首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Promoting endothelial cell affinity and antithrombogenicity of polytetrafluoroethylene (PTFE) by mussel-inspired modification and RGD/heparin grafting
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Promoting endothelial cell affinity and antithrombogenicity of polytetrafluoroethylene (PTFE) by mussel-inspired modification and RGD/heparin grafting

机译:促进聚四氟乙烯(PTFE)的内皮细胞亲和力和抗静电性,贻贝风格的改性和RGD /肝素接枝

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When used as small-diameter vascular grafts (SDVGs), synthetic biomedical materials like polytetrafluoroethylene (PTFE) may induce thrombosis and intimal hyperplasia due to the lack of an endothelial cell layer. Modification of the PTFE in an aqueous solution is difficult because of its hydrophobicity. Herein, aiming to simultaneously promote endothelial cell affinity and antithrombogenicity, a mussel-inspired modification approach was employed to enable the grafting of various bioactive molecules like RGD and heparin. This approach involves a series of pragmatic steps including oxygen plasma treatment, dopamine (DA) coating, polyethylenimine (PEI) grafting, and RGD or RGD/heparin immobilization. Successful modification in each step was verified via Fourier transform infrared (FTIR) spectroscopy and X-ray photoelectron spectroscopy (XPS). Plasma treatment increased the hydrophilicity of PTFE, thereby allowing it to be efficiently coated with dopamine. Grafting of dopamine, RGD, and heparin led to an increase in surface roughness and a decrease in water contact angle due to increased surface energy. Platelet adhesion increased after dopamine and RGD modification, but it dramatically decreased when heparin was introduced. All of these modifications, especially the incorporation of RGD, showed favorable effects on endothelial cell attachment, viability, and proliferation. Due to strong cell-substrate interactions between endothelial cells and RGD, the RGD/heparin-grafted PTFE demonstrated high endothelial cell affinity. This facile modification method is highly suitable for all hydrophobic surfaces and provides a promising technique for SDVG modification to stimulate fast endothelialization and effective antithrombosis.
机译:当用作小直径血管移植物(SDVGS)时,由于缺乏内皮细胞层,诸如聚四氟乙烯(PTFE)等合成生物医学材料可能会诱导血栓形成和内膜增生。由于其疏水性,难以改变水溶液中的PTFE。这里,旨在同时促进内皮细胞亲和力和抗诱导性,采用贻贝启动的修饰方法来使得能够接枝像RGD和肝素等各种生物活性分子。该方法涉及一系列务实步骤,包括氧等离子体处理,多巴胺(DA)涂层,聚乙烯菊氨酸(PEI)接枝和RGD或RGD /肝素固定化。通过傅立叶变换红外(FTIR)光谱和X射线光电子能谱(XPS)验证了每个步骤中的成功修改。等离子体处理增加了PTFE的亲水性,从而允许其有效地涂有多巴胺。由于表面能增加,多巴胺,RGD和肝素的接枝导致表面粗糙度的增加和水接触角的降低。血小板粘附在多巴胺和RGD改性后增加,但在引入肝素时显着降低。所有这些修改,特别是RGD的掺入,对内皮细胞附着,活力和增殖表现出有利影响。由于内皮细胞和RGD之间的细胞底物相互作用,RGD /肝素接枝的PTFE展示了高内皮细胞亲和力。这种容易改性方法非常适合所有疏水表面,并为SDVG改性提供了一种有希望的技术,以刺激快速内皮化和有效的抗血栓形成。

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