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载药微球的药物洗脱支架:PLGA 载药微球在水凝胶涂层中的整合用于亲水性抗再狭窄药物的局部和持续释放。

Microsphere-integrated drug-eluting stents: PLGA microsphere integration in hydrogel coating for local and prolonged delivery of hydrophilic antirestenosis agents.

机构信息

Department of Materials and Production Engineering, University Federico II, Piazzale Tecchio 80, Naples, Italy.

出版信息

J Biomed Mater Res A. 2011 May;97(2):201-11. doi: 10.1002/jbm.a.33039. Epub 2011 Mar 10.

DOI:10.1002/jbm.a.33039
PMID:21394898
Abstract

The development of a novel generation of drug-eluting stent (DES) relies upon the idea to obtain very flexible platforms able to overcome some issues associated to available devices and widen their field of application, especially to the currently emerging biotech therapeutics. Here, we propose a new concept of DES named microsphere-integrated drug-eluting stent (MIDES) composed of drug eluting biodegradable poly(D,L-lactide-co-glycolide) microspheres--encapsulating an hydrophilic model molecule (dextran)--fully integrated in a poly(2-hydroxy-ethyl-methacrylate) coating. By implementing a modified spray-coating technique, we have been able to achieve a thin (10 μm), smooth, and homogeneous hydrogel surface embedding underneath a population of two different microparticles formulations--Dex502H and Dex506. The amount of drug can be tailored, resulting in a dextran loading as high as 1.4 μg/cm, by simply reiteration of coating layer deposition making the MIDES a custom-made device where the release kinetics can be further modified by opportunely choosing microsphere properties. DES use is nowadays restricted to delivery of hydrophobic pharmaceuticals; release of hydrophilic therapeutics from MIDES can, however, be finely controlled by specifically engineering biodegradable microspheres. By varying polymer resomer, we obtained a tunable release rate in the first month of delivery. Depending on the microspheres properties release profile changes drastically moving from a biphasic release, in the case of Dex502H, with a burst of about 20% in the first day to a more sustained release for Dex506 particles. As proof of principle, we also demonstrated that MIDES approach can allows the delivery of two different agents opening up the way to a multitherapy in restenosis treatment.

摘要

新一代药物洗脱支架 (DES) 的开发依赖于获得非常灵活的平台的想法,该平台能够克服现有设备相关的一些问题,并拓宽其应用领域,尤其是新兴的生物技术治疗领域。在这里,我们提出了一种名为微球整合药物洗脱支架 (MIDES) 的新型 DES 概念,它由载药可生物降解的聚(D,L-丙交酯-共-乙交酯)微球组成 - 包封亲水性模型分子 (葡聚糖) - 完全整合在聚(2-羟乙基-甲基丙烯酸酯)涂层中。通过实施改良的喷雾涂层技术,我们能够实现 10μm 厚的、光滑且均匀的水凝胶表面,其下面嵌入了两种不同微球制剂的群体 - Dex502H 和 Dex506。通过简单地重复涂层沉积,可以调整药物的含量,使葡聚糖的载药量高达 1.4μg/cm,从而使 MIDES 成为一种定制设备,可以通过选择合适的微球特性进一步调整释放动力学。DES 的使用目前仅限于疏水性药物的输送;然而,通过专门设计可生物降解的微球,可以精细地控制亲水治疗剂从 MIDES 中的释放。通过改变聚合物的 Resomer,可以在第一个月的输送中获得可调节的释放速率。根据微球的特性,释放曲线会发生剧烈变化,从 Dex502H 的双相释放到 Dex506 颗粒的更持续释放。作为原理验证,我们还证明了 MIDES 方法可以允许输送两种不同的药物,为再狭窄治疗中的多疗法开辟了道路。

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