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Properties of switch-like bioregulatory networks studied by simulation of the hypoxia response control system

机译:通过低氧响应控制系统的仿真研究类开关生物调节网络的特性

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A complex bioregulatory network could be more easily comprehended if its essential function could be described by a small "core" subsystem, and if its response characteristics were switch-like. We tested this proposition by simulation studies of the hypoxia response control network. We hypothesized that a small subsystem governs the basics of the cellular response to hypoxia and that this response has a sharp oxygen-dependent transition. A molecular interaction map of the network was prepared, and an evolutionarily conserved core subsystem was extracted that could control the activity of hypoxia response promoter elements on the basis of oxygen concentration. The core subsystem included the hypoxia-inducible transcription factor (HIFalpha:ARNT heterodimer), proline hydroxylase, and the von Hippel-Lindau protein. Simulation studies showed that the same core subsystem can exhibit switch-like responses both to oxygen level and to HIFalpha synthesis rate, thus suggesting a mechanism for hypoxia response promoter element-dependent responses common to both hypoxia and growth factor signaling. The studies disclosed the mechanism responsible for the sharp transitions. We show how parameter sets giving switch-like behavior can be found and how this type of behavior provides a foundation for quantitative studies in cells.
机译:如果一个小型的“核心”子系统可以描述一个复杂的生物调节网络的基本功能,并且其响应特性像开关一样,则可以更容易地理解它。我们通过对缺氧反应控制网络的仿真研究测试了这一命题。我们假设一个小的子系统控制着对缺氧的细胞反应的基础,并且这种反应具有一个强烈的氧依赖性转变。绘制了网络的分子相互作用图,并提取了一个进化上保守的核心子系统,该子系统可以根据氧浓度控制缺氧反应启动子元件的活性。核心子系统包括缺氧诱导型转录因子(HIFalpha:ARNT异二聚体),脯氨酸羟化酶和von Hippel-Lindau蛋白。仿真研究表明,相同的核心子系统对氧水平和HIFalpha合成速率均可以表现出类似开关的响应,从而为低氧和生长因子信号传导共同提供了一种低氧响应启动子依赖元件的响应机制。研究揭示了导致急剧转变的机制。我们展示了如何找到提供类似开关行为的参数集,以及这种行为如何为细胞中的定量研究提供基础。

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