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苯二氮䓬类药物与中枢神经系统甘氨酸受体的相互作用:可能的作用机制。

Interaction of benzodiazepines with central nervous glycine receptors: possible mechanism of action.

作者信息

Young A B, Zukin S R, Snyder S H

出版信息

Proc Natl Acad Sci U S A. 1974 Jun;71(6):2246-50. doi: 10.1073/pnas.71.6.2246.

Abstract

Interaction of 21 benzodiazepines with the glycine receptor in the brainstem and spinal cord of rat have been evaluated in terms of their displacement of [(3)H]strychinine binding. The rank order of potency of the 21 drugs in displacing specific [(3)H]strychinine binding correlates (p < 0.005) with their rank order of potency in a vareity of pharmacological and behavioral tests in humans and animals that predict clinical efficacy. There is a 50-fold variation in potency of the series of benzodiazepines with mean effective dose (ED(50)) values ranging from 19muM to > 1000 muM. Diazepam (Valium(R)) and chlordiazepoxide (Librium(R)) have ED(50)'s of 26 muM and 200 muM, respectively, whereas the ED(50) for glycine is 25 muM. The inhibitory effects of 10 of the agents in two other central nervous system membrane receptor assays, for the opiate receptor and the muscarinic cholinergic receptor, do not correlate with any of the in vivo pharmacologic and behavioral tests. The benzodiazepines may exert their antianxiety, anticonvulsant and muscle-relaxant effects by mimicking the effects of the neurotransmitter glycine at its central nervous system receptor sites.

摘要

通过[³H]士的宁结合的置换作用,评估了21种苯二氮䓬类药物与大鼠脑干和脊髓中甘氨酸受体的相互作用。这21种药物置换特异性[³H]士的宁结合的效价顺序,与它们在预测临床疗效的多种人体和动物药理学及行为学试验中的效价顺序相关(p < 0.005)。该系列苯二氮䓬类药物的效价有50倍的差异,平均有效剂量(ED50)值范围为19μM至>1000μM。地西泮(安定®)和氯氮䓬(利眠宁®)的ED50分别为26μM和200μM,而甘氨酸的ED50为25μM。在另外两种中枢神经系统膜受体试验中,即阿片受体和毒蕈碱胆碱能受体试验中,10种药物的抑制作用与任何体内药理学和行为学试验均不相关。苯二氮䓬类药物可能通过在中枢神经系统受体部位模拟神经递质甘氨酸的作用,发挥其抗焦虑、抗惊厥和肌肉松弛作用。

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