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DOM及几种分子修饰的辨别刺激特性。

Discriminative stimulus properties of DOM and several molecular modifications.

作者信息

Glennon R A, Young R, Rosecrans J A

出版信息

Pharmacol Biochem Behav. 1982 Apr;16(4):553-6. doi: 10.1016/0091-3057(82)90413-0.

Abstract

Rats trained to discriminate racemic 2,5-dimethoxy-4-methylphenylisopropylamine, (+/-)-DOM (1.0 mg/kg), from saline in a two-lever drug discrimination task were challenged with the optimal isomers of DOM as well as with several related agents which represent minor molecular modifications of the DOM structure. Generalization of the (+/-)-DOM stimulus was found to occur to R(-)-DOM, S(+)-DOM, (+/-)-2,5-dimethoxyphenylisopropylamine (2,5-DMA), R(-)-2,-5-DMA, and the 2-demethyl derivative of (+/-)-DOM. The 3-methyl positional isomer of (+/-)-DOM was found to produce only 34% DOM-appropriate responding at the highest dose tested while administration of S(+)-2,5-DMA and the 5-demethyl derivative of (+/-)-DOM resulted in disruption of behavior.

摘要

在双杠杆药物辨别任务中接受训练以区分外消旋2,5 - 二甲氧基 - 4 - 甲基苯异丙胺(±)-DOM(1.0毫克/千克)与生理盐水的大鼠,接受了DOM的最佳异构体以及几种代表DOM结构微小分子修饰的相关药物的挑战。发现(±)-DOM刺激的泛化发生在R(-)-DOM、S(+)-DOM、(±)-2,5 - 二甲氧基苯异丙胺(2,5 - DMA)、R(-)-2,5 - DMA以及(±)-DOM的2 - 去甲基衍生物上。发现(±)-DOM的3 - 甲基位置异构体在测试的最高剂量下仅产生34%的DOM适宜反应,而给予S(+)-2,5 - DMA和(±)-DOM的5 - 去甲基衍生物会导致行为紊乱。

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