Examining the hepatotoxic potential of cannabidiol, cannabidiol-containing hemp extract, and cannabinol at consumer-relevant exposure concentrations in primary human hepatocytes

IF 2.7 4区 医学 Q3 TOXICOLOGY Journal of Applied Toxicology Pub Date : 2024-06-26 DOI:10.1002/jat.4646
Anneliese Striz, Yang Zhao, Estatira Sepehr, Cory Vaught, Kirsten Eckstrum, Kyra Headrick, Jeffrey Yourick, Robert Sprando
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Abstract

Hemp extracts and consumer products containing cannabidiol (CBD) and/or other phytocannabinoids derived from hemp have entered the marketplace in recent years. CBD is an approved drug in the United States for the treatment of certain seizure disorders. While effects of CBD in the liver have been well characterized, data on the effects of other cannabinoids and hemp extracts in the liver and methods for studying these effects in vitro are limited. This study examined the hepatotoxic potential of CBD, CBD concentration-matched hemp extract, and cannabinol (CBN), at consumer-relevant concentrations determined by in silico modeling, in vitro using primary human hepatocytes. Primary human hepatocytes exposed to between 10-nM and 25-μM CBD, CBN, or hemp extract for 24 and 48 h were evaluated by measuring lactate dehydrogenase release, apoptosis, albumin secretion, urea secretion, and mitochondrial membrane potential. Cell viability was not significantly affected by CBD, CBN, or the hemp extract at any of the concentrations tested. Exposure to hemp extract induced a modest but statistically significant decrease in albumin secretion, urea secretion, and mitochondrial membrane potential at the highest concentration tested whereas CBD only induced a modest but statistically significant decrease in albumin secretion compared with vehicle control. Although this study addresses data gaps in the understanding of cannabinoid hepatoxicity in vitro, additional studies will be needed to determine how these results correlate with relevant consumer exposure and the biological effects of cannabinoids in human liver.

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研究大麻二酚、含大麻二酚的大麻提取物和大麻酚在初级人类肝细胞中与消费者相关的暴露浓度下的肝毒性潜力。
近年来,含有大麻二酚(CBD)和/或其他从大麻中提取的植物大麻素的大麻提取物和消费品已进入市场。大麻二酚是美国批准用于治疗某些癫痫发作疾病的药物。虽然 CBD 对肝脏的影响已被充分描述,但有关其他大麻素和大麻提取物对肝脏影响的数据以及体外研究这些影响的方法却很有限。本研究使用原代人类肝细胞,在体外研究了 CBD、CBD 浓度匹配的大麻提取物和大麻酚(CBN)的肝脏毒性潜力,其浓度是通过硅学建模确定的消费者相关浓度。将原代人类肝细胞暴露于 10-nM 至 25-μM 的 CBD、CBN 或大麻提取物中 24 小时和 48 小时,通过测量乳酸脱氢酶释放、细胞凋亡、白蛋白分泌、尿素分泌和线粒体膜电位进行评估。在任何测试浓度下,CBD、CBN 或大麻提取物对细胞活力都没有明显影响。在测试的最高浓度下,暴露于大麻提取物会导致白蛋白分泌、尿素分泌和线粒体膜电位略有下降,但在统计学上有显著影响;而与车辆对照相比,CBD 只导致白蛋白分泌略有下降,但在统计学上有显著影响。虽然这项研究填补了体外大麻素肝毒性认识方面的数据空白,但还需要进行更多的研究,以确定这些结果与消费者的相关接触以及大麻素在人体肝脏中的生物效应之间的关联。
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来源期刊
CiteScore
7.00
自引率
6.10%
发文量
145
审稿时长
1 months
期刊介绍: Journal of Applied Toxicology publishes peer-reviewed original reviews and hypothesis-driven research articles on mechanistic, fundamental and applied research relating to the toxicity of drugs and chemicals at the molecular, cellular, tissue, target organ and whole body level in vivo (by all relevant routes of exposure) and in vitro / ex vivo. All aspects of toxicology are covered (including but not limited to nanotoxicology, genomics and proteomics, teratogenesis, carcinogenesis, mutagenesis, reproductive and endocrine toxicology, toxicopathology, target organ toxicity, systems toxicity (eg immunotoxicity), neurobehavioral toxicology, mechanistic studies, biochemical and molecular toxicology, novel biomarkers, pharmacokinetics/PBPK, risk assessment and environmental health studies) and emphasis is given to papers of clear application to human health, and/or advance mechanistic understanding and/or provide significant contributions and impact to their field.
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