首页> 外文期刊>Journal of Materials Science. Materials in Medicine >In vitro study of drug-eluting stent coatings based on poly(L-lactide) incorporating cyclosporine A - drug release, polymer degradation and mechanical integrity
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In vitro study of drug-eluting stent coatings based on poly(L-lactide) incorporating cyclosporine A - drug release, polymer degradation and mechanical integrity

机译:含环孢菌素A的聚(L-丙交酯)药物洗脱支架涂层的体外研究-药物释放,聚合物降解和机械完整性

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摘要

In this study, absorbable polymer stent coatings for localized drug delivery based on poly(L-lactide) (PLLA) and cyclosporine A (CsA) were developed and tested in vitro. Metallic stents were coated with different compositions of PLLA/CsA (70/ 30, 60/40, 50/50% w/w) and β-sterilized. The specimens were used to assess the drug release kinetics with HPLC. Sterilization influenced polymer degradation was measured with GPC. Mechanical integrity of the stent coatings was studied with SEM. The interconnection of the coated stents with a balloon-catheter was characterized by the measurement of stent dislodgment force. A migration assay was used to determine the inhibitory effect of the model drug CsA on smooth muscle cell (SMC) migration. The release of CsA was established over time periods up to 24 days in sodium chloride solution and in porcine blood plasma. An inhibition of SMC migration (max. 26-33%) was found for CsA concentrations of 4 × 10~(-5) to 4 × 10~(-7) mol/l. Marked molecular weight reduction (70-80%) of the PLLA matrix occurred after β-sterilization. We also observed a substantial decrease of in vitro degradation time. The maintenance of the mechanical integrity of the polymer coating during crimping and dilation of the specimens could be verified, and a sufficient stent dislodgment force of 0.8-0.9 N was measured.
机译:在这项研究中,基于聚(L-丙交酯)(PLLA)和环孢菌素A(CsA)的用于局部药物递送的可吸收聚合物支架涂料已开发并在体外进行了测试。金属支架涂有不同成分的PLLA / CsA(70 / 30、60 / 40、50 / 50%w / w)并经过β灭菌。标本用于通过HPLC评估药物释放动力学。用GPC测量了灭菌对聚合物降解的影响。用SEM研究了支架涂层的机械完整性。涂层支架与球囊导管的相互连接通过测量支架位移力来表征。使用迁移测定法确定模型药物CsA对平滑肌细胞(SMC)迁移的抑制作用。在长达24天的时间内,在氯化钠溶液和猪血浆中建立了CsA的释放。发现CsA浓度为4×10〜(-5)到4×10〜(-7)mol / l时,SMC迁移受到抑制(最大26-33%)。 β-灭菌后,PLLA基质的分子量明显降低(70-80%)。我们还观察到了体外降解时间的大幅减少。可以验证在压接和试样膨胀期间保持聚合物涂层的机械完整性,并测得了足够的0.8-0.9 N的支架移位力。

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