Biological Response after 14-Day Cannabidiol and Propylene Glycol Inhalation in Sprague-Dawley Rats.

IF 3.1 4区 医学 Q2 PHARMACOLOGY & PHARMACY
Daniela Schwotzer, Justyna Kulpa, Andrew Gigliotti, Wendy Dye, Kristen Trexler, Hammad Irshad, Tim Lefever, Mark Ware, Marcel Bonn-Miller, Jacob McDonald
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Abstract

Objective: Cannabidiol (CBD), a phytocannabinoid of increasing interest for its purported therapeutic effects, is primarily consumed via ingestion and inhalation. While the toxicology of orally administered CBD has been reported, little is known about the effects of CBD inhalation. Doses selected for the present analysis allowed for evaluation of dose-response at concentrations >100-fold higher than typical human consumption levels. Materials and Methods: CBD (98.89% pure) was formulated in propylene glycol (PG) and aerosolized by nebulization to evaluate biological response after nose-only inhalation. Sprague Dawley rats (n = 35 males, 30 females) were exposed to 1.0 and 1.3 mg/L nominal concentrations of CBD and PG, respectively, for 12-180 min. Resulting average daily presented dose ranges were 8.9-138.5 mg/kg CBD and 11.3-176.0 mg/kg PG. Aerosols of 1.4 µm median diameter were achieved. Biological response indicators included clinical signs, clinical chemistry, hematology, body/organ weights, and pulmonary/systemic histopathology. Results: Inflammatory and necrotic responses were observed in the nose at the highest doses of CBD. Limited findings in the larynx and lung were mainly observed at higher doses. There were no histological findings in extrapulmonary organs. Dosimetry modeling differentiated the no observable adverse effect level between the nasal region and lungs to be 2.8 and 10.6 mg/kg CBD, respectively. Conclusions: Dose-depending findings of histological changes in the respiratory tract are observed at high doses. At lower doses consistent with typical over-the-counter vape products there appears to be substantial safety margin in the present study (93- and 353-fold lower for nose and lung, respectively).

Sprague-Dawley 大鼠吸入 14 天大麻二酚和丙二醇后的生物反应。
目的:大麻二酚(CBD)是一种植物大麻素,因其所谓的治疗效果而受到越来越多的关注。虽然口服 CBD 的毒理学已有报道,但对吸入 CBD 的影响却知之甚少。本分析所选择的剂量允许在浓度比典型的人类消费水平高 100 倍以上的情况下评估剂量反应。材料和方法将纯度为 98.89% 的 CBD 配制在丙二醇(PG)中,并通过雾化吸入来评估纯鼻吸入后的生物反应。斯普拉格道利大鼠(雄性 35 只,雌性 30 只)分别接触 1.0 和 1.3 mg/L 标称浓度的 CBD 和 PG 12-180 分钟。结果得出的日平均剂量范围为 8.9-138.5 毫克/千克 CBD 和 11.3-176.0 毫克/千克 PG。气溶胶的中值直径为 1.4 微米。生物反应指标包括临床症状、临床化学、血液学、体重/器官重量以及肺/系统组织病理学。结果:在CBD的最高剂量下,鼻腔出现了炎症和坏死反应。喉部和肺部的有限发现主要出现在较高剂量时。肺外器官没有组织学发现。剂量测定模型显示,鼻腔和肺部的无明显不良反应水平分别为 2.8 毫克/千克 CBD 和 10.6 毫克/千克 CBD。结论高剂量时可观察到呼吸道组织学变化的剂量依赖性结果。在本研究中,与典型的非处方 Vape 产品一致的较低剂量似乎有很大的安全余量(鼻腔和肺部分别低 93 倍和 353 倍)。
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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