CTLA-4-expressing ILC3s restrain interleukin-23-mediated inflammation.
Anees AhmedAnn M JosephJordan ZhouVeronika HornJazib UddinMengze LyuJérémy Gocnull nullRobbyn E SockolowJames Badger WingÉric VivierShimon SakaguchiGregory F SonnenbergPublished in: Nature (2024)
Interleukin (IL-)23 is a major mediator and therapeutic target in chronic inflammatory diseases that also elicits tissue protection in the intestine at homeostasis or following acute infection 1-4 . However, the mechanisms that shape these beneficial versus pathological outcomes remain poorly understood. To address this gap in knowledge, we performed single-cell RNA sequencing on all IL-23 receptor-expressing cells in the intestine and their acute response to IL-23, revealing a dominance of T cells and group 3 innate lymphoid cells (ILC3s). Unexpectedly, we identified potent upregulation of the immunoregulatory checkpoint molecule cytotoxic T-lymphocyte-associated antigen-4 (CTLA-4) on ILC3s. This pathway was activated by gut microbes and IL-23 in a FOXO1- and STAT3-dependent manner. Mice lacking CTLA-4 on ILC3s exhibited reduced regulatory T cells, elevated inflammatory T cells and more-severe intestinal inflammation. IL-23 induction of CTLA-4 + ILC3s was necessary and sufficient to reduce co-stimulatory molecules and increase PD-L1 bioavailability on intestinal myeloid cells. Finally, human ILC3s upregulated CTLA-4 in response to IL-23 or gut inflammation and correlated with immunoregulation in inflammatory bowel disease. These results reveal ILC3-intrinsic CTLA-4 as an essential checkpoint that restrains the pathological outcomes of IL-23, suggesting that disruption of these lymphocytes, which occurs in inflammatory bowel disease 5-7 , contributes to chronic inflammation.
Keyphrases
- oxidative stress
- induced apoptosis
- single cell
- regulatory t cells
- nk cells
- cell cycle arrest
- dna damage
- liver failure
- dendritic cells
- drug induced
- healthcare
- gene expression
- endoplasmic reticulum stress
- endothelial cells
- acute myeloid leukemia
- peripheral blood
- rna seq
- bone marrow
- metabolic syndrome
- transcription factor
- dna methylation
- anti inflammatory
- poor prognosis
- immune response
- binding protein
- insulin resistance