Microbiota-induced tissue signals regulate ILC3-mediated antigen presentation.
Frank Michael LehmannNicole von BurgRobert IvanekClaudia TeufelEdit HorvathAnnick PeterGleb TurchinovichDaniel StaehliTobias EichlisbergerMercedes Gomez de AgüeroMairene Coto-LlerenaMichaela Prchal-MurphyVeronika SexlMohamed Bentires-AljChristoph MüllerDaniela FinkePublished in: Nature communications (2020)
Although group 3 innate lymphoid cells (ILC3s) are efficient inducers of T cell responses in the spleen, they fail to induce CD4+ T cell proliferation in the gut. The signals regulating ILC3-T cell responses remain unknown. Here, we show that transcripts associated with MHC II antigen presentation are down-modulated in intestinal natural cytotoxicity receptor (NCR)- ILC3s. Further data implicate microbiota-induced IL-23 as a crucial signal for reversible silencing of MHC II in ILC3s, thereby reducing the capacity of ILC3s to present antigen to T cells in the intestinal mucosa. Moreover, IL-23-mediated MHC II suppression is dependent on mTORC1 and STAT3 phosphorylation in NCR- ILC3s. By contrast, splenic interferon-γ induces MHC II expression and CD4+ T cell stimulation by NCR- ILC3s. Our results thus identify biological circuits for tissue-specific regulation of ILC3-dependent T cell responses. These pathways may have implications for inducing or silencing T cell responses in human diseases.
Keyphrases
- nk cells
- cell proliferation
- high glucose
- endothelial cells
- magnetic resonance
- diabetic rats
- induced apoptosis
- magnetic resonance imaging
- machine learning
- artificial intelligence
- cell death
- cell cycle arrest
- big data
- drug induced
- binding protein
- protein kinase
- immune response
- oxidative stress
- contrast enhanced
- cell cycle
- deep learning