Abstract

Sarcopenia is the progressive loss of skeletal muscle mass and force/power that develops with aging. Accumulating data shows that it is principally the weakness that accompanies sarcopenia, not the loss of muscle size per se, that contributes to disability. We were the first group to propose that bone cells, specifically osteocytes, signal to muscle and play an important role in this process. We discovered that soluble factors from osteocytes from young mice (5 mo) accelerate myogenesis of both C2C12 cells and primary myoblasts, whereas no effect was observed with factors from osteocytes of aged mice (22 mo). We identified two known osteocyte factors, PGE2 and Wnt3a (i.e., osteokines), as potential mediators of osteocyte to muscle signaling, as they closely mimicked the effects of young osteocyte soluble factors on myogenesis. Both Wnt3a and PGE2 significantly upregulated genes that orchestrate growth, hypertrophy, mitochondrial biogenesis, and Ca2+- release/uptake in muscle. Wnt3a was associated with the translocation of ?-catenin to nuclei and was linked to two downstream genes of the Wnt/?-catenin pathway, Fhl1 and Numb that have direct roles in myogenesis. Our cell based results were further supported by our ex vivo, in vivo and clinical studies. The conditional deletion of one allele of ?-catenin in osteocytes led to a decrease in both muscle mass and function of skeletal muscles during aging, while conversely, skeletal muscle function was enhanced in the Lrp5G171V mouse, a model of increased skeletal Wnt/?-catenin signaling. Clinically, we have found that serum from healthy 60 yr old women, has high concentrations of WNT3a and increases myogenic differentiation of human primary myoblasts, while serum from osteoporotic women, which has 1/10 of the WNT3a serum levels of healthy women, decreases myogenesis. Ex vivo, PGE2 is able to mirror the effects of young osteocyte osteokines by enhancing force generation in young muscles, but not in aged muscles and the effects were linked to the expression of the EP4 receptor in muscles. Lipidomics profiling revealed that with age, levels of key lipid-signaling mediators of the arachidonic acid pathway decrease, however exercise rescues the levels of these lipids. These data suggest that with aging, bone to muscle signaling is defective or muscle response to PGE2 is impaired, potentially through EP4-PGE2 signaling in aged skeletal muscles. These studies support our hypothesis that bone to muscle signaling is altered with aging due to compromised Wnt/?-catenin and PGE2 signaling, contributing to sarcopenia-related muscle weakness. To test this hypothesis, we will conduct the following studies.
Aim 1 : Determine the role of Wnt/?-catenin signaling in bone-muscle crosstalk during aging/exercise.
Aim 2 : Determine the role of PGE2 signaling in bone-muscle crosstalk during aging/exercise. These studies will provide new mechanisms for regulation of muscle function by bone-signaling osteokines as well as provide a platform for new secreted factors involved in bone-muscle crosstalk during aging/exercise. These studies will generate important information for prevention and/or treatment of `osteosarcopenia'.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG039355-07
Application #
9789127
Study Section
Special Emphasis Panel (ZAG1)
Project Start
Project End
Budget Start
2019-06-01
Budget End
2020-05-31
Support Year
7
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Indiana University-Purdue University at Indianapolis
Department
Type
DUNS #
603007902
City
Indianapolis
State
IN
Country
United States
Zip Code
46202

  Publications

Bonewald, Lynda (2018) Use it or lose it to age: A review of bone and muscle communication. Bone 120:212-218
Kitase, Yukiko; Vallejo, Julian A; Gutheil, William et al. (2018) ?-aminoisobutyric Acid, l-BAIBA, Is a Muscle-Derived Osteocyte Survival Factor. Cell Rep 22:1531-1544
Pin, Fabrizio; Barreto, Rafael; Kitase, Yukiko et al. (2018) Growth of ovarian cancer xenografts causes loss of muscle and bone mass: a new model for the study of cancer cachexia. J Cachexia Sarcopenia Muscle 9:685-700
Morris, Josephine L; Cross, Stephen J; Lu, Yinhui et al. (2018) Live imaging of collagen deposition during skin development and repair in a collagen I - GFP fusion transgenic zebrafish line. Dev Biol 441:4-11
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
Tiede-Lewis, LeAnn M; Xie, Yixia; Hulbert, Molly A et al. (2017) Degeneration of the osteocyte network in the C57BL/6 mouse model of aging. Aging (Albany NY) 9:2190-2208
Wang, Zhiying; Bian, Liangqiao; Mo, Chenglin et al. (2017) Targeted quantification of lipid mediators in skeletal muscles using restricted access media-based trap-and-elute liquid chromatography-mass spectrometry. Anal Chim Acta 984:151-161
Jähn, Katharina; Kelkar, Shilpa; Zhao, Hong et al. (2017) Osteocytes Acidify Their Microenvironment in Response to PTHrP In Vitro and in Lactating Mice In Vivo. J Bone Miner Res 32:1761-1772
Huang, Jian; Romero-Suarez, Sandra; Lara, Nuria et al. (2017) Crosstalk between MLO-Y4 osteocytes and C2C12 muscle cells is mediated by the Wnt/?-catenin pathway. JBMR Plus 1:86-100
Bonewald, Lynda F (2017) The Role of the Osteocyte in Bone and Nonbone Disease. Endocrinol Metab Clin North Am 46:1-18

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