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载有壬二酸的液晶系统的配方与特性研究及其经皮给药。

Formulation and characterization of liquid crystal systems containing azelaic acid for topical delivery.

机构信息

Department of Pharmaceutical Technology, Hacettepe University, Faculty of Pharmacy, Ankara, Turkey.

出版信息

Drug Dev Ind Pharm. 2013 Feb;39(2):228-39. doi: 10.3109/03639045.2012.671829. Epub 2012 Apr 5.

Abstract

PURPOSE

The aim of this study is to prepare and characterize azelaic acid (AzA) containing liquid crystal (LC) drug delivery systems for topical use.

METHODS

Two ternary phase diagrams, containing liquid paraffin as the oil component and a mixture of two nonionic surfactants (Brij 721P and Brij 72), were constructed. Formulations chosen from the phase diagrams were characterized by polarized light microscopy, rheological analyses, differential scanning calorimetry (DSC), and small angle x-ray scattering spectroscopy.

RESULTS

Polarized light microscopy proved that except the oil/water emulsion (O/W E), other formulations showed lamellar LC structure. In vitro release studies indicated that the fastest release was achieved by the Lamellar LC (LLC) and O/W E systems, whereas slower release was obtained from the emulsion containing lamellar LC (E-LLC) and distorted lamellar LC (D-LLC) systems. Results of rheological measurements both supported the results of in vitro release studies and showed that the emulsion containing the LC (E-LLC) system had the most stable structure. The formulations and their effect on stratum corneum (SC) were evaluated by DSC studies. The lamellar LC (LLC), emulsion containing lamellar liquid crystal (E-LLC), and O/W E formulations had an effect on both lipid and protein components of SC, whereas distorted lamellar liquid crystal (D-LLC) system had an effect on only the lipid components of SC.

CONCLUSIONS

LLC systems could be considered promising for the topical delivery of AzA.

摘要

目的

本研究旨在制备并表征用于局部应用的含壬二酸(AzA)的液晶(LC)药物传递系统。

方法

构建了两个包含液体石蜡作为油相和两种非离子表面活性剂(Brij 721P 和 Brij 72)混合物的三元相图。从相图中选择的配方通过偏光显微镜、流变分析、差示扫描量热法(DSC)和小角 X 射线散射光谱法进行表征。

结果

偏光显微镜证明,除了油/水乳液(O/W E)外,其他配方均显示层状 LC 结构。体外释放研究表明,层状 LC(LLC)和 O/W E 系统的释放最快,而含有层状 LC 的乳液(E-LLC)和变形层状 LC(D-LLC)系统的释放较慢。流变学测量结果均支持体外释放研究结果,并表明含有 LC 的乳液(E-LLC)系统具有最稳定的结构。通过 DSC 研究评估了配方及其对角质层(SC)的影响。层状 LC(LLC)、含层状液晶的乳液(E-LLC)和 O/W E 制剂对 SC 的脂质和蛋白质成分均有影响,而变形层状液晶(D-LLC)系统仅对 SC 的脂质成分有影响。

结论

LLC 系统可被认为是 AzA 局部递送的有前途的制剂。

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