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非依赖海洛因和依赖海洛因的恒河猴在海洛因与食物之间的选择:纳洛酮、丁丙诺啡和美沙酮的作用

Choice between heroin and food in nondependent and heroin-dependent rhesus monkeys: effects of naloxone, buprenorphine, and methadone.

作者信息

Negus S Stevens

机构信息

Alcohol and Drug Abuse Research Center, Harvard Medical School, McLean Hospital, 115 Mill Street, Belmont, MA 02178-9106, USA.

出版信息

J Pharmacol Exp Ther. 2006 May;317(2):711-23. doi: 10.1124/jpet.105.095380. Epub 2006 Feb 2.

Abstract

Several medications are approved for treatment of opiate abuse, but determinants of their clinical effectiveness are not completely understood. States of opiate dependence or withdrawal may constitute one important set of determinants. To test this hypothesis, the effects of naloxone, buprenorphine, and methadone were assessed on choice between heroin and food in nondependent rhesus monkeys and in heroin-dependent monkeys undergoing withdrawal. A choice procedure was used to permit dissociation of medication effects on the relative reinforcing properties of heroin from nonselective effects on response rates. In nondependent monkeys, increasing unit doses of heroin (0-0.1 mg/kg/injection) maintained dose-dependent increases in heroin choice. Chronic 5-day treatment with naloxone (0.01-0.32 mg/kg/h) or buprenorphine (0.01-0.1 mg/kg/day) produced dose-dependent rightward shifts in heroin choice dose-effect curves, whereas chronic methadone (0.1-0.56 mg/kg/h) had little effect on heroin choice up to doses that suppressed responding. In heroin-dependent monkeys, opiate withdrawal produced overt abstinence signs as well as increases in heroin choice, manifested as leftward shifts in heroin choice dose-effect curves. The withdrawal-associated increases in heroin choice suggest that opiate withdrawal increased the relative reinforcing efficacy of heroin in comparison with food, an effect that may be related to relapse in humans. Methadone prevented withdrawal-associated increases in heroin choice, whereas buprenorphine was less effective. These findings suggest that agonist medications such as methadone may derive their clinical utility from their ability to attenuate withdrawal-associated increases in opiate reinforcement. Moreover, this procedure may be useful for exploring mechanisms underlying withdrawal-associated increases in opiate reinforcement and for testing candidate medications.

摘要

有几种药物已被批准用于治疗阿片类药物滥用,但它们临床疗效的决定因素尚未完全明确。阿片类药物依赖或戒断状态可能是一组重要的决定因素。为了验证这一假设,研究人员评估了纳洛酮、丁丙诺啡和美沙酮对非依赖恒河猴以及正在戒断的海洛因依赖恒河猴在海洛因与食物之间选择行为的影响。采用了一种选择程序,以区分药物对海洛因相对强化特性的影响与对反应率的非选择性影响。在非依赖恒河猴中,增加海洛因的单位剂量(0 - 0.1毫克/千克/注射)可使海洛因选择呈剂量依赖性增加。用纳洛酮(0.01 - 0.32毫克/千克/小时)或丁丙诺啡(0.01 - 0.1毫克/千克/天)进行为期5天的慢性治疗,可使海洛因选择剂量 - 效应曲线产生剂量依赖性右移,而慢性美沙酮(0.1 - 0.56毫克/千克/小时)在抑制反应的剂量范围内对海洛因选择几乎没有影响。在海洛因依赖恒河猴中,阿片类药物戒断会产生明显的戒断症状以及海洛因选择增加,表现为海洛因选择剂量 - 效应曲线左移。与戒断相关的海洛因选择增加表明,与食物相比,阿片类药物戒断增加了海洛因的相对强化效力,这种效应可能与人类的复吸有关。美沙酮可预防与戒断相关的海洛因选择增加,而丁丙诺啡的效果较差。这些发现表明,美沙酮等激动剂药物的临床效用可能源于它们减弱与戒断相关的阿片类药物强化增加的能力。此外,该程序可能有助于探索与戒断相关的阿片类药物强化增加的潜在机制,并用于测试候选药物。

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