Publication | Open Access
Simulated binding of transcription factors to active and inactive regions folds human chromosomes into loops, rosettes and topological domains
208
Citations
51
References
2016
Year
GeneticsMolecular BiologyGene Regulatory NetworkEpigeneticsProtein FoldingInterphase ChromosomesTranscription FactorsBiophysicsCell DivisionGenome StructureDna ReplicationNuclear OrganizationBiomolecular InteractionChromosomal RearrangementSimulated BindingChromatinPattern FormationChromatin RemodelingNatural SciencesTranscription FactoriesComputational BiologyMolecular BiophysicsSystems BiologyMedicineTopological Domains
Biophysicists are modeling conformations of interphase chromosomes, often basing the strengths of interactions between segments distant on the genetic map on contact frequencies determined experimentally. Here, instead, we develop a fitting-free, minimal model: bivalent or multivalent red and green 'transcription factors' bind to cognate sites in strings of beads ('chromatin') to form molecular bridges stabilizing loops. In the absence of additional explicit forces, molecular dynamic simulations reveal that bound factors spontaneously cluster-red with red, green with green, but rarely red with green-to give structures reminiscent of transcription factories. Binding of just two transcription factors (or proteins) to active and inactive regions of human chromosomes yields rosettes, topological domains and contact maps much like those seen experimentally. This emergent 'bridging-induced attraction' proves to be a robust, simple and generic force able to organize interphase chromosomes at all scales.
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