作者
Henry Kurniawan, Davide G Franchina, Luana Guerra, Lynn Bonetti, Leticia Soriano-Baguet, Melanie Grusdat, Lisa Schlicker, Oliver Hunewald, Catherine Dostert, Myriam P Merz, Carole Binsfeld, Gordon S Duncan, Sophie Farinelle, Yannic Nonnenmacher, Jillian Haight, Dennis Das Gupta, Anouk Ewen, Rabia Taskesen, Rashi Halder, Ying Chen, Christian Jäger, Markus Ollert, Paul Wilmes, Vasilis Vasiliou, Isaac S Harris, Christiane B Knobbe-Thomsen, Jonathan D Turner, Tak W Mak, Michael Lohoff, Johannes Meiser, Karsten Hiller, Dirk Brenner
发表日期
2020/5/5
期刊
Cell metabolism
卷号
31
期号
5
页码范围
920-936. e7
出版商
Elsevier
简介
Regulatory T cells (Tregs) maintain immune homeostasis and prevent autoimmunity. Serine stimulates glutathione (GSH) synthesis and feeds into the one-carbon metabolic network (1CMet) essential for effector T cell (Teff) responses. However, serine's functions, linkage to GSH, and role in stress responses in Tregs are unknown. Here, we show, using mice with Treg-specific ablation of the catalytic subunit of glutamate cysteine ligase (Gclc), that GSH loss in Tregs alters serine import and synthesis and that the integrity of this feedback loop is critical for Treg suppressive capacity. Although Gclc ablation does not impair Treg differentiation, mutant mice exhibit severe autoimmunity and enhanced anti-tumor responses. Gclc-deficient Tregs show increased serine metabolism, mTOR activation, and proliferation but downregulated FoxP3. Limitation of cellular serine in vitro and in vivo restores FoxP3 expression and …
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H Kurniawan, DG Franchina, L Guerra, L Bonetti… - Cell metabolism, 2020