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水凝胶形成微阵列贴片介导盐酸四环素的透皮给药。

Hydrogel-forming microarray patch mediated transdermal delivery of tetracycline hydrochloride.

作者信息

Zhao Li, Vora Lalitkumar K, Kelly Stephen A, Li Linlin, Larrañeta Eneko, McCarthy Helen O, Donnelly Ryan F

机构信息

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

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

出版信息

J Control Release. 2023 Apr;356:196-204. doi: 10.1016/j.jconrel.2023.02.031. Epub 2023 Mar 7.

DOI:10.1016/j.jconrel.2023.02.031
PMID:36868520
Abstract

Antibiotic resistance is one of the most serious health problems today and is expected to worsen in the coming decades. It has been suggested that antibiotic administration routes that bypass the human gut could potentially tackle this problem. In this work, an antibiotic hydrogel-forming microarray patch (HF-MAP) system, which can be used as an alternative antibiotic delivery technology, has been fabricated. Specifically, poly(vinyl alcohol)/poly(vinylpyrrolidone) (PVA/PVP) microarray showed excellent swelling properties with >600% swelling in PBS over 24 h. The tips on the HF-MAP were proven to be able to penetrate a skin model which is thicker than stratum corneum. The antibiotic (tetracycline hydrochloride) drug reservoir was mechanically robust and dissolved completely in an aqueous medium within a few minutes. In vivo animal studies using a Sprague Dawley rat model showed antibiotic administration using HF-MAP achieved a sustained release profile, in comparison with animals receiving oral gavage and intravenous (IV) injection, with a transdermal bioavailability of 19.1% and an oral bioavailability of 33.5%. The maximum drug plasma concentration for HF-MAP group reached 7.40 ± 4.74 μg/mL at 24 h, whereas the drug plasma concentration for both oral (5.86 ± 1.48 μg/mL) and IV (8.86 ± 4.19 μg/mL) groups peaked soon after drug administration and had decreased to below the limit of detection at 24 h. The results demonstrated that antibiotics can be delivered by HF-MAP in a sustained manner.

摘要

抗生素耐药性是当今最严重的健康问题之一,预计在未来几十年还会恶化。有人提出,绕过人体肠道的抗生素给药途径可能有助于解决这一问题。在这项工作中,一种可作为替代抗生素递送技术的抗生素水凝胶形成微阵列贴片(HF-MAP)系统已被制造出来。具体而言,聚乙烯醇/聚乙烯吡咯烷酮(PVA/PVP)微阵列在PBS中24小时内具有超过600%的优异溶胀性能。HF-MAP上的尖端被证明能够穿透比角质层更厚的皮肤模型。抗生素(盐酸四环素)药物储库机械强度高,能在几分钟内完全溶解于水性介质中。使用Sprague Dawley大鼠模型进行的体内动物研究表明,与接受灌胃和静脉注射的动物相比,使用HF-MAP给药实现了持续释放,经皮生物利用度为19.1%,口服生物利用度为33.5%。HF-MAP组在24小时时的最大血浆药物浓度达到7.40±4.74μg/mL,而口服组(5.86±1.48μg/mL)和静脉注射组(8.86±4.19μg/mL)在给药后不久血浆药物浓度就达到峰值,并在24小时时降至检测限以下。结果表明,抗生素可以通过HF-MAP持续递送。

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