Pharmacological Actions of NGB 2904, a Selective Dopamine D3 Receptor Antagonist, in Animal Models of Drug Addiction

Zheng-Xiong Xi, Eliot L. Gardner
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引用次数: 101

Abstract

As a continuation of our work with SB-277011A, we have examined the effects of another highly elective dopamine (DA) D3 receptor antagonist, N-(4-[4-{2,3-dichlorophenyl}-1-piperazinyl]butyl)-2-fluorenylcarboxamide (NGB 2904), in animal models of addiction. Our results indicate that by systemic administration, NGB 2904 inhibits intravenous cocaine self-administration maintained under a progressive-ratio (PR) reinforcement schedule, cocaine- or cocaine cue–induced reinstatement of cocaine-seeking behavior, and cocaine- or other addictive drug-enhanced brain stimulation reward (BSR). The action of NGB 2904 on PR cocaine self-administration was long-lasting (1–2 days) after a single injection, supporting its potential use in treatment of cocaine addiction. The effects of NGB 2904 in the BSR paradigm were dose-dependent for both NGB 2904 and cocaine; that is, only lower doses of NGB 2904 were effective, and their putative antiaddiction effect could be overcome by increasing the doses of cocaine or other addictive drugs. A dopamine-dependent mechanism is proposed to explain the effects of NGB 2904 on cocaine's actions in these animal models of drug addiction. The data reviewed in this paper suggest that NGB 2904 or other D3-selective antagonists may have potential in controlling motivation for drug-taking behavior or relapse to drug-seeking behavior, but may have a limited role in antagonizing the acute rewarding effects produced by cocaine or other addictive drugs. In addition, NGB 2904 may also act as a useful tool to study the role of D3 receptors in drug addiction.

Abstract Image

选择性多巴胺D3受体拮抗剂ngb2904在药物成瘾动物模型中的药理作用
作为SB-277011A研究的延续,我们研究了另一种高度选择性多巴胺(DA) D3受体拮抗剂N-(4-[4-{2,3-二氯苯基}-1-哌嗪基]丁基)-2-氟烯基carboxamide (NGB 2904)在成瘾动物模型中的作用。我们的研究结果表明,通过系统给药,NGB 2904可以抑制在递进比例(PR)强化计划下维持的静脉可卡因自我给药,可卡因或可卡因线索诱导的可卡因寻求行为恢复,以及可卡因或其他成瘾药物增强的脑刺激奖励(BSR)。NGB 2904在单次注射后对PR可卡因自我给药的作用持续时间长(1-2天),支持其在治疗可卡因成瘾方面的潜在应用。NGB 2904在BSR范式中的作用对NGB 2904和可卡因均呈剂量依赖性;也就是说,只有低剂量的NGB 2904是有效的,其假定的抗成瘾作用可以通过增加可卡因或其他成瘾药物的剂量来克服。我们提出了一种多巴胺依赖机制来解释NGB 2904在这些药物成瘾动物模型中对可卡因作用的影响。本文综述的数据表明,NGB 2904或其他d3选择性拮抗剂可能在控制吸毒行为动机或寻求毒品行为的复发方面具有潜力,但在对抗可卡因或其他成瘾药物产生的急性奖励效应方面可能作用有限。此外,NGB 2904也可以作为研究D3受体在药物成瘾中的作用的有用工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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