Author
Listed:
- Cheng Zhang
(Stanford University School of Medicine)
- Yoga Srinivasan
(Cardiovascular Research Institute, University of California, San Francisco, 555 Mission Bay Boulevard South, S452P, San Francisco, California 94158, USA)
- Daniel H. Arlow
(D. E. Shaw Research)
- Juan Jose Fung
(Stanford University School of Medicine
Present addresses: ProNovus Bioscience, LLC. 544 E Weddell Drive, Sunnyvale, California 94089, USA (J.J.F.); Northeast Normal University, Changchun, Jilin 130024, China (Y.Z.).)
- Daniel Palmer
(Cardiovascular Research Institute, University of California, San Francisco, 555 Mission Bay Boulevard South, S452P, San Francisco, California 94158, USA)
- Yaowu Zheng
(Cardiovascular Research Institute, University of California, San Francisco, 555 Mission Bay Boulevard South, S452P, San Francisco, California 94158, USA
Present addresses: ProNovus Bioscience, LLC. 544 E Weddell Drive, Sunnyvale, California 94089, USA (J.J.F.); Northeast Normal University, Changchun, Jilin 130024, China (Y.Z.).)
- Hillary F. Green
(D. E. Shaw Research)
- Anjali Pandey
(Portola Pharmaceuticals, 270 East Grand Avenue)
- Ron O. Dror
(D. E. Shaw Research)
- David E. Shaw
(D. E. Shaw Research)
- William I. Weis
(Stanford University School of Medicine
Stanford University School of Medicine, 299 Campus Drive)
- Shaun R. Coughlin
(Cardiovascular Research Institute, University of California, San Francisco, 555 Mission Bay Boulevard South, S452P, San Francisco, California 94158, USA)
- Brian K. Kobilka
(Stanford University School of Medicine)
Abstract
Protease-activated receptor 1 (PAR1) is the prototypical member of a family of G-protein-coupled receptors that mediate cellular responses to thrombin and related proteases. Thrombin irreversibly activates PAR1 by cleaving the amino-terminal exodomain of the receptor, which exposes a tethered peptide ligand that binds the heptahelical bundle of the receptor to affect G-protein activation. Here we report the 2.2-Å-resolution crystal structure of human PAR1 bound to vorapaxar, a PAR1 antagonist. The structure reveals an unusual mode of drug binding that explains how a small molecule binds virtually irreversibly to inhibit receptor activation by the tethered ligand of PAR1. In contrast to deep, solvent-exposed binding pockets observed in other peptide-activated G-protein-coupled receptors, the vorapaxar-binding pocket is superficial but has little surface exposed to the aqueous solvent. Protease-activated receptors are important targets for drug development. The structure reported here will aid the development of improved PAR1 antagonists and the discovery of antagonists to other members of this receptor family.
Suggested Citation
Cheng Zhang & Yoga Srinivasan & Daniel H. Arlow & Juan Jose Fung & Daniel Palmer & Yaowu Zheng & Hillary F. Green & Anjali Pandey & Ron O. Dror & David E. Shaw & William I. Weis & Shaun R. Coughlin & , 2012.
"High-resolution crystal structure of human protease-activated receptor 1,"
Nature, Nature, vol. 492(7429), pages 387-392, December.
Handle:
RePEc:nat:nature:v:492:y:2012:i:7429:d:10.1038_nature11701
DOI: 10.1038/nature11701
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Cited by:
- Yang Yang & Hye Jin Kang & Ruogu Gao & Jingjing Wang & Gye Won Han & Jeffrey F. DiBerto & Lijie Wu & Jiahui Tong & Lu Qu & Yiran Wu & Ryan Pileski & Xuemei Li & Xuejun Cai Zhang & Suwen Zhao & Terry K, 2023.
"Structural insights into the human niacin receptor HCA2-Gi signalling complex,"
Nature Communications, Nature, vol. 14(1), pages 1-11, December.
- Song-Meng Wang & Yan-Fang Wang & Liping Huang & Li-Shuo Zheng & Hao Nian & Yu-Tao Zheng & Huan Yao & Wei Jiang & Xiaoping Wang & Liu-Pan Yang, 2023.
"Chiral recognition of neutral guests by chiral naphthotubes with a bis-thiourea endo-functionalized cavity,"
Nature Communications, Nature, vol. 14(1), pages 1-9, December.
- Shota Suzuki & Kotaro Tanaka & Kouki Nishikawa & Hiroshi Suzuki & Atsunori Oshima & Yoshinori Fujiyoshi, 2023.
"Structural basis of hydroxycarboxylic acid receptor signaling mechanisms through ligand binding,"
Nature Communications, Nature, vol. 14(1), pages 1-13, December.
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