Authors
Tripti Gaur, Christopher J Lengner, Hayk Hovhannisyan, Ramesh A Bhat, Peter VN Bodine, Barry S Komm, Amjad Javed, Andre J Van Wijnen, Janet L Stein, Gary S Stein, Jane B Lian
Publication date
2005/9/30
Journal
Journal of Biological Chemistry
Volume
280
Issue
39
Pages
33132-33140
Publisher
American Society for Biochemistry and Molecular Biology
Description
Both activating and null mutations of proteins required for canonical WNT signaling have revealed the importance of this pathway for normal skeletal development. However, tissue-specific transcriptional mechanisms through which WNT signaling promotes the differentiation of bone-forming cells have yet to be identified. Here, we address the hypothesis that canonical WNT signaling and the bone-related transcription factor RUNX2/CBFA1/AML3 are functionally linked components of a pathway required for the onset of osteoblast differentiation. Our findings show that, in bone of the SFRP1 (secreted frizzled-related protein-1)-null mouse, which exhibits activated WNT signaling and a high bone mass phenotype, there is a significant increase in expression of T-cell factor (TCF)-1, Runx2, and the RUNX2 target gene osteocalcin. We demonstrate by mutational analysis that a functional TCF regulatory element …
Total citations
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Scholar articles
T Gaur, CJ Lengner, H Hovhannisyan, RA Bhat… - Journal of Biological Chemistry, 2005