Remodeling Translation Primes CD8+ T-cell Antitumor Immunity

Katie E. Hurst; Kiley A. Lawrence; Rob A. Robino; Lauren E. Ball; Dongjun Chung; Jessica E. Thaxton

doi:10.1158/2326-6066.cir-19-0516

Remodeling Translation Primes CD8+ T-cell Antitumor Immunity

Katie E. Hurst(Medical University of South Carolina), Kiley A. Lawrence(Medical University of South Carolina), Rob A. Robino(Medical University of South Carolina), Lauren E. Ball(Medical University of South Carolina), Dongjun Chung(Medical University of South Carolina), Jessica E. Thaxton(Medical University of South Carolina)

Cancer Immunology Research

February 19, 2020

10.1158/2326-6066.cir-19-0516

Cited by 22Open Access

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Abstract

Abstract The requisites for protein translation in T cells are poorly understood and how translation shapes the antitumor efficacy of T cells is unknown. Here we demonstrated that IL15-conditioned T cells were primed by the metabolic energy sensor AMP-activated protein kinase to undergo diminished translation relative to effector T cells. However, we showed that IL15-conditioned T cells exhibited a remarkable capacity to enhance their protein translation in tumors, which effector T cells were unable to duplicate. Studying the modulation of translation for applications in cancer immunotherapy revealed that direct ex vivo pharmacologic inhibition of translation elongation primed robust T-cell antitumor immunity. Our work elucidates that altering protein translation in CD8+ T cells can shape their antitumor capability.

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