Lysine vitcylation is a vitamin C-derived protein modification that enhances STAT1-mediated immune response.

赖氨酸维生素C化是一种维生素C衍生的蛋白质修饰,可增强STAT1介导的免疫反应

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作者:He Xiadi, Wang Qiwei, Cheng Xin, Wang Weihua, Li Yutong, Nan Yabing, Wu Jiang, Xiu Bingqiu, Jiang Tao, Bergholz Johann S, Gu Hao, Chen Fuhui, Fan Guangjian, Sun Lianhui, Xie Shaozhen, Zou Junjie, Lin Sheng, Wei Yun, Lee James, Asara John M, Zhang Ke, Cantley Lewis C, Zhao Jean J
Vitamin C (vitC) is essential for health and shows promise in treating diseases like cancer, yet its mechanisms remain elusive. Here, we report that vitC directly modifies lysine residues to form "vitcyl-lysine"-a process termed vitcylation. Vitcylation occurs in a dose-, pH-, and sequence-dependent manner in both cell-free systems and living cells. Mechanistically, vitC vitcylates signal transducer and activator of transcription-1 (STAT1)- lysine-298 (K298), impairing its interaction with T cell protein-tyrosine phosphatase (TCPTP) and preventing STAT1-Y701 dephosphorylation. This leads to enhanced STAT1-mediated interferon (IFN) signaling in tumor cells, increased major histocompatibility complex (MHC)/human leukocyte antigen (HLA) class I expression, and activation of anti-tumor immunity in vitro and in vivo. The discovery of vitcylation as a distinctive post-translational modification provides significant insights into vitC's cellular function and therapeutic potential, opening avenues for understanding its biological effects and applications in disease treatment.

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