In vivo CRISPR screening reveals nutrient signaling processes underpinning CD8+ T cell fate decisions
Author(s) -
Hongling Huang,
Peipei Zhou,
Jun Wei,
Lingyun Long,
Hao Shi,
Yogesh Dhungana,
Nicole M. Chapman,
Guotong Fu,
Jordy Saravia,
Jana Raynor,
Shaofeng Liu,
Gustavo Palacios,
YongDong Wang,
Chenxi Qian,
Jiyang Yu,
Hongbo Chi
Publication year - 2021
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2021.02.021
Subject(s) - biology , crispr , cell fate determination , underpinning , microbiology and biotechnology , in vivo , cell , computational biology , genetics , transcription factor , gene , civil engineering , engineering
How early events in effector T cell (TEFF) subsets tune memory T cell (TMEM) responses remains incompletely understood. Here, we systematically investigated metabolic factors in fate determination of TEFF and TMEM cells using in vivo pooled CRISPR screening, focusing on negative regulators of TMEM responses. We found that amino acid transporters Slc7a1 and Slc38a2 dampened the magnitude of TMEM differentiation, in part through modulating mTORC1 signaling. By integrating genetic and systems approaches, we identified cellular and metabolic heterogeneity among TEFF cells, with terminal effector differentiation associated with establishment of metabolic quiescence and exit from the cell cycle. Importantly, Pofut1 (protein-O-fucosyltransferase-1) linked GDP-fucose availability to downstream Notch-Rbpj signaling, and perturbation of this nutrient signaling axis blocked terminal effector differentiation but drove context-dependent TEFF proliferation and TMEM development. Our study establishes that nutrient uptake and signaling are key determinants of T cell fate and shape the quantity and quality of TMEM responses.
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