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阿扑吗啡与“非典型多巴胺激动剂”(吡贝地尔和S3608)对运动活性影响的比较研究

A comparative study of the locomotor activity effects of apomorphine and the "atypical dopamine agonists" (piribedil and S3608).

作者信息

Offermeier J, van Rooyen J M

出版信息

Life Sci. 1986 Mar 10;38(10):895-903. doi: 10.1016/0024-3205(86)90257-2.

Abstract

Apomorphine and the "atypical dopamine agonists" (piribedil and S3608) dose dependently increase locomotor activity (LA) in rats. The LA effects of all 3 drugs are readily attenuated by pretreatment with pimozide or sulpiride. Reserpine pretreatment or bilateral 6-hydroxydopamine lesions of the nucleus accumbens (NAS) potentiates apomorphine-induced LA but attenuates piribedil- and S3608-induced LA. The latter suggests an indirect mode of action for piribedil and for S3608. However, piribedil and S3608 at concentrations up to 10(-4)M do not cause release or inhibition of 3H-dopamine uptake in synaptosomes prepared from the rat NAS. Sulpiride antagonism of apomorphine-induced LA is surmountable by increasing the dose of apomorphine. Antagonism of piribedil- or S3608-induced LA by sulpiride is not surmountable by increasing the dose of either of the "atypical dopamine agonists". Furthermore, pretreatment with either piribedil or S3608 substantially increases the peak LA inducible by apomorphine. The effects of simultaneous injections of piribedil and S3608 are, however, not additive. These findings suggest that the LA stimulant effects of piribedil and S3608 are mediated via receptors or systems which differ from the receptors involved in the mediation of apomorphine-induced LA.

摘要

阿扑吗啡和“非典型多巴胺激动剂”(匹莫齐特和S3608)可使大鼠的运动活性(LA)呈剂量依赖性增加。预先用匹莫齐特或舒必利处理可使这三种药物的LA效应轻易减弱。利血平预处理或伏隔核(NAS)的双侧6-羟基多巴胺损伤可增强阿扑吗啡诱导的LA,但会减弱匹莫齐特和S3608诱导的LA。后者提示匹莫齐特和S3608的作用方式为间接作用。然而,浓度高达10^(-4)M的匹莫齐特和S3608不会导致从大鼠NAS制备的突触体中3H-多巴胺的释放或摄取抑制。增加阿扑吗啡的剂量可克服舒必利对阿扑吗啡诱导的LA的拮抗作用。增加“非典型多巴胺激动剂”中任何一种的剂量都无法克服舒必利对匹莫齐特或S3608诱导的LA的拮抗作用。此外,预先用匹莫齐特或S3608处理可显著增加阿扑吗啡诱导的LA峰值。然而,同时注射匹莫齐特和S3608的效应并非相加。这些发现表明,匹莫齐特和S3608的LA刺激效应是通过与介导阿扑吗啡诱导的LA所涉及的受体不同的受体或系统介导的。

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