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苯二氮䓬反向激动剂Ro 15 - 4513和FG 7142对乙醇作用于小脑浦肯野神经元的拮抗作用:电生理研究

Antagonism of ethanol effects on cerebellar Purkinje neurons by the benzodiazepine inverse agonists Ro 15-4513 and FG 7142: electrophysiological studies.

作者信息

Palmer M R, van Horne C G, Harlan J T, Moore E A

机构信息

Department of Pharmacology, University of Colorado Health Sciences Center, Denver.

出版信息

J Pharmacol Exp Ther. 1988 Dec;247(3):1018-24.

PMID:2849654
Abstract

Ro 15-4513, a benzodiazepine inverse agonist, has been reported to antagonize the ataxic effects of ethanol. The present study investigates the Ro 15-4513 sensitivity of rat cerebellar Purkinje neurons to the depressant effects of locally applied ethanol. Local applications of ethanol by pressure ejection from multibarrel micropipettes caused reversible and dose-dependent depressions of the neuronal firing rates of single cerebellar Purkinje neurons. The ethanol-induced depressions could be antagonized by local applications of Ro 15-4513 applied from another barrel of the same micropipette. This antagonism was not competitive, suggesting that Ro 15-4513 does not interfere directly with the initial step of the ethanol mechanism of action. A beta-carboline inverse agonist, FG 7142, was more efficacious than Ro 15-4513 for antagonizing the ethanol-induced depressions, but appeared to be less potent. Recovery of ethanol-induced depressions of Purkinje neurons firing rates after Ro 15-4513 antagonism was not usually observed for 1 hr or more after the antagonist application. In contrast to ethanol effects, qualitatively similar gamma-aminobutyric acid-induced depressions of these same neurons were not antagonized by the doses of Ro 15-4513 used. We conclude that the electrophysiological depressant effects of ethanol on cerebellar neuronal activity can be antagonized by the benzodiazepine inverse agonists, Ro 15-4513 and FG 7142.

摘要

Ro 15 - 4513是一种苯二氮䓬类反向激动剂,据报道它能拮抗乙醇的共济失调作用。本研究调查了大鼠小脑浦肯野神经元对局部应用乙醇的抑制作用的Ro 15 - 4513敏感性。通过多管微量移液器压力喷射局部应用乙醇,可引起单个小脑浦肯野神经元的神经元放电频率出现可逆且剂量依赖性的降低。乙醇诱导的放电频率降低可被从同一微量移液器的另一管中局部应用Ro 15 - 4513所拮抗。这种拮抗作用不是竞争性的,这表明Ro 15 - 4513并不直接干扰乙醇作用机制的初始步骤。一种β - 咔啉反向激动剂FG 7142在拮抗乙醇诱导的放电频率降低方面比Ro 15 - 4513更有效,但似乎效力较低。在应用拮抗剂后,通常在1小时或更长时间内未观察到Ro 15 - 4513拮抗后乙醇诱导的浦肯野神经元放电频率降低的恢复。与乙醇的作用相反,这些相同神经元的γ - 氨基丁酸诱导的性质相似的放电频率降低未被所用剂量的Ro 15 - 4513所拮抗。我们得出结论,乙醇对小脑神经元活动的电生理抑制作用可被苯二氮䓬类反向激动剂Ro 15 - 4513和FG 7142所拮抗。

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