Abstract

Dentin matrix protein 1 (DMP1) and dentin sialophosphoprotein (DSPP) are essential for the formation of dentin. Previous in vitro studies have indicated that DMP1 might regulate the expression of DSPP during dentinogenesis. To examine whether DMP1 controls dentinogenesis through the regulation of DSPP in vivo, we cross-bred transgenic mice expressing normal DSPP driven by a 3.6-kb rat Col1a1 promoter with Dmp1 KO mice to generate mice expressing the DSPP transgene in the Dmp1 KO genetic background (referred to as "Dmp1 KO/DSPP Tg mice"). We used morphological, histological, and biochemical techniques to characterize the dentin and alveolar bone of Dmp1 KO/DSPP Tg mice compared with Dmp1 KO and wild-type mice. Our analyses showed that the expression of endogenous DSPP was remarkably reduced in the Dmp1 KO mice. Furthermore, the transgenic expression of DSPP rescued the tooth and alveolar bone defects of the Dmp1 KO mice. In addition, our in vitro analyses showed that DMP1 and its 57-kDa C-terminal fragment significantly up-regulated the Dspp promoter activities in a mesenchymal cell line. In contrast, the expression of DMP1 was not altered in the Dspp KO mice. These results provide strong evidence that DSPP is a downstream effector molecule that mediates the roles of DMP1 in dentinogenesis.

Highlights

  • Previous in vitro studies indicated that dentin matrix protein 1 (DMP1) might regulate dentin sialophosphoprotein (DSPP) expression in odontoblasts

  • Efforts have been made in recent years to define the functional relationship between DMP1 and DSPP in dentinogenesis because Dmp1 KO mice and Dspp KO mice have the same dentin mineralization defect [7, 18]

  • We found that the Dspp expression was remarkably reduced in the Dmp1 KO mice, that the transgenic expression of DSPP rescued the tooth and alveolar bone defects of the Dmp1 KO mice, that DMP1 stimulated the Dspp promoter activity in vitro, and that Dmp1 expression was not altered in the Dspp KO mice

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Summary

Background

Previous in vitro studies indicated that dentin matrix protein 1 (DMP1) might regulate dentin sialophosphoprotein (DSPP) expression in odontoblasts. Our in vitro analyses showed that DMP1 and its 57-kDa C-terminal fragment significantly up-regulated the Dspp promoter activities in a mesenchymal cell line. Our analyses showed that the transgenic expression of DSPP rescued the tooth and alveolar bone defects of the Dmp KO mice. Our in vitro analyses showed that fulllength DMP1 and its 57-kDa C-terminal fragment significantly stimulated Dspp promoter activities in a mesenchymal cell line. These findings lend support to the belief that DSPP is a downstream effector molecule regulated by DMP1 during dentinogenesis

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