Structure-Based Discovery of a Subtype-Selective Inhibitor Targeting a Transient Receptor Potential Vanilloid Channel

被引:15
|
作者
Chai, Hao [1 ,2 ,5 ]
Cheng, Xi [1 ,2 ]
Zhou, Bin [1 ,2 ,5 ]
Zhao, Lifen [1 ,2 ]
Lin, Xianhua [3 ,4 ]
Huang, Dongping [3 ,4 ]
Lu, Weiqiang [3 ,4 ]
Lv, Hao [1 ,2 ,5 ]
Tang, Feng [1 ,2 ]
Zhang, Qiansen [3 ,4 ]
Huang, Wei [1 ,2 ,5 ]
Li, Yang [1 ,2 ,5 ]
Yang, Huaiyu [3 ,4 ]
机构
[1] Chinese Acad Sci, Shanghai Inst Mat Med, State Key Lab Drug Res, 555 Zuchongzhi Rd, Shanghai 201203, Peoples R China
[2] Chinese Acad Sci, Shanghai Inst Mat Med, CAS Key Lab Receptor Res, 555 Zuchongzhi Rd, Shanghai 201203, Peoples R China
[3] East China Normal Univ, Shanghai Key Lab Regulatory Biol, Inst Biomed Sci, 500 Dongchuan Rd, Shanghai 200241, Peoples R China
[4] East China Normal Univ, Sch Life Sci, 500 Dongchuan Rd, Shanghai 200241, Peoples R China
[5] Univ Chinese Acad Sci, 19A Yuquan Rd, Beijing 100049, Peoples R China
基金
中国国家自然科学基金;
关键词
LYSOPHOSPHATIDIC ACID; TRPV1; STRUCTURES; CELL-MIGRATION; ACTIVATION; AUTOTAXIN; MECHANISMS; TRANSITION; EFFICIENT; DYNAMICS; DOCKING;
D O I
10.1021/acs.jmedchem.8b01496
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Discovery of potent selective inhibitors targeting a protein from a highly conserved family is challenging. Using a strategy combining structural and evolutionary information, we discovered transient receptor potential (TRP) subtype-selective inhibitors (transient receptor potential vanilloid type 2 (TRPV2) inhibitors). We unveiled three ligand-binding sites of TRPV2 and compounds that bind to these sites. Structural optimization of the best-hit compound provided a potent selective TRPV2 inhibitor, SET2. The molecular basis and subtype-selective inhibition mechanism were quantitatively characterized and experimentally verified. Then, as an effective chemical probe, SET2 was used to investigate the function role of TRPV2. SET2-induced inhibition of TRPV2 reduced prostate cancer migration, which indicated TRPV2 as an antimetastasis therapeutic target. In addition, functional assays suggested that TRPV2 was coupled to a validated metastasis mediator, LPAR1. The discovery of the potent selective inhibitor potentially leads to novel avenues for pharmacological applications and therapeutic development targeting the TRPV2 channel.
引用
收藏
页码:1373 / 1384
页数:12
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