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Differential reliance on lipid metabolism as a salvage pathway underlies functional differences of T cell subsets in poor nutrient environments

Abstract: T cells compete with malignant cells for limited nutrients within the solid tumor microenvironment. We found that effector memory CD4 T cells respond distinctly from other T cell subsets to limiting glucose and can maintain high levels of interferon-? (IFN-?) production in a nutrient-poor environment. Unlike naive (TN) or central memory T (TCM) cells, effector memory T (TEM) cells fail to upregulate fatty acid synthesis, oxidative phosphorylation, and reductive glutaminolysis in limiting glucose. Interference of fatty acid synthesis in naive T cells dramatically upregulates IFN-?, while increasing exogenous lipids in media inhibits production of IFN-? by all subsets, suggesting that relative ratio of fatty acid metabolism to glycolysis is a direct predictor of T cell effector activity. Together, these data suggest that effector memory T cells are programmed to have limited ability to synthesize and metabolize fatty acids, which allows them to maintain T cell function in nutrient-depleted microenvironments. Ecker et al. distinguish unique metabolic and functional properties of naive and memory T cell subsets during glucose limitation. During glucose starvation, T cells begin to differentially rely on fatty acid synthesis and glutamine utilization to survive. Unexpectedly, reliance on fatty acid synthesis alters the ability to produce IFN-?.

 Fuente: Cell Reports, 2018, 23(3), 741-755

 Editorial: Cell Press Elsevier

 Año de publicación: 2018

 Nº de páginas: 16

 Tipo de publicación: Artículo de Revista

 DOI: 10.1016/j.celrep.2018.03.084

 ISSN: 2211-1247

 Url de la publicación: https://doi.org/10.1016/j.celrep.2018.03.084

Autoría

ECKER, CHRISTOPHER

GUO, LILI

VOICU, STEFANA

MEDVEC, ANDREW

CORTINA, LUIS

PAJDA, JACKIE

ANDOLINA, MELANIE

TORRES-CASTILLO, MARIA

DONATO, JENNIFER L.

MANSOUR, SARYA

ZYNDA, EVAN R.

LIN, PEI-YI

VARELA-ROHENA, ANGEL

BLAIR, IAN A.

RILEY, JAMES L.