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犬类中大麻二酚的药代动力学。

Pharmacokinetics of cannabidiol in dogs.

作者信息

Samara E, Bialer M, Mechoulam R

机构信息

Department of Pharmacy, School of Pharmacy, Hebrew University, Jerusalem, Israel.

出版信息

Drug Metab Dispos. 1988 May-Jun;16(3):469-72.

PMID:2900742
Abstract

Cannabidiol (CBD) is one of the major nonpsychoactive cannabinoids produced by Cannabis sativa L. Recent studies have shown that CBD has a high protective index, comparable to that of phenobarbital and phenytoin. Because CBD has been reported to possess both anticonvulsant and antiepileptic activity, its pharmacokinetics were studied in dogs after the administration of two iv doses (45 and 90 mg) and one oral dose (180 mg) to dogs. After iv administration, CBD was rapidly distributed, followed by a prolonged elimination. It has a terminal half-life of 9 hr. CBD plasma levels declined in a triphasic fashion. The total body clearance of CBD was 17 liters/hr (after the 45-mg dose) and 16 liters/hr (after the 90-mg dose). This clearance value, after its normalization to blood clearance using mathematical equations, approaches the value of the hepatic blood flow; the extraction ratio in the liver is 0.74. CBD was observed to have a large volume of distribution, approximately 100 liters. In the dose range of 45 to 90 mg, the increase in the AUC was proportional to the dose, a fact that indicates that the pharmacokinetic profile of CBD in this dose range was not dose dependent. In three of the six dogs studied, CBD could not be detected in the plasma after oral administration. In the other three, the oral bioavailability ranged from 13 to 19%. The results of this study show that CBD is barely absorbed after oral administration to dogs. This low bioavailability may be due to a first pass effect.

摘要

大麻二酚(CBD)是大麻植株产生的主要非精神活性大麻素之一。最近的研究表明,CBD具有较高的保护指数,与苯巴比妥和苯妥英相当。由于据报道CBD具有抗惊厥和抗癫痫活性,因此在给犬静脉注射两个剂量(45毫克和90毫克)和一个口服剂量(180毫克)后,对其药代动力学进行了研究。静脉注射后,CBD迅速分布,随后消除过程延长。其终末半衰期为9小时。CBD血浆水平呈三相下降。CBD的全身清除率为17升/小时(45毫克剂量后)和16升/小时(90毫克剂量后)。使用数学方程将该清除率值归一化为血清除率后,接近肝血流量的值;肝脏中的提取率为0.74。观察到CBD的分布容积较大,约为100升。在45至90毫克的剂量范围内,AUC的增加与剂量成正比,这一事实表明该剂量范围内CBD的药代动力学特征不依赖于剂量。在研究的6只犬中,有3只口服给药后血浆中未检测到CBD。在另外3只犬中,口服生物利用度为13%至19%。本研究结果表明,犬口服CBD后几乎不被吸收。这种低生物利用度可能是由于首过效应。

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