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首页> 外文期刊>Journal of Medicinal Chemistry >High Affinity Dopamine D-3 Receptor (D3R)-Selective Antagonists Attenuate Heroin Self-Administration in Wild-Type but not D3R Knockout Mice
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High Affinity Dopamine D-3 Receptor (D3R)-Selective Antagonists Attenuate Heroin Self-Administration in Wild-Type but not D3R Knockout Mice

机译:高亲和力多巴胺D-3受体(D3R)选择性拮抗剂在野生型中可减轻海洛因的自我给药,但对D3R敲除小鼠则无作用。

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摘要

The dopamine D-3 receptor (D3R) is a promising target for the development of pharmacotherapeutics to treat substance use disorders. Several D3R-selective antagonists are effective in animal models of drug abuse, especially in models of relapse. Nevertheless, poor bioavailability, metabolic instability, and/or predicted toxicity have impeded success in translating these drug candidates to clinical use. Herein, we report a series of D3R-selective 4-phenylpiperazines with improved metabolic stability. A subset of these compounds was evaluated for D3R functional efficacy and off-target binding at selected 5-HT receptor subtypes, where significant overlap in SAR with D3R has been observed. Several high affinity D3R antagonists, including compounds 16 (K-i = 0.12 nM) and 32 (K-i = 0.35 nM), showed improved metabolic stability compared to the parent compound, PG648 (6). Notably, 16 and the classic D3R antagonist SB277011A (2) were effective in reducing selfadministration of heroin in wild-type but not D3R knockout mice.
机译:多巴胺D-3受体(D3R)是用于治疗药物滥用的药物治疗学的有希望的目标。几种D3R选择性拮抗剂在药物滥用的动物模型中有效,尤其是在复发模型中。然而,不良的生物利用度,代谢不稳定性和/或预期的毒性阻碍了将这些候选药物转化为临床用途的成功。在这里,我们报告一系列具有改善的代谢稳定性的D3R选择性4-苯基哌嗪。评估了这些化合物的一个子集的D3R功能功效和所选5-HT受体亚型的脱靶结合,其中观察到SAR与D3R显着重叠。与母体化合物PG648相比,几种高亲和力D3R拮抗剂,包括化合物16(K-1 = 0.12 nM)和32(K-1 = 0.35 nM),显示出更高的代谢稳定性。值得注意的是,16和经典的D3R拮抗剂SB277011A(2)在减少野生型海洛因而不是D3R敲除小鼠中可有效减少海洛因的自我给药。

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