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通过远紫外停流圆二色性和8-苯胺基-1-萘磺酸盐结合测定的大肠杆菌色氨酸脱辅基阻遏物早期折叠中间体的结构与稳定性

Structure and stability of an early folding intermediate of Escherichia coli trp aporepressor measured by far-UV stopped-flow circular dichroism and 8-anilino-1-naphthalene sulfonate binding.

作者信息

Mann C J, Matthews C R

机构信息

Department of Chemistry, Pennsylvania State University, University Park 16802.

出版信息

Biochemistry. 1993 May 25;32(20):5282-90. doi: 10.1021/bi00071a002.

Abstract

The refolding kinetics of Escherichia coli trp aporepressor were monitored using stopped-flow far-ultraviolet circular dichroism and 8-anilino-1-naphthalene sulfonate fluorescence spectroscopy. Significant gains in secondary structure and the development of hydrophobic surface, respectively, were observed within the dead time of mixing (4-5 ms). These initial increases, or burst phase amplitudes, plotted as a function of final urea concentration, exhibited sigmoidal, coincident unfolding transition curves. The transition curves were fit to a two-state model, and the resulting free energies of folding in the absence of denaturant were found to be similar (approximately 3.3 kcal/mol). Three subsequent slow refolding phases exhibited relaxation times and amplitudes similar to those previously observed for tryptophan fluorescence [Gittelman, M. S., & Matthews, C. R. (1990) Biochemistry 29, 7011-7021]. These results support the proposals that a stable, monomeric intermediate is rapidly formed during the folding of trp aporepressor and that this species contains a significant amount of secondary structure and hydrophobic surface. This early intermediate is then processed through folding and association reactions that result in the formation of the remaining secondary, tertiary, and quaternary structure.

摘要

利用停流远紫外圆二色光谱和8-苯胺基-1-萘磺酸荧光光谱监测了大肠杆菌色氨酸脱辅基阻遏蛋白的重折叠动力学。在混合的死时间(4 - 5毫秒)内,分别观察到二级结构的显著增加和疏水表面的形成。这些初始增加量或爆发相振幅作为最终尿素浓度的函数绘制,呈现出S形的、重合的解折叠转变曲线。将转变曲线拟合到二态模型,发现在没有变性剂的情况下得到的折叠自由能相似(约3.3千卡/摩尔)。随后的三个缓慢重折叠阶段表现出的弛豫时间和振幅与先前观察到的色氨酸荧光相似[Gittelman, M. S., & Matthews, C. R. (1990) Biochemistry 29, 7011 - 7021]。这些结果支持了以下观点:在色氨酸脱辅基阻遏蛋白折叠过程中会迅速形成一个稳定的单体中间体,并且该物种含有大量的二级结构和疏水表面。然后这个早期中间体通过折叠和缔合反应进行处理,从而导致其余二级、三级和四级结构的形成。

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