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用于模拟血管流动的亲水化海藻酸盐水凝胶的开发及其在生物相关药物洗脱支架测试中的应用。

Development of hydrophobized alginate hydrogels for the vessel-simulating flow-through cell and their usage for biorelevant drug-eluting stent testing.

机构信息

Institute of Pharmacy, Center of Drug Absorption and Transport, University of Greifswald, Felix-Hausdorff-Straße 3, 17487, Greifswald, Germany.

出版信息

AAPS PharmSciTech. 2013 Sep;14(3):1209-18. doi: 10.1208/s12249-013-0011-9. Epub 2013 Aug 6.

DOI:10.1208/s12249-013-0011-9
PMID:23918507
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3755162/
Abstract

The vessel-simulating flow-through cell (vFTC) has been used to examine release and distribution from drug-eluting stents in an in vitro model adapted to the stent placement in vivo. The aim of this study was to examine the effect of the admixture of different hydrophobic additives to the vessel wall simulating hydrogel compartment on release and distribution from model substance-coated stents. Four alginate-based gel formulations containing reversed-phase column microparticles LiChroprep® RP-18 or medium-chain triglycerides in form of preprocessed oil-in-water emulsions Lipofundin® MCT in different concentrations were successfully developed. Alginate and modified gels were characterized regarding the distribution coefficient for the fluorescent model substances, fluorescein and triamterene, and release as well as distribution of model substances from coated stents were investigated in the vFTC. Distribution coefficients for the hydrophobic model substance triamterene and the hydrophobized gel formulations were up to four times higher than for the reference gel. However, comparison of the obtained release profiles yielded no major differences in dissolution and distribution behavior for both fluorescent model substances (fluorescein, triamterene). Comparison of the test results with mathematically modeled data acquired using finite element methods demonstrated a good agreement between modeled data and experimental results indicating that gel hydrophobicity will only influence release in cases of fast releasing stent coatings.

摘要

血管模拟流通池(vFTC)已被用于研究药物洗脱支架在体外模型中的释放和分布,该模型适用于模拟体内支架放置。本研究的目的是研究将不同疏水性添加剂混合到血管壁模拟水凝胶隔室中对模型物质涂层支架的释放和分布的影响。成功开发了四种基于海藻酸盐的凝胶配方,其中含有反相柱微颗粒 LiChroprep®RP-18 或作为预加工油包水乳剂形式的中链甘油三酯 Lipofundin®MCT,浓度不同。对荧光模型物质荧光素和三氨喋呤的分布系数以及涂层支架的模型物质释放和分布进行了研究。疏水性模型物质三氨喋呤和疏水性凝胶配方的分配系数比参考凝胶高四倍。然而,对获得的释放曲线的比较表明,两种荧光模型物质(荧光素、三氨喋呤)的溶解和分布行为没有明显差异。将测试结果与使用有限元方法获得的数学模型数据进行比较表明,模型数据与实验结果之间具有良好的一致性,这表明在快速释放支架涂层的情况下,凝胶疏水性只会影响释放。

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