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对κ阿片受体激动剂沙维诺林A作为猴子药物自我给药惩罚剂的评估。

Assessment of the kappa opioid agonist, salvinorin A, as a punisher of drug self-administration in monkeys.

作者信息

Freeman Kevin B, Naylor Jennifer E, Prisinzano Thomas E, Woolverton William L

机构信息

Division of Neurobiology and Behavior Research, Department of Psychiatry and Human Behavior, The University of Mississippi Medical Center, Jackson, MS, 39216, USA,

出版信息

Psychopharmacology (Berl). 2014 Jul;231(14):2751-8. doi: 10.1007/s00213-014-3436-2. Epub 2014 Jan 31.

Abstract

RATIONALE

Drugs can function as punishers. However, work on the study of drugs as punishers is limited, as is the range of compounds known to function as punishers. Kappa opioid agonists, which have received much experimental attention as potential therapeutics for drug abuse, reportedly produce aversive effects. However, kappa agonists have yet to be tested as punishers of behavior.

OBJECTIVE

The goal of the current study was to determine if a kappa agonist could function as a punisher of drug self-administration.

METHOD

In separate experiments, monkeys were allowed to choose in a two-lever choice design between intravenous injections of equal doses of either cocaine (0.1 mg/kg/injection on each lever) or remifentanil (0.1 μg/kg/injection on each lever) when one of the two options was mixed with various doses of the kappa agonist, salvinorin A.

RESULTS

Choice for the cocaine and remifentanil options that were combined with salvinorin A decreased as a function of salvinorin A dose in all monkeys. However, operant response rates were not systematically affected by salvinorin A administration.

CONCLUSION

The present findings demonstrate that the kappa agonist, salvinorin A, can punish self-administration of a psychotimulant, cocaine, and a mu opioid, remifentanil. In consideration of these findings, it may be possible to curtail the abuse of some drugs by contingently delivering kappa agonists (e.g., as combination formularies for prescription medications).

摘要

理论依据

药物可起到惩罚物的作用。然而,关于药物作为惩罚物的研究工作有限,已知能起到惩罚物作用的化合物种类也有限。κ阿片受体激动剂作为药物滥用的潜在治疗方法受到了大量实验关注,据报道会产生厌恶效应。然而,κ激动剂尚未被测试作为行为的惩罚物。

目的

本研究的目的是确定一种κ激动剂是否能作为药物自我给药的惩罚物。

方法

在单独的实验中,当两种选择之一与不同剂量的κ激动剂沙维诺林A混合时,猴子在双杠杆选择设计中选择静脉注射等剂量的可卡因(每根杠杆每次注射0.1毫克/千克)或瑞芬太尼(每根杠杆每次注射0.1微克/千克)。

结果

在所有猴子中,与沙维诺林A联合使用的可卡因和瑞芬太尼选择随着沙维诺林A剂量的增加而减少。然而,沙维诺林A的给药并未系统地影响操作反应率。

结论

本研究结果表明,κ激动剂沙维诺林A可以惩罚精神兴奋剂可卡因和μ阿片类药物瑞芬太尼的自我给药。考虑到这些发现,通过偶然给予κ激动剂(例如,作为处方药的组合配方)来减少某些药物的滥用可能是可行的。

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