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Multiunit Floating Drug Delivery System of Rosiglitazone Maleate: Development, Characterization, Statistical Optimization of Drug Release and In Vivo Evaluation

机译:马来酸罗格列酮多单元浮动药物递送系统:药物释放的开发,表征,统计优化和体内评估

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摘要

A multiunit floating drug delivery system of rosiglitazone maleate has been developed by encapsulating the drug into Eudragit® RS100 through nonaqueous emulsification/solvent evaporation method. The in vitro performances of microspheres were evaluated by yield (%), particle size analysis, drug entrapment efficiency, in vitro floating behavior, surface topography, drug–polymer compatibility, crystallinity of the drug in the microspheres, and drug release studies. In vitro release was optimized by a {3, 3} simplex lattice mixture design to achieve predetermined target release. The in vivo performance of the optimized formulation was evaluated in streptozotocin-induced diabetic rats. The results showed that floating microspheres could be successfully prepared with good yields (69–75%), high entrapment (78-97%), narrow size distribution, and desired target release with the help of statistical design of experiments from very small number of formulations. In vivo evaluation in albino rats suggested that floating microspheres of rosiglitazone could be a promising approach for better glycemic control.
机译:通过非水乳化/溶剂蒸发法将药物封装到RS100中,已经开发了马来酸罗格列酮的多单元浮动药物递送系统。通过收率(%),粒度分析,药物截留效率,体外漂浮行为,表面形貌,药物-聚合物相容性,药物在微球中的结晶度和药物释放研究来评估微球的体外性能。通过{3,3}单纯形晶格混合物设计优化了体外释放,以实现预定的目标释放。在链脲佐菌素诱导的糖尿病大鼠中评估了优化制剂的体内性能。结果表明,可以通过非常少量的实验统计设计,成功地制备出具有良好收率(69-75%),高截留率(78-97%),窄尺寸分布和所需目标释放的漂浮微球。配方。在白化病大鼠中的体内评估表明,罗格列酮的漂浮微球可能是更好控制血糖的一种有前途的方法。

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