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基于微乳的甲磺酸雷沙吉兰透皮凝胶:用于帕金森病治疗的体外和体内评估。

Microemulsion-based gel for the transdermal delivery of rasagiline mesylate: In vitro and in vivo assessment for Parkinson's therapy.

机构信息

Department of Pharmaceutical Sciences and Technology, Institute of Chemical Technology, Matunga, Mumbai 400019, Maharashtra, India; Department of Chemical Sciences, Bernal Institute, University of Limerick, Limerick, Ireland.

Department of Pharmaceutical Sciences and Technology, Institute of Chemical Technology, Matunga, Mumbai 400019, Maharashtra, India; R&D, Loreal R&D, Mumbai, India.

出版信息

Eur J Pharm Biopharm. 2021 Aug;165:66-74. doi: 10.1016/j.ejpb.2021.04.026. Epub 2021 May 7.

DOI:10.1016/j.ejpb.2021.04.026
PMID:33971272
Abstract

Rasagiline mesylate (RSM) is a selective and irreversible monoamine oxidase B inhibitor used for the treatment of Parkinson's disease (PD). However, its unfavorable biopharmaceutical properties, such as extensive degradation in the gastrointestinal tract and first-pass metabolism are responsible for its low oral bioavailability and suboptimal therapeutic efficacy. Here, we report the feasibility of delivering RSM via the transdermal route using RSM containing microemulsion-based gel (RSM-MEG) to achieve effective management of PD. Our in vitro skin permeation studies of RSM-MEG showed significantly higher (at least ~1.5-fold) permeation across rat skin compared to the conventional RSM hydrogel. Our skin irritation studies in rabbits showed that RSM-MEG is safe for transdermal application. Finally, using the rat model of rotenone-induced Parkinsonism, we demonstrated that the topical application of RSM-MEG was equally effective in reversing PD symptoms when compared to oral RSM therapy. Thus, our study confirmed the feasibility and potential of transdermal delivery of RSM via simple topical application of RSM-MEG, and this approach could be an alternative therapeutic intervention for the treatment of Parkinson's disease.

摘要

甲磺酸雷沙吉兰(RSM)是一种选择性和不可逆的单胺氧化酶 B 抑制剂,用于治疗帕金森病(PD)。然而,其不利的生物制药特性,如在胃肠道中的广泛降解和首过代谢,导致其口服生物利用度低和治疗效果不佳。在这里,我们报告了使用含有微乳基凝胶的 RSM(RSM-MEG)通过透皮途径输送 RSM 的可行性,以实现对 PD 的有效管理。我们对 RSM-MEG 的体外皮肤渗透研究表明,与常规 RSM 水凝胶相比,RSM-MEG 在大鼠皮肤上的渗透明显更高(至少高出 1.5 倍)。我们在兔子中的皮肤刺激性研究表明,RSM-MEG 适用于透皮应用。最后,使用鱼藤酮诱导的帕金森病大鼠模型,我们证明与口服 RSM 治疗相比,RSM-MEG 的局部应用在逆转 PD 症状方面同样有效。因此,我们的研究证实了通过简单的 RSM-MEG 局部应用透皮递送 RSM 的可行性和潜力,这种方法可能是治疗帕金森病的一种替代治疗干预措施。

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