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可卡因条件反射:8-羟基二苯丙氨酸自身受体剂量水平的逆转作用。

Cocaine conditioning: reversal by autoreceptor dose levels of 8-OHDPAT.

作者信息

Carey Robert J, Damianopoulos Ernest N, Shanahan Arielle B

机构信息

Research Service (151), VA Medical Center, 800 Irving Avenue, Syracuse, NY 13210, USA.

出版信息

Pharmacol Biochem Behav. 2009 Jan;91(3):447-52. doi: 10.1016/j.pbb.2008.08.027. Epub 2008 Sep 9.

Abstract

In order to investigate the contribution of serotonergic effects of cocaine to Pavlovian conditioning of cocaine locomotor stimulant effects, two experiments were conducted in which groups of rats (N=10) received cocaine treatments (10 mg/kg) paired or unpaired to placement in an open-field environment. Initially, a cocaine conditioned locomotion stimulant effect was established. Next, additional Coc-P and Coc-UP pairings were carried out in conjunction with pretreatment injections of the 5-HT1A agonist, 8-OHDPAT (0.01, 0.025 and 0.05 mg/kg) or saline. In experiment 1, the Coc-P group which received the saline pretreatment again exhibited conditioning but in the 8-OHDPAT pretreatment Coc-P group conditioning was eliminated. In the second experiment, the protocol of the first experiment was repeated but expanded in the post-conditioning phase to include an 8-OHDPAT plus the 5-HT1A antagonist pretreatment Coc-P group. As in the first experiment, the 8-OHDPAT pretreatment Coc-P group did not exhibit a cocaine conditioned locomotion stimulant effect; whereas, the saline pretreatment Coc-P and the 8-OHDPAT plus WAY-100635 pretreatment Coc-P groups did exhibit the cocaine conditioned locomotion stimulant effect. These findings are consistent with an important role for serotonin in the maintenance of cocaine Pavlovian conditioned effects.

摘要

为了研究可卡因的血清素能效应在可卡因运动刺激效应的巴甫洛夫条件反射中的作用,进行了两项实验,将大鼠分组(N = 10),给予可卡因处理(10毫克/千克),并将其与放置在旷场环境中进行配对或非配对。最初,建立了可卡因条件性运动刺激效应。接下来,结合5-HT1A激动剂8-OHDPAT(0.01、0.025和0.05毫克/千克)或生理盐水的预处理注射,进行额外的可卡因-配对(Coc-P)和可卡因-非配对(Coc-UP)配对。在实验1中,接受生理盐水预处理的Coc-P组再次表现出条件反射,但在接受8-OHDPAT预处理的Coc-P组中,条件反射被消除。在第二个实验中,重复了第一个实验的方案,但在条件反射后阶段进行了扩展,纳入了一个8-OHDPAT加5-HT1A拮抗剂预处理的Coc-P组。与第一个实验一样,接受8-OHDPAT预处理的Coc-P组未表现出可卡因条件性运动刺激效应;而接受生理盐水预处理的Coc-P组和接受8-OHDPAT加WAY-100635预处理的Coc-P组确实表现出可卡因条件性运动刺激效应。这些发现与血清素在维持可卡因巴甫洛夫条件效应中的重要作用一致。

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