| Literature DB >> 31091446 |
Jing Qiu1, Matteo Villa1, David E Sanin1, Michael D Buck1, David O'Sullivan1, Reagan Ching1, Mai Matsushita1, Katarzyna M Grzes1, Frances Winkler2, Chih-Hao Chang3, Jonathan D Curtis1, Ryan L Kyle1, Nikki Van Teijlingen Bakker1, Mauro Corrado1, Fabian Haessler1, Francesca Alfei4, Joy Edwards-Hicks1, Leonard B Maggi5, Dietmar Zehn4, Takeshi Egawa6, Bertram Bengsch7, Ramon I Klein Geltink1, Thomas Jenuwein1, Edward J Pearce8, Erika L Pearce9.
Abstract
Competition for nutrients like glucose can metabolically restrict T cells and contribute to their hyporesponsiveness during cancer. Metabolic adaptation to the surrounding microenvironment is therefore key for maintaining appropriate cell function. For instance, cancer cells use acetate as a substrate alternative to glucose to fuel metabolism and growth. Here, we show that acetate rescues effector function in glucose-restricted CD8+ T cells. Mechanistically, acetate promotes histone acetylation and chromatin accessibility and enhances IFN-γ gene transcription and cytokine production in an acetyl-CoA synthetase (ACSS)-dependent manner. Ex vivo acetate treatment increases IFN-γ production by exhausted T cells, whereas reducing ACSS expression in T cells impairs IFN-γ production by tumor-infiltrating lymphocytes and tumor clearance. Thus, hyporesponsive T cells can be epigenetically remodeled and reactivated by acetate, suggesting that pathways regulating the use of substrates alternative to glucose could be therapeutically targeted to promote T cell function during cancer.Entities:
Keywords: T cell exhaustion; T cell hyporesponsiveness; T cells; acetate; acetyl-CoA synthetase; chromatin remodeling; effector functions; tumor immunity; tumor-infiltrating lymphocytes
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Year: 2019 PMID: 31091446 PMCID: PMC6544383 DOI: 10.1016/j.celrep.2019.04.022
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423