Pharmacokinetics of Cannabidiol: A Systematic Review and Meta-Regression Analysis.

IF 3.1 4区 医学 Q2 PHARMACOLOGY & PHARMACY
Cannabis and Cannabinoid Research Pub Date : 2024-08-01 Epub Date: 2023-08-29 DOI:10.1089/can.2023.0025
Ehsan Moazen-Zadeh, Alexandra Chisholm, Keren Bachi, Yasmin L Hurd
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引用次数: 0

Abstract

Background: In this review, we provide an updated assessment of available evidence on the pharmacokinetics (PK) of CBD and explore the impact of different factors on PK outcomes. Materials and Methods: This systematic review and meta-regression analysis was preregistered (PROSPERO: CRD42021269857). We systematically searched Medline, Embase, PsycInfo, and Web of Science Core Collection up to November 19, 2022. Trials of CBD in healthy adults were included if they reported at least one of the PK parameters of interest, including Tmax, Cmax, AUC0-t, AUC0-inf, and T1/2, in serum or plasma. Studies of patient populations or CBD co-administration with other medications were excluded. The National Heart, Lung, and Blood Institute's Quality Assessment Tool for Before-After Studies with no Control Group was used. Random-effects multivariable meta-regression analysis was conducted. Results: A total of 112 trial arms from 39 studies were included; 26 trial arms had a "Good" quality, 70 "Fair," and 16 "Poor." Eight arms used inhalation CBD, 29 oromucosal, 73 oral, and 2 intravenous. CBD formulations could be categorized to nanotech (n=14), oil-based (n=21), alcohol-based (n=10), water-based (n=12), Sativex (n=17), and Epidiolex® (n=22). For single-dose studies, CBD doses ranged between 2 and 100 mg in inhalation, 5-50 mg in oromucosal, and 0.42-6000 mg in oral administration. Sixty-six trial arms had only male participants or a higher number of male than female participants. The duration of the PK session was between 4 and 164 h. A higher CBD dose was associated with higher Cmax, AUC0-t, and AUC0-inf. Compared with oral administration, oromucosal administration was associated with lower Cmax, AUC0-t, and AUC0-inf. Fed status was associated with higher Cmax and AUC0-t when compared with the fasting status. A higher ratio of female participants was associated with lower Tmax in oral administration and higher Cmax. Conclusion: As expected, CBD dose, route of administration, and diet were major determinants of CBD PK with oral routes providing higher bioavailability and nanotechnology formulations a faster onset. Although CBD appeared to have a faster onset and longer duration in women, more studies are required to delineate the role of biological sex. Factors that influence CBD PK have implications for medication development and appropriate dosing in clinical practice.

大麻二酚的药代动力学:系统综述和荟萃回归分析。
背景:在这篇综述中,我们对CBD的药代动力学(PK)的现有证据进行了最新评估,并探讨了不同因素对PK结果的影响。材料和方法:该系统综述和元回归分析是预先注册的(PROSPERO:CD42021269857)。截至2022年11月19日,我们系统搜索了Medline、Embase、PsycInfo和Web of Science核心收藏。如果健康成年人报告了血清或血浆中至少一个感兴趣的PK参数,包括Tmax、Cmax、AUC0-t、AUC0-inf和T1/2,则纳入CBD试验。排除了对患者群体或CBD与其他药物联合给药的研究。使用美国国家心肺血液研究所的无对照组前后研究质量评估工具。进行随机效应多变量元回归分析。结果:共纳入39项研究的112个试验组;26个试验组的质量为“良好”,70个为“一般”,16个为“较差”。8个试验组使用吸入CBD,29个为口腔粘膜,73个为口服,2个为静脉注射。CBD制剂可分为纳米技术(n=14)、油基(n=21)、醇基(n=10)、水性(n=12)、Sativex(n=17)和Epidiolex®(n=22)。对于单剂量研究,CBD剂量在2至100之间 mg吸入,5-50 口腔粘膜中为mg,0.42-6000 mg口服给药。66个试验组只有男性参与者,或者男性参与者的数量高于女性。PK的持续时间在4到164之间 h.较高的CBD剂量与较高的Cmax、AUC0-t和AUC0-inf相关。与口服给药相比,口腔粘膜给药与较低的Cmax、AUC0-t和AUC0-inf相关。与禁食状态相比,进食状态与较高的Cmax和AUC0-t相关。女性参与者比例越高,口服给药的Tmax越低,Cmax越高。结论:正如预期的那样,CBD剂量、给药途径和饮食是CBD PK的主要决定因素,口服途径提供了更高的生物利用度,纳米技术制剂起效更快。尽管CBD在女性中的发病速度更快,持续时间更长,但还需要更多的研究来描述生物学性别的作用。影响CBD PK的因素对药物开发和临床实践中的适当剂量有影响。
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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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
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