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3-PPP(一种选择性多巴胺能自身受体激动剂)对患有持续性抗精神病药物所致运动障碍的卷尾猴的抗运动障碍作用。

Antidyskinetic action of 3-PPP, a selective dopaminergic autoreceptor agonist, in Cebus monkeys with persistent neuroleptic-induced dyskinesias.

作者信息

Häggström J E, Gunne L M, Carlsson A, Wikström H

出版信息

J Neural Transm. 1983;58(3-4):135-42. doi: 10.1007/BF01252800.

Abstract

Four Cebus apella monkeys with persistent dyskinetic movements induced by earlier long-term administration of haloperidol were subjected to a trial of the dyskinesia-modifying effects of a novel dopamine autoreceptor agonist 3-PPP (3[3-hydroxyphenyl]-N-n-propyl-piperidine). Three monkeys had choreic dyskinesia involving trunk and extremities whereas one had a buccolingual form including tongue protrusion with choreoathetotic twitching and twisting movements of the tongue. Two monkeys (1 choreic, 1 buccolingual) responded with dose-dependent symptom alleviation to 3-PPP, 1-4 mg/kg, with no signs of concomitant sedation or catalepsy. In the monkey with buccolingual dyskinesia all dyskinetic signs disappeared completely 2 hours after 2 mg/kg of 3-PPP. This animal participated in a separate study where the same doses of 3-PPP but also its enantiomers were given. The (-) enantiomer was a more potent antidyskinetic agent than the (+) enantiomer, the racemate falling between these two. Four mg/kg of the (+) enantiomer precipitated an amphetamine-like excitation and after 4 hours aggravation of dyskinesia was noted. These observations support the notion that the (+) enantiomer has both postsynaptic and presynaptic stimulatory effects, whereas the (-) enantiomer acts as a presynaptic dopamine receptor agonist.

摘要

对4只因早期长期服用氟哌啶醇而出现持续性运动障碍的僧帽猴进行了新型多巴胺自身受体激动剂3-PPP(3-[3-羟苯基]-N-正丙基哌啶)改善运动障碍作用的试验。3只猴子出现涉及躯干和四肢的舞蹈样运动障碍,而1只猴子表现为颊舌型运动障碍,包括伸舌以及舌的舞蹈手足徐动样抽搐和扭转运动。2只猴子(1只舞蹈样、1只颊舌型)对3-PPP(1-4mg/kg)有剂量依赖性的症状缓解反应,无伴随镇静或僵住症的迹象。在患有颊舌型运动障碍的猴子中,给予2mg/kg的3-PPP后2小时,所有运动障碍体征完全消失。这只猴子参与了另一项研究,在该研究中给予相同剂量的3-PPP及其对映体。(-)对映体是比(+)对映体更强效的抗运动障碍药物,外消旋体的作用介于两者之间。4mg/kg的(+)对映体引发了类似苯丙胺的兴奋作用,4小时后观察到运动障碍加重。这些观察结果支持以下观点,即(+)对映体具有突触后和突触前刺激作用,而(-)对映体作为突触前多巴胺受体激动剂起作用。

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