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多巴胺能系统可能参与潜在抗抑郁药依西他普明的作用机制。

Possible involvement of the dopaminergic system in the mode of action of the potential antidepressant trazium esilate.

作者信息

Gyertyán I, Petöcz L, Bajnógel J, Szücs Z, Hegedüs M, Gyüre K, Gacsályi I, Krizsán D, Fekete M I

机构信息

EGIS Pharmaceuticals, Division of Pharmacology, Budapest, Hungary.

出版信息

Arzneimittelforschung. 1989 Jul;39(7):775-81.

PMID:2551306
Abstract

Trazium esilate (EGYT-3615) is structurally an as-triazino isoquinolinium salt which showed considerable activity in pharmacological tests characteristic for antidepressants (antagonism of tetrabenazine, potentiation of yohimbine, behavioral despair). The compound exhibited minimal sedative effect. Some findings suggest that it influences the central dopaminergic system. The drug potentiated actions of amphetamine such as stereotypy and hypermotility. It differentially blocked the hypothermic and the stereotypy inducing action of apomorphine. Trazium esilate also inhibited the cataleptic state provoked by bulbocapnine in mice. In higher dose it decreased the plasma prolactin level in rats. The compound potentiated the effect of norepinephrine on isolated vas deferens of the rat. Trazium esilate is a weak displacer on a1-, a2- and D2-receptors, however, it induced a2-receptor desenzitization after repeated treatment. It had no influence on rat brain cortical noradrenaline and striatal dopamine release evoked by high K+ concentration, but it increased the spontaneous dopamine outflow in rat striatum. The compound also elevated the striatal dopamine and DOPAC levels both after acute and chronic treatment.

摘要

乙磺司他嗪(EGYT - 3615)在结构上是一种三嗪并异喹啉鎓盐,在具有抗抑郁药特征的药理试验(对丁苯那嗪的拮抗作用、对育亨宾的增强作用、行为绝望试验)中显示出相当的活性。该化合物的镇静作用极小。一些研究结果表明它会影响中枢多巴胺能系统。该药物增强了苯丙胺的作用,如刻板行为和运动亢进。它对阿扑吗啡的降温作用和诱导刻板行为的作用有不同程度的阻断。乙磺司他嗪还抑制了小鼠中由千金藤碱诱发的僵住状态。在较高剂量下,它会降低大鼠血浆催乳素水平。该化合物增强了去甲肾上腺素对大鼠离体输精管的作用。乙磺司他嗪是α1、α2和D2受体的弱置换剂,然而,重复给药后它会诱导α2受体脱敏。它对高钾浓度诱发的大鼠脑皮质去甲肾上腺素释放和纹状体多巴胺释放没有影响,但它增加了大鼠纹状体中多巴胺的自发外流。急性和慢性给药后,该化合物还会提高纹状体多巴胺和3,4 - 二羟基苯乙酸(DOPAC)水平。

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