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蛋白质结构、动力学和功能的网络描述中的紊乱蛋白质和网络紊乱:假说和综合评述。

Disordered proteins and network disorder in network descriptions of protein structure, dynamics and function: hypotheses and a comprehensive review.

机构信息

Department of Medical Chemistry, Semmelweis University, H-1444 Budapest, P. O. Box 260, Hungary.

出版信息

Curr Protein Pept Sci. 2012 Feb;13(1):19-33. doi: 10.2174/138920312799277992.

Abstract

During the last decade, network approaches became a powerful tool to describe protein structure and dynamics. Here we review the links between disordered proteins and the associated networks, and describe the consequences of local, mesoscopic and global network disorder on changes in protein structure and dynamics. We introduce a new classification of protein networks into 'cumulus-type', i.e., those similar to puffy (white) clouds, and 'stratus-type', i.e., those similar to flat, dense (dark) low-lying clouds, and relate these network types to protein disorder dynamics and to differences in energy transmission processes. In the first class, there is limited overlap between the modules, which implies higher rigidity of the individual units; there the conformational changes can be described by an 'energy transfer' mechanism. In the second class, the topology presents a compact structure with significant overlap between the modules; there the conformational changes can be described by 'multi-trajectories'; that is, multiple highly populated pathways. We further propose that disordered protein regions evolved to help other protein segments reach 'rarely visited' but functionally-related states. We also show the role of disorder in 'spatial games' of amino acids; highlight the effects of intrinsically disordered proteins (IDPs) on cellular networks and list some possible studies linking protein disorder and protein structure networks.

摘要

在过去的十年中,网络方法已成为描述蛋白质结构和动力学的有力工具。在这里,我们回顾了无序蛋白质与相关网络之间的联系,并描述了局部、介观和全局网络无序对蛋白质结构和动力学变化的影响。我们将蛋白质网络分为“积云型”,即类似于蓬松(白色)云的网络,和“层积云型”,即类似于平坦、密集(黑色)低空云的网络,并将这些网络类型与蛋白质无序动力学和能量传递过程的差异联系起来。在第一类中,模块之间的重叠有限,这意味着各个单元的刚性更高;在这种情况下,构象变化可以用“能量转移”机制来描述。在第二类中,拓扑结构紧凑,模块之间有很大的重叠;在这种情况下,构象变化可以用“多轨迹”来描述,即多个高度占据的途径。我们进一步提出,无序蛋白质区域的进化是为了帮助其他蛋白质片段达到“很少访问”但功能相关的状态。我们还展示了无序在氨基酸“空间博弈”中的作用;强调了无序蛋白质(IDP)对细胞网络的影响,并列出了一些可能的将蛋白质无序与蛋白质结构网络联系起来的研究。

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