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人载脂蛋白 A1 在固/液和液/气界面。

Human Apolipoprotein A1 at Solid/Liquid and Liquid/Gas Interfaces.

出版信息

J Phys Chem B. 2018 Apr 12;122(14):3953-3960. doi: 10.1021/acs.jpcb.7b12481. Epub 2018 Mar 28.

Abstract

An X-ray reflectivity study on the adsorption behavior of human apolipoprotein A1 (apoA1) at hydrophilic and hydrophobic interfaces is presented. It is shown that the protein interacts via electrostatic and hydrophobic interactions with the interfaces, resulting in the absorption of the protein. pH dependent measurements at the solid/liquid interface between silicon dioxide and aqueous protein solution show that in a small pH range between pH 4 and 6, adsorption is increased due to electrostatic attraction. Here, the native shape of the protein seems to be conserved. In contrast, the adsorption at the liquid/gas interface is mainly driven by hydrophobic effects, presumably by extending the hydrophobic regions of the amphipathic helices, and results in a conformational change of the protein during adsorption. However, the addition of differently charged membrane-forming lipids at the liquid/gas interface illustrates the ability of apoA1 to include lipids, resulting in a depletion of the lipids from the interface.

摘要

本文报道了人载脂蛋白 A1(apoA1)在亲水和疏水界面上吸附行为的 X 射线反射率研究。结果表明,蛋白质通过静电和疏水相互作用与界面相互作用,导致蛋白质的吸收。在二氧化硅和蛋白质水溶液之间的固/液界面上进行的 pH 依赖性测量表明,在 pH 4 到 6 的小 pH 范围内,由于静电吸引,吸附增加。在该范围内,蛋白质的天然形状似乎得以保留。相比之下,在气/液界面上的吸附主要由疏水作用驱动,可能是通过扩展两亲性螺旋的疏水区,导致蛋白质在吸附过程中发生构象变化。然而,在气/液界面添加带不同电荷的形成膜的脂质表明 apoA1 具有包含脂质的能力,导致脂质从界面中耗尽。

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