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抗抑郁药急性和慢性给药对中枢胆碱能神经系统的影响。与抗胆碱能药物的比较。

Effects of acute and chronic administration of antidepressant drugs on the central cholinergic nervous system. Comparison with anticholinergic drugs.

作者信息

Goldman M E, Erickson C K

出版信息

Neuropharmacology. 1983 Oct;22(10):1215-22. doi: 10.1016/0028-3908(83)90084-9.

DOI:10.1016/0028-3908(83)90084-9
PMID:6646355
Abstract

The purpose of this investigation was to study the effects of antidepressant drugs on the central cholinergic system of the rat after acute and chronic administration. Drugs (antidepressants and non-antidepressants) were first divided into highly potent, moderately potent or weak anticholinergic categories based upon the ability of each compound to displace [3H]-QNB [( 3H]quinuclidinyl benzilate from synaptosomal membranes. One antidepressant drug and one non-antidepressant drug, with similar anticholinergic properties, were chosen as representative agents of each category of anticholinergic potency. Acute administration of amitriptyline or atropine (highly potent anticholinergics) increased the level of high affinity uptake of choline in the hippocampus and striatum. Imipramine and thioridazine (moderately potent anticholinergics) increased the uptake of choline only in the striatum. After acute administration, the effects of nomifensine and d-amphetamine (weak anticholinergics) differed on striatal uptake of choline. Following 30 days pretreatment with any drug, an acute challenge dose of that drug no longer altered the uptake of choline in either region. After chronic administration, amitriptyline increased the density of muscarinic receptors in the cortex whereas atropine increased the density of receptors in the cortex, hippocampus and striatum. The other agents did not alter receptor parameters in the regions examined. Since the central cholinergic actions of the antidepressants were similar to the central actions of the non-antidepressants, it is concluded that the effects of the antidepressants on the central cholinergic nervous system are more closely related to the side effects of these agents than to their therapeutic mechanism of action.

摘要

本研究的目的是探讨抗抑郁药物急性和慢性给药后对大鼠中枢胆碱能系统的影响。首先根据每种化合物从突触体膜置换[3H]-QNB([3H]喹核醇基苯甲酸酯)的能力,将药物(抗抑郁药和非抗抑郁药)分为高效、中效或低效抗胆碱能类别。选择一种抗胆碱能特性相似的抗抑郁药和一种非抗抑郁药作为各抗胆碱能效力类别的代表药物。急性给予阿米替林或阿托品(高效抗胆碱能药)可提高海马和纹状体中胆碱的高亲和力摄取水平。丙咪嗪和硫利达嗪(中效抗胆碱能药)仅增加纹状体中胆碱的摄取。急性给药后,诺米芬辛和右旋苯丙胺(低效抗胆碱能药)对纹状体胆碱摄取的影响不同。用任何一种药物预处理30天后,该药物的急性挑战剂量不再改变任一区域中胆碱的摄取。慢性给药后,阿米替林增加皮质中毒蕈碱受体的密度,而阿托品增加皮质、海马和纹状体中受体的密度。其他药物在所检查的区域中未改变受体参数。由于抗抑郁药的中枢胆碱能作用与非抗抑郁药的中枢作用相似,因此得出结论,抗抑郁药对中枢胆碱能神经系统的影响与其副作用的关系比与其治疗作用机制的关系更为密切。

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