Journal
JOURNAL OF BONE AND MINERAL RESEARCH
Volume 28, Issue 4, Pages 960-969Publisher
WILEY
DOI: 10.1002/jbmr.1824
Keywords
AGING; NF-B; OSTEOBLAST; OSTEOCLAST; SirT1
Categories
Funding
- American Federation for Aging Research
- Vanderbilt Department of Medicine
- Vanderbilt Orthopaedic Institute Pilot Award
Ask authors/readers for more resources
Silent information regulator T1 (SirT1) is linked to longevity and negatively controls NF-B signaling, a crucial mediator of survival and regulator of both osteoclasts and osteoblasts. Here we show that NF-B repression by SirT1 in both osteoclasts and osteoblasts is necessary for proper bone remodeling and may contribute to the mechanisms linking aging and bone loss. Osteoclast- or osteoblast-specific SirT1 deletion using the Sirtflox/flox mice crossed to lysozyme M-cre and the 2.3kb col1a1-cre transgenic mice, respectively, resulted in decreased bone mass caused by increased resorption and reduced bone formation. In osteoclasts, lack of SirT1 promoted osteoclastogenesis in vitro and activated NF-B by increasing acetylation of Lysine 310. Importantly, this increase in osteoclastogenesis was blocked by pharmacological inhibition of NF-B. In osteoblasts, decreased SirT1 reduced osteoblast differentiation, which could also be rescued by inhibition of NF-B. In further support of the critical role of NF-B signaling in bone remodeling, elevated NF-B activity in IB+/ mice uncoupled bone resorption and formation, leading to reduced bone mass. These findings support the notion that SirT1 is a genetic determinant of bone mass, acting in a cell-autonomous manner in both osteoblasts and osteoclasts, through control of NF-B and bone cell differentiation. (c) 2013 American Society for Bone and Mineral Research.
Authors
I am an author on this paper
Click your name to claim this paper and add it to your profile.
Reviews
Recommended
No Data Available