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Drug-inorganic-polymer nanohybrid for transdermal delivery

机译:用于透皮递送的药物-无机-聚合物纳米杂化物

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For transdermal drug delivery, we prepared a drug-inorganic nanohybrid (FB-LDH) by intercalating a transdermal model drug, flurbiprofen (FB), into the layered double hydroxides (LDHs) via coprecipitation reaction. The X-ray diffraction patterns and FT-IR spectra of the FB-LDH indicated that the FB molecules were successfully intercalated via electrostatic interaction within the LDH lattices. The in vitro drug release revealed that the Eudragit? S-100 in release media could facilitate the drug out-diffusion by effectively replacing the intercalated drug and also enlarging the lattice spacing of the FB-LDH. In this work, a hydrophobic gel suspension of the FB-LDH was suggested as a transdermal controlled delivery formulation, where the suspensions were mixed with varying amounts of Eudragit? S-100 aqueous solution. The Frantz diffusion cell experiments using mouse full-skins showed that a lag time and steady-state flux of the drug could be controlled from 12.8 h and 3.28 ??g cm-2 h-1 to less than 1 h and 14.57 ??g cm-2 h-1, respectively, by increasing the mass fraction of Eudragit? S-100 solution in gel suspensions from 0% to 20% (w/w), respectively. Therefore, we conclude gel formulation of the FB-LDH have a potential for transdermal controlled drug delivery. ? 2013 Elsevier B.V. All rights reserved.
机译:对于透皮药物递送,我们通过共沉淀反应将透皮模型药物氟比洛芬(FB)插入层状双氢氧化物(LDHs)中,从而制备了一种药物-无机纳米混合物(FB-LDH)。 FB-LDH的X射线衍射图和FT-IR光谱表明,FB分子通过LDH晶格内的静电相互作用成功嵌入。体外药物释放显示Eudragit?释放介质中的S-100可以通过有效替换嵌入的药物并扩大FB-LDH的晶格间距来促进药物向外扩散。在这项工作中,FB-LDH的疏水性凝胶悬浮液被建议作为一种透皮控制递送制剂,其中该悬浮液与不同量的Eudragit®混合。 S-100水溶液。使用小鼠全皮肤进行的Frantz扩散池实验表明,该药物的滞后时间和稳态通量可以控制在12.8 h和3.28 ?? g cm-2 h-1到不到1 h和14.57 ?? g cm-2 h-1,分别通过增加Eudragit?的质量分数得到。凝胶悬浮液中的S-100溶液浓度分别为0%至20%(w / w)。因此,我们得出结论,FB-LDH的凝胶制剂具有经皮控制药物传递的潜力。 ? 2013 Elsevier B.V.保留所有权利。

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