Mechanical loading stimulates dentin matrix protein 1 (DMP1) expression in osteocytes in vivo

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Gluhak-Heinrich, Jelica¹; Ye, Ling²; Bonewald, Lynda F.²; Feng, Jian Q.²; MacDougall, Mary³; Harris, Stephen E.²; Pavlin, Dubravko¹

Mechanical loading stimulates dentin matrix protein 1 (DMP1) expression in osteocytes in vivo

J Bone Miner Res. May 2003;18(5):807-817

©203 American Society for Bone and Mineral Research

Affiliations

¹Department of Orthodontics, The University of Texas Health Science Center at San Antonio, San Antonio, Texas, USA

²Department of Oral Biology, The University of Missouri at Kansas City, School of Dentistry, Kansas City, Missouri, USA

³Department of Pediatric Dentistry, The University of Texas Health Science Center at San Antonio, San Antonio, Texas, USA
Abstract and keywords

Dentin matrix protein 1 (DMP1) was originally postulated to be dentin specific. Further analysis showed that DMP1 is also expressed in mature cartilage and bone. In bone tissue, DMP1 is expressed predominantly in late osteoblasts and osteocytes. DMP1 belongs to the SIBLING (Small Integrin Binding Ligand N-linked Glycoprotein) family of cellular matrix proteins that also includes osteopontin, bone sialoprotein, dentin sialophosphoprotein, and others. In this study, we examined the effect of mechanical loading on expression of DMP1 mRNA and DMP1 protein in alveolar bone in the mouse tooth movement model by in situ hybridization and immunocytochemistry. The expression of DMP1 mRNA was determined quantitatively in mechanically loaded and control sites of dento-alveolar tissue at several time points from 6 h to 7 days after loading. The tooth movement model allows simultaneous evaluation of bone resorption and bone formation sites. Expression of DMP1 mRNA in osteocytes increased 2-fold as early as 6 h after treatment in both the bone formation and bone resorption sites. After 4 days, DMP1 expression in osteocytes increased to a maximum of 3.7-fold in the bone formation sites and 3.5-fold in the resorption sites. Osteoblasts responded in the opposite manner and showed a transient 45% decrease of DMP1 mRNA in bone formation sites and a constant decrease of DMP1 mRNA during the entire course of treatment in the bone resorption sites, with a peak inhibition of 67% at day 2. By immunocytochemistry using a C-terminal region peptide antibody to DMP1, we found that there was a transient decrease in immunoreactivity at 3 days after treatment on both the formation side and the resorption side compared with the matched contralateral control tissue. However by 7 days of loading, there was a dramatic increase in DMP1 protein immunoreactivity on both the formation side and the resorption side. These results represent changes in epitope availability using this antibody or true changes in protein levels. The observations imply that the DMP1 protein is undergoing dynamic changes in either synthesis or other protein/matrix interaction after mechanical loading of alveolar bone. The findings indicate that DMP1 is involved in the responses of osteocytes and osteoblasts to mechanical loading of bone. These results support the hypothesis that osteocytes alter their matrix microenvironment in response to mechanical loading.

Keywords: dentin matrix protein 1; mechanical load; osteocytes; osteoblasts; tooth movement
Links

DOI: 10.1359/jbmr.2003.18.5.807

PubMed: 12733719

WoS: 000182328000002

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