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Surface Nanostructuring of Parylene-C Coatings for Blood Contacting Implants

机译:用于血液接触植入物的Parylene-C涂层的表面纳米结构

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摘要

This paper investigates the effects on the blood compatibility of surface nanostructuring of Parylene-C coating. The proposed technique, based on the consecutive use of O2 and SF6 plasma, alters the surface roughness and enhances the intrinsic hydrophobicity of Parylene-C. The degree of hydrophobicity of the prepared surface can be precisely controlled by opportunely adjusting the plasma exposure times. Static contact angle measurements, performed on treated Parylene-C, showed a maximum contact angle of 158°. The nanostructured Parylene-C retained its hydrophobicity up to 45 days, when stored in a dry environment. Storing the samples in a body-mimicking solution caused the contact angle to progressively decrease. However, at the end of the measurement, the plasma treated surfaces still exhibited a higher hydrophobicity than the untreated counterparts. The proposed treatment improved the performance of the polymer as a water diffusion barrier in a body simulating environment. Modifying the nanotopography of the polymer influences the adsorption of different blood plasma proteins. The adsorption of albumin—a platelet adhesion inhibitor—and of fibrinogen—a platelet adhesion promoter—was studied by fluorescence microscopy. The adsorption capacity increased monotonically with increasing hydrophobicity for both studied proteins. The effect on albumin adsorption was considerably higher than on fibrinogen. Study of the proteins simultaneous adsorption showed that the albumin to fibrinogen adsorbed ratio increases with substrate hydrophobicity, suggesting lower thrombogenicity of the nanostructured surfaces. Animal experiments proved that the treated surfaces did not trigger any blood clot or thrombus formation when directly exposed to the arterial blood flow. The findings above, together with the exceptional mechanical and insulation properties of Parylene-C, support its use for packaging implants chronically exposed to the blood flow.
机译:本文研究了Parylene-C涂层表面纳米结构对血液相容性的影响。基于连续使用O2和SF6等离子体,提出的技术改变了表面粗糙度并增强了Parylene-C的固有疏水性。制备的表面的疏水度可以通过适当地调节等离子体暴露时间来精确地控制。在经过处理的Parylene-C上进行的静态接触角测量显示最大接触角为158°。当存放在干燥环境中时,纳米结构的Parylene-C可以保留长达45天的疏水性。将样品存储在模拟人体的溶液中导致接触角逐渐减小。然而,在测量结束时,经等离子体处理的表面仍显示出比未处理的对应表面更高的疏水性。所提出的处理改善了聚合物在人体模拟环境中作为水扩散阻挡层的性能。修改聚合物的纳米形貌会影响不同血浆蛋白的吸附。通过荧光显微镜研究了白蛋白(一种血小板粘附抑制剂)和纤维蛋白原(一种血小板粘附促进剂)的吸附。两种研究蛋白的吸附能力均随着疏水性的增加而单调增加。对白蛋白吸附的影响明显高于对纤维蛋白原的吸附。对蛋白质同时吸附的研究表明,白蛋白与纤维蛋白原的吸附比率随底物疏水性的增加而增加,表明纳米结构表面的血栓形成性较低。动物实验证明,直接暴露于动脉血流时,处理过的表面不会引发任何血块或血栓形成。以上发现以及Parylene-C的出色机械和绝缘性能,支持其用于包装长期暴露于血流的植入物。

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