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. 2020 Dec;21(12):1540-1551.
doi: 10.1038/s41590-020-0793-3. Epub 2020 Oct 5.

Disturbed mitochondrial dynamics in CD8+ TILs reinforce T cell exhaustion

Yi-Ru Yu #  1   2 Hana Imrichova #  3 Haiping Wang  1   2 Tung Chao  1   2 Zhengtao Xiao  4 Min Gao  5 Marcela Rincon-Restrepo  1   2 Fabien Franco  1   2 Raphael Genolet  1   2 Wan-Chen Cheng  1   2 Camilla Jandus  1   2 George Coukos  1   2 Yi-Fan Jiang  6 Jason W Locasale  4 Alfred Zippelius  7   8 Pu-Ste Liu  9 Li Tang  5 Christoph Bock  3   10 Nicola Vannini  1   2 Ping-Chih Ho  11   12
Affiliations

Disturbed mitochondrial dynamics in CD8+ TILs reinforce T cell exhaustion

Yi-Ru Yu et al. Nat Immunol. 2020 Dec.

Abstract

The metabolic challenges present in tumors attenuate the metabolic fitness and antitumor activity of tumor-infiltrating T lymphocytes (TILs). However, it remains unclear whether persistent metabolic insufficiency can imprint permanent T cell dysfunction. We found that TILs accumulated depolarized mitochondria as a result of decreased mitophagy activity and displayed functional, transcriptomic and epigenetic characteristics of terminally exhausted T cells. Mechanistically, reduced mitochondrial fitness in TILs was induced by the coordination of T cell receptor stimulation, microenvironmental stressors and PD-1 signaling. Enforced accumulation of depolarized mitochondria with pharmacological inhibitors induced epigenetic reprogramming toward terminal exhaustion, indicating that mitochondrial deregulation caused T cell exhaustion. Furthermore, supplementation with nicotinamide riboside enhanced T cell mitochondrial fitness and improved responsiveness to anti-PD-1 treatment. Together, our results reveal insights into how mitochondrial dynamics and quality orchestrate T cell antitumor responses and commitment to the exhaustion program.

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