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Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation

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Title: Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
Authors: Crump, NT
Hadjinicolaou, A
Xia, M
Walsby-Tickle, J
Gileadi, U
Chen, J-L
Setshedi, M
Olsen, LR
Lau, I-J
Godfrey, L
Quek, L
Yu, Z
Ballabio, E
Barnkob, MB
Napolitani, G
Salio, M
Koohy, H
Kessler, BM
Taylor, S
Vyas, P
McCullagh, JSO
Milne, TA
Cerundolo, V
Item Type: Journal Article
Abstract: Depleting the microenvironment of important nutrients such as arginine is a key strategy for immune evasion by cancer cells. Many tumors overexpress arginase, but it is unclear how these cancers, but not T cells, tolerate arginine depletion. In this study, we show that tumor cells synthesize arginine from citrulline by upregulating argininosuccinate synthetase 1 (ASS1). Under arginine starvation, ASS1 transcription is induced by ATF4 and CEBPβ binding to an enhancer within ASS1. T cells cannot induce ASS1, despite the presence of active ATF4 and CEBPβ, as the gene is repressed. Arginine starvation drives global chromatin compaction and repressive histone methylation, which disrupts ATF4/CEBPβ binding and target gene transcription. We find that T cell activation is impaired in arginine-depleted conditions, with significant metabolic perturbation linked to incomplete chromatin remodeling and misregulation of key genes. Our results highlight a T cell behavior mediated by nutritional stress, exploited by cancer cells to enable pathological immune evasion.
Issue Date: 11-May-2021
Date of Acceptance: 16-Apr-2021
URI: http://hdl.handle.net/10044/1/109197
DOI: 10.1016/j.celrep.2021.109101
ISSN: 2211-1247
Publisher: Elsevier
Journal / Book Title: Cell Reports
Volume: 35
Issue: 6
Copyright Statement: © 2021 The Author(s). This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/)
Publication Status: Published
Article Number: 109101
Online Publication Date: 2021-05-11
Appears in Collections:Department of Immunology and Inflammation



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