Abstract

Osteoporosis afflicts 25 million women and men in the US per year and burdens the health care system with over 20 billion dollars per year. As the US population ages and lives longer, development of prevention strategies and new treatments for bone loss become even more crucial. The Principal Investigator identified a gene, Lrp5, responsible for high bone mass in a human kindred and evidence now exists that this molecule is involved in bone mass regulation through its role in the mechanotransduction pathway. In this proposal, we have developed a unifying hypothesis and model that integrates PGE2 and the Wnt/(-catenin signaling pathways and accounts for the role of Lrp5 in regulating bone cell function in response to loading. We will test the hypothesis that crosstalk between the prostaglandin and Wnt/( catenin signaling pathways in osteocytes is a key early event in the bone response to mechanical loading that sets into play an amplification mechanism to propagate the signal to load, resulting in a bone formation response. We propose that loading is first perceived by osteocytes followed by signal propagation to lining cells and osteoblasts on the bone surface. It is known that an early osteocyte response to mechanical loading is PGE2 release which functions in an autocrine/paracrine fashion to induce new bone formation. We propose this early event results in cross-talk with and activation of the Wnt/(-catenin pathway in a first step that is independent of Lrp5 receptor activation. This initial activation alters the expression of key factors that initiate the activation of Lrp5 through a paracrine/autocrine feedback mechanism, generating a secondary activation (amplification) of the Wnt/(-catenin pathway at the level of Lrp5. To test this hypothesis the following Specific Aims are proposed: 1) Determine when and which cell types (osteocytes, lining cells and osteoblasts) activate the Wnt/(-catenin signaling pathway in the adult skeleton in response to changes in mechanical load. 2) Determine the temporal relationship and crosstalk between the PGE2 and the Wnt/(-catenin signaling pathways in the bone cell response to mechanical loading. 3) Determine the mechanism by which the expression of known modulators of Lrp5 (Wnts, Dkks, Wise, Sost) are altered by mechanical loading in adult bone cells.
These specific aims will be accomplished using complementary in vitro, in vivo and transgenic approaches to dissect the molecular mechanism for PGE2 initiated activation of (-catenin signaling and the role of Lrp5 in the response of bone to mechanical loading. These studies will provide a unifying model for integrating two pathways known to be important for bone responsiveness to mechanical loading, prostaglandin and Wnt/(-catenin signaling, and will result in a conceptual framework to integrate other important signaling pathways in bone (ATP, Ca2+ fluxes, integrin, etc.) into a paradigm that ultimately explains how bone responds to mechanical loading at the cellular and molecular level. This will lead to new approaches to treating and/or preventing osteoporosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR053949-03
Application #
7672243
Study Section
Skeletal Biology Development and Disease Study Section (SBDD)
Program Officer
Sharrock, William J
Project Start
2007-09-15
Project End
2012-08-31
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
3
Fiscal Year
2009
Total Cost
$313,943
Indirect Cost

  Institution

Name
University of Missouri Kansas City
Department
Dentistry
Type
Schools of Dentistry
DUNS #
010989619
City
Kansas City
State
MO
Country
United States
Zip Code
64110

  Publications

Begonia, Mark; Dallas, Mark; Johnson, Mark L et al. (2017) Comparison of strain measurement in the mouse forearm using subject-specific finite element models, strain gaging, and digital image correlation. Biomech Model Mechanobiol 16:1243-1253
Begonia, Mark T; Dallas, Mark; Vizcarra, Bruno et al. (2015) Non-contact strain measurement in the mouse forearm loading model using digital image correlation (DIC). Bone 81:593-601
Lara-Castillo, N; Johnson, M L (2015) LRP receptor family member associated bone disease. Rev Endocr Metab Disord 16:141-8
Lara-Castillo, N; Kim-Weroha, N A; Kamel, M A et al. (2015) In vivo mechanical loading rapidly activates ?-catenin signaling in osteocytes through a prostaglandin mediated mechanism. Bone 76:58-66
Thiagarajan, Ganesh; Lu, Yunkai; Dallas, Mark et al. (2014) Experimental and finite element analysis of dynamic loading of the mouse forearm. J Orthop Res 32:1580-8
Javaheri, Behzad; Stern, Amber Rath; Lara, Nuria et al. (2014) Deletion of a single ?-catenin allele in osteocytes abolishes the bone anabolic response to loading. J Bone Miner Res 29:705-15
Lu, Yunkai; Thiagarajan, Ganesh; Nicolella, Daniel P et al. (2012) Load/strain distribution between ulna and radius in the mouse forearm compression loading model. Med Eng Phys 34:350-6
Johnson, Mark L (2012) LRP5 and bone mass regulation: Where are we now? Bonekey Rep 1:1
Jähn, K; Lara-Castillo, N; Brotto, L et al. (2012) Skeletal muscle secreted factors prevent glucocorticoid-induced osteocyte apoptosis through activation of ?-catenin. Eur Cell Mater 24:197-209; discussion 209-10
Kitase, Yukiko; Barragan, Leonardo; Qing, Hai et al. (2010) Mechanical induction of PGE2 in osteocytes blocks glucocorticoid-induced apoptosis through both the ?-catenin and PKA pathways. J Bone Miner Res 25:2657-68

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