大麻二酚改善斑马鱼氟哌啶醇诱导的运动功能障碍:与多巴胺激活药物的比较研究。

Akihiro Hasumi, Hideyuki Maeda
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摘要

背景:从大麻植物中提取的大麻二酚(CBD)被认为具有药用价值,因为它具有抗炎和抗氧化的神经保护作用。最近的大鼠行为研究报道了CBD介导5-羟色胺(5-HT1A)受体的作用,以改善多巴胺(D2)受体阻断引起的运动功能障碍。特别是,它对纹状体D2受体阻断的影响是与各种锥体外运动功能障碍引起的神经系统疾病相关的重要功能。与该部位相关的多巴胺能神经退行性变可诱发帕金森病(PD),这种病通常影响老年人。它还会引起药物性帕金森病。本研究探讨了CBD(不直接作用于D2受体)对抗精神病药物(氟哌啶醇)诱导的药物性运动功能障碍的改善作用。方法:使用抗精神病药物氟哌啶醇建立斑马鱼幼虫药物性帕金森病模型。我们评估了行走距离和重复光刺激反应。此外,我们研究了几种浓度的CBD是否能改善帕金森模型的症状,并将其与抗帕金森药物罗匹尼罗的效果进行了比较。结果:通过测量斑马鱼行走的距离和它们对光刺激的反应,相当于氟哌啶醇浓度一半的CBD几乎完全逆转了氟哌啶醇引起的运动功能障碍。虽然在与CBD相同的浓度下,罗匹尼罗也能显著逆转氟哌啶醇的作用,但CBD比罗匹尼罗更有效。结论:通过D2受体阻断改善cbd诱导的运动功能障碍是治疗氟哌啶醇诱导的运动功能障碍的潜在新机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Cannabidiol improves haloperidol-induced motor dysfunction in zebrafish: a comparative study with a dopamine activating drug.

Background: Cannabidiol (CBD) extracted from the cannabis plant is believed to have a medicinal value due to its neuroprotective effect via anti-inflammatory and antioxidant action. Recent behavioral studies in rats have reported that CBD mediates serotonin (5-HT1A) receptor action to improve motor dysfunction induced by dopamine (D2) receptor blockade. In particular, its effect on D2 receptor blockade in the striatum is an important function associated with neurological disorders resulting from various extrapyramidal motor dysfunctions. Dopaminergic neurodegeneration associated with this site is known for inducing Parkinson's disease (PD), which often affects the elderly. It is also known to cause drug-induced Parkinsonism. This study examines the ameliorating effect of CBD, which does not act directly on D2 receptors, against drug-induced motor dysfunction induced by the antipsychotic drug (haloperidol).

Methods: We created a drug-induced Parkinsonism model in zebrafish larvae using an antipsychotic drug (haloperidol). We evaluated the distance traveled and repetitive light-stimulation response. Furthermore, we examined whether administration of several concentrations of CBD ameliorates symptoms of the Parkinsonism model and compared its effects with those of antiparkinsonian drug ropinirole.

Results: CBD concentrations equal to half of haloperidol's resulted in an almost complete reversal of haloperidol-induced motor dysfunction, as measured by the distance traveled by the zebrafish and their response to light-stimulus. While ropinirole also significantly reversed haloperidol's effects at the same concentration as CBD, CBD was more effective than ropinirole.

Conclusions: CBD-induced motor dysfunction improvement via D2 receptor blockade is a potential novel mechanism for the treatment of haloperidol-induced motor dysfunction.

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