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新型潜在抗焦虑化合物F 2692(1-(3'-三氟甲基苯基)-1,4-二氢-3-氨基-4-氧代-6-甲基哒嗪)的神经药理学。2. 在大鼠高架十字迷宫试验中对其产生耐受性和依赖性的潜力以及对苯二氮䓬戒断影响的评估。

Neuropharmacology of a new potential anxiolytic compound, F 2692, 1-(3'-trifluoromethyl phenyl) 1, 4-dihydro 3-amino 4-oxo 6-methyl pyridazine. 2. Evaluation of its tolerance and dependence producing potential and of its effects on benzodiazepine withdrawal in the elevated plus-maze test in rats.

作者信息

Chopin P, Assié M B, Briley M

机构信息

Centre de Recherche Pierre Fabre, Castres, France.

出版信息

Psychopharmacology (Berl). 1993;110(1-2):19-26. doi: 10.1007/BF02246946.

Abstract

After 21 days administration, diazepam (0.3-3 mg/kg/day) exhibited, 30 min after the last injection, tolerance to the sedative effect and "anxiolytic" activity as recorded in the elevated plus-maze test in rats. A dose-dependent increase of "anxiety" was also observed 24 h after withdrawal from 21 or 90 days of diazepam treatment. In contrast, under the same experimental conditions, F 2692 [1-(3'-trifluoromethyl phenyl) 1,4-dihydro 3-amino 4-oxo 6-methyl pyridazine] (3-30 mg/kg/day) exhibited no tolerance to either the sedative effect or the "anxiolytic" activity and showed no "anxiogenic rebound" response after withdrawal. Chronic diazepam pretreatment for 21 days modified neither the sedative effect nor the dose-dependent "anxiolytic" effect of F 2692. Furthermore, F 2692 could reverse the anxiogenic response after withdrawal from 21 days administration of diazepam. Finally, administration of diazepam for 3 weeks followed by a daily administration of F 2692 for a week induced no increase of "anxiety" 24 h after withdrawal.

摘要

在给予地西泮(0.3 - 3毫克/千克/天)21天后,在最后一次注射30分钟后,大鼠高架十字迷宫试验记录显示其对镇静作用和“抗焦虑”活性产生了耐受性。在停止给予地西泮21天或90天后的24小时,还观察到“焦虑”呈剂量依赖性增加。相比之下,在相同实验条件下,F 2692 [1 - (3'-三氟甲基苯基) 1,4 - 二氢 - 3 - 氨基 - 4 - 氧代 - 6 - 甲基哒嗪](3 - 30毫克/千克/天)对镇静作用或“抗焦虑”活性均未产生耐受性,且在停药后未表现出“致焦虑反弹”反应。对地西泮进行21天的慢性预处理,既未改变F 2692的镇静作用,也未改变其剂量依赖性“抗焦虑”作用。此外,F 2692可以逆转在给予地西泮21天后停药引起的致焦虑反应。最后,先给予地西泮3周,然后每天给予F 2692一周,停药24小时后未引起“焦虑”增加。

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