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Surface Modification with Dopamine and Heparin/Poly-L-Lyslne Nanoparticles Provides a Favorable Release Behavior for the Healing of Vascular Stent Lesions

机译:多巴胺和肝素/聚-L-赖氨酸纳米粒子的表面改性为血管支架病变的愈合提供了有利的释放行为

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Surface biofunctional modification of coronary artery stents to prevent thrombosis and restenosis formation, as well as accelerate endothelialization, has become a new hot spot. However, bioactive coatings on implants are not yet sufficiently developed for long-term activity, as they quickly lose efficiency in vivo and finally fail. On the basis of a novel time-ordered concept of biofunctionality for vascular stents, heparin/poly L-3ysine nanoparticle (NP) was developed and immobilized on a polydopamine-coated titanium surface, with the aim of regulating and maintaining the intravascular biological response within the normal range after biomaterial implantation. An in vitro dynamic release model was established to mimic the blood flow condition in vivo with three phases: (l) An early phase (l—7 days) with release of predominantly anticoagulant and anti-inflammatory substances and to a minor degree antiproliferative effects against smooth muscle cells (SMCs); (2) this is followed by a phase (7—14 days) of supported endothelial cell (ECs) proliferation and suppressed SMC proliferation with persisting high antithrombogenicity and anti-inflammatory properties of the surface. (3) Finally, a stable stage (14—28 days) with adequate biomolecules on the surface that maintain hemocompatibility and anti inflammation as well as inhibit SMCs proliferation and promote ECs growth. In vivo animal tests further confirmed that the NP-modified surface provides a favorable release behavior to apply a stage-adjusted remedy. We suggested that these observations provide important guidance and potential means for reasonable and suitable platform construction on a stent surface.
机译:冠状动脉支架的表面生物功能修饰,以防止血栓形成和再狭窄的形成以及加速内皮化,已成为一个新的热点。但是,植入物上的生物活性涂层尚不能充分开发用于长期活动,因为它们会很快失去体内功效,最终失效。基于新颖的血管支架生物功能的有序概念,开发了肝素/聚L-3赖氨酸纳米颗粒(NP)并将其固定在聚多巴胺涂层的钛表面上,目的是调节和维持血管内生物反应生物材料植入后的正常范围。建立了一个体外动态释放模型来模拟体内血液流动状况,分为三个阶段:(l)早期阶段(1-7天),主要释放出抗凝和抗炎物质,并在较小程度上抑制针对平滑肌细胞(SMC); (2)随后是阶段性(7-14天)受支持的内皮细胞(EC)增殖并抑制SMC增殖,同时保持表面的高抗血栓形成性和抗炎性。 (3)最后,一个稳定的阶段(14-28天),其表面上有足够的生物分子,可以维持血液相容性和抗炎症作用,并抑制SMC增殖并促进ECs生长。体内动物试验进一步证实,NP修饰的表面可提供有利的释放行为,以应用经过阶段调整的药物。我们建议这些观察结果为在支架表面上合理和合适的平台构造提供重要的指导和潜在的手段。

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