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AMPA受体GluR-C亚基在觅酒行为及复吸中的作用。

Involvement of the AMPA receptor GluR-C subunit in alcohol-seeking behavior and relapse.

作者信息

Sanchis-Segura Carles, Borchardt Thilo, Vengeliene Valentina, Zghoul Tarek, Bachteler Daniel, Gass Peter, Sprengel Rolf, Spanagel Rainer

机构信息

Department of Psychopharmacology, Central Institute of Mental Health, University of Heidelberg, 68072 Mannheim, Germany.

出版信息

J Neurosci. 2006 Jan 25;26(4):1231-8. doi: 10.1523/JNEUROSCI.4237-05.2006.

Abstract

Craving and relapse are core symptoms of drug addiction and alcoholism. It is suggested that, after chronic drug consumption, long-lasting neuroplastic changes within the glutamatergic system are important determinants of addictive behavior. Here, we show that the AMPA type glutamate receptor plays a crucial role in alcohol craving and relapse. We observed, in two animal models of alcohol craving and relapse, that the AMPA antagonist GYKI 52466 [1-(4-aminophenyl)-4-methyl-7, 8-methylenedioxy-5H-2, 3-benzodiazepine] dose-dependently reduced cue-induced reinstatement of alcohol-seeking behavior and the alcohol deprivation effect. The involvement of the AMPA receptor in these phenomena was further studied using mice deficient for the GluR-C AMPA subunit [GluR-C knock-out (KO)]. GluR-C KOs displayed a blunted, cue-induced reinstatement response and alcohol deprivation effect, when compared with wild-type controls; however, no differences between genotypes could be observed regarding ethanol self-administration under operant or home cage drinking conditions. These results imply a role for GluR-C in alcohol relapse, although this phenotype could also be attributable to a reduction in the total number of AMPA receptors in specific brain areas. In conclusion, AMPA receptors seem to be involved in the neuroplastic changes underlying alcohol seeking behavior and relapse. Thus, AMPA receptors represent a novel therapeutic target in preventing relapse.

摘要

渴求与复发是药物成瘾和酒精成瘾的核心症状。有研究表明,长期药物使用后,谷氨酸能系统内持久的神经可塑性变化是成瘾行为的重要决定因素。在此,我们表明AMPA型谷氨酸受体在酒精渴求与复发中起关键作用。在两种酒精渴求与复发的动物模型中,我们观察到AMPA拮抗剂GYKI 52466 [1-(4-氨基苯基)-4-甲基-7, 8-亚甲二氧基-5H-2, 3-苯并二氮杂䓬] 剂量依赖性地减少线索诱导的觅酒行为恢复及酒精剥夺效应。使用缺乏GluR-C AMPA亚基的小鼠 [GluR-C基因敲除 (KO)] 进一步研究了AMPA受体在这些现象中的作用。与野生型对照相比,GluR-C基因敲除小鼠表现出减弱的线索诱导恢复反应和酒精剥夺效应;然而,在操作性或笼内饮水条件下,关于乙醇自我给药,各基因型之间未观察到差异。这些结果表明GluR-C在酒精复发中起作用,尽管这种表型也可能归因于特定脑区AMPA受体总数的减少。总之,AMPA受体似乎参与了觅酒行为和复发背后的神经可塑性变化。因此,AMPA受体是预防复发的一个新的治疗靶点。

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