化学
细胞保护
结肠炎
敌手
核出口信号
药理学
基因敲除
细胞生物学
药物发现
癌症研究
生物化学
细胞核
受体
内科学
生物
医学
氧化应激
细胞凋亡
基因
作者
Xibao Tian,Jiali Gao,Meishuo Liu,Yuqin Lei,Fangjun Wang,Jin Chen,Peng Chu,Jiujiao Gao,Feida Long,Minzhi Liang,Xiangyu Long,Huiying Chu,Cuixia Liu,Xueliang Li,Qingxiang Sun,Guohui Li,Yongliang Yang
标识
DOI:10.1021/acs.jmedchem.9b01663
摘要
Exportin-1 (also named as CRM1) plays a prominent role in autoimmune disorders and has emerged as a potential therapeutic target for colitis. Here we report on the rational structure-based discovery of a small-molecule antagonist of exportin-1, LFS-829, with low-range nanomolar activities. The co-crystallographic structure, surface plasmon resonance binding assay, and cell-based phenotypic nuclear export functional assay validated that exportin-1 is a key target of LFS-829. Moreover, we demonstrated that the C528S mutation or the knockdown on exportin-1 can abolish the cellular activities of LFS-829. Strikingly, oral administration of LFS-829 can significantly reverse the pathological features of colitis model mice. We revealed that LFS-829 can attenuate dual NF-κB signaling and the Nrf2 cytoprotection pathway via targeting exportin-1 in colitis mice. Moreover, LFS-829 has a very low risk of cardiotoxicity and acute toxicity. Therefore, LFS-829 holds great promise for the treatment of colitis and may warrant translation for use in clinical trials.
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