首页> 外文期刊>Langmuir: The ACS Journal of Surfaces and Colloids >Plasma proteins adsorption mechanism on polyethylene-grafted poly(ethylene glycol) surface by quartz crystal microbalance with dissipation
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Plasma proteins adsorption mechanism on polyethylene-grafted poly(ethylene glycol) surface by quartz crystal microbalance with dissipation

机译:耗散石英晶体微天平在聚乙烯接枝聚乙二醇表面吸附血浆蛋白的机理

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Protein adsorption has a vital role in biomaterial surface science because it is directly related to the hemocompatibility of blood-contacting materials. In this study, monomethoxy poly(ethylene glycol) (mPEG) with two different molecular weights was grafted on polyethylene as a model to elucidate the adsorption mechanisms of plasma protein through quartz crystal microbalance with dissipation (QCM-D). Combined with data from platelet adhesion, whole blood clotting time, and hemolysis rate, the blood compatibility of PE-g-mPEG film was found to have significantly improved. Two adsorption schemes were developed for real-time monitoring of protein adsorption. Results showed that the preadsorbed bovine serum albumin (BSA) on the surfaces of PE-g-mPEG films could effectively inhibit subsequent adsorption of fibrinogen (Fib). Nonspecific protein adsorption of BSA was determined by surface coverage, not by the chain length of PEG. Dense PEG brush could release more trapped water molecules to resist BSA adsorption. Moreover, the preadsorbed Fib could be gradually displaced by high-concentration BSA. However, the adsorption and displacement of Fib was determined by surface hydrophilicity.
机译:蛋白质吸附在生物材料表面科学中具有至关重要的作用,因为它与血液接触材料的血液相容性直接相关。在这项研究中,将具有两种不同分子量的单甲氧基聚(乙二醇)(mPEG)嫁接到聚乙烯上作为模型,通过具有耗散的石英晶体微天平(QCM-D)阐明血浆蛋白的吸附机理。结合血小板粘附,全血凝固时间和溶血速率的数据,发现PE-g-mPEG膜的血液相容性有了显着改善。开发了两种吸附方案,用于实时监测蛋白质的吸附。结果表明,PE-g-mPEG薄膜表面上预先吸附的牛血清白蛋白(BSA)可以有效抑制随后的纤维蛋白原(Fib)吸附。 BSA的非特异性蛋白质吸附取决于表面覆盖率,而不是取决于PEG的链长。浓密的PEG刷可以释放更多的水分子以抵抗BSA的吸附。而且,预吸附的Fib可能会被高浓度BSA逐渐取代。但是,Fib的吸附和置换取决于表面亲水性。

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