Literature DB >> 18759300

Repression of chondrogenesis through binding of notch signaling proteins HES-1 and HEY-1 to N-box domains in the COL2A1 enhancer site.

Shawn P Grogan1, Tsaiwei Olee, Koji Hiraoka, Martin K Lotz.   

Abstract

OBJECTIVE: Notch signaling is implicated in the repression of mesenchymal stem cell (MSC) chondrogenic differentiation. The purpose of this study was to examine the mechanism of this repression and how it is modulated to permit chondrogenesis.
METHODS: Notch intracellular domain (NICD) protein levels were monitored via Western blotting throughout chondrogenic differentiation of human MSCs in pellet cultures. Overexpression of Notch signaling components and their effect on chondrogenesis was achieved by transfecting plasmids coding for NICD, HES-1, and HERP-2/HEY-1. COL2A1 and AGGRECAN expression was monitored via quantitative polymerase chain reaction analysis. Chromatin immunoprecipitation (ChIP) was used to test whether HES-1 and HEY-1 bind putative N-box domains in intron 1 of COL2A1.
RESULTS: High levels of NICD proteins were reduced during chondrogenesis of human MSCs, and this was mediated by transforming growth factor beta3 (TGFbeta3). COL2A1 gene expression was repressed following overexpression of NICD (2-fold) and HES-1 (3-fold) and was markedly repressed by overexpression of HEY-1 (80-fold). HEY-1 repressed AGGRECAN expression 10-fold, while NICD and HES-1 had no effect. We identified 2 putative N-box domains adjacent to, and part of, the SOX9 enhancer binding site located in intron 1 of COL2A1. ChIP studies showed that endogenous HES-1 and HEY-1 bound to these sites. Transducin-like enhancer, the HES-1 corepressor protein, was displaced during chondrogenic differentiation and following TGFbeta3 treatment.
CONCLUSION: These results reveal novel mechanisms by which Notch signaling represses gene expression. Notch signaling proteins act on the SOX9 binding site in the COL2A1 enhancer and prevent SOX9-mediated transcriptional activation of COL2A1 and, thus, chondrogenic differentiation.

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Year:  2008        PMID: 18759300      PMCID: PMC2786215          DOI: 10.1002/art.23730

Source DB:  PubMed          Journal:  Arthritis Rheum        ISSN: 0004-3591


  50 in total

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Review 3.  Toward the rational design of cell fate modifiers: notch signaling as a target for novel biopharmaceuticals.

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5.  HERP, a novel heterodimer partner of HES/E(spl) in Notch signaling.

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  41 in total

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Review 3.  Reconstruction of an in vitro niche for the transition from intervertebral disc development to nucleus pulposus regeneration.

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Review 4.  Notch Signaling and the Skeleton.

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7.  Notch1 signaling regulates chondrogenic lineage determination through Sox9 activation.

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9.  MicroRNA-140 is expressed in differentiated human articular chondrocytes and modulates interleukin-1 responses.

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10.  Mesenchymal progenitor cell markers in human articular cartilage: normal distribution and changes in osteoarthritis.

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