多巴胺D2受体拮抗剂——非典型抗精神病药remoxipride的药理学研究。

R. Nadal
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引用次数: 23

摘要

Remoxipride是一种取代苯甲酰胺,作为多巴胺D2受体的弱但非常选择性拮抗剂。它是在80年代末由Astra (Roxiam)引入的,并被作为非典型抗精神病药开处方。本文综述了其对中脑边缘和黑质纹状体多巴胺能系统的选择性作用。在动物实验中,在阻断多巴胺激动剂诱导的多动症的剂量下,remoxipride具有最小的催化作用。这些发现预示着抗精神病药物活性与锥体外系症状的可能性较低。Remoxipride在最近的精神分裂症动物模型中似乎也有效,如潜在抑制或脉冲前抑制。在临床研究中,remoxipride显示出相对较低的锥体外系副作用发生率,其对催乳素释放的影响是短期的,通常是轻微的。临床疗效与氟哌啶醇或氯丙嗪相似。尽管在1993年,由于一些接受remoxipride的患者出现再生障碍性贫血的报道,其临床使用受到严格限制,但该药物已被发现对多巴胺D2受体表现出相对较高的选择性,使remoxipride成为神经化学和行为研究的有趣工具。
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Pharmacology of the atypical antipsychotic remoxipride, a dopamine D2 receptor antagonist.
Remoxipride is a substituted benzamide that acts as a weak but very selective antagonist of dopamine D2 receptors. It was introduced by Astra (Roxiam) at the end of the eighties and was prescribed as an atypical antipsychotic. This article reviews its putative selective effects on mesolimbic versus nigrostriatal dopaminergic systems. In animals, remoxipride has minimal cataleptic effects at doses that block dopamine agonist-induced hyperactivity. These findings are predictive of antipsychotic activity with a low likelihood of extrapyramidal symptoms. Remoxipride also appears to be effective in more recent animal models of schizophrenia, such as latent inhibition or prepulse inhibition. In clinical studies, remoxipride shows a relatively low incidence of extrapyramidal side effects and its effects on prolactin release are short-lasting and generally mild. The clinical efficacy of remoxipride is similar to that of haloperidol or chlorpromazine. Although its clinical use was severely restricted in 1993, due to reports of aplastic anemia in some patients receiving remoxipride, this drug has been found to exhibit relatively high selectivity for dopamine D2 receptors making remoxipride an interesting tool for neurochemical and behavioral studies.
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