucial in promoting type 2 inflammation that contributes to both anti-parasite immunity and allergic diseases. However, the molecular checkpoints in ILC2s that determine whether to immediately launch a proinflammatory response are unknown. Here, we found that retinoid X receptor gamma (Rxrg) was highly expressed in small intestinal ILC2s and rapidly suppressed by alarmin cytokines. Genetic deletion of Rxrg did not impact ILC2 development but facilitated ILC2 responses and the tissue inflammation induced by alarmins. Mechanistically, RXRγ maintained the expression of its target genes that support intracellular cholesterol efflux, which in turn reduce ILC2 proliferation. Furthermore, RXRγ expression prevented ILC2 response to mild stimulations, including low doses of alarmin cytokine and mechanical skin injury. Together, we propose that RXRγ expression and its mediated lipid metabolic states function as a cell-intrinsic checkpoint that confers the threshold of ILC2 activation in the small intestine.
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| http://dx.doi.org/10.1016/j.immuni.2023.08.019 | DOI Listing |
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