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Formulation and Optimization of Eudragit RS PO-Tenofovir Nanocarriers Using Box-Behnken Experimental Design

机译:基于Box-Behnken实验设计的Eudragit RS PO-替诺福韦纳米载体的配制和优化

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The objective of present study was to develop an optimized polymeric nanoparticle system for the antiretroviral drug tenofovir. A modified nanoprecipitation method was used to prepare Eudragit RS PO nanoparticles of the drug. The effect of amount of polymer, surfactant concentration, and sonication time on particle size, particle distribution, encapsulation efficiency (EE), and zeta potential were assessed and optimized utilizing a three-factor, three-level Box-Behnken Design (BBD) of experiment. Fifteen formulations of nanoparticles were prepared as per BBD and evaluated for particle size, polydispersity index (PDI), EE, and zeta potential. The results showed that the measured mean particle sizes were in the range of 233 to 499 nm, PDI ranged from 0.094 to 0.153, average zeta potential ranged from −19.9 to −45.8 mV, and EE ranged between 98 and 99%. The optimized formulation was characterized forin vitrodrug release and structural characterization. The mean particle size of this formulation was 233 nm with a PDI of 0.0107. It had a high EE of 98% and average zeta potential of −35 mV, an indication of particle stability. The FTIR showed some noncovalent interactions between the drug and polymer but a sustained release was observedin vitrofor up to 80 hours.
机译:本研究的目的是为抗逆转录病毒药物替诺福韦开发一种优化的聚合物纳米颗粒系统。一种改进的纳米沉淀方法用于制备该药物的Eudragit RS PO纳米颗粒。使用三因素,三级Box-Behnken设计(BBD)对聚合物的量,表面活性剂浓度和超声处理时间对粒度,颗粒分布,包封效率(EE)和Zeta电位的影响进行了评估和优化。实验。根据BBD制备了15种纳米颗粒制剂,并对其粒径,多分散指数(PDI),EE和Zeta电位进行了评估。结果表明,测得的平均粒径在233至499nm之间,PDI在0.094至0.153之间,平均zeta电位在-19.9至-45.8VmV之间,EE在98%至99%之间。针对体外药物释放和结构表征对优化的制剂进行了表征。该配方的平均粒径为233 nm,PDI为0.0107。它具有98%的高EE和-35 mV的平均zeta电位,表明了颗粒的稳定性。 FTIR显示药物与聚合物之间存在一些非共价相互作用,但在体外观察到长达80小时的持续释放。

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