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**关键词**:TiO2;吸附;纤维连接蛋白;血纤维蛋白原;白蛋白;时间分辨动力学;结构变化;竞争研究

Adsorption of fibronectin, fibrinogen, and albumin on TiO2: time-resolved kinetics, structural changes, and competition study.

机构信息

Department of Material Science and Metallurgy, Technical University of Catalonia, Barcelona, Spain.

出版信息

Biointerphases. 2012 Dec;7(1-4):48. doi: 10.1007/s13758-012-0048-4. Epub 2012 Aug 9.

Abstract

An understanding of protein adsorption process is crucial for designing biomaterial surfaces. In this work, with the use of a quartz-crystal microbalance with dissipation monitoring, we researched the following: (a) the kinetics of adsorption on TiO(2) surfaces of three extensively described proteins that are relevant for metallic implant integration [i.e., albumin (BSA), fibrinogen (Fbg), and fibronectin (Fn)]; and (b) the competition of those proteins for adsorbing on TiO(2) in a two-step experiment consisted of sequentially exposing the surfaces to different monoprotein solutions. Each protein showed a different process of adsorption and properties of the adlayer-calculated using the Voigt model. The competition experiments showed that BSA displaced larger proteins such as Fn and Fbg when BSA was introduced as the second protein in the system, whereas the larger proteins laid on top of BSA forming an adsorbed protein bi-layer when those were introduced secondly in the system.

摘要

了解蛋白质吸附过程对于设计生物材料表面至关重要。在这项工作中,我们使用石英晶体微天平(带有耗散监测功能)研究了以下内容:(a)在与金属植入物整合相关的三种广泛描述的蛋白质(即白蛋白(BSA)、纤维蛋白原(Fbg)和纤维连接蛋白(Fn))在 TiO2 表面上的吸附动力学;(b)在两步实验中,这些蛋白质在 TiO2 上的竞争,该实验由依次将表面暴露于不同的单蛋白溶液组成。每种蛋白质的吸附过程和使用 Voigt 模型计算得到的吸附层性质都不同。竞争实验表明,当 BSA 作为系统中的第二种蛋白质引入时,BSA 会取代 Fn 和 Fbg 等较大的蛋白质,而当较大的蛋白质在系统中被引入时,它们会覆盖在 BSA 上形成吸附蛋白质双层。

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