Publication | Open Access
Transcriptional regulatory network controlling the ontogeny of hematopoietic stem cells
48
Citations
56
References
2020
Year
Hsc OntogenyTranscriptomics TechnologyGene Regulatory NetworkEpigeneticsTranscriptional RegulationStem Cell MobilizationStem CellsTranscription FactorsTranscriptional Regulatory NetworkGene ExpressionFunctional GenomicsCell BiologyCell LineageDevelopmental BiologyGene RegulationStem Cell ResearchTranscription Factors Sp3Cell Fate DeterminationSystems BiologyMedicine
Hematopoietic stem cell (HSC) ontogeny is accompanied by dynamic changes in gene regulatory networks. We performed RNA-seq and histone mark ChIP-seq to define the transcriptomes and epigenomes of cells representing key developmental stages of HSC ontogeny in mice. The five populations analyzed were embryonic day 10.5 (E10.5) endothelium and hemogenic endothelium from the major arteries, an enriched population of prehematopoietic stem cells (pre-HSCs), fetal liver HSCs, and adult bone marrow HSCs. Using epigenetic signatures, we identified enhancers for each developmental stage. Only 12% of enhancers are primed, and 78% are active, suggesting the vast majority of enhancers are established de novo without prior priming in earlier stages. We constructed developmental stage-specific transcriptional regulatory networks by linking enhancers and predicted bound transcription factors to their target promoters using a novel computational algorithm, target inference via physical connection (TIPC). TIPC predicted known transcriptional regulators for the endothelial-to-hematopoietic transition, validating our overall approach, and identified putative novel transcription factors, including the broadly expressed transcription factors SP3 and MAZ. Finally, we validated a role for SP3 and MAZ in the formation of hemogenic endothelium. Our data and computational analyses provide a useful resource for uncovering regulators of HSC formation.
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