File S E, Pellow S
MRC Neuropharmacology Research Group School of Pharmacy, University of London, U.K.
Behav Brain Res. 1988 Sep 1;30(1):31-6. doi: 10.1016/0166-4328(88)90005-8.
The benzodiazepine receptor inverse agonists, methyl 6,7-dimethoxy-4-ethyl-beta-carboline-3-carboxylate (DMCM) and N-methyl-beta-carboline-3-carboxamide (FG 7142), were given to rats at various stages of a passive avoidance task. When the drugs were given before trial 1, low doses enhanced, and high doses impaired, performance as assessed 24 h later. A group given drugs on both trials showed that the impairment was not due to state-dependent effects. When the drugs were given immediately after trial 1, or before trial 2, they were without effect, except for the low dose of DMCM which impaired consolidation. It is discussed whether the changes in passive avoidance performance are due to direct or indirect effects. Between-trial habituation of exploratory head-dipping was measured in a holeboard. When FG 7142 was given before trial 1, the high dose impaired between-trial response decrement; but this was because it decreased the level of head-dipping on trial 1. When FG 7142 was given immediately after trial 1, or before trial 2, it was without effect on between-trial habituation.
将苯二氮䓬受体反向激动剂6,7-二甲氧基-4-乙基-β-咔啉-3-羧酸甲酯(DMCM)和N-甲基-β-咔啉-3-甲酰胺(FG 7142)在被动回避任务的不同阶段给予大鼠。在试验1之前给药时,低剂量增强了24小时后评估的表现,高剂量则损害了表现。在两次试验中都给药的一组显示,损害并非由于状态依赖性效应。当在试验1后立即给药或在试验2之前给药时,除了低剂量的DMCM损害巩固外,它们没有效果。讨论了被动回避表现的变化是由于直接还是间接效应。在洞板中测量了试验间探索性探首的习惯化。在试验1之前给予FG 7142时,高剂量损害了试验间反应递减;但这是因为它降低了试验1时的探首水平。当在试验1后立即给予FG 7142或在试验2之前给予时,它对试验间习惯化没有影响。
