Literature DB >> 29746183

Msx2 Marks Spatially Restricted Populations of Mesenchymal Precursors.

N Sakagami1, Y Matsushita1, S Syklawer-Howle1, H M Kronenberg2, W Ono1, N Ono1.   

Abstract

Craniofacial development requires a set of patterning codes that define the identities of postmigratory mesenchymal cells in a region-specific manner, in which locally expressed morphogens, including fibroblast growth factors (FGFs) and bone morphogenetic proteins (BMPs), provide instructive cues. Msx2, a bona fide target of BMP signaling, is a transcription factor regulating Runx2 and osterix (Osx), whose mutations are associated with cranial deformities in humans. Here we show that Msx2 defines osteo-chondro precursor cells in specific regions of the craniofacial mesenchyme at the postmigratory stage, particularly in the mandibular process and the posterior cranial vault. Analysis of Msx2-creER mice revealed that early mesenchymal cells in proximity to the BMP4-expressing mesenchyme were marked upon tamoxifen injection, and their descendants contributed to diverse types of mesenchymal cells in the later stage, such as chondrocytes and perichondrial cells of the transient cartilage, as well as osteoblasts and suture mesenchymal cells. By contrast, Osx-creER marked osteoblast precursors at the later stage, and their descendants continued to become osteoblasts well into the postnatal stage. Therefore, Msx2 marks spatially restricted populations of mesenchymal precursor cells with diverse differentiation potential, suggesting that extrinsic molecular cues can dictate the nature of postmigratory mesenchymal cells in craniofacial development.

Entities:  

Keywords:  cell differentiation; chondrocytes; cranial sutures; maxillofacial development; osteoblasts; transcription factors

Mesh:

Substances:

Year:  2018        PMID: 29746183      PMCID: PMC6151915          DOI: 10.1177/0022034518771014

Source DB:  PubMed          Journal:  J Dent Res        ISSN: 0022-0345            Impact factor:   6.116


  24 in total

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4.  Augmented BMP signaling in the neural crest inhibits nasal cartilage morphogenesis by inducing p53-mediated apoptosis.

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5.  Ectodermally derived FGF8 defines the maxillomandibular region in the early chick embryo: epithelial-mesenchymal interactions in the specification of the craniofacial ectomesenchyme.

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6.  Premature suture closure and ectopic cranial bone in mice expressing Msx2 transgenes in the developing skull.

Authors:  Y H Liu; R Kundu; L Wu; W Luo; M A Ignelzi; M L Snead; R E Maxson
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7.  A robust and high-throughput Cre reporting and characterization system for the whole mouse brain.

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8.  A phylogenetically conserved cis-regulatory module in the Msx2 promoter is sufficient for BMP-dependent transcription in murine and Drosophila embryos.

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Review 9.  Signals and switches in Mammalian neural crest cell differentiation.

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10.  Augmentation of Smad-dependent BMP signaling in neural crest cells causes craniosynostosis in mice.

Authors:  Yoshihiro Komatsu; Paul B Yu; Nobuhiro Kamiya; Haichun Pan; Tomokazu Fukuda; Gregory J Scott; Manas K Ray; Ken-Ichi Yamamura; Yuji Mishina
Journal:  J Bone Miner Res       Date:  2013-06       Impact factor: 6.741

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Journal:  J Dent Res       Date:  2019-10-17       Impact factor: 6.116

Review 2.  The diverse origin of bone-forming osteoblasts.

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Review 3.  BMP Signaling in the Development and Regeneration of Cranium Bones and Maintenance of Calvarial Stem Cells.

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