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“类蛋白质”和“非类蛋白质”杂聚物之间的差异。

Difference between "proteinlike" and "nonproteinlike" heteropolymers.

作者信息

Chen H, Zhou X, Ou-Yang Z C

机构信息

Center for Advanced Study, Tsinghua University, Beijing 100084, People's Republic of China.

出版信息

Phys Rev E Stat Nonlin Soft Matter Phys. 2001 Mar;63(3 Pt 1):031913. doi: 10.1103/PhysRevE.63.031913. Epub 2001 Feb 27.

Abstract

Based on a simple two-dimensional (2D) hydrophobic-polar (H-P) lattice model, properties of amino acid chains are studied by enumeration and Monte-Carlo simulation methods. Among them some chains with large average energy gap (E(g);) are thought to be "proteinlike" while the others are "nonproteinlike." The large E(g); between the low excited conformations and the native conformation guarantees not only the thermodynamic stability of protein but also its fast-folding property. The phase transition from molten globule to the native conformation for the "proteinlike" polymer is found to be of first order, while that for the "nonproteinlike" polymer is not. Some properties of chains as a function of E(g); shows that the transition from "nonproteinlike" to "proteinlike" heteropolymers is continuous. The simulation of folding at different temperature indicates that the main reason why some polymers fold slowly to its native conformation is their low folding temperature which makes the effective energy barrier (E(b)/T(f)) much higher than "proteinlike" chains.

摘要

基于一个简单的二维(2D)疏水-极性(H-P)晶格模型,通过枚举和蒙特卡罗模拟方法研究了氨基酸链的性质。其中,一些具有大平均能隙(E(g))的链被认为是“类蛋白质的”,而其他的则是“非类蛋白质的”。低激发构象与天然构象之间的大E(g)不仅保证了蛋白质的热力学稳定性,还保证了其快速折叠特性。发现“类蛋白质”聚合物从熔融球状体到天然构象的相变是一级相变,而“非类蛋白质”聚合物的相变则不是。链的一些性质作为E(g)的函数表明,从“非类蛋白质”到“类蛋白质”杂聚物的转变是连续的。不同温度下的折叠模拟表明,一些聚合物缓慢折叠到其天然构象的主要原因是它们的折叠温度低,这使得有效能垒(E(b)/T(f))比“类蛋白质”链高得多。

相似文献

1
Difference between "proteinlike" and "nonproteinlike" heteropolymers.“类蛋白质”和“非类蛋白质”杂聚物之间的差异。
Phys Rev E Stat Nonlin Soft Matter Phys. 2001 Mar;63(3 Pt 1):031913. doi: 10.1103/PhysRevE.63.031913. Epub 2001 Feb 27.
2
Factors governing the foldability of proteins.影响蛋白质可折叠性的因素。
Proteins. 1996 Dec;26(4):411-41. doi: 10.1002/(SICI)1097-0134(199612)26:4<411::AID-PROT4>3.0.CO;2-E.

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