Molecular dynamics simulations of β2-microglobulin interaction with hydrophobic surfaces

IF 3.743 Q2 Biochemistry, Genetics and Molecular Biology Molecular BioSystems Pub Date : 2017-10-09 DOI:10.1039/C7MB00464H
Cedrix J. Dongmo Foumthuim, Alessandra Corazza, Gennaro Esposito and Federico Fogolari
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引用次数: 5

Abstract

Hydrophobic surfaces are known to adsorb and unfold proteins, a process that has been studied only for a few proteins. Here we address the interaction of β2-microglobulin, a paradigmatic protein for the study of amyloidogenesis, with hydrophobic surfaces. A system with 27 copies of the protein surrounded by a model cubic hydrophobic box is studied by implicit solvent molecular dynamics simulations. Most proteins adsorb on the walls of the box without major distortions in local geometry, whereas free molecules maintain proper structures and fluctuations as observed in explicit solvent molecular dynamics simulations. The major conclusions from the simulations are as follows: (i) the adopted implicit solvent model is adequate to describe protein dynamics and thermodynamics; (ii) adsorption occurs readily and is irreversible on the simulated timescale; (iii) the regions most involved in molecular encounters and stable interactions with the walls are the same as those that are important in protein–protein and protein–nanoparticle interactions; (iv) unfolding following adsorption occurs at regions found to be flexible by both experiments and simulations; (v) thermodynamic analysis suggests a very large contribution from van der Waals interactions, whereas unfavorable electrostatic interactions are not found to contribute much to adsorption energy. Surfaces with different degrees of hydrophobicity may occur in vivo. Our simulations show that adsorption is a fast and irreversible process which is accompanied by partial unfolding. The results and the thermodynamic analysis presented here are consistent with and rationalize previous experimental work.

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β2-微球蛋白与疏水表面相互作用的分子动力学模拟
已知疏水表面可以吸附和展开蛋白质,这一过程只对少数蛋白质进行了研究。在这里,我们讨论了β2-微球蛋白与疏水表面的相互作用,β2-微球蛋白是研究淀粉样蛋白形成的典型蛋白。采用隐式溶剂分子动力学模拟方法,研究了27个蛋白质拷贝被模型立方疏水盒包围的体系。大多数蛋白质吸附在盒子壁上,在局部几何结构上没有重大扭曲,而自由分子保持适当的结构和波动,这在显式溶剂分子动力学模拟中观察到。模拟的主要结论如下:(1)所采用的隐式溶剂模型足以描述蛋白质动力学和热力学;(ii)吸附容易发生,并且在模拟时间尺度上是不可逆的;(iii)与分子相遇和与壁稳定相互作用最相关的区域与蛋白质-蛋白质和蛋白质-纳米颗粒相互作用中重要的区域相同;(iv)吸附后展开发生在实验和模拟发现的柔性区域;(v)热力学分析表明,范德华相互作用对吸附能的贡献很大,而不利的静电相互作用对吸附能的贡献不大。在体内可能存在不同疏水性程度的表面。模拟结果表明,吸附是一个快速、不可逆的过程,并伴有部分展开。本文给出的结果和热力学分析与以往的实验工作一致,并使之合理化。
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来源期刊
Molecular BioSystems
Molecular BioSystems 生物-生化与分子生物学
CiteScore
2.94
自引率
0.00%
发文量
0
审稿时长
2.6 months
期刊介绍: Molecular Omics publishes molecular level experimental and bioinformatics research in the -omics sciences, including genomics, proteomics, transcriptomics and metabolomics. We will also welcome multidisciplinary papers presenting studies combining different types of omics, or the interface of omics and other fields such as systems biology or chemical biology.
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