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    Pbx1 represses osteoblastogenesis by blocking Hoxa10-mediated recruitment of chromatin remodeling factors

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    Authors
    Gordon, Jonathan A. R.
    Hassan, Mohammad Q.
    Saini, Sharanjot
    Montecino, Martin A.
    Van Wijnen, Andre J.
    Stein, Gary S.
    Stein, Janet L.
    Lian, Jane B.
    UMass Chan Affiliations
    Department of Cell Biology
    Document Type
    Journal Article
    Publication Date
    2010-07-01
    Keywords
    3T3 Cells
    Animals
    Base Sequence
    Cell Differentiation
    Cell Line
    Chromatin Assembly and Disassembly
    Gene Expression Regulation, Developmental
    Homeodomain Proteins
    Humans
    Integrin-Binding Sialoprotein
    Mice
    Models, Biological
    Multipotent Stem Cells
    Mutation
    Osteoblasts
    Osteocalcin
    Osteogenesis
    Promoter Regions, Genetic
    RNA, Small Interfering
    Rats
    Sialoglycoproteins
    Transcription Factors
    Transcriptional Activation
    Cell Biology
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    Abstract
    Abdominal-class homeodomain-containing (Hox) factors form multimeric complexes with TALE-class homeodomain proteins (Pbx, Meis) to regulate tissue morphogenesis and skeletal development. Here we have established that Pbx1 negatively regulates Hoxa10-mediated gene transcription in mesenchymal cells and identified components of a Pbx1 complex associated with genes in osteoblasts. Expression of Pbx1 impaired osteogenic commitment of C3H10T1/2 multipotent cells and differentiation of MC3T3-E1 preosteoblasts. Conversely, targeted depletion of Pbx1 by short hairpin RNA (shRNA) increased expression of osteoblast-related genes. Studies using wild-type and mutated osteocalcin and Bsp promoters revealed that Pbx1 acts through a Pbx-binding site that is required to attenuate gene activation by Hoxa10. Chromatin-associated Pbx1 and Hoxa10 were present at osteoblast-related gene promoters preceding gene expression, but only Hoxa10 was associated with these promoters during transcription. Our results show that Pbx1 is associated with histone deacetylases normally linked with chromatin inactivation. Loss of Pbx1 from osteoblast promoters in differentiated osteoblasts was associated with increased histone acetylation and CBP/p300 recruitment, as well as decreased H3K9 methylation. We propose that Pbx1 plays a central role in attenuating the ability of Hoxa10 to activate osteoblast-related genes in order to establish temporal regulation of gene expression during osteogenesis.
    Source
    Gordon, Jonathan A. R., Hassan, Mohammad Q., Saini, Sharanjot, Montecino, Martin, van Wijnen, Andre J., Stein, Gary S., Stein, Janet L., Lian, Jane B. Pbx1 Represses Osteoblastogenesis by Blocking Hoxa10-Mediated Recruitment of Chromatin Remodeling Factors. Mol. Cell. Biol. 2010 30: 3531-3541. doi:10.1128/MCB.00889-09. Link to article on publisher's website
    DOI
    10.1128/MCB.00889-09
    Permanent Link to this Item
    http://hdl.handle.net/20.500.14038/49564
    PubMed ID
    20439491
    Related Resources
    Link to article in PubMed
    ae974a485f413a2113503eed53cd6c53
    10.1128/MCB.00889-09
    Scopus Count
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    UMass Chan Faculty and Researcher Publications

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