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为什么硅结合蛋白“Si-tag”能与硅表面强烈结合?固有无序多肽对固体表面的构象适应的意义。

Why does the silica-binding protein "Si-tag" bind strongly to silica surfaces? Implications of conformational adaptation of the intrinsically disordered polypeptide to solid surfaces.

机构信息

Department of Molecular Biotechnology, Graduate School of Advanced Sciences of Matter, Hiroshima University, 1-3-1 Kagamiyama, Higashi-Hiroshima, Hiroshima 739-8530, Japan.

出版信息

Colloids Surf B Biointerfaces. 2011 Sep 1;86(2):359-63. doi: 10.1016/j.colsurfb.2011.04.020. Epub 2011 Apr 21.

DOI:10.1016/j.colsurfb.2011.04.020
PMID:21592750
Abstract

We recently reported that the bacterial 50S ribosomal protein L2 binds strongly to silica surfaces even in the presence of high salt concentrations, detergents, and denaturants such as 8 M urea. We designated L2 as Si-tag, a fusion tag for immobilizing functional proteins on silica materials. Here we discuss the remarkable properties of the Si-tag polypeptide in order to understand the mechanism underlying this binding. Experimental and theoretical studies have shown that the 60-aa N-terminal region and the 71-aa C-terminal region, both of which are rich in positively charged residues, lack a well-defined three-dimensional structure under physiological conditions. This lack of a stable tertiary structure suggests that Si-tag belongs to a family of intrinsically disordered (ID) proteins that exist as dynamic ensembles of rapidly fluctuating structures in aqueous solution. Because of its inherent flexibility, Si-tag could form a large intermolecular interface and optimize its structure for surface interactions by conformational adaptation at the binding interface. Such conformational adaptation occurring concomitantly with binding is common to many ID proteins and is called "coupled folding and binding". Through this conformational adaptation, Si-tag could optimize the interactions between its positively charged side chains and ionized surface silanol groups and between its apolar side chains and hydrophobic surface siloxane sites. The cumulative contribution of these contacts would significantly strengthen the binding of Si-tag, resulting in strong, virtually irreversible binding. Our study suggests that flexible ID proteins have tremendous potential for connecting biomolecules to inorganic materials.

摘要

我们最近报道称,细菌 50S 核糖体蛋白 L2 即使在存在高盐浓度、洗涤剂和变性剂(如 8M 尿素)的情况下,也能与二氧化硅表面强烈结合。我们将 L2 命名为 Si-tag,这是一种将功能性蛋白质固定在二氧化硅材料上的融合标签。在这里,我们将讨论 Si-tag 多肽的显著特性,以了解这种结合的机制。实验和理论研究表明,富含正电荷的 60 个氨基酸 N 端区域和 71 个氨基酸 C 端区域在生理条件下都缺乏明确的三维结构。这种缺乏稳定的三级结构表明 Si-tag 属于无规卷曲(ID)蛋白家族,在水溶液中以快速波动结构的动态集合体形式存在。由于其固有灵活性,Si-tag 可以形成大的分子间界面,并通过在结合界面上的构象适应来优化其结构以进行表面相互作用。这种与结合同时发生的构象适应是许多 ID 蛋白的共同特征,被称为“偶联折叠和结合”。通过这种构象适应,Si-tag 可以优化其正电荷侧链与离子化表面硅醇基团之间以及非极性侧链与疏水性表面硅氧烷位点之间的相互作用。这些接触的累积贡献将显著增强 Si-tag 的结合,从而导致强的、几乎不可逆的结合。我们的研究表明,灵活的 ID 蛋白在将生物分子连接到无机材料方面具有巨大的潜力。

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