Abstract

Glucocorticoid administration is frequently used to suppress inflammation and treat a variety of conditions in the VA patient population. One of the most significant side effects of this therapy is bone loss and increased risk of fracture. We have developed a murine model of glucocorticoid-induced bone loss that mimics many of the structural and histological changes observed in humans. In addition, we have used mice with genetic deletion of the glucocorticoid receptor in specific cell types to identify the targets of glucocorticoid action on the skeleton. We found that deletion of the glucocorticoid receptor from osteoblast lineage cells prevents the stimulation of bone resorption and the suppression of bone formation caused by glucocorticoid administration. However, the molecular mechanisms by which glucocorticoids stimulate bone resorption and suppress bone formation by acting on this cell type remain unclear. Based on preliminary studies, we propose the central hypothesis that glucocorticoids stimulate bone resorption by suppressing expression of osteoprotegerin (OPG) and that they suppress bone formation by antagonizing canonical Wnt signaling. To address this hypothesis we will identify the molecular mechanisms by which glucocorticoids suppress expression of the OPG gene using a combination of large transcriptional reporter constructs and deletion of regulatory sequences from the endogenous OPG gene in cells and mice (Aim 1). We will also determine whether glucocorticoids suppress bone formation by stimulating the apoptosis of osteoblast lineage cells by blocking induction of apoptosis in this cell type. This will be accomplished by deletion of genes essential for apoptosis (Bak, Bax, and Caspase 8) in this cell lineage (Aim 2). Lastly, we will determine whether glucocorticoids suppress bone formation by opposing Wnt signaling by creating mice with constitutive activation of ?-catenin in osteoblasts and treating them with exogenous glucocorticoids. If our hypothesis is correct, this maneuver will prevent suppression of bone formation by glucocorticoids (Aim 3). Overall, the proposed studies will clarify the molecular changes by which glucocorticoid excess causes bone loss and may identify novel approaches to prevent this bone loss in patients that require chronic glucocorticoid therapy.

Public Health Relevance

Glucocorticoids are often used to treat inflammatory conditions, such as arthritis, as well as to prevent transplant rejection. One of the most significant side effects of glucocorticoid treatment is the loss of bone and the associated increase in fracture risk. Glucocorticoid treatment is common in the VA patient population and is therefore a significant problem for veterans. The goal of the proposed studies it to better understand how glucocorticoids cause bone loss and increase fracture risk. A better understanding of how glucocorticoids cause bone loss may lead to better or more effective interventions to prevent this bone loss.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01BX000294-10
Application #
9829488
Study Section
Special Emphasis Panel (ZRD1)
Project Start
2009-04-01
Project End
2022-12-31
Budget Start
2020-01-01
Budget End
2020-12-31
Support Year
10
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Central Arkansas Veterans Hlthcare Sys
Department
Type
DUNS #
082573742
City
North Little Rock
State
AR
Country
United States
Zip Code
72114

  Publications

O'Brien, Charles A; Morello, Roy (2018) Modeling Rare Bone Diseases in Animals. Curr Osteoporos Rep 16:458-465
Xiong, Jinhu; Almeida, Maria; O'Brien, Charles A (2018) The YAP/TAZ transcriptional co-activators have opposing effects at different stages of osteoblast differentiation. Bone 112:1-9
Weinstein, Robert S; Hogan, Erin A; Borrelli, Michael J et al. (2017) The Pathophysiological Sequence of Glucocorticoid-Induced Osteonecrosis of the Femoral Head in Male Mice. Endocrinology 158:3817-3831
Piemontese, Marilina; Almeida, Maria; Robling, Alexander G et al. (2017) Old age causes de novo intracortical bone remodeling and porosity in mice. JCI Insight 2:
Piemontese, Marilina; Xiong, Jinhu; Fujiwara, Yuko et al. (2016) Cortical bone loss caused by glucocorticoid excess requires RANKL production by osteocytes and is associated with reduced OPG expression in mice. Am J Physiol Endocrinol Metab 311:E587-93
Fujiwara, Yuko; Piemontese, Marilina; Liu, Yu et al. (2016) RANKL (Receptor Activator of NF?B Ligand) Produced by Osteocytes Is Required for the Increase in B Cells and Bone Loss Caused by Estrogen Deficiency in Mice. J Biol Chem 291:24838-24850
Piemontese, Marilina; Onal, Melda; Xiong, Jinhu et al. (2016) Low bone mass and changes in the osteocyte network in mice lacking autophagy in the osteoblast lineage. Sci Rep 6:24262
Xiong, Jinhu; Piemontese, Marilina; Onal, Melda et al. (2015) Osteocytes, not Osteoblasts or Lining Cells, are the Main Source of the RANKL Required for Osteoclast Formation in Remodeling Bone. PLoS One 10:e0138189
Piemontese, Marilina; Onal, Melda; Xiong, Jinhu et al. (2015) Suppression of autophagy in osteocytes does not modify the adverse effects of glucocorticoids on cortical bone. Bone 75:18-26
Xiong, Jinhu; Piemontese, Marilina; Thostenson, Jeff D et al. (2014) Osteocyte-derived RANKL is a critical mediator of the increased bone resorption caused by dietary calcium deficiency. Bone 66:146-54

Showing the most recent 10 out of 22 publications