n -苯丙基- n '-(3-甲氧基苯乙基)哌嗪(YZ-185)减弱小鼠可卡因的条件奖励特性。

ISRN Pharmacology Pub Date : 2013-09-05 eCollection Date: 2013-01-01 DOI:10.1155/2013/546314
Andrew S Sage, Scott C Vannest, Kuo-Hsien Fan, Matthew J Will, Susan Z Lever, John R Lever, Dennis K Miller
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引用次数: 7

摘要

西格玛受体拮抗剂在行为分析中减少可卡因的作用,包括条件位置偏好。先前的小鼠运动活性实验表明,sigma受体配体YZ-185 (n -苯丙基- n '-(3-甲氧基苯乙基)哌嗪)在低剂量(0.1 μ mol/kg)下增强可卡因诱导的多动,在高剂量(3.16-31.6 μ mol/kg)下剂量依赖性减弱可卡因诱导的多动。本研究探讨了YZ-185对小鼠可卡因条件奖励特性的影响。YZ-185(0.1、0.316、3.16和31.6 μ mol/kg)不具有产生条件位置偏好或厌恶的内在活性。高剂量YZ-185 (31.6 μ mol/kg)和低剂量YZ-185 (0.1 ~ 3.16 μ mol/kg)抑制了可卡因(66 μ mol/kg)的位置偏好。YZ-185没有改变可卡因位置偏好的表达。为了进一步表征YZ-185的行为特征,还确定了YZ-185在升高零迷宫和旋转路径中的作用;YZ-185在两项实验中均未产生显著变化,表明YZ-185探测的sigma受体不调节焦虑样或协调运动技能行为。综上所述,YZ-185在31.6 μ mol/kg剂量下是一种sigma受体拮抗剂,表明sigma受体可以介导可卡因条件奖励特性的形成。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

N-Phenylpropyl-N'-(3-methoxyphenethyl)piperazine (YZ-185) Attenuates the Conditioned-Rewarding Properties of Cocaine in Mice.

N-Phenylpropyl-N'-(3-methoxyphenethyl)piperazine (YZ-185) Attenuates the Conditioned-Rewarding Properties of Cocaine in Mice.

N-Phenylpropyl-N'-(3-methoxyphenethyl)piperazine (YZ-185) Attenuates the Conditioned-Rewarding Properties of Cocaine in Mice.

N-Phenylpropyl-N'-(3-methoxyphenethyl)piperazine (YZ-185) Attenuates the Conditioned-Rewarding Properties of Cocaine in Mice.

Sigma receptor antagonists diminish the effects of cocaine in behavioral assays, including conditioned place preference. Previous locomotor activity experiments in mice determined that the sigma receptor ligand YZ-185 (N-phenylpropyl-N'-(3-methoxyphenethyl)piperazine) enhanced cocaine-induced hyperactivity at a lower (0.1  μ mol/kg) dose and dose-dependently attenuated cocaine-induced hyperactivity at higher (3.16-31.6  μ mol/kg) doses. The present study investigated the effect of YZ-185 on cocaine's conditioned-rewarding properties in mice. YZ-185 (0.1, 0.316, 3.16, and 31.6  μ mol/kg) did not have intrinsic activity to produce conditioned place preference or aversion. A higher (31.6  μ mol/kg) YZ-185 dose, but not lower (0.1-3.16  μ mol/kg) YZ-185 doses, prevented the development of place preference to cocaine (66  μ mol/kg). YZ-185 did not alter the expression of cocaine place preference. To further characterize YZ-185's behavioral profile, its effects in the elevated zero maze and rotarod procedures were also determined; YZ-185 produced no significant change from baseline in either assay, indicating that the sigma receptors probed by YZ-185 do not regulate anxiety-like or coordinated motor skill behaviors. Overall, these results suggest that YZ-185 is a sigma receptor antagonist at the 31.6  μ mol/kg dose and demonstrate that sigma receptors can mediate the development of the conditioned-rewarding properties of cocaine.

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