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食物对人体中大麻二酚(CBD)配方、剂量和给药的影响:临床研究的系统评价。

Food effects on the formulation, dosing, and administration of cannabidiol (CBD) in humans: A systematic review of clinical studies.

机构信息

Department of Pharmaceutical Sciences, University of Michigan College of Pharmacy, Ann Arbor, Michigan, USA.

Skaggs School of Pharmacy and Pharmaceutical Sciences, University of California San Diego, La Jolla, California, USA.

出版信息

Pharmacotherapy. 2021 Apr;41(4):405-420. doi: 10.1002/phar.2512. Epub 2021 Mar 18.

DOI:10.1002/phar.2512
PMID:33583102
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8485703/
Abstract

Cannabidiol (CBD), a non-psychotropic phytocannabinoid from the Cannabis plant, is increasingly being pursued as a treatment for differing ailments. The bioavailability and pharmacokinetics of CBD are not well understood, and proper dosing schemes have not been adequately developed for its clinical use. CBD is a lipophilic molecule and exhibits low water solubility, so its formulation expectedly impacts its gastrointestinal absorption and subsequent blood plasma concentrations. In this review article, the food effects on CBD pharmacokinetics were analyzed. Clinical trials focusing on the performance of Epidiolex, the FDA-approved CBD formulation, were found in several databases and systematically analyzed in terms of administration method, dosing schedules, and patient characteristics. 44 data sets from clinical trials were found to be useful in the quantitative analysis. Following the normalization of all the pharmacokinetic data sets by dose and patient weight, CBD exhibited a much greater bioavailability in fed patients. For Epidiolex, administration in the fed state led to lower interindividual variability and more predictable pharmacokinetics. Considering all the different oral formulations of CBD, further analysis points to the main excipient of oral CBD formulations (refined sesame seed oil) as a major contributor to the dose-dependent variations in CBD pharmacokinetics, especially affecting the fasted state. We discuss the implications of these results on the downstream pharmacodynamics of endocannabinoid receptor modulation and its broad physiological implications.

摘要

大麻二酚(CBD)是一种来自大麻植物的非精神活性植物大麻素,作为一种治疗不同疾病的方法,其应用日益受到关注。然而,人们对 CBD 的生物利用度和药代动力学了解甚少,其临床应用也没有制定出适当的剂量方案。CBD 是一种亲脂性分子,水溶性较低,因此其制剂预计会影响其在胃肠道中的吸收和随后的血浆浓度。在这篇综述文章中,分析了食物对 CBD 药代动力学的影响。在几个数据库中找到了关于美国食品和药物管理局批准的 CBD 制剂 Epidiolex 的临床试验,并对给药方法、剂量方案和患者特征进行了系统分析。从临床试验中找到了 44 个有用的数据组进行定量分析。通过对所有药代动力学数据集进行归一化,按剂量和患者体重进行归一化后,发现进食患者的 CBD 生物利用度明显更高。对于 Epidiolex,进食状态下的给药导致个体间变异性降低,药代动力学更具可预测性。考虑到 CBD 的所有不同口服制剂,进一步的分析表明,口服 CBD 制剂的主要赋形剂(精制芝麻油)是 CBD 药代动力学剂量依赖性变化的主要原因,尤其是对禁食状态的影响。我们讨论了这些结果对下游内源性大麻素受体调节的药效学及其广泛的生理意义的影响。

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