[PDF][PDF] The CD28 signaling pathway regulates glucose metabolism

KA Frauwirth, JL Riley, MH Harris, RV Parry… - Immunity, 2002 - cell.com
KA Frauwirth, JL Riley, MH Harris, RV Parry, JC Rathmell, DR Plas, RL Elstrom, CH June
Immunity, 2002cell.com
Lymphocyte activation initiates a program of cell growth, proliferation, and differentiation that
increases metabolic demand. Although T cells increase glucose uptake and glycolysis
during an immune response, the signaling pathways that regulate these increases remain
largely unknown. Here we show that CD28 costimulation, acting through
phosphatidylinositol 3′-kinase (PI3K) and Akt, is required for T cells to increase their
glycolytic rate in response to activation. Furthermore, CD28 controls a primary response …
Abstract
Lymphocyte activation initiates a program of cell growth, proliferation, and differentiation that increases metabolic demand. Although T cells increase glucose uptake and glycolysis during an immune response, the signaling pathways that regulate these increases remain largely unknown. Here we show that CD28 costimulation, acting through phosphatidylinositol 3′-kinase (PI3K) and Akt, is required for T cells to increase their glycolytic rate in response to activation. Furthermore, CD28 controls a primary response pathway, inducing a level of glucose uptake and glycolysis in excess of that needed to maintain cellular ATP/ADP levels or macromolecular synthesis. These data suggest that CD28 costimulation functions to increase glycolytic flux, allowing T cells to anticipate energetic and biosynthetic needs associated with a sustained response.
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