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在全身和海马注射尼古丁后,高架十字迷宫焦虑测试中第1次和第2次试验的行为调节。

Modulation of behaviour on trials 1 and 2 in the elevated plus-maze test of anxiety after systemic and hippocampal administration of nicotine.

作者信息

Ouagazzal A M, Kenny P J, File S E

机构信息

Psychopharmacology Research Unit, Neuroscience Research Centre, GKT School of Biomedical Sciences, King's College, Guy's Campus, London, UK.

出版信息

Psychopharmacology (Berl). 1999 May;144(1):54-60. doi: 10.1007/s002130050976.

Abstract

RATIONALE

The elevated plus-maze provides a test situation in which distinctive states of anxiety are elicited on trials 1 and 2 and the dorsal hippocampus has previously been shown to mediate the anxiogenic effects of (-)-nicotine in the social interaction test.

OBJECTIVE

To determine the effects of a wide dose range of (-)-nicotine on trial 1 and 2 in the plus-maze after systemic administration and whether the dorsal hippocampus is a site mediating the anxiogenic effect of nicotine.

METHODS

(-)-Nicotine (0.001, 0.005, 0.01, 0.05, 0.1, 0.5 and 1 mg/kg) was injected IP 30 min before testing for 5 min in the plus-maze. Rats receiving dorsal hippocampal infusions received bilateral infusions of 0.5 microl of artificial CSF or (-)-nicotine (0.1, 1, 4 or 8 microg). The needle was left in place for 50 s after injection and testing took place 3 min later. Rats tested on trial 1 were naive to the plus-maze, those tested on trial 2 had received a previous 5-min undrugged exposure to the maze 48 h earlier.

RESULTS

Low doses of (-)-nicotine (0.001, 0.005, 0.01, 0.05 and 0.1 mg/kg, IP) were without effect on either trial, but higher doses (0.5 and 1 mg/kg, IP) had anxiogenic effects on both trials, as shown by decreases in percentage time spent and percentage entries onto the open arms. Infusion of (-)-nicotine (0.1, 1, 4 and 8 microg) bilaterally into the dorsal hippocampus was without effect on trial 1, but 1 microg had an anxiolytic effect on trial 2, shown by an increased percentage time spent on the open arms.

CONCLUSIONS

The results on both trials in the plus-maze after systemic administration of nicotine add to previous reports from the social interaction test that high doses of nicotine have anxiogenic effects. However, the effects of nicotine in the dorsal hippocampus are different in all three anxiety tests (anxiogenic in social interaction, ineffective on trial 1, anxiolytic on trial 2) showing that nicotinic cholinergic control in this brain region may vary depending on the state and/or type of anxiety generated by the test. The brain region(s) underlying the anxiogenic effects of IP nicotine on both trials in the plus-maze remain to be identified.

摘要

原理

高架十字迷宫提供了一种测试情境,在第1次和第2次试验中会引发不同的焦虑状态,并且先前已表明背侧海马体在社交互动测试中介导(-)-尼古丁的致焦虑作用。

目的

确定全身给药后不同剂量范围的(-)-尼古丁对高架十字迷宫第1次和第2次试验的影响,以及背侧海马体是否是介导尼古丁致焦虑作用的部位。

方法

在高架十字迷宫中测试前30分钟腹腔注射(-)-尼古丁(0.001、0.005、0.01、0.05、0.1、0.5和1毫克/千克),测试5分钟。接受背侧海马体注射的大鼠接受双侧注射0.5微升人工脑脊液或(-)-尼古丁(0.1、1、4或8微克)。注射后针头留置50秒,3分钟后进行测试。第1次试验的大鼠对高架十字迷宫不熟悉,第2次试验的大鼠在48小时前曾在无药物状态下接触该迷宫5分钟。

结果

低剂量的(-)-尼古丁(0.001、0.005、0.01、0.05和0.1毫克/千克,腹腔注射)对两次试验均无影响,但较高剂量(0.5和1毫克/千克,腹腔注射)在两次试验中均有致焦虑作用,表现为在开放臂上花费的时间百分比和进入开放臂的次数百分比降低。双侧背侧海马体注射(-)-尼古丁(0.1、1、4和8微克)对第1次试验无影响,但1微克在第2次试验中有抗焦虑作用,表现为在开放臂上花费的时间百分比增加。

结论

尼古丁全身给药后在高架十字迷宫两次试验中的结果补充了社交互动测试先前的报告,即高剂量尼古丁有致焦虑作用。然而,尼古丁在背侧海马体中的作用在所有三项焦虑测试中有所不同(在社交互动中致焦虑,在第1次试验中无作用,在第2次试验中有抗焦虑作用),表明该脑区的烟碱胆碱能控制可能因测试产生的焦虑状态和/或类型而异。腹腔注射尼古丁在高架十字迷宫两次试验中致焦虑作用的潜在脑区仍有待确定。

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