Lactate Dehydrogenase Inhibition Synergizes with IL-21 to Promote CD8 T Cell Stemness and Antitumor Immunity

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2020 Mar 4

PMID 32123114

Citations 111

Authors

Dalton Hermans

Sanjivan Gautam

Juan C Garcia-Canaveras

Daniel Gromer

Suman Mitra

Rosanne Spolski

Peng Li

Stephen Christensen

Rosa Nguyen

Jian-Xin Lin

Jangsuk Oh

Ning Du

Sharon Veenbergen

Jessica Fioravanti

Risa Ebina-Shibuya

Christopher Bleck

Leonard M Neckers

Joshua D Rabinowitz

Luca Gattinoni

Warren J Leonard

Affiliations

Soon will be listed here.

Abstract

Interleukin (IL)-2 and IL-21 dichotomously shape CD8 T cell differentiation. IL-2 drives terminal differentiation, generating cells that are poorly effective against tumors, whereas IL-21 promotes stem cell memory T cells (T) and antitumor responses. Here we investigated the role of metabolic programming in the developmental differences induced by these cytokines. IL-2 promoted effector-like metabolism and aerobic glycolysis, robustly inducing lactate dehydrogenase (LDH) and lactate production, whereas IL-21 maintained a metabolically quiescent state dependent on oxidative phosphorylation. LDH inhibition rewired IL-2-induced effects, promoting pyruvate entry into the tricarboxylic acid cycle and inhibiting terminal effector and exhaustion programs, including mRNA expression of members of the NR4A family of nuclear receptors, as well as and While deletion of prevented development of cells with antitumor effector function, transient LDH inhibition enhanced the generation of memory cells capable of triggering robust antitumor responses after adoptive transfer. LDH inhibition did not significantly affect IL-21-induced metabolism but caused major transcriptomic changes, including the suppression of IL-21-induced exhaustion markers LAG3, PD1, 2B4, and TIM3. LDH inhibition combined with IL-21 increased the formation of T cells, resulting in more profound antitumor responses and prolonged host survival. These findings indicate a pivotal role for LDH in modulating cytokine-mediated T cell differentiation and underscore the therapeutic potential of transiently inhibiting LDH during adoptive T cell-based immunotherapy, with an unanticipated cooperative antitumor effect of LDH inhibition and IL-21.

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