DWL-4-140: A allene small molecule targeting STING that alleviates lupus-like phenotype in Trex1-/- mice

DWL-4-140:一种靶向 STING 的丙二烯小分子,可缓解 Trex1-/- 小鼠的狼疮样表型

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作者:Hekang Du, Meng Kou, Weili Deng, Xueyuan Zhou, Xiaoxiong Zhang, Zhengrong Huang, Bowen Ren, Xingting Cai, Shan Xu, Yu Chen, Lizhu Chen, Chuanben Chen, Hongli Bao, Qi Chen, Daliang Li

Abstract

The innate immune system plays a critical role in the host response against pathogenic microbial infection. However, aberrant activation of the innate immune pathways is a characteristic feature of various diseases. Thus, targeted drugs must be developed based on the understanding of the innate immune signaling pathways. This study demonstrated that an allene small molecule (DWL-4-140) can efficiently and selectively exert regulatory effects on the stimulator of interferon genes (STING), resulting in the downregulation of DNA-induced interferon responses. Mechanistically, DWL-4-140 targeted the cyclized nucleotide-binding domain (CBD) of STING, inhibiting the assembly of the STING multimeric complex and the recruitment of downstream signaling mediators. In addition to downregulating the 10-carboxymethyl-9-acridanone-induced production of inflammatory factors, DWL-4-140 alleviated the pathological features of Trex1 deletion-induced lupus in mice. Thus, this study demonstrated that DWL-4-140 pharmacologically inhibits STING with potential therapeutic applications in auto-inflammatory diseases.

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