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Stochastic dynamics of genetic broadcasting networks

机译:基因广播网络的随机动力学

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摘要

The complex genetic programs of eukaryotic cells are often regulated by key transcription factors occupying or clearing out of a large number of genomic locations. Orchestrating the residence times of these factors is therefore important for the well organized functioning of a large network. The classic models of genetic switches sidestep this timing issue by assuming the binding of transcription factors to be governed entirely by thermodynamic protein-DNA affinities. Here we show that relying on passive thermodynamics and random release times can lead to a “time-scale crisis” for master genes that broadcast their signals to a large number of binding sites. We demonstrate that this time-scale crisis for clearance in a large broadcasting network can be resolved by actively regulating residence times through molecular stripping. We illustrate these ideas by studying a model of the stochastic dynamics of the genetic network of the central eukaryotic master regulator NFκB which broadcasts its signals to many downstream genes that regulate immune response, apoptosis, etc.
机译:真核细胞的复杂遗传程序通常由占据或清除大量基因组位置的关键转录因子调控。因此,编排这些因素的停留时间对于大型网络的良好组织功能非常重要。基因开关的经典模型通过假设转录因子的结合完全由热力学蛋白质-DNA亲和力来控制,从而规避了这一时序问题。在这里,我们证明了依靠被动热力学和随机释放时间会导致将基因信号传播到大量结合位点的主基因的“时间尺度危机”。我们证明,可以通过分子剥离主动调节停留时间来解决这种大型广播网络中的通关危机。我们通过研究中央真核生物主调节因子NFκB的遗传网络的随机动力学模型来阐明这些想法,该模型将其信号广播到许多调节免疫反应,细胞凋亡等的下游基因。

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  • 期刊名称 other
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  • 年(卷),期 -1(96),5-1
  • 年度 -1
  • 页码 052305
  • 总页数 19
  • 原文格式 PDF
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