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Physical understanding of complex multiscale biochemical models via algorithmic simplification: Glycolysis in Saccharomyces cerevisiae

机译:通过算法简化对复杂的多尺度生化模型的物理理解:酿酒酵母中的糖酵解

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Large-scale models of cellular reaction networks are usually highly complex and characterized by a wide spectrum of time scales, making a direct interpretation and understanding of the relevant mechanisms almost impossible. We address this issue by demonstrating the benefits provided by model reduction techniques. We employ the Computational Singular Perturbation (CSP) algorithm to analyze the glycolytic pathway of intact yeast cells in the oscillatory regime. As a primary object of research for many decades, glycolytic oscillations represent a paradigmatic candidate for studying biochemical function and mechanisms. Using a previously published full-scale model of glycolysis, we show that, due to fast dissipative time scales, the solution is asymptotically attracted on a low dimensional manifold. Without any further input from the investigator, CSP clarifies several long-standing questions in the analysis of glycolytic oscillations, such as the origin of the oscillations in the upper part of glycolysis, the importance of energy and redox status, as well as the fact that neither the oscillations nor cellcell synchronization can be understood in terms of glycolysis as a simple linear chain of sequentially coupled reactions.
机译:细胞反应网络的大规模模型通常非常复杂,并且具有广泛的时间尺度,因此几乎不可能直接解释和理解相关机制。我们通过展示模型简化技术提供的好处来解决此问题。我们采用计算奇异摄动(CSP)算法来分析完整的酵母细胞在振荡机制中的糖酵解途径。数十年来,糖酵解振荡作为研究的主要对象,代表了研究生化功能和机制的范例。使用先前发布的全面的糖酵解模型,我们显示,由于快速耗散的时间尺度,解决方案在低维流形上渐近吸引。没有研究者的任何进一步意见,CSP澄清了糖酵解振荡分析中的几个长期存在的问题,例如糖酵解上部振荡的起源,能量和氧化还原状态的重要性以及就糖酵解而言,振荡和细胞同步均无法理解为顺序耦合反应的简单线性链。

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