Distinct inactive conformations of the dopamine D2 and D3 receptors correspond to different extents of inverse agonism

J Robert Lane; Ara M Abramyan; Pramisha Adhikari; Alastair C Keen; Kuo-Hao Lee; Julie Sanchez; Ravi Kumar Verma; Herman D Lim; Hideaki Yano; Jonathan A Javitch; Lei Shi

doi:10.7554/eLife.52189

eLife (Jan 2020)

Distinct inactive conformations of the dopamine D2 and D3 receptors correspond to different extents of inverse agonism

J Robert Lane,
Ara M Abramyan,
Pramisha Adhikari,
Alastair C Keen,
Kuo-Hao Lee,
Julie Sanchez,
Ravi Kumar Verma,
Herman D Lim,
Hideaki Yano,
Jonathan A Javitch,
Lei Shi

Affiliations

J Robert Lane: Division of Pharmacology, Physiology and Neuroscience, School of Life Sciences, Queen’s Medical Centre, University of Nottingham, Nottingham, United Kingdom; Centre of Membrane Protein and Receptors, Universities of Birmingham and Nottingham, Nottingham, United Kingdom
Ara M Abramyan: Computational Chemistry and Molecular Biophysics Unit, National Institute on Drug Abuse - Intramural Research Program, National Institutes of Health, Baltimore, United States
Pramisha Adhikari: Computational Chemistry and Molecular Biophysics Unit, National Institute on Drug Abuse - Intramural Research Program, National Institutes of Health, Baltimore, United States
Alastair C Keen: Division of Pharmacology, Physiology and Neuroscience, School of Life Sciences, Queen’s Medical Centre, University of Nottingham, Nottingham, United Kingdom; Centre of Membrane Protein and Receptors, Universities of Birmingham and Nottingham, Nottingham, United Kingdom; Drug Discovery Biology, Department of Pharmacology and Medicinal Chemistry, Monash Institute of Pharmaceutical Sciences, Monash University, Parkville, Australia
Kuo-Hao Lee: Computational Chemistry and Molecular Biophysics Unit, National Institute on Drug Abuse - Intramural Research Program, National Institutes of Health, Baltimore, United States
Julie Sanchez: Division of Pharmacology, Physiology and Neuroscience, School of Life Sciences, Queen’s Medical Centre, University of Nottingham, Nottingham, United Kingdom; Centre of Membrane Protein and Receptors, Universities of Birmingham and Nottingham, Nottingham, United Kingdom
Ravi Kumar Verma: Computational Chemistry and Molecular Biophysics Unit, National Institute on Drug Abuse - Intramural Research Program, National Institutes of Health, Baltimore, United States
Herman D Lim: Drug Discovery Biology, Department of Pharmacology and Medicinal Chemistry, Monash Institute of Pharmaceutical Sciences, Monash University, Parkville, Australia
Hideaki Yano: Computational Chemistry and Molecular Biophysics Unit, National Institute on Drug Abuse - Intramural Research Program, National Institutes of Health, Baltimore, United States
Jonathan A Javitch: Department of Psychiatry, Vagelos College of Physicians and Surgeons, Columbia University, New York, United States; Division of Molecular Therapeutics, New York State Psychiatric Institute, New York, United States; Department of Pharmacology, Vagelos College of Physicians and Surgeons, Columbia University, New York, United States
Lei Shi: ORCiD; Computational Chemistry and Molecular Biophysics Unit, National Institute on Drug Abuse - Intramural Research Program, National Institutes of Health, Baltimore, United States

DOI: https://doi.org/10.7554/eLife.52189
Journal volume & issue: Vol. 9

Abstract

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By analyzing and simulating inactive conformations of the highly homologous dopamine D2 and D3 receptors (D2R and D3R), we find that eticlopride binds D2R in a pose very similar to that in the D3R/eticlopride structure but incompatible with the D2R/risperidone structure. In addition, risperidone occupies a sub-pocket near the Na+ binding site, whereas eticlopride does not. Based on these findings and our experimental results, we propose that the divergent receptor conformations stabilized by Na+-sensitive eticlopride and Na+-insensitive risperidone correspond to different degrees of inverse agonism. Moreover, our simulations reveal that the extracellular loops are highly dynamic, with spontaneous transitions of extracellular loop 2 from the helical conformation in the D2R/risperidone structure to an extended conformation similar to that in the D3R/eticlopride structure. Our results reveal previously unappreciated diversity and dynamics in the inactive conformations of D2R. These findings are critical for rational drug discovery, as limiting a virtual screen to a single conformation will miss relevant ligands.

Published in eLife

ISSN: 2050-084X (Online)
Publisher: eLife Sciences Publications Ltd
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General)
Website: https://elifesciences.org

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