JCI Insight (Aug 2020)

CD28 costimulation drives tumor-infiltrating T cell glycolysis to promote inflammation

  • Kathryn E. Beckermann,
  • Rachel Hongo,
  • Xiang Ye,
  • Kirsten Young,
  • Katie Carbonell,
  • Diana C. Contreras Healey,
  • Peter J. Siska,
  • Sierra Barone,
  • Caroline E. Roe,
  • Christof C. Smith,
  • Benjamin G. Vincent,
  • Frank M. Mason,
  • Jonathan M. Irish,
  • W. Kimryn Rathmell,
  • Jeffrey C. Rathmell

Journal volume & issue
Vol. 5, no. 16

Abstract

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Metabolic reprogramming dictates the fate and function of stimulated T cells, yet these pathways can be suppressed in T cells in tumor microenvironments. We previously showed that glycolytic and mitochondrial adaptations directly contribute to reducing the effector function of renal cell carcinoma (RCC) CD8+ tumor-infiltrating lymphocytes (TILs). Here we define the role of these metabolic pathways in the activation and effector functions of CD8+ RCC TILs. CD28 costimulation plays a key role in augmenting T cell activation and metabolism, and is antagonized by the inhibitory and checkpoint immunotherapy receptors CTLA4 and PD-1. While RCC CD8+ TILs were activated at a low level when stimulated through the T cell receptor alone, addition of CD28 costimulation greatly enhanced activation, function, and proliferation. CD28 costimulation reprogrammed RCC CD8+ TIL metabolism with increased glycolysis and mitochondrial oxidative metabolism, possibly through upregulation of GLUT3. Mitochondria also fused to a greater degree, with higher membrane potential and overall mass. These phenotypes were dependent on glucose metabolism, as the glycolytic inhibitor 2-deoxyglucose both prevented changes to mitochondria and suppressed RCC CD8+ TIL activation and function. These data show that CD28 costimulation can restore RCC CD8+ TIL metabolism and function through rescue of T cell glycolysis that supports mitochondrial mass and activity.

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