Literature DB >> 9074935

Timing of the expression of enamel gene products during mouse tooth development.

M Zeichner-David1, H Vo, H Tan, T Diekwisch, B Berman, F Thiemann, M D Alcocer, P Hsu, T Wang, J Eyna, J Caton, H C Slavkin, M MacDougall.   

Abstract

In order to understand the mechanisms involved in tooth development it is important to define the timing for tissue-specific gene expression. A consequence of ameloblast cell differentiation is the sequential expression of tissue-specific genes whose products form the enamel extracellular matrix. The ameloblast phenotype has been characterized as consisting of two major classes of proteins: amelogenins and non-amelogenin proteins such as anionic enamel proteins (enamelins, tuft proteins, tuftelin, sulfated proteins) and enamel proteases. The postulated functions for the anionic enamel proteins are as nucleators for hydroxyapatite crystal formation while amelogenins control the crystal size, growth and orientation. While the amelogenins have been well characterized, detailed knowledge for anionic enamel proteins has been sparse. In the present study, we designed experiments to characterize one of the anionic enamel proteins from mouse molars, tuftelin, and to determine the timing of expression of this protein during molar tooth development. Our results showed the initial detection of tuftelin transcripts within proliferating inner enamel epithelial cells at very early stages of tooth development (13 days of embryonic development equivalent to the bud stage of tooth development). These data provide direct evidence that invalidates previous dogmas that enamel proteins were synthesized by polarized, non-dividing, fully differentiated ameloblast cells. In addition, tuftelin was found to be synthesized also by dental papilla mesenchyme cells suggesting that this protein is not enamel-specific. These data taken together open the possibility that the tuftelin present in the dentino-enamel junction could be secreted by both, preodontoblast cells and preameloblast cells. It might also suggest a possible different role for tuftelin than nucleator of hydroxyapatite crystals.

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Year:  1997        PMID: 9074935

Source DB:  PubMed          Journal:  Int J Dev Biol        ISSN: 0214-6282            Impact factor:   2.203


  12 in total

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2.  Sequential distribution of keratan sulphate and chondroitin sulphate epitopes during ameloblast differentiation.

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3.  Transcription factor Sp3 is essential for post-natal survival and late tooth development.

Authors:  P Bouwman; H Göllner; H P Elsässer; G Eckhoff; A Karis; F Grosveld; S Philipsen; G Suske
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4.  Enamel-free teeth: Tbx1 deletion affects amelogenesis in rodent incisors.

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Journal:  Dev Biol       Date:  2009-02-20       Impact factor: 3.582

Review 5.  Current knowledge of tooth development: patterning and mineralization of the murine dentition.

Authors:  Javier Catón; Abigail S Tucker
Journal:  J Anat       Date:  2009-04       Impact factor: 2.610

6.  Ctip2/Bcl11b controls ameloblast formation during mammalian odontogenesis.

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Journal:  Proc Natl Acad Sci U S A       Date:  2009-02-26       Impact factor: 11.205

7.  De Novo Genome and Transcriptome Assembly of the Canadian Beaver (Castor canadensis).

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Journal:  G3 (Bethesda)       Date:  2017-02-09       Impact factor: 3.154

8.  Role of MIZ-1 in AMELX gene expression.

Authors:  Hee-Jin Noh; Dong-In Koh; Kon-O Lee; Bu-Nam Jeon; Min-Kyeong Kim; Malcom L Snead; Man-Wook Hur
Journal:  Biochem Biophys Rep       Date:  2016-10-15

Review 9.  Bcl11b/Ctip2 in Skin, Tooth, and Craniofacial System.

Authors:  Marie-Thérèse Daher; Pedro Bausero; Onnik Agbulut; Zhenlin Li; Ara Parlakian
Journal:  Front Cell Dev Biol       Date:  2020-12-10

10.  Stage-Specific Role of Amelx Activation in Stepwise Ameloblast Induction from Mouse Induced Pluripotent Stem Cells.

Authors:  Xinchao Miao; Kunimichi Niibe; Maolin Zhang; Zeni Liu; Praphawi Nattasit; Yumi Ohori-Morita; Takashi Nakamura; Xinquan Jiang; Hiroshi Egusa
Journal:  Int J Mol Sci       Date:  2021-07-03       Impact factor: 5.923

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