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首页> 外文期刊>Colloids and Surfaces, B. Biointerfaces >Drug delivery system based on cyclodextrin-naproxen inclusion complex incorporated in electrospun polycaprolactone nanofibers
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Drug delivery system based on cyclodextrin-naproxen inclusion complex incorporated in electrospun polycaprolactone nanofibers

机译:静电纺丝聚己内酯纳米纤维中基于环糊精-萘普生包合物的药物递送系统

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摘要

In this study, we select naproxen (NAP) as a reference drug and electrospun poly (ε-caprolactone) (PCL) nanofibers as a fibrous matrix for our drug-delivery system. NAP was complexed with betacyclodextrin (βCD) to form inclusion complex (NAP-βCD-IC) and then NAP-βCD-IC was incorporated into PCL nanofibers via electrospinning. The incorporation of NAP without CD-IC into electrospun PCL was also carried out for a comparative study. Our aim is to analyze the release profiles of NAP from PCL/NAP and PCL/NAP-βCD-IC nanofibers and we investigate the effect of CD-IC on the release behavior of NAP from the nanofibrous PCL matrix. The characterization of NAP-βCD-IC and the presence of CD-IC in PCL/NAP-βCD-IC nanofibers were studied by FTIR, XRD, TGA, NMR and SEM. The SEM imaging of the electrospun PCL/NAP and PCL/NAP-βCD-IC nanofibers reveal that the average fiber diameter of these nanofibers is around 300 nm, in addition, the aggregates of CD-IC in PCL/NAP-βCD-IC nanofibers is observed. The release study of NAP in buffer solution elucidate that the PCL/NAP-βCD-IC nanofibers have higher release amount of NAP than the PCL/NAP nanofibers due to the solubility enhancement of NAP by CD-IC.
机译:在这项研究中,我们选择萘普生(NAP)作为参考药物,并将电纺聚(ε-己内酯)(PCL)纳米纤维作为我们的药物输送系统的纤维基质。将NAP与β-环糊精(βCD)络合形成包合物(NAP-βCD-IC),然后通过电纺丝将NAP-βCD-IC掺入PCL纳米纤维中。还进行了不带CD-IC的NAP到静电纺PCL中的比较研究。我们的目的是分析NAP从PCL / NAP和PCL /NAP-βCD-IC纳米纤维中释放的特性,并研究CD-IC对NAP从纳米纤维PCL基质中释放行为的影响。通过FTIR,XRD,TGA,NMR和SEM研究了NAP-βCD-IC的表征和PCL /NAP-βCD-IC纳米纤维中CD-IC的存在。静电纺丝PCL / NAP和PCL /NAP-βCD-IC纳米纤维的SEM图像显示,这些纳米纤维的平均纤维直径约为300 nm,此外,PCL /NAP-βCD-IC纳米纤维中的CD-IC聚集体被观察到。 NAP在缓冲溶液中的释放研究表明,由于CD-IC增强了NAP的溶解度,PCL /NAP-βCD-IC纳米纤维的NAP释放量高于PCL / NAP纳米纤维。

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