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Novel bioresorbable stent coating for drug release in congenital heart disease applications

机译:新型生物可吸收支架涂料,用于先天性心脏病应用中的药物释放

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A novel double opposed helical poly-l-lactic acid (PLLA) bioresorbable stent has been designed for use in pediatrics. The aim was to test the PLLA stent biocompatibility. The PLLA stent was immersed into whole pig's blood in a closed loop circuit then fibrin and platelet association was assessed via enzyme-linked immunosorbent assay. D-Dimer was valued at 0.2 +/- 0.002 ng/mL and P-selectin 0.43 +/- 00.01 ng/mL indicating limited association of fibrin and platelets on the stent. To improve biocompatibility by targeting inflammatory cells, dexamethasone was incorporated on PLLA fibers with two coating methods. Both coatings were poly(l-lactide-co-glycolide) acid (PLGA) but one was made porous with sucrose while the other remained nonporous. There was no change in mechanical properties of the fiber with either coating of PLGA polymer. The total amount of dexamethasone released was then determined for each coating. The cumulative drug release for the porous fiber was significantly higher (approximate to 100%) over 8 weeks than the nonporous fiber (40%). Surface examination of the fiber with scanning electron microscopy showed more surface microfracturing in coatings that contain pores. The biocompatibility of this novel stent was demonstrated. Mechanical properties of the fiber were not altered by coating with PLGA polymer. Anti-inflammatory drug release was optimized using a porous PLGA polymer. (c) 2014 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 103A: 1761-1770, 2015.
机译:已经设计出一种新颖的双对置螺旋形聚-1-乳酸(PLLA)生物可吸收支架,用于儿科。目的是测试PLLA支架的生物相容性。将PLLA支架浸入闭环回路中的全猪血液中,然后通过酶联免疫吸附试验评估血纤蛋白和血小板的缔合。 D-二聚体的值为0.2 +/- 0.002 ng / mL,P-选择素的值为0.43 +/- 00.01 ng / mL,表明血纤维蛋白和血小板在支架上的结合有限。为了通过靶向炎性细胞提高生物相容性,地塞米松通过两种涂覆方法掺入PLLA纤维上。两种涂层均为聚(1-丙交酯-乙交酯)酸(PLGA),但其中一层用蔗糖制成多孔性,而另一层保持无孔。两种PLGA聚合物涂层的纤维的机械性能均没有变化。然后确定每种涂层释放的地塞米松的总量。在8周内,多孔纤维的累积药物释放明显高于无孔纤维(40%)(约100%)。用扫描电子显微镜对纤维进行表面检查发现,在含有孔的涂层中,表面发生了更多的微裂。证明了这种新型支架的生物相容性。纤维的机械性能不会因涂PLGA聚合物而改变。使用多孔PLGA聚合物优化了抗炎药物的释放。 (c)2014 Wiley Periodicals,Inc.J Biomed Mater Res Part A:103A:1761-1770,2015。

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