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首页> 外文期刊>Journal of biomedical materials research, Part A >Direct surface modification of metallic biomaterials via tyrosine oxidation aiming to accelerate the re‐endothelialization of vascular stents
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Direct surface modification of metallic biomaterials via tyrosine oxidation aiming to accelerate the re‐endothelialization of vascular stents

机译:通过酪氨酸氧化的直接表面改性旨在加速血管支架的重新内皮化

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Abstract Rapid in‐situ re‐endothelialization of coronary stents is one of the most effective approaches to inhibit late thrombosis and restenosis. Strut surfaces allowing excellent adhesion and migration of endothelial cells and endothelial progenitor cells may accelerate in‐situ re‐endothelialization. Here, a well‐known endothelial cell adhesive peptide, Arg‐Glu‐Asp‐Val (REDV), was directly immobilized onto metallic surfaces by means of single‐step tyrosine oxidation with copper chloride (II) and hydrogen peroxide, which we recently reported as a new biomaterial modification technique. REDV immobilization on a 316L stainless steel plate improved endothelial cell adhesion and effectively suppressed platelet adhesion in vitro . In addition, a Co‐Cr stent immobilized with Ac‐Tyr‐Gly‐Gly‐Gly‐Arg‐Glu‐Asp‐Val (Y‐REDV) was implanted into a rabbit abdominal aorta. On 7 days postimplantation, 80% of the strut surface of the Y‐REDV‐immobilized stent was covered by a thin neointimal layer and was similar in appearance to native endothelium. Restenosis and late thrombosis were not observed in the Y‐REDV‐immobilized stent for 42 days. These findings suggest that direct immobilization of Y‐REDV peptide onto metallic biomaterials by tyrosine oxidation is effective for promoting in‐situ re‐endothelialization in vascular stents. ? 2017 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 106A: 491–499, 2018.
机译:摘要冠状动脉支架的快速原位重新内皮化是抑制晚期血栓形成和再狭窄的最有效的方法之一。允许内皮细胞和内皮祖细胞的优异粘附和迁移的支柱表面可以加速原位再肝化。这里,通过用氯化铜(II)和过氧化氢,通过单步酪氨酸氧化直接将甲状腺细胞粘合剂肽(REDV)直接固定在金属表面上。作为一种新的生物材料改性技术。 316L不锈钢板上的REDV固定化改善内皮细胞粘附,有效地抑制了体外血小板粘附。此外,将用AC-Tyr-Gly-Gly-Arg-Glu-Asp-Val(Y-REDV)固定的CO-CR支架植入兔腹主动脉中。在7天后,由薄的新内膜层覆盖Y-Redv-固定支架的80%的支柱表面,并且在外观上与天然内皮相似。在Y-Redv-固定支架中未观察到再狭窄和晚期血栓形成42天。这些发现表明,通过酪氨酸氧化将Y-REDV肽直接固定到金属生物材料上,可有效地促进血管支架中的原位重新内皮化。还2017年Wiley期刊,Inc。J生物保罗第A部分:106A:491-499,2018。

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