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Design, preparation and performance of a novel drug-eluting stent with multiple layer coatings

机译:具有多层涂层的新型药物洗脱支架的设计,制备和性能

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摘要

Drug-eluting stents (DESs) can effectively control the harmful effects of coronary artery disease, because of their excellent ability to reduce in-stent restenosis. However, delayed re-endothelialization and late stent thrombosis have caused concern over the safety of DESs. In this study, according to time-ordered pathological responses after stent implantation, a hierarchical multiple drug-eluting stent was designed and prepared to overcome the existing DES limitations. A platelet membrane glycoprotein IIIa monoclonal antibody (SZ-21) and a vascular endothelial growth factor (VEGF(121)) were loaded into the inner coating of 316L stainless steel (316L SS) stents to inhibit thrombosis and promote re-endothelialization; rapamycin (RAPA) was loaded into the third layer to inhibit intima hyperplasia; a drug-free poly-L-lactic acid coating was located on the second and fourth layers and used as sustained release layers. The results showed that the three drugs exhibited sequential release kinetics without significant burst release. RAPA released quickly at the early stage, while SZ-21 and VEGF121 achieved a slow and prolonged release. In vitro experiments showed that the stents had excellent hemocompatibility and anti-inflammatory properties, and promoted the proliferation and migration of endothelial cells while inhibiting the proliferation and migration of smooth muscle cells. Finally the stents were implanted in the carotid arteries of New Zealand white rabbits. In vivo results showed that compared to 316L SS stents, the multiple drug-eluting stents could accelerate re-endothelialization and inhibit thrombosis, inflammation and in-stent restenosis after 4 weeks (12.79 +/- 2.45% vs. 25.27 +/- 4.81%) and 12 weeks (15.87 +/- 3.62% vs. 58.84 +/- 6.87%). These results indicate that the novel drug-eluting stent with multiple layer coatings will have a highly potential clinical application.
机译:药物洗脱支架(DESS)可以有效地控制冠状动脉疾病的有害影响,因为它们具有降低支架内恢复的绝佳能力。然而,延迟重新内皮化和晚期支架血栓形成对DES的安全引起了关注。在这项研究中,根据支架植入后的时间有序的病理反应,设计了一种分层多种药物洗脱支架并准备克服现有的DES限制。血小板膜糖蛋白IIIa单克隆抗体(SZ-21)和血管内皮生长因子(VEGF(121))加载到316L不锈钢(316LS)支架的内涂层中,以抑制血栓形成并促进重新内皮化;将雷帕霉素(RAPA)加载到第三层中以抑制内含内膜增生;无毒的多L-乳酸涂层位于第二和第四层上并用作持续剥离层。结果表明,三种药物表现出连续释放动力学,而无明显爆发。 RAPA在早期发布在早期阶段,而SZ-21和VEGF121则达到缓慢而延长的释放。体外实验表明,支架具有优异的血液相色性和抗炎性能,并促进内皮细胞的增殖和迁移,同时抑制平滑肌细胞的增殖和迁移。最后,在新西兰白兔的颈动脉中植入了支架。在体内结果表明,与316L SS支架相比,多种药物洗脱支架可以加速重新内皮化并抑制4周后血栓形成,炎症和支架内再狭窄(12.79 +/- 2.45%与25.27 +/- 4.81% )和12周(15.87 +/- 3.62%与58.84 +/- 6.87%)。这些结果表明,具有多层涂层的新型药物洗脱支架将具有高潜在的临床应用。

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  • 来源
    《Biomaterials Science》 |2017年第9期|共13页
  • 作者单位

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

    Gen Hosp PLA Rocket Force Beijing 100085 Peoples R China;

    Chongqing Univ Key Lab Biorheol Sci &

    Technol State &

    Local Joint Engn Lab Vasc Implants Chongq Bioengn Coll Minist Educ Chongqing 400044 Peoples R China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
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