Publication | Open Access
Collapse of the hepatic gene regulatory network in the absence of FoxA factors
56
Citations
41
References
2020
Year
GeneticsMolecular GeneticsFoxa GenesGene Regulatory NetworkEpigeneticsTranscriptional RegulationTranscription FactorsLiver DevelopmentMolecular SignalingFoxa FactorsLiver PhysiologyOrganogenesisGene ExpressionEpigenetic RegulationFunctional GenomicsTranscription RegulationChromatin FunctionGene FunctionChromatinDevelopmental BiologyHepatologyChromatin StructureNatural SciencesFoxa Transcription FactorsGene RegulationRegulatory Network ModellingLiver DiseaseSystems BiologyMedicineCell Development
The FoxA transcription factors are critical for liver development through their pioneering activity, which initiates a highly complex regulatory network thought to become progressively resistant to the loss of any individual hepatic transcription factor via mutual redundancy. To investigate the dispensability of FoxA factors for maintaining this regulatory network, we ablated all FoxA genes in the adult mouse liver. Remarkably, loss of FoxA caused rapid and massive reduction in the expression of critical liver genes. Activity of these genes was reduced back to the low levels of the fetal prehepatic endoderm stage, leading to necrosis and lethality within days. Mechanistically, we found FoxA proteins to be required for maintaining enhancer activity, chromatin accessibility, nucleosome positioning, and binding of HNF4α. Thus, the FoxA factors act continuously, guarding hepatic enhancer activity throughout adult life.
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