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进化保守的 Tyr169 稳定朊病毒蛋白的β2-α2 环。

Evolutionary conserved Tyr169 stabilizes the β2-α2 loop of the prion protein.

机构信息

Department of Biochemistry University of Zürich , Winterthurerstrasse 190, CH-8057 Zürich, Switzerland.

出版信息

J Am Chem Soc. 2015 Mar 4;137(8):2948-57. doi: 10.1021/ja511568m. Epub 2015 Feb 20.

Abstract

Experimental evidence indicates that the primary structure of the β2-α2 loop region (residues 165-175) in mammalian prion proteins (PrP) influences the conversion from the cellular species (PrP(C)) to the β-sheet-rich aggregate. Here, we captured the transition of the β2-α2 loop from 310-helical turn to β turn by unbiased molecular dynamics simulations of the single-point mutant Y169G. Multiple conformations along the spontaneous transition of the mutant were then used as starting point for sampling of the free-energy surface of the wild type and other single-point mutants. Using two different methods for the determination of free energy profiles, we found that the barrier for the 310-helical turn to β turn transition of the wild type is higher by about 2.5 kcal/mol than for the Y169G mutant, which is due to favorable stacking of the aromatic rings of Y169 and F175, and a stable hydrogen bond between the side chains of Y169 and D178. The transition of the β2-α2 loop to β turn increases the solvent-exposure of the hydrophobic stretch 169-YSNQNNF-175. The simulations indicate that the strictly conserved Y169 in mammalian prion proteins stabilizes the 310-helical turn in the β2-α2 loop, thus hindering the conversion to an aggregation-prone conformation.

摘要

实验证据表明,哺乳动物朊病毒蛋白(PrP)中β2-α2 环区(残基 165-175)的一级结构影响从细胞态(PrP(C)) 到富含β-折叠的聚集物的转化。在这里,我们通过对单点突变 Y169G 的无偏分子动力学模拟捕获了β2-α2 环从 310 螺旋转角到β转角的转变。然后,将突变体自发转变过程中的多个构象用作野生型和其他单点突变体的自由能表面采样的起点。使用两种不同的方法来确定自由能曲线,我们发现野生型 310 螺旋转角到β转角转变的势垒比 Y169G 突变体高约 2.5 kcal/mol,这是由于 Y169 和 F175 的芳环堆积有利,以及 Y169 和 D178 的侧链之间形成稳定的氢键。β2-α2 环向β转角的转变增加了疏水性延伸 169-YSNQNNF-175 的溶剂暴露。模拟表明,哺乳动物朊病毒蛋白中严格保守的 Y169 稳定了β2-α2 环中的 310 螺旋转角,从而阻碍了向易于聚集的构象的转化。

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