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一种用于抗青光眼药物持续释放的聚(ε-己内酯)装置。

A poly(ε-caprolactone) device for sustained release of an anti-glaucoma drug.

机构信息

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

出版信息

Biomed Mater. 2011 Apr;6(2):025003. doi: 10.1088/1748-6041/6/2/025003. Epub 2011 Feb 4.

DOI:10.1088/1748-6041/6/2/025003
PMID:21293056
Abstract

Implantable dorzolamide-loaded discs were prepared by blending poly(ε-caprolactone), PCL, with poly(ethylene oxide)-b-poly(propylene oxide)-b-poly(ethylene oxide), Lu. By blending, crystallinity, water uptake and mass loss were modified relative to the pure polymers. Burst was diminished by coating the discs with a PCL shell. All samples presented burst release except PCL-coated samples that showed controlled release during 18 days. For PCL-coated samples, barrier control of diffusion coupled with partition control from the core slowed down the release, while for 50/50 Lu/PCL-coated samples, the enhancement in the porosity of the core diminished partition control of drug release. Nonlinear regression analysis suggested that a degradation model fully describes the release curve considering a triphasic release mechanism: the instantaneous diffusion (burst), diffusion and polymer degradation stages. The MTT test indicated that the materials are not cytotoxic for corneal endothelial cells. A good in vitro-in vivo correlation was obtained, with similar amounts of drug released in vitro and in vivo. The discs decreased intraocular pressure (IOP) in normotensive rabbit eyes by 13.0% during 10 days for PCL-coated and by 13.0% during 4 days for 50/50 Lu/PCL-coated samples. The percentages of IOP decrease are similar to those obtained by dorzolamide eyedrop instillation (11.0%).

摘要

载有盐酸多佐胺的植入式圆盘通过聚(ε-己内酯)(PCL)与聚(氧化乙烯)-b-聚(氧化丙烯)-b-聚(氧化乙烯)(Lu)共混制备而成。通过共混,相对于纯聚合物,结晶度、吸水率和质量损失得到了改善。通过用 PCL 壳层涂覆圆盘,消除了突释。所有样品均表现出突释释放,除了 PCL 涂层样品在 18 天内显示出控制释放。对于 PCL 涂层样品,扩散的屏障控制与核心的分配控制相结合,减缓了药物释放。对于 50/50 Lu/PCL 涂层样品,核心的多孔性增强降低了药物释放的分配控制。非线性回归分析表明,降解模型充分描述了释放曲线,考虑了三相释放机制:瞬时扩散(突释)、扩散和聚合物降解阶段。MTT 试验表明,这些材料对角膜内皮细胞无细胞毒性。在体内和体外均获得了良好的相关性,在体外和体内释放了相似量的药物。在 10 天内,PCL 涂层的圆盘将正常眼压兔眼内压降低了 13.0%,而 50/50 Lu/PCL 涂层的圆盘在 4 天内将眼内压降低了 13.0%。眼压降低的百分比与多佐胺滴眼剂滴注(11.0%)获得的百分比相似。

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