首页> 外文期刊>Artificial cells, nanomedicine, and biotechnology. >Triamcinolone acetonide–Eudragitsup?/sup RS100 nanofibers and nanobeads: Morphological and physicochemical characterization
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Triamcinolone acetonide–Eudragitsup?/sup RS100 nanofibers and nanobeads: Morphological and physicochemical characterization

机译:醋酸曲安奈德-Eudragit ? RS100纳米纤维和纳米珠:形态和理化特性

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Abstract Context and objective: The aim of the present research was to fabricate triamcinolone acetonide (TA)-Eudragit? RS100 nanostructures using the electrospraying method. Materials and methods: The physicochemical properties of the electrosprayed formulations as well as drug release patterns were assessed. The particle size and morphology were evaluated using scanning electron microscopy. X-ray crystallography and differential scanning calorimetry were also conducted to investigate the crystallinity and polymorphic alterations of the drug in the formulations. Probable chemical interactions between the drug and the carrier during the preparation process were analyzed using FT-IR spectroscopy. The drug release kinetic was also considered to predict the release mechanism. Results and discussion: Increasing the concentration of injected polymer solution resulted in the formation of more fibers and fewer beads, with the particle diameter ranging from 60 nm to a few micrometers based on the drug: polymer ratio. The drug crystallinity was notably decreased during the electrospraying process; however, no interaction between drug and polymer was detected. The electrosprayed formulations with 1:10 drug: polymer ratio showed an almost similar drug release rate compared to the pure drug, while those with 1:5 ratio revealed slower release profiles. The release data were best fitted to the Weibull model, so that the corresponding shape factor values of the Weibull model were less than 0.75, indicating the diffusion controlled release mechanism. Conclusion: Our findings revealed that TA loaded Eudragit? RS100 nanofibers and nanobeads were properly prepared by the electrospraying method, which is a simple, surfactant-free and cost effective technique for producing drug: polymer nanostructures.
机译:摘要背景与目的:本研究的目的是制备曲安奈德(TA)-Eudragit?使用电喷涂方法的RS100纳米结构。材料和方法:评估了电喷雾制剂的理化性质以及药物释放模式。使用扫描电子显微镜评估粒度和形态。还进行了X射线晶体学和差示扫描量热法以研究制剂中药物的结晶度和多晶型变化。使用傅立叶变换红外光谱分析了药物和载体在制备过程中可能发生的化学相互作用。还考虑了药物释放动力学来预测释放机理。结果与讨论:增加注入的聚合物溶液的浓度导致形成更多的纤维和更少的珠子,基于药物:聚合物的比例,粒径范围为60 nm至几微米。在电喷雾过程中,药物的结晶度明显降低;但是,没有检测到药物和聚合物之间的相互作用。与纯药物相比,具有1:10药物:聚合物比率的电喷雾制剂显示出几乎相似的药物释放速率,而具有1:5比率的那些则显示出较慢的释放曲线。释放数据最适合于威布尔模型,因此威布尔模型的相应形状因子值小于0.75,表明了扩散控制释放机制。结论:我们的发现表明TA负载Eudragit吗? RS100纳米纤维和纳米珠通过电喷雾方法正确制备,这是一种简单,无表面活性剂且经济高效的生产药物:聚合物纳米结构的技术。

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