Literature DB >> 12640731

Epigenetic signals during odontoblast differentiation.

H Lesot1, S Lisi, R Peterkova, M Peterka, V Mitolo, J V Ruch.   

Abstract

Odontoblast terminal differentiation occurs according to a tooth-specific pattern and implies both temporospatially regulated epigenetic signaling and the expression of specific competence. Differentiation of odontoblasts (withdrawal from the cell cycle, cytological polarization, and secretion of predentin/dentin) is controlled by the inner dental epithelium, and the basement membrane (BM) plays a major role both as a substrate and as a reservoir of paracrine molecules. Cytological differentiation implies changes in the organization of the cytoskeleton and is controlled by cytoskeleton-plasma membrane-extracellular matrix interactions. Fibronectin is re-distributed during odontoblast polarization and interacts with cell-surface molecules. A non-integrin 165-kDa fibronectin-binding protein, transiently expressed by odontoblasts, is involved in microfilament reorganization. Growth factors (TGF beta 1, 2, 3/BMP2, 4, and 6), expressed in tooth germs, signal differentiation. Systemically derived molecules (IGF1) may also intervene. IGF1 stimulates cytological but not functional differentiation of odontoblasts: The two events can thus be separated. Immobilized TGF beta 1 (combined with heparin) induced odontoblast differentiation. Only immobilized TGF beta 1 and 3 or a combination of FGF1 and TGF beta 1 stimulated the differentiation of functional odontoblasts over extended areas and allowed for maintenance of gradients of differentiation. Presentation of active molecules in vitro appeared to be of major importance; the BM should fulfill this role in vivo by immobilizing and spatially presenting TGF beta s. Attempts are being made to investigate the mechanisms which spatially control the initiation of odontoblast differentiation and those which regulate its propagation. Analysis of molar development suggested that odontoblast differentiation and crown morphogenesis are interdependent, although the possibility of co-regulation requires further investigation.

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Year:  2001        PMID: 12640731     DOI: 10.1177/08959374010150012001

Source DB:  PubMed          Journal:  Adv Dent Res        ISSN: 0895-9374


  24 in total

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2.  Dact1-3 mRNAs exhibit distinct expression domains during tooth development.

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4.  Transcriptome-based systematic identification of extracellular matrix proteins.

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Journal:  Proc Natl Acad Sci U S A       Date:  2008-08-29       Impact factor: 11.205

5.  Dentinogenic potential of human adult dental pulp cells during the extended primary culture.

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Review 6.  Can interaction of materials with the dentin-pulp complex contribute to dentin regeneration?

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7.  Osterix regulates tooth root formation in a site-specific manner.

Authors:  T H Kim; C H Bae; J C Lee; J E Kim; X Yang; B de Crombrugghe; E S Cho
Journal:  J Dent Res       Date:  2015-01-07       Impact factor: 6.116

8.  Generation and characterization of DSPP-Cerulean/DMP1-Cherry reporter mice.

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9.  Cytomegalovirus inhibition of embryonic mouse tooth development: a model of the human amelogenesis imperfecta phenocopy.

Authors:  Tina Jaskoll; George Abichaker; Nolan Jangaard; Pablo Bringas; Michael Melnick
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Review 10.  Morphogenetic fields within the human dentition: a new, clinically relevant synthesis of an old concept.

Authors:  Grant Townsend; Edward F Harris; Herve Lesot; Francois Clauss; Alan Brook
Journal:  Arch Oral Biol       Date:  2008-08-29       Impact factor: 2.633

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