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尼古丁和烟碱受体对焦虑和抑郁的影响。

Effect of nicotine and nicotinic receptors on anxiety and depression.

作者信息

Picciotto Marina R, Brunzell Darlene H, Caldarone Barbara J

机构信息

Department of Psychiatry, Yale University School of Medicine, 34 Park Street, New Haven, CT 06508, USA.

出版信息

Neuroreport. 2002 Jul 2;13(9):1097-106. doi: 10.1097/00001756-200207020-00006.

Abstract

Nicotine has been shown to have effects on anxiety and depression in both human and animal studies. These studies suggest that nicotinic acetylcholine receptors (nAChRs) can modulate the function of pathways involved in stress response, anxiety and depression in the normal brain, and that smoking can result in alterations of anxiety level and mood. The effects of nicotine are complex however, and nicotine treatment can be either anxiolytic or anxiogenic depending on the anxiety model tested, the route of nicotine administration and the time course of administration. The paradoxical effects of nicotine on emotionality are likely due to the broad expression of nAChRs throughout the brain, the large number of nAChR subtypes that have been identified and the ability of nicotine treatment to both activate and desensitize nAChRs. Activation of nAChRs has been shown to modulate many systems associated with stress response including stress hormone pathways, monoaminergic transmission and release of classical neurotransmitters throughout the brain. Local administration studies in animals have identified brain areas that may be involved in the anxiogenic and anxiolytic actions of nicotine including the lateral septum, the dorsal raphe nuclei, the mesolimbic dopamine system and the hippocampus. The ensemble of studies to date suggest that under certain conditions nicotine can act as an anxiolytic and an antidepressant, but that following chronic use, adaptations to nicotine can occur resulting in increased anxiety and depression following withdrawal.

摘要

在人体和动物研究中均已表明,尼古丁对焦虑和抑郁有影响。这些研究表明,烟碱型乙酰胆碱受体(nAChRs)可调节正常大脑中参与应激反应、焦虑和抑郁的通路功能,且吸烟可导致焦虑水平和情绪的改变。然而,尼古丁的作用较为复杂,根据所测试的焦虑模型、尼古丁给药途径和给药时间进程,尼古丁治疗可能具有抗焦虑或致焦虑作用。尼古丁对情绪的矛盾作用可能归因于nAChRs在全脑的广泛表达、已鉴定出的大量nAChR亚型以及尼古丁治疗激活和使nAChRs脱敏的能力。已表明nAChRs的激活可调节许多与应激反应相关的系统,包括应激激素通路、单胺能传递以及全脑经典神经递质的释放。动物局部给药研究已确定了可能参与尼古丁致焦虑和抗焦虑作用的脑区,包括外侧隔核、中缝背核、中脑边缘多巴胺系统和海马体。迄今为止的一系列研究表明,在某些情况下尼古丁可起到抗焦虑和抗抑郁作用,但长期使用后,机体可能会对尼古丁产生适应性变化,导致戒断后焦虑和抑郁增加。

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