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D1受体缺陷小鼠中保留的可卡因条件性位置偏爱

Retained cocaine conditioned place preference in D1 receptor deficient mice.

作者信息

Miner L L, Drago J, Chamberlain P M, Donovan D, Uhl G R

机构信息

Molecular Neurobiology Branch, Addiction Research Center, National Institute on Drug Abuse, Baltimore, MD 21224, USA.

出版信息

Neuroreport. 1995 Nov 27;6(17):2314-6. doi: 10.1097/00001756-199511270-00011.

Abstract

The role of the D1 dopamine receptor subtype in mediating cocaine effects was examined in mice in which the D1 receptor gene had been ablated by homologous recombination. Cocaine reward was assessed by conditioned place preference experiments using mice which had either one allele (+/-) or both alleles (-/-) of the D1 dopamine receptor gene disrupted and in their wild type (+/+) littermates. Cocaine conditioning resulted in similar increases in preference for drug-paired environments in mice of each of the three genotypes. Cocaine did not alter locomotor activity levels in homozygous, D1 knockout mice -/-, whereas increased activity was noted in both +/+ and +/- animals. These results are consistent with the idea that the D1 receptor is involved in the locomotor stimulant effects of cocaine, but has little role in a major test of the rewarding and reinforcing effects of the drug.

摘要

在通过同源重组使D1受体基因缺失的小鼠中,研究了D1多巴胺受体亚型在介导可卡因效应中的作用。使用D1多巴胺受体基因一个等位基因(+/-)或两个等位基因(-/-)被破坏的小鼠及其野生型(+/+)同窝小鼠,通过条件性位置偏爱实验评估可卡因奖赏效应。可卡因条件反射导致三种基因型小鼠对药物配对环境的偏爱均有类似增加。可卡因并未改变纯合D1基因敲除小鼠(-/-)的运动活动水平,而在野生型(+/+)和杂合子(+/-)动物中均观察到活动增加。这些结果与以下观点一致:D1受体参与可卡因的运动兴奋作用,但在该药物奖赏和强化作用的主要测试中作用不大。

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