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An entropic characterization of protein interaction networks and cellular robustness

机译:蛋白质相互作用网络和细胞鲁棒性的熵表征

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摘要

The structure of molecular networks is believed to determine important aspects of their cellular function, such as the organismal resilience against random perturbations. Ultimately, however, cellular behaviour is determined by the dynamical processes, which are constrained by network topology. The present work is based on a fundamental relation from dynamical systems theory, which states that the macroscopic resilience of a steady state is correlated with the uncertainty in the underlying microscopic processes, a property that can be measured by entropy. Here, we use recent network data from large-scale protein interaction screens to characterize the diversity of possible pathways in terms of network entropy. This measure has its origin in statistical mechanics and amounts to a global characterization of both structural and dynamical resilience in terms of microscopic elements. We demonstrate how this approach can be used to rank network elements according to their contribution to network entropy and also investigate how this suggested ranking reflects on the functional data provided by gene knockouts and RNAi experiments in yeast and Caenorhabditis elegans. Our analysis shows that knockouts of proteins with large contribution to network entropy are preferentially lethal. This observation is robust with respect to several possible errors and biases in the experimental data. It underscores the significance of entropy as a fundamental invariant of the dynamical system, and as a measure of structural and dynamical properties of networks. Our analytical approach goes beyond the phenomenological studies of cellular robustness based on local network observables, such as connectivity. One of its principal achievements is to provide a rationale to study proxies of cellular resilience and rank proteins according to their importance within the global network context.
机译:据信分子网络的结构决定了其细胞功能的重要方面,例如抵抗随机扰动的生物适应力。然而,最终,蜂窝行为是由动态过程决定的,而动态过程受网络拓扑的约束。本工作基于动力系统理论的基本关系,该关系指出,稳态的宏观弹性与潜在的微观过程中的不确定性相关,该特性可以通过熵来衡量。在这里,我们使用来自大规模蛋白质相互作用屏幕的最新网络数据,以网络熵来表征可能途径的多样性。这项措施起源于统计力学,相当于微观元素对结构和动态弹性的全面表征。我们演示了如何使用此方法根据网络元素对网络熵的贡献来对网络元素进行排名,并且还研究此建议的排名如何反映酵母和秀丽隐杆线虫中基因敲除和RNAi实验提供的功能数据。我们的分析表明,对网络熵有重大贡献的蛋白质敲除具有致命的杀伤力。对于实验数据中的几种可能的误差和偏差,这种观察是可靠的。它强调了熵作为动力学系统的基本不变性以及作为网络结构和动力学特性的度量的重要性。我们的分析方法超越了基于本地网络可观察性(例如连通性)的细胞健壮性的现象学研究。它的主要成就之一是为研究细胞弹性代理并根据其在全球网络环境中的重要性对蛋白质进行排名提供了理论依据。

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