Literature DB >> 30445456

Runx2 regulates cranial suture closure by inducing hedgehog, Fgf, Wnt and Pthlh signaling pathway gene expressions in suture mesenchymal cells.

Xin Qin1, Qing Jiang1,2, Toshihiro Miyazaki1, Toshihisa Komori1,2.   

Abstract

Cleidocranial dysplasia (CCD, #119600), which is characterized by hypoplastic clavicles, open fontanelles, supernumerary teeth and a short stature, is caused by heterozygous mutations in RUNX2. However, it currently remains unclear why suture closure is severely impaired in CCD patients. The closure of posterior frontal (PF) and sagittal (SAG) sutures was completely interrupted in Runx2+/- mice, and the proliferation of suture mesenchymal cells and their condensation were less than those in wild-type mice. To elucidate the underlying molecular mechanisms, differentially expressed genes between wild-type and Runx2+/- PF and SAG sutures were identified by microarray and real-time reverse transcription polymerase chain reaction analyses. The expression of hedgehog, Fgf, Wnt and Pthlh signaling pathway genes, including Gli1, Ptch1, Ihh, Fgfr2, Fgfr3, Tcf7, Wnt10b and Pth1r, which were directly regulated by Runx2, was reduced in the sutures, but not the calvarial bone tissues of Runx2+/- mice. Bone formation and suture closure were enhanced in an organ culture of Runx2+/- calvariae with ligands or agonists of hedgehog, Fgf, Wnt and Pthlh signaling, while they were suppressed and suture mesenchymal cell proliferation was decreased in an organ culture of wild-type calvariae with their antagonists. These results indicate that more than a half dosage of Runx2 is required for the proliferation of suture mesenchymal cells, their condensation and commitment to osteoblast-lineage cells, and the induction of hedgehog, Fgf, Wnt and Pthlh signaling pathway gene expressions in sutures, but not in calvarial bone tissues, and also that the activation of hedgehog, Fgf, Wnt and Pthlh signaling pathways is necessary for suture closure.
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Year:  2019        PMID: 30445456     DOI: 10.1093/hmg/ddy386

Source DB:  PubMed          Journal:  Hum Mol Genet        ISSN: 0964-6906            Impact factor:   6.150


  24 in total

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Review 2.  Signaling network regulating osteogenesis in mesenchymal stem cells.

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Review 3.  Signaling Pathways in Bone Development and Their Related Skeletal Dysplasia.

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4.  MACF1 promotes osteoblast differentiation by sequestering repressors in cytoplasm.

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Journal:  Cell Death Differ       Date:  2021-03-04       Impact factor: 12.067

5.  RAB23 coordinates early osteogenesis by repressing FGF10-pERK1/2 and GLI1.

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6.  Runx2 Regulates Mouse Tooth Root Development Via Activation of WNT Inhibitor NOTUM.

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Review 7.  Bcl11b/Ctip2 in Skin, Tooth, and Craniofacial System.

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Review 8.  Molecular Mechanism of Runx2-Dependent Bone Development.

Authors:  Toshihisa Komori
Journal:  Mol Cells       Date:  2020-02-29       Impact factor: 5.034

9.  Antxr1, Which is a Target of Runx2, Regulates Chondrocyte Proliferation and Apoptosis.

Authors:  Qing Jiang; Xin Qin; Carolina Andrea Yoshida; Hisato Komori; Kei Yamana; Shinsuke Ohba; Hironori Hojo; Brad St Croix; Viviane K S Kawata-Matsuura; Toshihisa Komori
Journal:  Int J Mol Sci       Date:  2020-03-31       Impact factor: 5.923

10.  Expression of a Constitutively Active Form of Hck in Chondrocytes Activates Wnt and Hedgehog Signaling Pathways, and Induces Chondrocyte Proliferation in Mice.

Authors:  Viviane K S Kawata Matsuura; Carolina Andrea Yoshida; Hisato Komori; Chiharu Sakane; Kei Yamana; Qing Jiang; Toshihisa Komori
Journal:  Int J Mol Sci       Date:  2020-04-12       Impact factor: 5.923

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