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取代苯乙胺对脑血清素能机制的比较作用。

Comparative effects of substituted phenylethylamines on brain serotonergic mechanisms.

作者信息

Chung Hwang E, Van Woert M H

出版信息

J Pharmacol Exp Ther. 1980 May;213(2):254-60.

PMID:6965983
Abstract

A series of substituted phenylethylamines were examined for their relative potencies to 1) release and inhibit accumulation of labeled serotonin in brain synaptosomes, 2) compete with serotonin receptor binding and 3) induce the "serotonin syndrome" in mice. In general, the relative potencies of the phenylethylamine derivatives to produce the serotonin syndrome did not correlates well with their effects on synaptosomal uptake or release of serotonin or serotonin receptor binding. However, para chloro substitution was more effective than meta or ortho chlorophenylethylamine and para methoxy substitution more effective than ortho methoxyphenylethylamine for [3H]serotonin uptake inhibition and release and induction of the serotonin syndrome. Lineweaver Burk kinetic analysis indicated that para chlorophenylethylamine was a competitive inhibitor of [3H]serotonin uptake in vitro with a Ki of 4.3 x 10(-7) M. Fluoxetine, a specific serotonin uptake inhibitor, blocked p-chlorophenylethylamine and p-methoxyphenylethylamine-induced [3H]serotonin release. The ability of phenylethylamine derivatives to release preferentially [3H]serotonin in vitro without damaging serotonergic neurons and to consistently and rapidly produce the serotonin syndrome in vivo should make these compounds useful pharmacological tools for investigating brain serotonin metabolism.

摘要

对一系列取代苯乙胺进行了研究,考察它们在以下方面的相对效力:1)释放并抑制脑突触体中标记血清素的积累;2)与血清素受体结合竞争;3)在小鼠中诱发“血清素综合征”。一般来说,苯乙胺衍生物产生血清素综合征的相对效力与其对突触体摄取或释放血清素或血清素受体结合的影响相关性不佳。然而,对氯取代比对氯或邻氯苯乙胺更有效,对甲氧基取代比邻甲氧基苯乙胺在抑制[3H]血清素摄取、释放及诱发血清素综合征方面更有效。Lineweaver Burk动力学分析表明,对氯苯乙胺在体外是[3H]血清素摄取的竞争性抑制剂,其Ki为4.3×10(-7)M。氟西汀,一种特异性血清素摄取抑制剂,可阻断对氯苯乙胺和对甲氧基苯乙胺诱导的[3H]血清素释放。苯乙胺衍生物在体外优先释放[3H]血清素而不损伤血清素能神经元,以及在体内持续快速产生血清素综合征的能力,应使这些化合物成为研究脑血清素代谢的有用药理学工具。

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