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结构紊乱在RNA和蛋白质伴侣功能中的作用。

The role of structural disorder in the function of RNA and protein chaperones.

作者信息

Tompa Peter, Csermely Peter

机构信息

Institute of Enzymology, Biological Research Center, Hungarian Academy of Sciences, 1518 Budapest, P.O. Box 7, Hungary.

出版信息

FASEB J. 2004 Aug;18(11):1169-75. doi: 10.1096/fj.04-1584rev.

Abstract

Chaperones are highly sophisticated protein machines that assist the folding of RNA molecules or other proteins. Their function is generally thought to require a fine-tuned and highly conserved structure: despite the recent recognition of the widespread occurrence of structural disorder in the proteome, this structural trait has never been generally considered in molecular chaperones. In this review we give evidence for the prevalence of functional regions without a well-defined 3-D structure in RNA and protein chaperones. By considering a variety of individual examples, we suggest that the structurally disordered chaperone regions either function as molecular recognition elements that act as solubilizers or locally loosen the structure of the kinetically trapped folding intermediate via transient binding to facilitate its conformational search. The importance of structural disorder is underlined by a predictor of natural disordered regions, which shows an extremely high proportion of such regions, unparalleled in any other protein class, within RNA chaperones: 54.2% of their residues fall into disordered regions and 40% fall within disordered regions longer than 30 consecutive residues. Structural disorder also prevails in protein chaperones, for which frequency values are 36.7% and 15%, respectively. In keeping with these and other details, a novel "entropy transfer" model is presented to account for the mechanistic role of structural disorder in chaperone function.

摘要

分子伴侣是高度复杂的蛋白质机器,可协助RNA分子或其他蛋白质折叠。一般认为它们的功能需要精细调节且高度保守的结构:尽管最近人们认识到蛋白质组中广泛存在结构无序现象,但这种结构特征在分子伴侣中从未被普遍考虑过。在本综述中,我们提供证据表明,RNA和蛋白质分子伴侣中普遍存在没有明确三维结构的功能区域。通过考虑各种具体例子,我们认为结构无序的分子伴侣区域要么作为分子识别元件发挥作用,充当增溶剂,要么通过瞬时结合局部松开动力学捕获的折叠中间体的结构,以促进其构象搜索。天然无序区域预测器强调了结构无序的重要性,该预测器显示,在RNA分子伴侣中,此类区域的比例极高,在任何其他蛋白质类别中都无与伦比:其54.2%的残基属于无序区域,40%位于连续30个以上残基的无序区域内。结构无序在蛋白质分子伴侣中也很普遍,其频率值分别为36.7%和15%。基于这些及其他细节,我们提出了一种新颖的“熵转移”模型,以解释结构无序在分子伴侣功能中的机制作用。

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