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喷他佐辛透皮给药系统的制剂与体外评价

Formulation and in vitro evaluation of pentazocine transdermal delivery system.

作者信息

Furuishi Takayuki, Io Takeshi, Fukami Toshiro, Suzuki Toyofumi, Tomono Kazuo

机构信息

Research Unit of Pharmaceutics, College of Pharmacy, Nihon University, Chiba, Japan.

出版信息

Biol Pharm Bull. 2008 Jul;31(7):1439-43. doi: 10.1248/bpb.31.1439.

Abstract

The aim of this study was to prepare a pentazocine (PTZ) matrix-type transdermal drug delivery system (TDDS) using acrylic pressure-sensitive adhesives. Among the five Duro-Tak adhesive polymers tested (87-9301, 87-2677, 87-201A, 87-2196, 87-2852), in vitro dissolution studies demonstrated the highest PTZ release flux from the Duro-Tak 87-9301 matrix. In addition, the effects of permeation enhancers, isopropyl myristate (IPM) and glyceryl monocaprylate (GEFA-C(8)), and drug content on PTZ skin permeation from prepared patches were evaluated using Franz diffusion cells fitted with hairless mouse skin. IPM and GEFA-C(8) were found to produce effective flux of PTZ at a patch concentration of 10% w/w and 5% w/w, respectively. The PTZ flux increased linearly as the loading dose increased up to 30%, whereas no further increase in flux was observed at loading doses of 40% and 50% due to drug crystallization in the matrix. Thus, the highest skin permeation rate (24.2 microg/cm(2)/h) was achieved when 30% of PTZ was loaded in Duro-Tak 87-9301 with 10% IPM and 5% GEFA-C(8). These results demonstrate the feasibility of a novel narcotic-antagonist analgesic matrix-type TDDS for PTZ.

摘要

本研究的目的是使用丙烯酸类压敏胶制备喷他佐辛(PTZ)基质型透皮给药系统(TDDS)。在所测试的五种Duro-Tak胶黏聚合物(87-9301、87-2677、87-201A、87-2196、87-2852)中,体外溶出度研究表明,Duro-Tak 87-9301基质的PTZ释放通量最高。此外,使用装有无毛小鼠皮肤的Franz扩散池评估了渗透促进剂肉豆蔻酸异丙酯(IPM)和单辛酸甘油酯(GEFA-C(8))以及药物含量对所制备贴剂中PTZ皮肤渗透的影响。发现IPM和GEFA-C(8)分别在贴剂浓度为10% w/w和5% w/w时能产生有效的PTZ通量。PTZ通量随载药量增加至30%呈线性增加,而在载药量为40%和50%时,由于基质中药物结晶,未观察到通量进一步增加。因此,当在含有10% IPM和5% GEFA-C(8)的Duro-Tak 87-9301中加载30%的PTZ时,实现了最高的皮肤渗透速率(24.2微克/平方厘米/小时)。这些结果证明了一种新型的麻醉拮抗剂镇痛基质型PTZ透皮给药系统的可行性。

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