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Spontaneous Emulsification of Nifedipine-Loaded Self-Nanoemulsifying Drug Delivery System

机译:硝苯地平载自纳米乳化递药系统的自发乳化

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摘要

Self-nanoemulsifying drug delivery system (SNEDDS) can be used to improve dissolution of poorly water-soluble drugs. The objective of this study was to prepare SNEDDS by using ternary phase diagram and investigate their spontaneous emulsifying property, dissolution of nifedipine (NDP), as well as the pharmacokinetic profile of selected SNEDDS formulation. The results showed that the composition of the SNEDDS was a great importance for the spontaneous emulsification. Based on ternary phase diagram, the region giving the SNEDDS with emulsion droplet size of less than 300 nm after diluting in aqueous medium was selected for further formulation. The small-angle X-ray scattering curves showed no sharp peak after dilution at different percentages of water, suggesting non-ordered structure. The system was found to be robust in different dilution volumes; the droplet size was in nanometer range. In vitro dissolution study showed remarkable increase in dissolution of NDP from SNEDDS formulations compared with NDP powders. The pharmacokinetic study of selected SNEDDS formulation in male Wistar rats revealed the improved maximum concentration and area under the curve. Our results proposed that the developed SNEDDS formations could be promising to improve the dissolution and oral bioavailability of NDP.
机译:自纳米乳化药物递送系统(SNEDDS)可用于改善水溶性差的药物的溶出度。这项研究的目的是通过使用三元相图制备SNEDDS,并研究其自发乳化特性,硝苯地平(NDP)的溶出度以及所选SNEDDS制剂的药代动力学特征。结果表明,SNEDDS的组成对于自发乳化非常重要。根据三元相图,选择在水性介质中稀释后乳化液滴尺寸小于300 nm的SNEDDS区域,以进一步配制。小角度X射线散射曲线显示在不同百分比的水稀释后没有尖锐的峰,表明无序结构。发现该系统在不同的稀释体积下都非常稳定。液滴尺寸在纳米范围内。体外溶出度研究表明,与NDP粉末相比,SNEDDS配方中NDP的溶出度显着增加。选定的SNEDDS制剂在雄性Wistar大鼠中的药代动力学研究表明,曲线下的最大浓度和面积有所改善。我们的研究结果表明,发达的SNEDDS地层有望改善NDP的溶出度和口服生物利用度。

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