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研究斑马鱼二氢叶酸还原酶蛋白新变体的折叠展开过程。

Investigation of folding unfolding process of a new variant of dihydrofolate reductase protein from Zebrafish.

机构信息

Amity Institute of Biotechnology, Molecular Biophysics Laboratory, Amity University, Sector 125, Noida, Uttar Pradesh 201313, India; Kusuma School of Biological Sciences, Indian Institute of Technology Delhi, HauzKhas, New Delhi- 110016, India.

Kusuma School of Biological Sciences, Indian Institute of Technology Delhi, HauzKhas, New Delhi- 110016, India.

出版信息

Int J Biol Macromol. 2016 Oct;91:736-43. doi: 10.1016/j.ijbiomac.2016.06.017. Epub 2016 Jun 7.

DOI:10.1016/j.ijbiomac.2016.06.017
PMID:27287769
Abstract

The folding and unfolding mechanisms of a small monomeric protein, Dihydrofolate reductase (1.5.1.3.) from a new variant, Zebrafish (zDHFR) has been studied through GdnHCl denaturation, followed by its refolding through dilution of the denaturant. Intrinsic and extrinsic fluorescence, far-UV CD and enzyme activity were employed to monitor structural and functional changes due to chemical denaturation. The unfolding transitions monitored by intrinsic fluorescence showed that GdnHCl based denaturation of zDHFR is reversible. At low concentration of the denaturant, zDHFR forms intermediate species as reflected by increased fluorescence intensity compared to the native and fully unfolded form. Equilibrium unfolding transition study of zDHFR induced by GdnHCl exhibited three- state process. The non- coincidence of fluorescence and far-UVCD based transitions curves support the establishment of three state model of zDHFR protein which involves native, intermediate and unfolded forms. Analysis of the equilibrium unfolding transition suggests the presence of non- native intermediate species. A comparative study of various species of DHFR shows that zDHFR has comparable thermodynamic stability with human counterpart and thus proved to be a good in vitro model system for structure- function relationship studies. Understanding various conformational states during the folding unfolding process of the zDHFR protein may provide important clues towards designing inhibitors against this important protein involved in cell cycle regulation.

摘要

新型变体斑马鱼二氢叶酸还原酶(1.5.1.3.)的单体小蛋白折叠和展开机制通过 GdnHCl 变性进行了研究,然后通过稀释变性剂使其复性。本研究采用内源和外源荧光、远紫外 CD 和酶活性监测化学变性引起的结构和功能变化。内源荧光监测的展开转变表明,基于 GdnHCl 的 zDHFR 变性是可逆的。在低浓度的变性剂下,与天然和完全展开形式相比,zDHFR 形成中间体物种,荧光强度增加。GdnHCl 诱导的 zDHFR 的平衡展开过渡研究表现出三态过程。荧光和远紫外 CD 基过渡曲线的不一致支持 zDHFR 蛋白的三态模型的建立,该模型涉及天然、中间和展开形式。平衡展开过渡分析表明存在非天然中间体物种。DHFR 各种物种的比较研究表明,zDHFR 与人源对应物具有可比的热力学稳定性,因此被证明是研究结构-功能关系的良好体外模型系统。了解 zDHFR 蛋白折叠展开过程中的各种构象状态可能为设计针对该重要细胞周期调节蛋白的抑制剂提供重要线索。

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