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

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 arginin...

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Autores principales: Crump, Nicholas T., Hadjinicolaou, Andreas V., Xia, Meng, Walsby-Tickle, John, Gileadi, Uzi, Chen, Ji-Li, Setshedi, Mashiko, Olsen, Lars R., Lau, I-Jun, Godfrey, Laura, Quek, Lynn, Yu, Zhanru, Ballabio, Erica, Barnkob, Mike B., Napolitani, Giorgio, Salio, Mariolina, Koohy, Hashem, Kessler, Benedikt M., Taylor, Stephen, Vyas, Paresh, McCullagh, James S.O., Milne, Thomas A., Cerundolo, Vincenzo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8131582/
https://www.ncbi.nlm.nih.gov/pubmed/33979616
http://dx.doi.org/10.1016/j.celrep.2021.109101
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author Crump, Nicholas T.
Hadjinicolaou, Andreas V.
Xia, Meng
Walsby-Tickle, John
Gileadi, Uzi
Chen, Ji-Li
Setshedi, Mashiko
Olsen, Lars R.
Lau, I-Jun
Godfrey, Laura
Quek, Lynn
Yu, Zhanru
Ballabio, Erica
Barnkob, Mike B.
Napolitani, Giorgio
Salio, Mariolina
Koohy, Hashem
Kessler, Benedikt M.
Taylor, Stephen
Vyas, Paresh
McCullagh, James S.O.
Milne, Thomas A.
Cerundolo, Vincenzo
author_facet Crump, Nicholas T.
Hadjinicolaou, Andreas V.
Xia, Meng
Walsby-Tickle, John
Gileadi, Uzi
Chen, Ji-Li
Setshedi, Mashiko
Olsen, Lars R.
Lau, I-Jun
Godfrey, Laura
Quek, Lynn
Yu, Zhanru
Ballabio, Erica
Barnkob, Mike B.
Napolitani, Giorgio
Salio, Mariolina
Koohy, Hashem
Kessler, Benedikt M.
Taylor, Stephen
Vyas, Paresh
McCullagh, James S.O.
Milne, Thomas A.
Cerundolo, Vincenzo
author_sort Crump, Nicholas T.
collection PubMed
description 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.
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spelling pubmed-81315822021-05-21 Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation Crump, Nicholas T. Hadjinicolaou, Andreas V. Xia, Meng Walsby-Tickle, John Gileadi, Uzi Chen, Ji-Li Setshedi, Mashiko Olsen, Lars R. Lau, I-Jun Godfrey, Laura Quek, Lynn Yu, Zhanru Ballabio, Erica Barnkob, Mike B. Napolitani, Giorgio Salio, Mariolina Koohy, Hashem Kessler, Benedikt M. Taylor, Stephen Vyas, Paresh McCullagh, James S.O. Milne, Thomas A. Cerundolo, Vincenzo Cell Rep Article 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. Cell Press 2021-05-11 /pmc/articles/PMC8131582/ /pubmed/33979616 http://dx.doi.org/10.1016/j.celrep.2021.109101 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Crump, Nicholas T.
Hadjinicolaou, Andreas V.
Xia, Meng
Walsby-Tickle, John
Gileadi, Uzi
Chen, Ji-Li
Setshedi, Mashiko
Olsen, Lars R.
Lau, I-Jun
Godfrey, Laura
Quek, Lynn
Yu, Zhanru
Ballabio, Erica
Barnkob, Mike B.
Napolitani, Giorgio
Salio, Mariolina
Koohy, Hashem
Kessler, Benedikt M.
Taylor, Stephen
Vyas, Paresh
McCullagh, James S.O.
Milne, Thomas A.
Cerundolo, Vincenzo
Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
title Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
title_full Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
title_fullStr Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
title_full_unstemmed Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
title_short Chromatin accessibility governs the differential response of cancer and T cells to arginine starvation
title_sort chromatin accessibility governs the differential response of cancer and t cells to arginine starvation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8131582/
https://www.ncbi.nlm.nih.gov/pubmed/33979616
http://dx.doi.org/10.1016/j.celrep.2021.109101
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