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Neuron. 2008 Jul 10;59(1):11-34. doi: 10.1016/j.neuron.2008.06.012.
3
Stress-induced reinstatement of cocaine seeking is mediated by the kappa opioid system.应激诱导的可卡因觅求恢复由κ阿片系统介导。
Psychopharmacology (Berl). 2008 Sep;200(1):59-70. doi: 10.1007/s00213-008-1122-y. Epub 2008 Jun 25.
4
Striatal and ventral pallidum dynorphin concentrations are markedly increased in human chronic cocaine users.在慢性可卡因成瘾的人类中,纹状体和腹侧苍白球中的强啡肽浓度显著升高。
Neuropharmacology. 2008 Jul;55(1):41-6. doi: 10.1016/j.neuropharm.2008.04.019. Epub 2008 Apr 29.
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The dysphoric component of stress is encoded by activation of the dynorphin kappa-opioid system.压力中的烦躁不安成分是由强啡肽κ-阿片系统的激活所编码的。
J Neurosci. 2008 Jan 9;28(2):407-14. doi: 10.1523/JNEUROSCI.4458-07.2008.
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Kappa agonist-induced reinstatement of cocaine seeking in squirrel monkeys: a role for opioid and stress-related mechanisms.κ激动剂诱导松鼠猴可卡因觅求行为的恢复:阿片类和应激相关机制的作用
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A role for mu opioid receptors in cocaine-induced activity, sensitization, and reward in the rat.μ阿片受体在大鼠可卡因诱导的活动、敏化和奖赏中的作用。
Psychopharmacology (Berl). 2007 Dec;195(2):265-72. doi: 10.1007/s00213-007-0883-z. Epub 2007 Aug 9.
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Enhanced sensitivity to stress and drug/alcohol craving in abstinent cocaine-dependent individuals compared to social drinkers.与社交饮酒者相比,戒除可卡因依赖的个体对应激以及药物/酒精渴望的敏感性增强。
Neuropsychopharmacology. 2008 Mar;33(4):796-805. doi: 10.1038/sj.npp.1301470. Epub 2007 Jun 13.
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Stress and drug-cue-induced craving in opioid-dependent individuals in naltrexone treatment.纳曲酮治疗中阿片类药物依赖个体的应激与药物线索诱发的渴望
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抑制κ阿片受体可减轻长期接触可卡因的大鼠可卡因摄入量的增加。

Inhibition of kappa opioid receptors attenuated increased cocaine intake in rats with extended access to cocaine.

作者信息

Wee Sunmee, Orio Laura, Ghirmai Senait, Cashman John R, Koob George F

机构信息

Committee on the Neurobiology of Addictive Disorders SP30-2400, The Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

Psychopharmacology (Berl). 2009 Sep;205(4):565-75. doi: 10.1007/s00213-009-1563-y. Epub 2009 May 30.

DOI:10.1007/s00213-009-1563-y
PMID:19484223
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2739447/
Abstract

OBJECTIVE

Previous studies demonstrated that the dynorphin/kappa opioid system was up-regulated upon repeated cocaine self-administration. In the present study, we tested the hypothesis that increased cocaine self-administration with extended access was associated with increased activity of the kappa opioid system in rats.

MATERIALS AND METHODS

Rats self-administered 0.5 mg/kg per injection of cocaine on a fixed-ratio (FR) schedule in either 1-h (short access, ShA) or 6-h (long access, LgA) sessions. After cocaine intake in the LgA rats increased to a maximum, the effects of kappa opioid receptor antagonists and a partial agonist were tested on cocaine intake in ShA and LgA rats.

RESULTS

Cocaine self-administration increased under FR and progressive-ratio (PR) schedules in LgA rats. Nor-BNI (15-30 mg/kg), a kappa receptor antagonist, decreased cocaine intake in LgA rats under a PR schedule (ShA, +1.7%; LgA, -27.4% from baseline), whereas naltrexone (0.3-10 mg/kg) and SG-II-49 (0.025-0.1 mg/kg), a nonspecific opioid receptor antagonist and a partial agonist, respectively, decreased cocaine intake in both groups (PR data: SG-II-49, ShA -28.6%, LgA -19.8%; naltrexone, ShA -34.6%, LgA -11.8% compared with vehicle data).

CONCLUSIONS

The present study demonstrated that the antagonism of kappa opioid receptors attenuated only the increased cocaine intake in LgA rats under a PR schedule, whereas the antagonism of micro and kappa receptors decreased cocaine intake in both ShA and LgA groups. The data suggest that increased motivation for cocaine in rats with extended access may be related to increased kappa opioid activity and may contribute to compulsive use.

摘要

目的

先前的研究表明,强啡肽/κ阿片系统在反复可卡因自我给药后会上调。在本研究中,我们检验了以下假设:延长获取时间后可卡因自我给药增加与大鼠κ阿片系统活性增加有关。

材料与方法

大鼠在1小时(短获取时间,ShA)或6小时(长获取时间,LgA)的实验时段内,按照固定比例(FR)程序,每次注射0.5mg/kg可卡因进行自我给药。在LgA组大鼠的可卡因摄入量增加到最大值后,测试κ阿片受体拮抗剂和部分激动剂对ShA组和LgA组大鼠可卡因摄入量的影响。

结果

在FR和累进比率(PR)程序下,LgA组大鼠的可卡因自我给药量增加。κ受体拮抗剂Nor-BNI(15 - 30mg/kg)在PR程序下降低了LgA组大鼠的可卡因摄入量(ShA组,较基线增加1.7%;LgA组,较基线减少27.4%),而纳曲酮(0.3 - 10mg/kg)和SG-II-49(0.025 - 0.1mg/kg),分别为非特异性阿片受体拮抗剂和部分激动剂,在两组中均降低了可卡因摄入量(PR数据:SG-II-49,ShA组减少28.6%,LgA组减少19.8%;纳曲酮,ShA组减少34.6%,LgA组减少11.8%,与溶媒数据相比)。

结论

本研究表明,κ阿片受体拮抗仅在PR程序下减弱了LgA组大鼠增加的可卡因摄入量,而μ和κ受体拮抗在ShA组和LgA组中均降低了可卡因摄入量。数据表明,延长获取时间的大鼠对可卡因的动机增加可能与κ阿片活性增加有关,并且可能导致强迫性使用。