First Author | Kram V | Year | 2017 |
Journal | Sci Rep | Volume | 7 |
Issue | 1 | Pages | 12627 |
PubMed ID | 28974711 | Mgi Jnum | J:255469 |
Mgi Id | MGI:6109212 | Doi | 10.1038/s41598-017-12651-6 |
Citation | Kram V, et al. (2017) Small leucine rich proteoglycans, a novel link to osteoclastogenesis. Sci Rep 7(1):12627 |
abstractText | Biglycan (Bgn) and Fibromodulin (Fmod) are subtypes of the small leucine-rich family of proteoglycans (SLRP). In this study we examined the skeletal phenotype of BgnFmod double knockout (BgnFmod KO) mice and found they were smaller in size and have markedly reduced bone mass compared to WT. The low bone mass (LBM) phenotype is the result of both the osteoblasts and osteoclasts from BgnFmod KO mice having higher differentiation potential and being more active compared to WT mice. Using multiple approaches, we showed that both Bgn and Fmod directly bind TNFalpha as well as RANKL in a dose dependent manner and that despite expressing higher levels of both TNFalpha and RANKL, BgnFmod KO derived osteoblasts cannot retain these cytokines in the vicinity of the cells, which leads to elevated TNFalpha and RANKL signaling and enhanced osteoclastogenesis. Furthermore, adding either Bgn or Fmod to osteoclast precursor cultures significantly attenuated the cells ability to form TRAP positive, multinucleated giant cells. In summary, our data indicates that Bgn and Fmod expressed by the bone forming cells, are novel coupling ECM components that control bone mass through sequestration of TNFalpha and/or RANKL, thereby adjusting their bioavailability in order to regulate osteoclastogenesis. |