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连续给予大鼠右旋苯丙胺治疗可降低可卡因的强化效果:治疗期间主动自我给药的重要性。

Reduction of the reinforcing effectiveness of cocaine by continuous D-amphetamine treatment in rats: importance of active self-administration during treatment period.

作者信息

Zimmer Benjamin A, Chiodo Keri A, Roberts David C S

机构信息

Department of Physiology and Pharmacology, Wake Forest University Health Sciences, Medical Center BLVD, Winston-Salem, NC, 27157, USA,

出版信息

Psychopharmacology (Berl). 2014 Mar;231(5):949-54. doi: 10.1007/s00213-013-3305-4. Epub 2013 Oct 22.

Abstract

RATIONALE

Continuous administration of D-amphetamine has shown promise as a treatment for psychostimulant addiction. In rodent studies, constant infusion of D-amphetamine (5 mg/kg/day) has been shown to reduce cocaine-reinforced responding in the dose range of 0.19-0.75 mg/kg/inf.

OBJECTIVES

The present study tested whether these effects were a reflection of pharmacological interactions between D-amphetamine and cocaine or if they resulted from associative learning mechanisms

METHODS

After stable progressive ratio (PR) baselines were established, rats were implanted with subcutaneous osmotic minipumps filled with either D-amphetamine (5 mg/kg/day-groups 1 and 2) or saline (group 3). During the treatment period, groups 1 and 3 self-administered cocaine at a dose that was previously shown to produce the most robust effects in combination with D-amphetamine treatment (0.19 mg/kg/inf), while group 2 received passive cocaine infusions.

RESULTS

In replication of previous studies, D-amphetamine treatment resulted in a significant (35 %) decrease in breakpoints relative to saline controls. By contrast, no reductions in breakpoints were observed in animals that received passive cocaine infusions during the treatment period (group 2).

CONCLUSIONS

Active self-administration of cocaine during the treatment period appears to be an important factor in reducing cocaine-reinforced breakpoints. These findings suggest learning mechanisms are involved in the therapeutic effects of continuous D-amphetamine, and pharmacological interaction mechanisms such as cross-tolerance cannot completely account for the observed decreases in cocaine seeking.

摘要

原理

持续给予右旋苯丙胺已显示出作为治疗精神兴奋剂成瘾的潜力。在啮齿动物研究中,持续输注右旋苯丙胺(5毫克/千克/天)已显示在0.19 - 0.75毫克/千克/次的剂量范围内可减少可卡因强化反应。

目的

本研究测试这些效应是右旋苯丙胺与可卡因之间药理相互作用的反映,还是由联想学习机制导致的。

方法

在建立稳定的累进比率(PR)基线后,给大鼠皮下植入充满右旋苯丙胺(5毫克/千克/天,第1组和第2组)或生理盐水(第3组)的渗透微型泵。在治疗期间,第1组和第3组以先前显示与右旋苯丙胺治疗联合产生最强效应的剂量(0.19毫克/千克/次)自行给予可卡因,而第2组接受被动可卡因输注。

结果

与先前研究一致,右旋苯丙胺治疗导致断点相对于生理盐水对照组显著降低(35%)。相比之下,在治疗期间接受被动可卡因输注的动物(第2组)中未观察到断点降低。

结论

治疗期间主动自行给予可卡因似乎是降低可卡因强化断点的一个重要因素。这些发现表明学习机制参与了持续给予右旋苯丙胺的治疗效果,并且诸如交叉耐受等药理相互作用机制不能完全解释观察到的可卡因觅求行为的减少。

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