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蛋白质折叠:理论与实验的匹配

Protein folding: matching theory and experiment.

作者信息

Laurents D V, Baldwin R L

机构信息

Biochemistry Department, Beckman Center, Stanford Medical Center, Stanford, California 94305-5307, USA.

出版信息

Biophys J. 1998 Jul;75(1):428-34. doi: 10.1016/S0006-3495(98)77530-7.

Abstract

The impact of folding funnels and folding simulations on the way experimentalists interpret results is examined. The image of the transition state has changed from a unique species that has a strained configuration, with a correspondingly high free energy, to a more ordinary folding intermediate, whose balance between limited conformational entropy and stabilizing contacts places it at the top of the free energy barrier. Evidence for a broad transition barrier comes from studies showing that mutations can change the position of the barrier. The main controversial issue now is whether populated folding intermediates are productive on-pathway intermediates or dead-end traps. Direct experimental evidence is needed. Theories suggesting that populated intermediates are trapped in a glasslike state are usually based on mechanisms which imply that trapping would only be extremely short-lived (e.g., nanoseconds) in water at 25 degrees C. There seems to be little experimental evidence for long-lived trapping in monomers, if folding aggregates are excluded. On the other hand, there is good evidence for kinetic trapping in dimers. alpha-Helix formation is currently the fastest known process in protein folding, and incipient helices are present at the start of folding. Fast helix formation has the effect of narrowing drastically the choice of folding routes. Thus helix formation can direct folding. It changes the folding metaphor from pouring liquid down a folding funnel to a train leaving a switchyard with only a few choices of exit tracks.

摘要

本文考察了折叠漏斗和折叠模拟对实验人员解读结果方式的影响。过渡态的概念已从具有应变构型、相应自由能较高的独特物种,转变为更普通的折叠中间体,其在有限构象熵和稳定接触之间的平衡使其处于自由能垒的顶部。存在宽泛过渡垒的证据来自于表明突变可改变垒位置的研究。目前主要的争议问题是,大量存在的折叠中间体是有成效的折叠途径中间体还是死端陷阱。这需要直接的实验证据。认为大量存在的中间体被困于类玻璃态的理论通常基于一些机制,这些机制意味着在25摄氏度的水中,捕获仅会持续极短时间(例如纳秒)。如果不考虑折叠聚集体,似乎几乎没有关于单体中长寿命捕获的实验证据。另一方面,有充分证据表明二聚体中存在动力学捕获。α-螺旋形成是目前已知蛋白质折叠中最快的过程,在折叠开始时就存在初始螺旋。快速螺旋形成会极大地缩小折叠途径的选择范围。因此,螺旋形成可引导折叠。它将折叠的比喻从把液体倒入折叠漏斗转变为一列火车离开调车场,只有几条出口轨道可供选择。

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