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    Date Issued2019 (2)2018 (1)AuthorBobola, Nicoletta (3)
    Donaldson, Ian J. (3)
    Ladam, Franck (3)Sagerstrom, Charles G. (3)Maehr, Rene (2)View MoreUMass Chan AffiliationDepartment of Biochemistry and Molecular Pharmacology (3)Diabetes Center of Excellence (2)Program in Molecular Medicine (2)Graduate School of Biomedical Sciences (1)Document TypeJournal Article (2)Preprint (1)KeywordDevelopmental Biology (3)Genetic Phenomena (2)pioneer factor (2)Amino Acids, Peptides, and Proteins (1)Biochemistry, Biophysics, and Structural Biology (1)View MoreJournalbioRxiv (1)Developmental biology (1)eLife (1)

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    Combinatorial action of NF-Y and TALE at embryonic enhancers defines distinct gene expression programs during zygotic genome activation in zebrafish

    Stanney, William; Ladam, Franck; Donaldson, Ian J.; Parsons, Teagan J.; Maehr, Rene; Bobola, Nicoletta; Sagerstrom, Charles G. (2019-12-17)
    Animal embryogenesis is initiated by maternal factors, but zygotic genome activation (ZGA) shifts regulatory control to the embryo during blastula stages. ZGA is thought to be mediated by maternally provided transcription factors (TFs), but few such TFs have been identified in vertebrates. Here we report that NF-Y and TALE TFs bind zebrafish genomic elements associated with developmental control genes already at ZGA. In particular, co-regulation by NF-Y and TALE is associated with broadly acting genes involved in transcriptional control, while regulation by either NF-Y or TALE defines genes in specific developmental processes, such that NF-Y controls a cilia gene expression program while TALE controls expression of hox genes. We also demonstrate that NF-Y and TALE-occupied genomic elements function as enhancers during embryogenesis. We conclude that combinatorial use of NF-Y and TALE at developmental enhancers permits the establishment of distinct gene expression programs at zebrafish ZGA.
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    TALE and NF-Y co-occupancy marks enhancers of developmental control genes during zygotic genome activation in zebrafish [preprint]

    Stanney, William J. III; Ladam, Franck; Donaldson, Ian J.; Parsons, Teagan J.; Maehr, Rene; Bobola, Nicoletta; Sagerstrom, Charles G. (2019-07-31)
    Animal embryogenesis is initiated by maternal factors, but zygotic genome activation (ZGA) shifts control to the embryo at early blastula stages. ZGA is thought to be mediated by specialized maternally deposited transcription factors (TFs), but here we demonstrate that NF-Y and TALE – TFs with known later roles in embryogenesis – co-occupy unique genomic elements at zebrafish ZGA. We show that these elements are selectively associated with early-expressed genes involved in transcriptional regulation and possess enhancer activity in vivo. In contrast, we find that elements individually occupied by either NF-Y or TALE are associated with genes acting later in development – such that NF-Y controls a cilia gene expression program while TALE TFs control expression of hox genes. We conclude that NF-Y and TALE have a shared role at ZGA, but separate roles later during development, demonstrating that combinations of known TFs can regulate subsets of key developmental genes at vertebrate ZGA.
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    TALE factors use two distinct functional modes to control an essential zebrafish gene expression program

    Ladam, Franck; Stanney, William; Donaldson, Ian J.; Yildiz, Ozge; Bobola, Nicoletta; Sagerstrom, Charles G. (2018-06-18)
    TALE factors are broadly expressed embryonically and known to function in complexes with transcription factors (TFs) like Hox proteins at gastrula/segmentation stages, but it is unclear if such generally expressed factors act by the same mechanism throughout embryogenesis. We identify a TALE-dependent gene regulatory network (GRN) required for anterior development and detect TALE occupancy associated with this GRN throughout embryogenesis. At blastula stages, we uncover a novel functional mode for TALE factors, where they occupy genomic DECA motifs with nearby NF-Y sites. We demonstrate that TALE and NF-Y form complexes and regulate chromatin state at genes of this GRN. At segmentation stages, GRN-associated TALE occupancy expands to include HEXA motifs near PBX:HOX sites. Hence, TALE factors control a key GRN, but utilize distinct DNA motifs and protein partners at different stages - a strategy that may also explain their oncogenic potential and may be employed by other broadly expressed TFs.
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