| The Japanese Dental Science Review | |
| Vol. 44 No. 1 2008 | |
| ISSN: 1882-7616 UBIC: 99 | |
| Summary | |
| Wnt proteins (Wnts) are palmitoylated and glycosylated ligands that play a central role
in the early development of organs and tissues. The discovery that loss-of-function mutations in low density
lipoprotein receptor-related protein 5 (LRP5), a Wnt co-receptor, led to low bone mass in humans revealed the
possible role of Wnt signaling in the regulation of bone remodeling. Many findings obtained from detailed analyses
of mice having mutations of Wnt signaling molecules have confirmed that Wnt signaling has potential roles in bone
remodeling in both physiological and pathological conditions. There are two pathways of Wnt signaling: β-catenin-
dependent canonical and -independent non-canonical pathways. Wnts act on osteoblast precursor cells and promote
their differentiation into mature osteoblasts through the β-catenin- dependent canonical pathway. In addition, Wnts
suppress bone resorption by regulating the receptor activator of NF-KB ligand (RANKL)/osteoprotegerin (OPG) ratio
through the same pathway in mature osteoblasts. In contrast, recent studies have shown that the activation
of the β-catenin-independent non-canonical pathway enhances the RANKL-induced osteoclast formation in
mouse macrophage cultures. These results indicate that Wnt-mediated signals are involved in several aspects of
bone formation and bone resorption. This review will summarize the current knowledge of the roles of Wnt signaling
in bone formation and resorption. © 2008 Japanese Association for Dental Science. Published by Elsevier Ireland.
All rights reserved.
Key words: Wnt; LRP; Osteoblasts; Osteoclasts; β-catenin; Bone |
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