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毒蕈碱激动剂的辨别刺激特性。

Discriminative stimulus properties of muscarinic agonists.

作者信息

Jung M, Costa L, Shearman G T, Kelly P H

机构信息

Preclinical Research, Sandoz A.G., Basel, Switzerland.

出版信息

Psychopharmacology (Berl). 1987;93(2):139-45. doi: 10.1007/BF00179923.

Abstract

In a two-lever, food-reinforced drug-discrimination paradigm separate groups of rats were trained to discriminate either arecoline, pilocarpine or oxotremorine from saline. The discriminative cues of all three agonists were potently blocked by scopolamine, but only by 30-60 fold higher doses of methylscopolamine. The three agonists all suppressed overall response rate. These rate-suppressant effects were not blocked by scopolamine in doses which blocked the discriminative cues. In generalization tests, arecoline elicited selection of the drug-appropriate lever in all groups of trained animals. Pilocarpine was discriminated as drug by all pilocarpine-trained animals and by a majority of oxotremorine-trained animals, but was not significantly discriminated by the arecoline-trained group. Oxotremorine was discriminated by all oxotremorine-trained animals but only by some pilocarpine-trained animals, and was not significantly discriminated by the arecoline-trained group. Morphine, haloperidol, chlordiazepoxide, pentobarbital and nicotine were not generalized to any of the training drugs. The discriminative stimuli produced by the training drugs are therefore specific and exhibit properties indicative of an origin at central muscarinic receptors but may not be identical.

摘要

在一种双杠杆、食物强化的药物辨别范式中,将不同组的大鼠训练成从盐水中辨别出槟榔碱、毛果芸香碱或氧化震颤素。所有三种激动剂的辨别线索均被东莨菪碱有效阻断,但仅被高30 - 60倍剂量的甲基东莨菪碱阻断。这三种激动剂均抑制了总体反应率。在阻断辨别线索的剂量下,东莨菪碱并未阻断这些速率抑制作用。在泛化试验中,槟榔碱在所有受过训练的动物组中都引发了对药物匹配杠杆的选择。毛果芸香碱在所有受过毛果芸香碱训练的动物以及大多数受过氧化震颤素训练的动物中被辨别为药物,但在受过槟榔碱训练的组中未被显著辨别。氧化震颤素在所有受过氧化震颤素训练的动物中被辨别出来,但仅在一些受过毛果芸香碱训练的动物中被辨别出来,并且在受过槟榔碱训练的组中未被显著辨别。吗啡、氟哌啶醇、氯氮卓、戊巴比妥和尼古丁均未被泛化为任何一种训练药物。因此,训练药物产生的辨别刺激是特异性的,并且表现出指示中枢毒蕈碱受体起源的特性,但可能并不完全相同。

相似文献

1
Discriminative stimulus properties of muscarinic agonists.毒蕈碱激动剂的辨别刺激特性。
Psychopharmacology (Berl). 1987;93(2):139-45. doi: 10.1007/BF00179923.

本文引用的文献

1
Pharmacology of pamine bromide.帕明溴化物的药理学。
J Pharmacol Exp Ther. 1954 Feb;110(2):188-204.

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