刺
干扰素基因刺激剂
小分子
先天免疫系统
棕榈酰化
炎症体
细胞生物学
干扰素
生物
跨膜蛋白
化学
免疫系统
半胱氨酸
炎症
生物化学
免疫学
受体
工程类
酶
航空航天工程
作者
Simone M. Haag,Muhammet F. Gülen,Luc Reymond,Antoine Gibelin,Laurence Abrami,Alexiane Decout,Michaël Heymann,F. Gisou van der Goot,Gerardo Turcatti,Rayk Behrendt,Andrea Ablasser
出处
期刊:Nature
[Springer Nature]
日期:2018-07-01
卷期号:559 (7713): 269-273
被引量:731
标识
DOI:10.1038/s41586-018-0287-8
摘要
Aberrant activation of innate immune pathways is associated with a variety of diseases. Progress in understanding the molecular mechanisms of innate immune pathways has led to the promise of targeted therapeutic approaches, but the development of drugs that act specifically on molecules of interest remains challenging. Here we report the discovery and characterization of highly potent and selective small-molecule antagonists of the stimulator of interferon genes (STING) protein, which is a central signalling component of the intracellular DNA sensing pathway1,2. Mechanistically, the identified compounds covalently target the predicted transmembrane cysteine residue 91 and thereby block the activation-induced palmitoylation of STING. Using these inhibitors, we show that the palmitoylation of STING is essential for its assembly into multimeric complexes at the Golgi apparatus and, in turn, for the recruitment of downstream signalling factors. The identified compounds and their derivatives reduce STING-mediated inflammatory cytokine production in both human and mouse cells. Furthermore, we show that these small-molecule antagonists attenuate pathological features of autoinflammatory disease in mice. In summary, our work uncovers a mechanism by which STING can be inhibited pharmacologically and demonstrates the potential of therapies that target STING for the treatment of autoinflammatory disease.
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