| Literature DB >> 31747582 |
Eric H Ma1, Mark J Verway2, Radia M Johnson3, Dominic G Roy2, Mya Steadman4, Sebastian Hayes4, Kelsey S Williams5, Ryan D Sheldon5, Bozena Samborska2, Penelope A Kosinski4, Hyeryun Kim4, Takla Griss2, Brandon Faubert6, Stephanie A Condotta7, Connie M Krawczyk8, Ralph J DeBerardinis9, Kelly M Stewart4, Martin J Richer7, Victor Chubukov4, Thomas P Roddy4, Russell G Jones10.
Abstract
Naive CD8+ T cells differentiating into effector T cells increase glucose uptake and shift from quiescent to anabolic metabolism. Although much is known about the metabolism of cultured T cells, how T cells use nutrients during immune responses in vivo is less well defined. Here, we combined bioenergetic profiling and 13C-glucose infusion techniques to investigate the metabolism of CD8+ T cells responding to Listeria infection. In contrast to in vitro-activated T cells, which display hallmarks of Warburg metabolism, physiologically activated CD8+ T cells displayed greater rates of oxidative metabolism, higher bioenergetic capacity, differential use of pyruvate, and prominent flow of 13C-glucose carbon to anabolic pathways, including nucleotide and serine biosynthesis. Glucose-dependent serine biosynthesis mediated by the enzyme Phgdh was essential for CD8+ T cell expansion in vivo. Our data highlight fundamental differences in glucose use by pathogen-specific T cells in vivo, illustrating the impact of environment on T cell metabolic phenotypes.Entities:
Year: 2019 PMID: 31747582 DOI: 10.1016/j.immuni.2019.09.003
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745