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重复蛋白未折叠状态的表征

Characterization of the unfolded state of repeat proteins.

作者信息

Mor Amit, Haran Gilad, Levy Yaakov

出版信息

HFSP J. 2008 Dec;2(6):405-15. doi: 10.2976/1.3021145. Epub 2008 Nov 12.

Abstract

The unfolded state ensemble of proteins has been described as a structurally featureless state. While this approach is supported by the fact that many unfolded proteins follow the scaling law behavior of a random coil, there is evidence that the unfolded states of various proteins are stabilized by native or non-native interactions. Recently, the existence of extensive non-native structure was reported for a repeat protein, which resulted in a scaling law exponent that is significantly smaller than that of a random polymer [Cortajarena et al., J. Mol. Biol. 382(1), 203-212 (2008)]. It was concluded that the high compactness of this protein stems from a significant fraction of interacting PP(II) helical segments in the unfolded state. In this study, we aim at providing possible molecular understanding of this anomalous compactness of the unfolded state and to investigate its origin. Using a hierarchy of computational models, we ask whether in general the unfolded state of a repeat protein is likely to be intrinsically more compact than the unfolded state of globular proteins, or whether this phenomenon depends mostly on the occurrence of a specific sequence that promotes PP(II) conformations. Our results suggest that the formation of the PP(II) conformation is indeed essential, yet the recurring sequence of repeat proteins promotes the interactions between these PP(II) segments and the formation of non-native interactions in the unfolded state.

摘要

蛋白质的未折叠状态系综被描述为一种无结构特征的状态。虽然许多未折叠蛋白质遵循随机卷曲的标度律行为这一事实支持了这种方法,但有证据表明,各种蛋白质的未折叠状态通过天然或非天然相互作用得以稳定。最近,有报道称一种重复蛋白存在广泛的非天然结构,这导致其标度律指数明显小于随机聚合物的标度律指数[科尔塔哈雷纳等人,《分子生物学杂志》382(1),203 - 212(2008)]。得出的结论是,这种蛋白质的高度紧凑性源于未折叠状态下相当一部分相互作用的多聚脯氨酸II型(PP(II))螺旋片段。在本研究中,我们旨在对未折叠状态的这种异常紧凑性提供可能的分子理解,并探究其起源。使用一系列计算模型,我们要问的是,一般来说,重复蛋白的未折叠状态是否本质上比球状蛋白的未折叠状态更紧凑,或者这种现象是否主要取决于促进PP(II)构象的特定序列的出现。我们的结果表明,PP(II)构象的形成确实至关重要,然而重复蛋白的重复序列促进了这些PP(II)片段之间的相互作用以及未折叠状态下非天然相互作用的形成。

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