Amino acid availability acts as a metabolic rheostat to determine the magnitude of ILC2 responses

Author:

Hodge Suzanne H.,Krauss Maria Z.,Kaymak Irem,King James,Howden Andrew J.M.,Panic Gordana,Grencis Richard K.,Swann Jonathan R.,Sinclair Linda V.,Hepworth Matthew R.ORCID

Abstract

AbstractGroup 2 innate lymphoid cells (ILC2) are functionally poised, tissue-resident lymphocytes that respond rapidly to damage and infection at mucosal barrier sites. ILC2 reside within complex microenvironments where they are subject to cues from the diet, commensal microbiota and invading pathogens – most notably helminths. Emerging evidence suggests ILC2 are acutely sensitive not only to canonical activating signals, but also perturbations in nutrient and metabolite availability. In the context of helminth infection, we identify amino acid availability as a nutritional cue in regulating ILC2 responses. ILC2 were found to be uniquely pre-primed to import amino acids via the large neutral amino acid transporters Slc7a5 and Slc7a8. Cell-intrinsic deletion of these transporters impaired ILC2 expansion, but not cytokine production, in part via tuning of mTOR activation. These findings implicate the import of amino acids as a metabolic requisite for optimal ILC2 responses, and further highlight nutritional cues as critical regulators of innate immune responses within mucosal barrier tissues.

Publisher

Cold Spring Harbor Laboratory

Reference44 articles.

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