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DOE Optimization of Nano-based Carrier of Pregabalin as Hydrogel: New Therapeutic Chemometric Approaches for Controlled Drug Delivery Systems

机译:DOE优化普瑞巴林作为水凝胶的纳米基载体:药物控制系统的新疗法和化学计量学方法

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摘要

Niosomes entrapping pregabalin (PG) were prepared using span 60 and cholesterol in different molar ratios by hydration method, the remaining PG from the hydrating solution was separated from vesicles by freeze centrifugation. Optimization of nano-based carrier of pregabalin (PG) was achieved. Quality by Design strategy was successfully employed to obtain PG-loaded niosomes with the desired properties. The optimal particle size, drug release and entrapment efficiency were attained by Minitab® program using design of experiment (DOE) that predicted the best parameters by investigating the combined effect of different factors simultaneously. Pareto chart was used in the screening step to exclude the insignificant variables while response surface methodology (RSM) was used in the optimization step to study the significant factors. Best formula was selected to prepare topical hydrogels loaded with niosomal PG using HPMC and Carbopol 934. It was verified, by means of mechanical and rheological tests, that addition of the vesicles to the gel matrix affected significantly gel network. In vitro release and ex vivo permeation experiments were carried out. Delivery of PG molecules followed a Higuchi, non Fickian diffusion. The present work will be of interest for pharmaceutical industry as a controlled transdermal alternative to the conventional oral route.
机译:通过水合法使用跨度60和胆固醇以不同的摩尔比制备包埋普瑞巴林(PG)的脂质体,通过冷冻离心将水合溶液中剩余的PG与囊泡分离。实现了普瑞巴林(PG)纳米基载体的优化。设计质量策略已成功用于获得具有所需特性的PG负载的脂质体。 Minitab ®程序使用实验设计(DOE)获得了最佳粒径,药物释放和包封效率,该实验设计通过同时研究不同因素的综合作用来预测最佳参数。在筛选步骤中使用帕累托图排除不重要的变量,而在优化步骤中使用响应面方法(RSM)研究重要因素。选择了最佳配方,可使用HPMC和Carbopol 934制备负载有碘代PG的局部水凝胶。通过机械和流变学测试证实,向凝胶基质中添加囊泡会显着影响凝胶网络。进行了体外释放和离体渗透实验。 PG分子的传递遵循Higuchi(非Fickian)扩散。作为常规口服途径的受控透皮替代品,当前的工作对于制药工业将是有意义的。

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