Propylene glycol and Kolliphor as solvents for systemic delivery of cannabinoids via intraperitoneal and subcutaneous routes in preclinical studies: a comparative technical note.

Kaveh Momenzadeh, Diana Yeritsyan, Nadim Kheir, Rosalyn M Nazarian, Ara Nazarian
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引用次数: 1

Abstract

Background: Substance administration to laboratory animals necessitates careful consideration and planning in order to enhance agent distribution while reducing any harmful effects from the technique. There are numerous methods for administering cannabinoids; however, several parameters must be considered, including delivery frequency, volume of administration, vehicle, and the level of competence required for staff to use these routes properly. There is a scarcity of information about the appropriate delivery method for cannabinoids in animal research, particularly those that need the least amount of animal manipulation during the course of the investigation. This study aims to assess the feasibility and potential side effects of intraperitoneal and subcutaneous injection of CBD and THC using propylene glycol or Kolliphor in animal models. By evaluating the ease of use and histopathological side effects of these solvents, this study intends to help researchers better understand an accessible long-term delivery route of administration in animal experiments while minimizing the potential confounding effects of the delivery method on the animal.

Methods: Intraperitoneal and subcutaneous methods of systemic cannabis administration were tested in rat models. Subcutaneous delivery via needle injection and continuous osmotic pump release were evaluated using propylene glycol or Kolliphor solvents. In addition, the use of a needle injection and a propylene glycol solvent for intraperitoneal (IP) administration was investigated. Skin histopathological changes were evaluated following a trial of subcutaneous injections of cannabinoids utilizing propylene glycol solvent.

Discussion: Although IP delivery of cannabinoids with propylene glycol as solvent is a viable method and is preferable to oral treatment in order to reduce gastrointestinal tract degradation, it has substantial feasibility limitations. We conclude that subcutaneous delivery utilizing osmotic pumps with Kolliphor as a solvent provides viable and consistent route of administration for long-term systemic cannabinoid delivery in the preclinical context.

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丙二醇和Kolliphor作为溶剂在临床前研究中通过腹腔和皮下途径给药大麻素:一个比较的技术说明。
背景:实验动物的物质管理需要仔细考虑和规划,以加强药物分布,同时减少技术的任何有害影响。有许多方法可以管理大麻素;但是,必须考虑几个参数,包括交付频率、管理数量、车辆和工作人员正确使用这些路线所需的能力水平。关于大麻素在动物研究中的适当递送方法的信息缺乏,特别是那些在调查过程中需要最少动物操作的信息。本研究旨在评估丙二醇或Kolliphor在动物模型上腹腔和皮下注射CBD和THC的可行性和潜在的副作用。通过评估这些溶剂的易用性和组织病理学副作用,本研究旨在帮助研究人员更好地了解动物实验中可行的长期给药途径,同时最大限度地减少给药方法对动物的潜在混淆效应。方法:采用大鼠腹腔注射和皮下注射两种给药方法。使用丙二醇或Kolliphor溶剂评估针注射皮下给药和连续渗透泵释放。此外,还研究了针注射和丙二醇溶剂用于腹腔(IP)给药的使用。皮肤组织病理学变化评估后皮下注射大麻素利用丙二醇溶剂的试验。讨论:虽然以丙二醇为溶剂的大麻素IP递送是一种可行的方法,并且比口服治疗更可取,以减少胃肠道降解,但它具有实质性的可行性局限性。我们得出的结论是,在临床前背景下,利用渗透泵与Kolliphor作为溶剂的皮下递送为长期系统性大麻素递送提供了可行和一致的管理途径。
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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