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拥挤剂对变性状态下多结构域蛋白质动力学的影响:一种溶剂化方法。

Influence of crowding agents on the dynamics of a multidomain protein in its denatured state: a solvation approach.

机构信息

Department of Chemistry, Indian Institute of Technology Delhi, Hauz Khas, New Delhi, 110016, India.

出版信息

Eur Biophys J. 2020 May;49(3-4):289-305. doi: 10.1007/s00249-020-01435-y. Epub 2020 May 12.

Abstract

It is now well appreciated that the crowded intracellular environment significantly modulates an array of physiological processes including protein folding-unfolding, aggregation, and dynamics to name a few. In this work we have studied the dynamics of domain I of the protein human serum albumin (HSA) in its urea-induced denatured states, in the presence of a series of commonly used macromolecular crowding agents. HSA was labeled at Cys-34 (a free cysteine) in domain I with the fluorophore 6-bromoacetyl-2-dimethylaminonaphthalene (BADAN) to act as a solvation probe. In partially denatured states (2-6 M urea), lower crowder concentrations (~ < 125 g/L) induced faster dynamics, while the dynamics became slower beyond 150 g/L of crowders. We propose that this apparent switch in dynamics is an evidence of a crossover from soft (enthalpic) to hard-core (entropic) interactions between the protein and crowder molecules. That soft interactions are also important for the crowders used here was further confirmed by the appreciable shift in the wavelength of the emission maximum of BADAN, in particular for PEG8000 and Ficoll 70 at concentrations where the excluded volume effect is not dominant.

摘要

现在人们已经充分认识到,拥挤的细胞内环境显著调节了一系列生理过程,包括蛋白质折叠-展开、聚集和动力学等。在这项工作中,我们研究了在一系列常用的高分子拥挤试剂存在的情况下,蛋白质人血清白蛋白(HSA)结构域 I 的动力学。在结构域 I 中的半胱氨酸 34 位(游离半胱氨酸)用荧光团 6-溴乙酰基-2-二甲氨基萘(BADAN)标记 HSA,作为溶剂探针。在部分变性状态(2-6 M 脲)下,较低的拥挤剂浓度(~ < 125 g/L)诱导更快的动力学,而超过 150 g/L 的拥挤剂时动力学变得更慢。我们提出,这种动力学的明显转变是蛋白质与拥挤分子之间从软(焓)相互作用到硬核(熵)相互作用的交叉的证据。对于这里使用的拥挤剂,软相互作用也很重要,这可以通过 BADAN 的发射最大值的波长明显偏移进一步证实,特别是对于 PEG8000 和 Ficoll 70,在这些浓度下,排除体积效应不是主要的。

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