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自发性尼古丁戒断增强大鼠的应激反应。

Spontaneous nicotine withdrawal potentiates the effects of stress in rats.

作者信息

Jonkman Sietse, Risbrough Victoria B, Geyer Mark A, Markou Athina

机构信息

Department of Psychiatry, School of Medicine, University of California San Diego, La Jolla, CA 92093-0603, USA.

出版信息

Neuropsychopharmacology. 2008 Aug;33(9):2131-8. doi: 10.1038/sj.npp.1301607. Epub 2007 Nov 21.

Abstract

Anxiety is a common symptom of nicotine withdrawal in humans, and may predict an inability to abstain from cigarette smoking. It is not clear if self-reports of anxiety during abstinence reflect increased baseline anxiety and/or increased responses to exogenous stressors. We hypothesized that nicotine withdrawal selectively exacerbates reactivity to aversive stimuli in rodents. Here, we investigated the effect of withdrawal from chronic nicotine administration (3.16 mg/kg per day base, delivered via subcutaneous osmotic minipumps) in the light-enhanced startle (LES) test in Wistar rats. In this procedure, baseline startle responding in the dark is compared to startle responding when the chamber is brightly lit. Bright illumination is aversive for rats and potentiates the startle response. Hence, this procedure allows comparisons of withdrawal effects on startle reactivity between relatively neutral and stressful contexts. We found that spontaneous nicotine withdrawal (24 h post-pump removal) did not influence baseline startle responding, but produced a selective increase in LES. Precipitated nicotine withdrawal through injections of one of two nicotinic acetylcholine receptor (nAChR) antagonists, dihydro-beta-erythroidine hydrobromide (DHbetaE: 0, 1.5, 3, or 6 mg/kg) or mecamylamine (0, 1, 2, or 4 mg/kg), did not influence baseline startle responding or LES. These results suggest that spontaneous nicotine withdrawal selectively potentiates responses to anxiogenic stimuli, but does not by itself produce a strong anxiogenic effect. These findings support the hypothesis that nicotine withdrawal exacerbates stress responding, and indicate LES may be a useful model to examine withdrawal effects on anxiety.

摘要

焦虑是人类尼古丁戒断的常见症状,可能预示着无法戒烟。目前尚不清楚戒断期间焦虑的自我报告是否反映了基线焦虑的增加和/或对外源性应激源的反应增加。我们假设尼古丁戒断会选择性地加剧啮齿动物对厌恶刺激的反应性。在此,我们在Wistar大鼠的光增强惊吓(LES)试验中研究了慢性尼古丁给药(每天3.16mg/kg碱,通过皮下渗透微型泵给药)戒断的影响。在这个过程中,将黑暗中的基线惊吓反应与箱体明亮照明时的惊吓反应进行比较。明亮照明对大鼠来说是厌恶的,并增强惊吓反应。因此,这个过程允许比较相对中性和应激环境下戒断对惊吓反应性的影响。我们发现,自发尼古丁戒断(取出泵后24小时)不影响基线惊吓反应,但会使LES选择性增加。通过注射两种烟碱型乙酰胆碱受体(nAChR)拮抗剂之一氢溴酸二氢β-刺桐定(DHβE:0、1.5、3或6mg/kg)或美加明(0、1、2或4mg/kg)引发尼古丁戒断,不影响基线惊吓反应或LES。这些结果表明,自发尼古丁戒断选择性地增强了对焦虑原性刺激的反应,但本身不会产生强烈的焦虑原性效应。这些发现支持了尼古丁戒断会加剧应激反应的假设,并表明LES可能是研究戒断对焦虑影响的有用模型。

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