Occupancy of dopamine D2 and D3 receptors by a novel D3 partial agonist BP1.4979: a [11C]-(+)-PHNO PET study in humans

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作者
Patricia Di Ciano
Esmaeil Mansouri
Junchao Tong
Alan A. Wilson
Sylvain Houle
Isabelle Boileau
Thierry Duvauchelle
Philippe Robert
Jean Charles Schwartz
Bernard Le Foll
机构
[1] Centre for Addiction and Mental Health,Translational Addiction Research Laboratory
[2] Centre for Addiction and Mental Health,Addiction Imaging Research Group
[3] University of Toronto,Institute of Medical Sciences
[4] Centre for Addiction and Mental Health,Preclinical imaging, Research Imaging Centre
[5] Centre for Addiction and Mental Health,Human Brain Laboratory, Research Imaging Centre
[6] Centre for Addiction and Mental Health,Campbell Family Mental Health Research Institute
[7] Centre for Addiction and Mental Health,Research Imaging Centre
[8] University of Toronto,Department of Psychiatry
[9] Centre for Addiction and Mental Health,Addiction Program
[10] Bioprojet,Department of Pharmacology and Toxicology
[11] Bioprojet Biotech,undefined
[12] University of Toronto,undefined
来源
Neuropsychopharmacology | 2019年 / 44卷
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摘要
There has been considerable interest in the development of dopamine D3 receptor (DRD3) partial agonists and antagonists for the treatment of substance use disorders. Pre-clinical evidence overwhelmingly supports the use of these drugs, but translation to humans has remained elusive due to the lack of selective compounds that are suitable for use in humans. Although it has been established for full antagonists, little in vivo occupancy data are available with DRD3 partial agonists. Here we investigate for the first time in healthy controls, the in vivo occupancy of a novel D3 partial agonist (BP1.4979) at the DRD3 and DRD2. Participants received either a single dose (1, 3, 10 or 30 mg) or a subchronic regimen (5–7 days, q.d. or b.i.d) of BP1.4979, with the last dose given at 1, 12 or 24 h prior to scanning with [11C]-(+)-PHNO. Single and subchronic administration of BP1.4979 dose-dependently occupied the DRD3 and DRD2, and this occupancy was preferential for the DRD3, notably at longer time points after administration of BP1.4979. Also consistent with preference for the DRD3, prolactin levels were minimally increased, and no subjective effects of BP1.4979 were reported. Serum levels of BP1.4979 were higher than its active metabolite, BP1.6239, while no notable increases in the inactive metabolite, BP1.6197, were found. These findings indicate the range of doses that can be used to occupy selectively the DRD3 over the DRD2 with BP1.4979 and speak to the use of in vivo imaging approaches in dose finding studies.
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页码:1284 / 1290
页数:6
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