New therapies that protect or restore bone quality have great potential to significantly improve skeletal health. Development of these therapies requires the identification of the cellular and molecular mechanisms that regulate bone quality. Therefore, the long-term goal of this research is to identify mechanisms by which biological and physical cues control bone extracellular matrix (ECM) material properties. To that end, this renewal application builds on our discovery that TGF regulates the material properties of bone ECM and remains one of just a handful of factors yet shown to do so. Recent work, supported by the first funding cycle, establishes osteocytes and MMP13 as key participants in the control of bone quality through a dynamic process called perilacunar remodeling (PLR). In PLR, osteocytes secrete proteases such as MMP13 to resorb the perilacunar bone matrix. PLR is essential for the maintenance of bone quality, systemic mineral homeostasis, and the canalicular channels that facilitate osteocyte nourishment, communication, and mechanosensation. Our recent data suggests that disruption of PLR in human bone may contribute to the bone fragility in diseases such as osteonecrosis of the femoral head or osteoradionecrosis of the jaw. However, major gaps surround the understanding of the role or regulation of PLR in healthy bone or in skeletal disease. Preliminary data raise the possibility that PLR is regulated by mechanical load and by TGF, a mechanism that has the potential to couple the maintenance of bone quality by PLR to changing physical and biological demands on the skeleton. This proposal tests the hypothesis that osteocytes regulate bone ECM material properties through perilacunar remodeling in a load- and TGF-dependent manner to control bone quality and cellular tension. Specifically, this project aims to: 1) determine the extent to which perilacunar remodeling is mechanosensitive and TGF-regulated, 2) identify mechanisms by which mechanical load regulates the effects of TGF on bone, and 3) determine the functional impact of PLR on bone ECM quality and osteocyte tension. PLR activity and regulation will be evaluated using a combination of histologic, radiologic, bioengineering, and molecular approaches. These studies will assess the effects on PLR of osteocyte-specific MMP13-deficiency, applied mechanical loads, and pharmacologic inhibition of the TGF type I receptor. In vivo and in vitro gain and loss of function studies will be used to determine the extent to which these factors operate in an epistatic pathway. In addition, this project examines the effect of dynamically regulated perilacunar bone ECM material properties on osteocyte cellular tension, signaling, and function. This project is significant because it will elucidate the regulation of osteocyte mediated PLR and bone quality by TGF and physical cues, revealing new mechanisms that can be therapeutically targeted to prevent bone fragility and maintain skeletal health.

Public Health Relevance

Bone resistance to fracture is a product of bone mass and bone quality. Though vigorous study of mechanisms regulating bone mass yielded new osteoporosis therapies, very little is known about the mechanisms regulating bone quality. Since deficits in bone quality contribute significantly to bone fragility, including that of aging, diabeic, and steroid-treated bone, this project aims to identify cellular and molecular mechanisms that maintain bone quality; in expectation that these insights will lead to the development of new therapies to prevent or treat bone fragility.

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE019284-08
Application #
9119517
Study Section
Skeletal Biology Development and Disease Study Section (SBDD)
Program Officer
Wan, Jason
Project Start
2008-07-01
Project End
2019-07-31
Budget Start
2016-08-01
Budget End
2017-07-31
Support Year
8
Fiscal Year
2016
Total Cost
Indirect Cost
Name
University of California San Francisco
Department
Orthopedics
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94118
Tamplen, Matthew; Fowler, Tristan; Markey, Jeffery et al. (2018) Treatment with anti-Sclerostin antibody to stimulate mandibular bone formation. Head Neck 40:1453-1460
Alliston, Tamara; Hernandez, Christopher J; Findlay, David M et al. (2018) Bone marrow lesions in osteoarthritis: What lies beneath. J Orthop Res 36:1818-1825
Acevedo, Claire; Sylvia, Meghan; Schaible, Eric et al. (2018) Contributions of Material Properties and Structure to Increased Bone Fragility for a Given Bone Mass in the UCD-T2DM Rat Model of Type 2 Diabetes. J Bone Miner Res 33:1066-1075
Alemi, A Sean; Mazur, Courtney M; Fowler, Tristan W et al. (2018) Glucocorticoids cause mandibular bone fragility and suppress osteocyte perilacunar-canalicular remodeling. Bone Rep 9:145-153
Ford, Audrey C; Chui, Wan Fung; Zeng, Anne Y et al. (2018) A modular approach to creating large engineered cartilage surfaces. J Biomech 67:177-183
Tang, Xinyan; Alliston, Tamara; Coughlin, Dezba et al. (2018) Dynamic imaging demonstrates that pulsed electromagnetic fields (PEMF) suppress IL-6 transcription in bovine nucleus pulposus cells. J Orthop Res 36:778-787
Dole, Neha S; Mazur, Courtney M; Acevedo, Claire et al. (2017) Osteocyte-Intrinsic TGF-? Signaling Regulates Bone Quality through Perilacunar/Canalicular Remodeling. Cell Rep 21:2585-2596
Ouyang, Ann; Cerchiari, Alec E; Tang, Xinyan et al. (2017) Effects of cell type and configuration on anabolic and catabolic activity in 3D co-culture of mesenchymal stem cells and nucleus pulposus cells. J Orthop Res 35:61-73
Whitaker, Amanda T; Berthet, Ellora; Cantu, Andrea et al. (2017) Smad4 regulates growth plate matrix production and chondrocyte polarity. Biol Open 6:358-364
Fowler, Tristan W; Acevedo, Claire; Mazur, Courtney M et al. (2017) Glucocorticoid suppression of osteocyte perilacunar remodeling is associated with subchondral bone degeneration in osteonecrosis. Sci Rep 7:44618

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