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蛋白质结晶中的成核前体。

Nucleation precursors in protein crystallization.

作者信息

Vekilov Peter G, Vorontsova Maria A

机构信息

Department of Chemical and Biomolecular Engineering, University of Houston, Houston, TX 77204-4004, USA.

出版信息

Acta Crystallogr F Struct Biol Commun. 2014 Mar;70(Pt 3):271-82. doi: 10.1107/S2053230X14002386. Epub 2014 Feb 20.

Abstract

Protein crystal nucleation is a central problem in biological crystallography and other areas of science, technology and medicine. Recent studies have demonstrated that protein crystal nuclei form within crucial precursors. Here, methods of detection and characterization of the precursors are reviewed: dynamic light scattering, atomic force microscopy and Brownian microscopy. Data for several proteins provided by these methods have demonstrated that the nucleation precursors are clusters consisting of protein-dense liquid, which are metastable with respect to the host protein solution. The clusters are several hundred nanometres in size, the cluster population occupies from 10(-7) to 10(-3) of the solution volume, and their properties in solutions supersaturated with respect to crystals are similar to those in homogeneous, i.e. undersaturated, solutions. The clusters exist owing to the conformation flexibility of the protein molecules, leading to exposure of hydrophobic surfaces and enhanced intermolecular binding. These results indicate that protein conformational flexibility might be the mechanism behind the metastable mesoscopic clusters and crystal nucleation. Investigations of the cluster properties are still in their infancy. Results on direct imaging of cluster behaviors and characterization of cluster mechanisms with a variety of proteins will soon lead to major breakthroughs in protein biophysics.

摘要

蛋白质晶体成核是生物晶体学以及科学、技术和医学等其他领域的核心问题。最近的研究表明,蛋白质晶体核在关键前体中形成。本文综述了前体的检测和表征方法:动态光散射、原子力显微镜和布朗显微镜。这些方法提供的几种蛋白质的数据表明,成核前体是由蛋白质密集液体组成的聚集体,相对于主体蛋白质溶液而言是亚稳的。聚集体尺寸为几百纳米,聚集体数量占溶液体积的10^(-7)至10^(-3),并且它们在相对于晶体过饱和的溶液中的性质与在均匀(即不饱和)溶液中的性质相似。聚集体的存在归因于蛋白质分子的构象灵活性,导致疏水表面暴露和分子间结合增强。这些结果表明,蛋白质构象灵活性可能是亚稳介观聚集体和晶体成核背后的机制。对聚集体性质的研究仍处于起步阶段。关于聚集体行为的直接成像以及用多种蛋白质表征聚集体机制的结果,将很快在蛋白质生物物理学领域取得重大突破。

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