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通过口腔黏膜延长阿扑吗啡的递送,开发用于帕金森病的非侵入性持续给药方法:在猪体内的研究。

Prolonged Delivery of Apomorphine Through the Buccal Mucosa, Towards a Noninvasive Sustained Administration Method in Parkinson's Disease: In Vivo Investigations in Pigs.

机构信息

Institute for Drug Research, School of Pharmacy, Faculty of Medicine, The Hebrew University of Jerusalem, P.O. Box 12065, Jerusalem 91120, Israel.

Institute for Drug Research, School of Pharmacy, Faculty of Medicine, The Hebrew University of Jerusalem, P.O. Box 12065, Jerusalem 91120, Israel.

出版信息

J Pharm Sci. 2021 Apr;110(4):1824-1833. doi: 10.1016/j.xphs.2020.12.010. Epub 2020 Dec 14.

DOI:10.1016/j.xphs.2020.12.010
PMID:33333142
Abstract

In the current work, prolonged systemic delivery of apomorphine via buccal mucosa was shown to be a promising treatment for Parkinson's disease as a substitute for clinically utilized subcutaneous infusions. Due to extensive 'first-pass' metabolism, apomorphine is administered parenterally to bypass liver metabolism. Drawbacks of parenteral administration cause low patient compliance and adherence to treatment. On the other hand, while also bypassing the liver, delivery through buccal mucosa has a superior safety profile, is less costly, lacks pain and discomfort, and possesses excellent accessibility, overall augmenting patient compliance. Current in vivo study in pigs showed: (1) steady plateau levels of apomorphine in plasma were obtained 30 min following administration and remained constant for 8 h until a delivery device was removed, (2) bioavailability of apomorphine was 55%-80% as opposed to <2% peroral and (3) simulation of the pharmacokinetic profile obtained in pigs predicted therapeutically relevant levels of apomorphine in human. Furthermore, antipyrine was incorporated as a permeation marker to enable mechanistic investigation of apomorphine release from the delivery device and its permeation through the buccal mucosa. In addition, limitations of an Ussing diffusion chamber as an ex vivo research tool were also discussed.

摘要

在当前的工作中,通过颊黏膜长时间系统递送阿扑吗啡被证明是治疗帕金森病的一种很有前途的方法,可以替代临床上使用的皮下输注。由于广泛的“首过”代谢,阿扑吗啡被给予肠胃外途径以绕过肝脏代谢。肠胃外给药的缺点导致患者对治疗的依从性和顺应性低。另一方面,虽然通过颊黏膜给药也绕过了肝脏,但它具有更好的安全性、成本更低、无疼痛和不适,并且具有极好的可及性,总体上提高了患者的依从性。目前在猪体内的研究表明:(1)给药后 30 分钟,血浆中阿扑吗啡达到稳定的平台水平,并在 8 小时内保持不变,直到卸下给药装置;(2)阿扑吗啡的生物利用度为 55%-80%,而口服给药则小于 2%;(3)在猪中模拟获得的药代动力学特征预测了人类中阿扑吗啡的治疗相关水平。此外,还将安替比林作为渗透标记物加入,以能够对从给药装置释放的阿扑吗啡及其通过颊黏膜的渗透进行机制研究。此外,还讨论了 Ussing 扩散室作为体外研究工具的局限性。

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引用本文的文献

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Curr Drug Targets. 2024;25(15):987-1011. doi: 10.2174/0113894501312703240826070530.
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The Management of Parkinson's Disease: An Overview of the Current Advancements in Drug Delivery Systems.帕金森病的管理:药物递送系统当前进展概述
Pharmaceutics. 2023 May 15;15(5):1503. doi: 10.3390/pharmaceutics15051503.
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A deep eutectic-based, self-emulsifying subcutaneous depot system for apomorphine therapy in Parkinson's disease.
基于深共晶溶剂的阿扑吗啡皮下储库系统用于帕金森病的治疗。
Proc Natl Acad Sci U S A. 2022 Mar 1;119(9). doi: 10.1073/pnas.2110450119.