Abstract

The functional syncytium comprising osteocytes, osteoblastic cells, marrow stromal cells, and endothelial cells of the blood vessels is thought to be the mechanosensory apparatus by which bone, as an organ, detects the need for mechanical adaptation and microdamage repair and initiates the appropriate adaptive responses. Consistent with this, studies leading to this project have revealed that the increased bone fragility that results from glucocorticoid excess in mice and humans is associated with increased bone fragility that results from glucocorticoid excess in mice and humans is associated with increased osteocyte apoptosis. Conversely, bisphosphonates and intermittent PTH, two treatments that are effective in steroid-induced osteoporosis (as well as estrogens, androgens, and calcitonin) prevent osteocyte and osteoblast apoptosis in vitro and in vivo. In addition, it has been demonstrated in vitro than the anti-apoptotic effect of bisphosphonates and estrogens results from rapid activation of the extracellular signal-regulated kinases (ERKs) and that mechanical signals also cause ERK activation in osteocytic cells. Collectively, these lines of evidence give credence to the hypotheses that disruption of the osteocyte network by apoptosis, resulting from hormonal or strain changes, may contribute to microdamage accumulation and increased bone fragility; whereas prevention of osteocyte viability may increase bone strength. Hormonal, pharmacological, and mechanical signals converge on common signal transduction pathways that influence the viability of osteocytes and the integrity of the lacuno-canalicular network, to orchestrate the appropriate addition or removal of bone and participate in the detection and repair of fatigue microdamage. To advance this hypothesis, the effects of pro- and anti-apoptotic agents (glucocorticoids and bisphosphonates) as well as mechanical signals on focal adhesion molecules (FAK and Pyk2), MAP kinases, intracellular calcium, and connexin channels and hemichannels will be determined in vitro. Further, the contribution of osteocyte apoptosis to mechanical strength will be studied using a murine model of glucocorticoid excess treated with bisphosphonates. These studiers should chart the signaling pathways controlling osteocyte viability and advanced our understanding of the contribution of altered prevalence of osteocyte apoptosis to bone strength.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG013918-07
Application #
6596382
Study Section
Special Emphasis Panel (ZAG1)
Project Start
2002-06-15
Project End
2003-05-31
Budget Start
Budget End
Support Year
7
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Arkansas for Medical Sciences
Department
Type
DUNS #
City
Little Rock
State
AR
Country
United States
Zip Code
72205

  Publications

Farr, Joshua N; Almeida, Maria (2018) The Spectrum of Fundamental Basic Science Discoveries Contributing to Organismal Aging. J Bone Miner Res 33:1568-1584
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
Kim, Ha-Neui; Chang, Jianhui; Shao, Lijian et al. (2017) DNA damage and senescence in osteoprogenitors expressing Osx1 may cause their decrease with age. Aging Cell 16:693-703
Ucer, Serra; Iyer, Srividhya; Kim, Ha-Neui et al. (2017) The Effects of Aging and Sex Steroid Deficiency on the Murine Skeleton Are Independent and Mechanistically Distinct. J Bone Miner Res 32:560-574
Iyer, Srividhya; Han, Li; Ambrogini, Elena et al. (2017) Deletion of FoxO1, 3, and 4 in Osteoblast Progenitors Attenuates the Loss of Cancellous Bone Mass in a Mouse Model of Type 1 Diabetes. J Bone Miner Res 32:60-69
Almeida, Maria; Laurent, Michaƫl R; Dubois, Vanessa et al. (2017) Estrogens and Androgens in Skeletal Physiology and Pathophysiology. Physiol Rev 97:135-187
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:
Ye, Shiqiao; Fujiwara, Toshifumi; Zhou, Jian et al. (2016) LIS1 Regulates Osteoclastogenesis through Modulation of M-SCF and RANKL Signaling Pathways and CDC42. Int J Biol Sci 12:1488-1499
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

Showing the most recent 10 out of 162 publications