Affiliation:
1. Department of Orthopaedic Surgery University of Arkansas for Medical Sciences Little Rock Arkansas USA
2. Center for Musculoskeletal Disease Research University of Arkansas for Medical Sciences Little Rock Arkansas USA
3. Division of Endocrinology University of Arkansas for Medical Sciences Little Rock Arkansas USA
Abstract
AbstractAs we age, our bones undergo a process of loss, often accompanied by muscle weakness and reduced physical activity. This is exacerbated by decreased responsiveness to mechanical stimulation in aged skeleton, leading to the hypothesis that decreased mechanical stimulation plays an important role in age‐related bone loss. Piezo1, a mechanosensitive ion channel, is critical for bone homeostasis and mechanotransduction. Here, we observed a decrease in Piezo1 expression with age in both murine and human cortical bone. Furthermore, loss of Piezo1 in osteoblasts and osteocytes resulted in an increase in age‐associated cortical bone loss compared to control mice. The loss of cortical bone was due to an expansion of the endosteal perimeter resulting from increased endocortical resorption. In addition, expression of Tnfrsf11b, encoding anti‐osteoclastogenic protein OPG, decreases with Piezo1 in vitro and in vivo in bone cells, suggesting that Piezo1 suppresses osteoclast formation by promoting Tnfrsf11b expression. Our results highlight the importance of Piezo1‐mediated mechanical signaling in protecting against age‐associated cortical bone loss by inhibiting bone resorption in mice.
Funder
National Institute of Arthritis and Musculoskeletal and Skin Diseases
National Institute of General Medical Sciences
Cited by
5 articles.
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