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向大鼠伏隔核、杏仁核或纹状体内微量注射多巴胺D-1拮抗剂SCH 23390对可卡因自身给药的影响。

Effects of the dopamine D-1 antagonist SCH 23390 microinjected into the accumbens, amygdala or striatum on cocaine self-administration in the rat.

作者信息

Caine S B, Heinrichs S C, Coffin V L, Koob G F

机构信息

Department of Neuropharmacology, Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

Brain Res. 1995 Sep 18;692(1-2):47-56. doi: 10.1016/0006-8993(95)00598-k.

DOI:10.1016/0006-8993(95)00598-k
PMID:8548319
Abstract

This study tested the hypothesis that blockade of D-1 dopamine receptors in the nucleus accumbens shell, central nucleus of the amygdala or dorsal striatum by intracerebral microinjection of the dopamine antagonist SCH 23390 produces an attenuation of the effects of self-administered cocaine. Microinjection of SCH 23390 (0-4.0 micrograms total dose) into any of the three brain regions dose-dependently increased the rate of cocaine self-administration, consistent with a partial attenuation of the effects of cocaine under these conditions (0.25 mg cocaine i.v.; fixed-ratio 5 timeout 20 s). The regional rank order potency of SCH 23390 was accumbens > amygdala > striatum, striatal injections being equipotent with subcutaneous administration. Moreover, SCH 23390 produced rapid effects on cocaine self-administration only when injected into the accumbens or amygdala. The time course of this regional selectivity was consistent with the rate of diffusion of SCH 23390 from the site of injection as measured by quantitative autoradiography, demonstrating that the regional selectivity of intracerebral injections of SCH 23390 is time-dependent. These results support a role for D-1 dopamine receptors in the nucleus accumbens and amygdala in the effects of self-administered cocaine, and suggest that D-1 receptors in certain portions of the 'extended amygdala' may be an important substrate for the reinforcing actions of cocaine.

摘要

本研究检验了以下假设

通过脑内微量注射多巴胺拮抗剂SCH 23390阻断伏隔核壳、杏仁核中央核或背侧纹状体中的D-1多巴胺受体,会减弱自我给药可卡因的作用。向三个脑区中的任何一个微量注射SCH 23390(总剂量0 - 4.0微克),可卡因自我给药速率呈剂量依赖性增加,这与在这些条件下(静脉注射0.25毫克可卡因;固定比率5,超时20秒)可卡因作用的部分减弱一致。SCH 23390的区域效价顺序为伏隔核>杏仁核>纹状体,纹状体注射与皮下给药等效。此外,只有当注入伏隔核或杏仁核时,SCH 23390才会对可卡因自我给药产生快速作用。这种区域选择性的时间进程与通过定量放射自显影测量的SCH 23390从注射部位的扩散速率一致,表明脑内注射SCH 23390的区域选择性是时间依赖性的。这些结果支持伏隔核和杏仁核中的D-1多巴胺受体在自我给药可卡因的作用中发挥作用,并表明“扩展杏仁核”某些部分的D-1受体可能是可卡因强化作用的重要底物。

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