Molecular recognition and activation of the prostacyclin receptor by anti-pulmonary arterial hypertension drugs

被引:1
|
作者
Wang, James Jiqi [1 ,2 ,3 ]
Jin, Sanshan [4 ,5 ]
Zhang, Heng [1 ]
Xu, Youwei [1 ]
Hu, Wen [1 ]
Jiang, Yi [4 ,5 ]
Chen, Chen [2 ,3 ]
Wang, Dao Wen [2 ,3 ]
Xu, H. Eric [1 ,5 ,6 ]
Wu, Canrong [1 ]
机构
[1] Chinese Acad Sci, Shanghai Inst Mat Med, State Key Lab Drug Res, Shanghai 201203, Peoples R China
[2] Huazhong Univ Sci & Technol, Dept Internal Med, Div Cardiol, Wuhan 430000, Peoples R China
[3] Huazhong Univ Sci & Technol, Tongji Hosp, Tongji Med Coll, Hubei Key Lab Genet & Mol Mech Cardiol Disorders, Wuhan 430000, Peoples R China
[4] Lingang Lab, Shanghai 200031, Peoples R China
[5] ShanghaiTech Univ, Sch Life Sci & Technol, Shanghai 201210, Peoples R China
[6] Univ Chinese Acad Sci, Beijing 100049, Peoples R China
基金
中国博士后科学基金; 中国国家自然科学基金; 国家重点研发计划;
关键词
CRYO-EM STRUCTURE; PROSTANOID RECEPTORS; MANAGEMENT; SOFTWARE; SURVIVAL; THERAPY; BINDING;
D O I
10.1126/sciadv.adk5184
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
The prostacyclin (PGI(2)) receptor (IP) is a G(s)-coupled receptor associated with blood pressure regulation, allergy, and inflammatory response. It is a main therapeutic target for pulmonary arterial hypertension (PAH) and several other diseases. Here we report cryo-electron microscopy (cryo-EM) structures of the human IP-G(s) complex bound with two anti-PAH drugs, treprostinil and MRE-269 (active form of selexipag), at global resolutions of 2.56 and 2.41 angstrom, respectively. These structures revealed distinct features governing IP ligand binding, receptor activation, and G protein coupling. Moreover, comparison of the activated IP structures uncovered the mechanism and key residues that determine the superior selectivity of MRE-269 over treprostinil. Combined with molecular docking and functional studies, our structures provide insight into agonist selectivity, ligand recognition, receptor activation, and G protein coupling. Our results provide a structural template for further improving IP-targeting drugs to reduce off-target activation of prostanoid receptors and adverse effects.
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页数:11
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