4.7 Article

Stochastic dynamics of genetic broadcasting networks

期刊

PHYSICAL REVIEW E
卷 96, 期 5, 页码 -

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AMER PHYSICAL SOC
DOI: 10.1103/PhysRevE.96.052305

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  1. D. R. Bullard-Welch Chair at Rice University [C-0016]
  2. PPG from the National Institute of General Medical Sciences [P01 GM071862]

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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 NF kappa B which broadcasts its signals to many downstream genes that regulate immune response, apoptosis, etc.

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