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Design, Development and Optimization of Nimesulide-Loaded Liposomal Systems for Topical Application

机译:局部应用尼美舒利脂质体系统的设计,开发和优化

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Nimesulide, a non-steroidal anti-inflammatory drug, was incorporated into multilamellar liposomes to improve its performance on topical administration. The drug was loaded onto liposomes employing thin film hydration technique. Various process and formulation variables were investigated to obtain the liposomal products of desired quality. Liposomes were monitored for percent drug entrapment, after separating the unentrapped drug by mini column centrifugation, for vesicular properties (such as size distribution profile, morphological attributes and agglomeration tendency), drug diffused through synthetic semipermeable membrane, and drug leakage. Systematic optimization studies were carried out using 32 factorial design to select the optimized liposomal composition with reference to percent drug entrapment, drug diffusion and leakage. The optimized batch of liposomes was subjected to drug permeation and drug retention studies employing rat skin and human cadaver skin. In comparison to methanolic solution of pure nimesulide, liposomal formulations were found to retain higher amounts of nimesulide in the skin. Anti-inflammatory studies, using carragenan-induced rat paw edema model, indicated significantly better performance of liposomally entrapped nimesulide in comparison to the marketed gel formulation and the Carbopol gel containing nimesulide.
机译:尼美舒利是一种非甾体类抗炎药,已掺入多层脂质体中,以改善局部给药的性能。采用薄膜水化技术将药物加载到脂质体上。研究了各种工艺和配方变量以获得所需质量的脂质体产品。在通过微型柱离心分离未捕获的药物后,监测脂质体的药物截留百分比,水泡性质(例如大小分布图,形态特征和聚集趋势),药物通过合成半透膜扩散和药物渗漏的情况。使用32因子设计进行了系统优化研究,以根据药物截留,药物扩散和泄漏的百分比选择优化的脂质体组成。使用大鼠皮肤和人尸体皮肤对优化的一批脂质体进行药物渗透和药物保留研究。与纯尼美舒利的甲醇溶液相比,脂质体制剂被发现在皮肤中保留了更高量的尼美舒利。使用角叉菜胶诱导的大鼠爪水肿模型进行的抗炎研究表明,与市售的凝胶制剂和含尼美舒利的Carbopol凝胶相比,脂质体包裹的尼美舒利的性能明显更好。

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