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动态光散射在研究电解质溶液中蛋白质相互作用方面的应用。

Dynamic light scattering application to study protein interactions in electrolyte solutions.

作者信息

Li Shaoxin, Xing Da, Li Junfeng

机构信息

Institute of Laser Life Science, South China Normal University, Guangzhou, 510631 P.R. China.

出版信息

J Biol Phys. 2004 Jan;30(4):313-24. doi: 10.1007/s10867-004-0997-z.

Abstract

The concentration dependence of the diffusion coefficient of particles suspended in solution depends primarily on the occupied volume fraction and on repulsive and attractive forces. This dependency is expressed by the interaction parameter, which can be assessed experimentally by light scattering measurements and have been determined for the diffusion coefficient of BSA under different salt concentration conditions in the present work. The result shows that the diffusion coefficient of protein grows up with increasing protein concentration, and when the ionic strength turns up gradually the diffusion coefficient decreases with protein concentration's increasing. The concentration dependence of BSA diffusion coefficients is interpreted in the context of a two-body potential of mean force, which includes repulsive hard-sphere and Coulombic interactions and attractive dispersion. With the increase of ionic strength, Debye screening decreases, protein interaction changes from repulsion to attraction, and protein begins to aggregate. By means of the concentration dependence of BSA diffusion coefficients, one can obtain the parameters of protein interactions and can find that protein bears a net effective charge of -9.0 e and has a Hamaker constant of 2.8k(B)T. This work demonstrates that DLS is an effective technique of studying protein interactions.

摘要

溶液中悬浮颗粒扩散系数的浓度依赖性主要取决于占据的体积分数以及排斥力和吸引力。这种依赖性由相互作用参数表示,该参数可通过光散射测量进行实验评估,并且在本工作中已针对不同盐浓度条件下牛血清白蛋白(BSA)的扩散系数进行了测定。结果表明,蛋白质的扩散系数随蛋白质浓度的增加而增大,并且当离子强度逐渐升高时,扩散系数随蛋白质浓度的增加而减小。BSA扩散系数的浓度依赖性是在平均力二体势的背景下进行解释的,该势包括排斥性硬球和库仑相互作用以及吸引性色散。随着离子强度的增加,德拜屏蔽减弱,蛋白质相互作用从排斥变为吸引,并且蛋白质开始聚集。借助BSA扩散系数的浓度依赖性,可以获得蛋白质相互作用的参数,并且可以发现蛋白质带有-9.0 e的净有效电荷,并且具有2.8k(B)T的哈梅克常数。这项工作表明动态光散射(DLS)是研究蛋白质相互作用的有效技术。

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