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药物溶解度、状态和载药量对双组分电纺纤维中控制释放的影响。

Effects of drug solubility, state and loading on controlled release in bicomponent electrospun fibers.

机构信息

Department of Chemical Engineering, University of Coimbra, Pólo II, Pinhal de Marrocos, 3030-290 Coimbra, Portugal.

出版信息

Int J Pharm. 2010 Sep 15;397(1-2):50-8. doi: 10.1016/j.ijpharm.2010.06.045. Epub 2010 Jul 3.

Abstract

Bicomponent fibers of two semi-crystalline (co)polymers, poly(varepsilon-caprolactone), and poly(oxyethylene-b-oxypropylene-b-oxyethylene), were obtained by electrospinning. Acetazolamide and timolol maleate were loaded in the fibers in different concentrations (below and above the drug solubility limit in polymer) in order to determine the effect of drug solubility in polymer, drug state, drug loading and fiber composition on fiber morphology, drug distribution and release kinetics. The high loadings fibers (with drug in crystalline form) showed higher burst and faster release than low drug content fibers, indicating the release was more sustained when the drug was encapsulated inside the fibers, in amorphous form. Moreover, timolol maleate was released faster than acetazolamide, indicating that drug solubility in polymer influences the partition of drug between polymer and elution medium, while fiber composition also controlled drug release. At low loadings, total release was not achieved (cumulative release percentages smaller than 100%), suggesting that drug remained trapped in the fibers. The modeling of release data implied a three stage release mechanism: a dissolution stage, a desorption and subsequent diffusion through water-filled pores, followed by polymer degradation control.

摘要

通过静电纺丝获得了两种半结晶(共)聚合物,聚(ε-己内酯)和聚(氧化乙烯-b-氧化丙烯-b-氧化乙烯)的双组份纤维。将乙酰唑胺和马来酸噻吗洛尔以不同浓度(低于和高于药物在聚合物中的溶解度极限)负载到纤维中,以确定药物在聚合物中的溶解度、药物状态、药物负载和纤维组成对纤维形态、药物分布和释放动力学的影响。高载药量纤维(药物呈结晶状态)的突释和释放速度比低药物含量纤维更快,表明药物以无定形形式包裹在纤维内时释放更持久。此外,马来酸噻吗洛尔的释放速度比乙酰唑胺快,表明药物在聚合物中的溶解度影响药物在聚合物和洗脱介质之间的分配,而纤维组成也控制药物释放。在低载药量下,未达到完全释放(累积释放百分比小于 100%),表明药物仍被困在纤维中。释放数据的建模表明存在三个阶段的释放机制:溶解阶段、随后通过充满水的孔的解吸和扩散,以及聚合物降解控制。

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