高CBD含量大麻药用提取物对原代小脑颗粒细胞培养物中罗替酮的神经保护作用及制剂的相关性。

IF 3.1 4区 医学 Q2 PHARMACOLOGY & PHARMACY Cannabis and Cannabinoid Research Pub Date : 2024-06-01 Epub Date: 2023-05-08 DOI:10.1089/can.2022.0289
Carolina Echeverry, Analía Richeri, Jimena Fagetti, Gaby F Martínez, Federico Vignolo, Giselle Prunell, Leticia Cuñetti, Marcela Martínez Busi, Sandra Pérez, Verónica Sánchez de Medina, Carlos Ferreiro, Cecilia Scorza
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引用次数: 0

摘要

简介:临床前研究支持药用大麻提取物治疗不同病症(如癫痫)的益处,但其神经保护潜力尚未得到广泛研究。材料和方法:Epifractan(EPI)是一种大麻药用提取物,含有大量大麻二酚(CBD)、萜类化合物和黄酮类化合物等成分、微量Δ9-四氢大麻酚和酸型 CBD。我们通过免疫细胞化学分析法分析了神经元和星形胶质细胞的细胞活力和形态,从而确定了 EPI 抵消鱼藤酮诱导的神经毒性的能力。将 EPI 的效果与 XALEX(一种从植物中提取的高度纯化的 CBD 制剂(XAL))和纯 CBD 晶体(CBD)进行了比较。结果显示结果表明,EPI能在很大浓度范围内显著降低鱼藤酮诱导的神经毒性,而本身不会引起神经毒性。EPI 的效果与 XAL 相似,这表明 EPI 中的单个物质之间没有发生相加或协同作用。相比之下,CBD 的情况与 EPI 和 XAL 不同,因为在检测的较高浓度下,CBD 本身就会产生神经毒性效应。EPI 配方中使用的中链甘油三酯油可以解释这种差异。结论我们的数据支持 EPI 的神经保护作用,它可以在不同的神经退行性过程中提供神经保护。研究结果强调了 CBD 作为 EPI 活性成分的作用,但同时也证明需要适当的配方来稀释药用大麻产品,这对于避免高剂量的神经毒性至关重要。
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Neuroprotective Effect of a Pharmaceutical Extract of Cannabis with High Content on CBD Against Rotenone in Primary Cerebellar Granule Cell Cultures and the Relevance of Formulations.

Introduction: Preclinical research supports the benefits of pharmaceutical cannabis-based extracts for treating different medical conditions (e.g., epilepsy); however, their neuroprotective potential has not been widely investigated. Materials and Methods: Using primary cultures of cerebellar granule cells, we evaluated the neuroprotective activity of Epifractan (EPI), a cannabis-based medicinal extract containing a high level of cannabidiol (CBD), components like terpenoids and flavonoids, trace levels of Δ9-tetrahydrocannabinol, and the acid form of CBD. We determined the ability of EPI to counteract the rotenone-induced neurotoxicity by analyzing cell viability and morphology of neurons and astrocytes by immunocytochemical assays. The effect of EPI was compared with XALEX, a plant-derived and highly purified CBD formulation (XAL), and pure CBD crystals (CBD). Results: The results revealed that EPI induced a significant reduction in the rotenone-induced neurotoxicity in a wide range of concentrations without causing neurotoxicity per se. EPI showed a similar effect to XAL suggesting that no additive or synergistic interactions between individual substances present in EPI occurred. In contrast, CBD did show a different profile to EPI and XAL because a neurotoxic effect per se was observed at higher concentrations assayed. Medium-chain triglyceride oil used in EPI formulation could explain this difference. Conclusion: Our data support a neuroprotective effect of EPI that may provide neuroprotection in different neurodegenerative processes. The results highlight the role of CBD as the active component of EPI but also support the need for an appropriate formulation to dilute pharmaceutical cannabis-based products that could be critical to avoid neurotoxicity at very high doses.

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来源期刊
Cannabis and Cannabinoid Research
Cannabis and Cannabinoid Research PHARMACOLOGY & PHARMACY-
CiteScore
6.80
自引率
7.90%
发文量
164
期刊最新文献
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