| Literature DB >> 29980617 |
Kai Yang1, Daniel Bastardo Blanco2,3, Xiang Chen4, Pradyot Dash2, Geoffrey Neale5, Celeste Rosencrance4, John Easton4, Wenan Chen4, Changde Cheng4, Yogesh Dhungana2, Anil Kc2, Walid Awad2, Xi-Zhi J Guo2,3, Paul G Thomas2, Hongbo Chi1.
Abstract
The interaction between extrinsic factors and intrinsic signal strength governs thymocyte development, but the mechanisms linking them remain elusive. We report that mechanistic target of rapamycin complex 1 (mTORC1) couples microenvironmental cues with metabolic programs to orchestrate the reciprocal development of two fundamentally distinct T cell lineages, the αβ and γδ T cells. Developing thymocytes dynamically engage metabolic programs including glycolysis and oxidative phosphorylation, as well as mTORC1 signaling. Loss of RAPTOR-mediated mTORC1 activity impairs the development of αβ T cells but promotes γδ T cell generation, associated with disrupted metabolic remodeling of oxidative and glycolytic metabolism. Mechanistically, we identify mTORC1-dependent control of reactive oxygen species production as a key metabolic signal in mediating αβ and γδ T cell development, and perturbation of redox homeostasis impinges upon thymocyte fate decisions and mTORC1-associated phenotypes. Furthermore, single-cell RNA sequencing and genetic dissection reveal that mTORC1 links developmental signals from T cell receptors and NOTCH to coordinate metabolic activity and signal strength. Our results establish mTORC1-driven metabolic signaling as a decisive factor for reciprocal αβ and γδ T cell development and provide insight into metabolic control of cell signaling and fate decisions.Entities:
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Year: 2018 PMID: 29980617 PMCID: PMC6230375 DOI: 10.1126/sciimmunol.aas9818
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468