Hit-to-Lead Optimization of the Natural Product Oridonin as Novel NLRP3 Inflammasome Inhibitors with Potent Anti-Inflammation Activity

被引:7
作者
He, Chen [1 ,2 ]
Liu, Junkai [1 ,2 ]
Li, Junda [1 ,2 ]
Wu, Hongyu [1 ,2 ]
Jiao, Chenyang [2 ,3 ]
Ze, Xiaotong [1 ,2 ]
Xu, Shengtao [1 ,2 ]
Zhu, Zheying [4 ]
Guo, Wenjie [3 ]
Xu, Jinyi [1 ,2 ]
Yao, Hong [1 ,2 ]
机构
[1] China Pharmaceut Univ, Sch Pharm, State Key Lab Nat Med, Nanjing 211198, Jiangsu, Peoples R China
[2] China Pharmaceut Univ, Sch Pharm, Dept Med Chem, Nanjing 211198, Jiangsu, Peoples R China
[3] Nanjing Univ, Sch Life Sci, State Key Lab Pharmaceut Biotechnol, Nanjing 210093, Peoples R China
[4] Univ Nottingham, Sch Pharm, Div Mol Therapeut & Formulat, Nottingham NG7 2RD, England
来源
JOURNAL OF MEDICINAL CHEMISTRY | 2024年 / 67卷 / 11期
基金
中国国家自然科学基金;
关键词
NF-KAPPA-B; NALP3; INFLAMMASOME; ACTIVATION; MECHANISM; IDENTIFICATION; IL-1-BETA; CASPASE-8; CRYSTALS; DISEASE; INNATE;
D O I
10.1021/acs.jmedchem.4c00504
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Targeting NLRP3 inflammasome with inhibitors is a novel strategy for NLRP3-driven diseases. Herein, hit compound 5 possessing an attractive skeleton was identified from our in-house database of oridonin, and then a potential lead compound 32 was obtained by optimization of 5, displaying two-digit nanomolar inhibition on NLRP3. Moreover, compound 32 showed enhanced safety index (SI) relative to oridonin (IC50 = 77.2 vs 780.4 nM, SI = 40.5 vs 8.5) and functioned through blocking ASC oligomerization and interaction of NLRP3-ASC/NEK7, thereby suppressing NLRP3 inflammasome assembly and activation. Furthermore, diverse agonists-induced activations of NLRP3 could be impeded by compound 32 without altering NLRC4 or AIM2 inflammasome. Crucially, compound 32 possessed tolerable pharmaceutical properties and significant anti-inflammatory activity in MSU-induced gouty arthritis model. Therefore, this work enriched the SAR of NLRP3 inflammasome inhibitors and provided a potential candidate for the treatment of NLRP3-associated diseases.
引用
收藏
页码:9406 / 9430
页数:25
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