Abstract

Turnover of cells and matrix occurs in all organs and tissues and is essential to maintain health and mechanical integrity. In bone, cell and matrix turnover occur through bone remodeling. Dysregulation of bone remodeling is the fundamental driver underlying all forms of Osteoporosis. Osteoporosis results from the accelerated birth of new remodeling units and/or alterations in osteoclast or osteoblast kinetics within remodeling units, leading to excessive resorption, too little formation or both. Regulation of the bone remodeling effector cells, osteoclasts and osteoblasts, is well understood. However, our understanding of the critical Activation step or the On-Switch to start bone remodeling is very limited. Recently, we discovered that osteocyte apoptosis activates bone resorption at bone microdamage sites. Furthermore, we found that estrogen loss and disuse cause osteocyte apoptosis that activates bone resorption as well. Finally, we discovered that in bone microdamage-induced remodeling, RANKL production is triggered in viable osteocytes (i.e., the Bystanders) immediately neighboring apoptotic osteocytes. Apoptotic osteocytes themselves do not produce osteoclastogenic cytokines. However, it is the dying osteocytes, not bone microdamage, which triggers this Bystander signaling in viable osteocytes - RANKL production is not turned-on when osteocyte apoptosis is inhibited. How apoptotic osteocytes trigger RANKL production in viable neighbor osteocytes is not known. Our preliminary studies suggest that gap junctions and Pannexin 1 channels play critical roles in this process. Experiments: In the current studies, we will use a combination of immunohistochemical approaches (osteocyte apoptosis vs. RANKL and OPG expressing osteocytes) and bone histomorphometric approaches to assess osteocyte apoptosis and production of osteoclastogenic cytokines by viable osteocyte. 1) In Aim 1, we will use mouse models of estrogen loss and disuse (OVX, HLS) to test whether RANKL production from viable Bystander osteocytes is the generalized mechanism for bone remodeling activation in response to a range of physiological stimuli. 2) In Aim 2, we will determine the role of gap junctions (GJ) vs Cx43 hemichannels in regulating the spread of osteocyte apoptosis and extent of osteoclastogenic signaling at bone microdamage sites. We will use a mouse ulnar fatigue to produce microcracks in bone in vivo. Pharmacological and peptide inhibition of GJ and Cx43 channels will be used to establish their regulation of the extent of osteocyte apoptosis and RANKL expression. 3) Finally, recent studies show apoptotic cells acutely release find me signals that stimulate recruitment of phagocytes that remove dying cells. Primary among these acute signals are nucleotides released through apoptosis-induced opening of Pannexin 1 channels.
In Aim 3, we will determine the role of Pannexin 1 and associated nucleotide signaling in coupling osteocyte apoptosis at bone microdamage sites to activation of Bystander osteocyte signaling using Panx1 knockout mice.

Public Health Relevance

Osteoporosis results from the accelerated birth of new remodeling sites and/or to alterations to the activities of the cells, osteoclasts or osteoblasts, within those remodeling sites, leading to excessive resorption, too little formation or both. Understanding of the critical Activation step or the 'On-Switch' to start bone remodeling is very limited. Our studies have revealed that osteocyte apoptosis, i.e., regulated death of osteocytes, controls activation of bone remodeling in response to skeletal unloading, fatigue (wear & tear) bone microdamage and estrogen loss. In the case of fatigue microdamage in bone, the controlled death of groups of osteocytes triggers their viable neighbor osteocytes to produce RANKL biochemical signals to recruit osteoclasts that resorb bone at the start of remodeling. In the current studies we will test whether this osteocyte apoptosis triggering of signaling from non-dying neighbor cells is actually a universal mechanism for a range of challenges that turn on bone remodeling and can lead to bone loss. In a related series of studies, we will examine how dying osteocytes signal their surviving neighbors to 'call for help.' We will explore parallels wit the cell death and the 'help' signaling responses evoked from surviving cells in stroke and heart attack, with particular focus on the role of gap junctions channels and pannexin channels. Understanding these biological mechanisms may open a new window for novel therapeutic targets that to modulate bone remodeling and prevent osteoporosis and bone fragility.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR041210-22
Application #
9015406
Study Section
Skeletal Biology Structure and Regeneration Study Section (SBSR)
Program Officer
Lester, Gayle E
Project Start
1992-09-15
Project End
2020-02-29
Budget Start
2016-03-01
Budget End
2017-02-28
Support Year
22
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
City College of New York
Department
Engineering (All Types)
Type
Biomed Engr/Col Engr/Engr Sta
DUNS #
603503991
City
New York
State
NY
Country
United States
Zip Code
10031

  Publications

Cabahug-Zuckerman, Pamela; Stout Jr, Randy F; Majeska, Robert J et al. (2018) Potential role for a specialized ?3 integrin-based structure on osteocyte processes in bone mechanosensation. J Orthop Res 36:642-652
Liu, Zhongbo; Han, Tianzhen; Werner, Haim et al. (2018) Reduced Serum IGF-1 Associated With Hepatic Osteodystrophy Is a Main Determinant of Low Cortical but Not Trabecular Bone Mass. J Bone Miner Res 33:123-136
Kennedy, Oran D; Lendhey, Matin; Mauer, Peter et al. (2017) Microdamage induced by in vivo Reference Point Indentation in mice is repaired by osteocyte-apoptosis mediated remodeling. Bone 95:192-198
Kaya, Serra; Basta-Pljakic, Jelena; Seref-Ferlengez, Zeynep et al. (2017) Lactation-Induced Changes in the Volume of Osteocyte Lacunar-Canalicular Space Alter Mechanical Properties in Cortical Bone Tissue. J Bone Miner Res 32:688-697
Liu, Zhongbo; Han, Tianzhen; Fishman, Shannon et al. (2017) Ablation of Hepatic Production of the Acid-Labile Subunit in Bovine-GH Transgenic Mice: Effects on Organ and Skeletal Growth. Endocrinology 158:2556-2571
McCutcheon, Sean; Majeska, Robert; Schaffler, Mitchell et al. (2017) A multiscale fluidic device for the study of dendrite-mediated cell to cell communication. Biomed Microdevices 19:71
Lewis, Karl J; Frikha-Benayed, Dorra; Louie, Joyce et al. (2017) Osteocyte calcium signals encode strain magnitude and loading frequency in vivo. Proc Natl Acad Sci U S A 114:11775-11780
Cheung, Wing Yee; Fritton, J Christopher; Morgan, Stacy Ann et al. (2016) Pannexin-1 and P2X7-Receptor Are Required for Apoptotic Osteocytes in Fatigued Bone to Trigger RANKL Production in Neighboring Bystander Osteocytes. J Bone Miner Res 31:890-9
Seref-Ferlengez, Zeynep; Maung, Stephanie; Schaffler, Mitchell B et al. (2016) P2X7R-Panx1 Complex Impairs Bone Mechanosignaling under High Glucose Levels Associated with Type-1 Diabetes. PLoS One 11:e0155107
Frikha-Benayed, Dorra; Basta-Pljakic, Jelena; Majeska, Robert J et al. (2016) Regional differences in oxidative metabolism and mitochondrial activity among cortical bone osteocytes. Bone 90:15-22

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