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用于研究牛血清白蛋白中结构域异步展开的位点选择性探针。

Site-selective probe for investigating the asynchronous unfolding of domains in bovine serum albumin.

机构信息

School of Chemistry and Chemical Engineering, Sun Yat-Sen University, Guangzhou 510275, PR China.

出版信息

Talanta. 2011 May 15;84(3):881-6. doi: 10.1016/j.talanta.2011.02.027. Epub 2011 Feb 23.

Abstract

A convenient method is proposed for precise investigation of the asynchronous structural transition of the domains in bovine serum albumin (BSA) during unfolding process. The method is based on a site-selective probe, alizarin red S (ARS), which has a high affinity to the subdomain IIA of BSA. BSA-ARS complex was formed and gradually unfolded by urea from 0 to 8.0M. The unfolding occurred in different domains of BSA resulted in distinct alterations of the microenvironment of the bound ARS. The spectral response of BSA-ARS complex, including the color, the UV absorption at 530 and 432 nm, and the intrinsic fluorescence at 342 and 310 nm with the excitation wavelength of 280 nm, showed slight changes in the urea concentration from 0 to 4.5M, drastic changes from 4.5 to 6.0M, and almost no changes from 6.0 to 8.0M. The redox behavior of bound ARS between 0.3 and 0.8 V also showed the same trend. Consequently, a two-step, three-state transition process was monitored by naked eyes, UV-vis spectroscopy and electrochemistry. It is the first report to realize the indicator of the intermediate state during the unfolding process of BSA through convenient methods instead of expensive approaches. The work provides a facile method for the investigation of the unfolding process of multidomain proteins.

摘要

提出了一种方便的方法,用于精确研究牛血清白蛋白(BSA)在展开过程中结构域的异步结构转变。该方法基于一种对 BSA 亚域 IIA 具有高亲和力的选择性探针,茜素红 S(ARS)。BSA-ARS 复合物形成,并逐渐由脲从 0 到 8.0M 展开。BSA 的不同结构域的展开导致结合的 ARS 的微环境发生明显变化。BSA-ARS 复合物的光谱响应,包括颜色、530nm 和 432nm 的紫外吸收以及 280nm 激发波长下 342nm 和 310nm 的固有荧光,在脲浓度从 0 到 4.5M 时略有变化,在 4.5 到 6.0M 时变化剧烈,在 6.0 到 8.0M 时几乎没有变化。结合的 ARS 在 0.3 至 0.8V 之间的氧化还原行为也表现出相同的趋势。因此,可以通过肉眼、紫外可见光谱和电化学监测到两步、三态转变过程。这是第一个通过方便的方法而不是昂贵的方法来实现 BSA 展开过程中中间态指示剂的报道。该工作为研究多结构域蛋白的展开过程提供了一种简便的方法。

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