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直接压片:一种结合水凝胶形成微针阵列的新型含药储库用于经皮给药。

Directly Compressed Tablets: A Novel Drug-Containing Reservoir Combined with Hydrogel-Forming Microneedle Arrays for Transdermal Drug Delivery.

作者信息

McAlister Emma, Dutton Bridie, Vora Lalitkumar K, Zhao Li, Ripolin Anastasia, Zahari Dk Siti Zawanah Binti Pg Hj, Quinn Helen L, Tekko Ismaiel A, Courtenay Aaron J, Kelly Stephen A, Rodgers Aoife M, Steiner Lilach, Levin Galit, Levy-Nissenbaum Etgar, Shterman Nava, McCarthy Helen O, Donnelly Ryan F

机构信息

School of Pharmacy, Queen's University Belfast, 97 Lisburn Road, Belfast, BT9 7BL, Ireland.

Health and Social Care Board, 12-22 Linenhall Street, Belfast, BT2 8BS, Ireland.

出版信息

Adv Healthc Mater. 2021 Feb;10(3):e2001256. doi: 10.1002/adhm.202001256. Epub 2020 Dec 14.

DOI:10.1002/adhm.202001256
PMID:33314714
Abstract

Microneedle (MN) patches consist of a hydrogel-forming MN array and a drug-containing reservoir. Drug-containing reservoirs documented in the literature include polymeric films and lyophilized wafers. While effective, both reservoir formulations are aqueous based, and so degradation can occur during formulation and drying for drugs inherently unstable in aqueous media. The preparation and characterization of novel, nonaqueous-based, directly compressed tablets (DCTs) for use in combination with hydrogel-forming MN arrays are described for the first time. In this work, a range of drug molecules are investigated. Precipitation of amoxicillin (AMX) and primaquine (PQ) in conventional hydrogel-forming MN arrays leads to use of poly(vinyl alcohol)-based MN arrays. Following in vitro permeation studies, in vivo pharmacokinetic studies are conducted in rats with MN patches containing AMX, levodopa/carbidopa (LD/CD), and levofloxacin (LVX). Therapeutically relevant concentrations of AMX (≥2 µg mL ), LD (≥0.5 µg mL ), and LVX (≥0.2 µg mL ) are successfully achieved at 1, 2, and 1 h, respectively. Thus, the use of DCTs offers promise to expand the range of drug molecules that can be delivered transdermally using MN patches.

摘要

微针(MN)贴片由形成水凝胶的微针阵列和含药储库组成。文献中记载的含药储库包括聚合物薄膜和冻干薄片。虽然这两种储库制剂都有效,但它们都是水基的,因此对于在水性介质中固有不稳定的药物,在制剂和干燥过程中可能会发生降解。首次描述了与形成水凝胶的微针阵列结合使用的新型非水基直接压片(DCT)的制备和表征。在这项工作中,研究了一系列药物分子。阿莫西林(AMX)和伯氨喹(PQ)在传统的形成水凝胶的微针阵列中沉淀,导致使用基于聚乙烯醇的微针阵列。在体外渗透研究之后,对含有AMX、左旋多巴/卡比多巴(LD/CD)和左氧氟沙星(LVX)的微针贴片在大鼠中进行了体内药代动力学研究。分别在1、2和1小时成功达到了治疗相关浓度的AMX(≥2μg/mL)、LD(≥0.5μg/mL)和LVX(≥0.2μg/mL)。因此,使用DCT有望扩大可以使用微针贴片经皮递送的药物分子范围。

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