Abstract

Previously we found that the adapter protein SHN3 had a major effect to suppress bone formation by osteoblasts in vivo by inhibiting the activity of the mitogen activated protein kinase (MAPK) ERK. We also identified that WNTs have a previously unidentified activity to activate this SHN3/ERK pathway. Here we seek to make critical extensions of these observations by determining how SHN3 inhibits ERK and how this pathway influences models of skeletal disease in vivo. This area of study is significant as osteoporosis is a highly prevalent disorder of low bone mass and skeletal fragility. Half of all women will experience of an osteoporotic fracture during their lifetime, with each of these fractures incurring significant morbidity and mortality. Based on the profound ability of SHN3 to suppress bone formation, building a better understanding of this pathway will yield new methods to control the activity of osteoblasts to form bone, potentially offering approaches to treat osteoporosis and other disorders of low bone mass. The three overlapping areas to be investigated in this project are: 1. Determine the contribution of SHN3 to skeletal disease models while we have established that SHN3 strongly suppresses bone formation in mice at baseline, the specific contribution of SHN3 to murine models of post-menopausal osteoporosis and skeletal fracture are unknown and will be studied in SHN3-deficient mice. 2. Determine how SHN3 inhibits the ERK pathway in osteoblasts While we have established that SHN3 acts in osteoblasts primarily by suppressing the activity of ERK, the relevant ERK substrates and how SHN3 shapes the kinetics of the ERK response are unknown and will be studied using phosphoproteomics and a quantitative ERK activity biosensor. Determining the relevant substrates of ERK may identify downstream effectors of the SHN3/ERK pathway that are themselves amenable to therapeutic targeting. Additionally, the mechanism for the activation of the ERK/SHN3 pathway by WNTs is unknown, and this will be addressed by a focused screen to determine the MAP3K required for proximal activation of this pathway. 3. Determine if chromatin acts as a scaffold to orchestrate the activity of the SHN3/ERK complex in osteoblasts. Both SHN3 and ERK have previously been identified to bind DNA, raising the possibility that regulation of ERK activity by SHN3 occurs in chromatin bound complexes. In this aim, a complimentary series of chromatin immunoprecipitation-sequencing experiments will be utilized to explore if chromatin orchestrates the function of the SHN3/ERK pathway.

Public Health Relevance

Osteoporosis (skeletal fragility due to low bone mass) affects more than 10 million Americans over the age of 50, resulting in a 1 in 2 and 1 in 4 lifetime risk o an osteoporotic fracture in women and men, respectively. We have identified a gene named SHN3 that has a strong effect to block new bone formation by turning down signals that drive osteoblasts to make bone. In this project, we will determine how SHN3 controls the pathways that drive bone formation by osteoblasts and determine if SHN3 contributes to a model of postmenopausal osteoporosis or to a model of fracture healing.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Office of The Director, National Institutes of Health (OD)
Type
Early Independence Award (DP5)
Project #
1DP5OD021351-01
Application #
9001643
Study Section
Special Emphasis Panel ()
Program Officer
Basavappa, Ravi
Project Start
2015-09-18
Project End
2020-08-31
Budget Start
2015-09-18
Budget End
2016-08-31
Support Year
1
Fiscal Year
2015
Total Cost
$404,985
Indirect Cost
$154,985

  Institution

Name
Weill Medical College of Cornell University
Department
Pathology
Type
DUNS #
060217502
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Xu, Ren; Yallowitz, Alisha; Qin, An et al. (2018) Targeting skeletal endothelium to ameliorate bone loss. Nat Med 24:823-833
Debnath, Shawon; Yallowitz, Alisha R; McCormick, Jason et al. (2018) Discovery of a periosteal stem cell mediating intramembranous bone formation. Nature 562:133-139
Xu, Zhan; Greenblatt, Matthew B; Yan, Guang et al. (2017) SMURF2 regulates bone homeostasis by disrupting SMAD3 interaction with vitamin D receptor in osteoblasts. Nat Commun 8:14570
Greenblatt, Matthew B; Tsai, Joy N; Wein, Marc N (2017) Bone Turnover Markers in the Diagnosis and Monitoring of Metabolic Bone Disease. Clin Chem 63:464-474
Xu, Ren; Zhang, Chao; Shin, Dong Yeon et al. (2017) c-Jun N-Terminal Kinases (JNKs) Are Critical Mediators of Osteoblast Activity In Vivo. J Bone Miner Res 32:1811-1815
Greenblatt, Matthew Blake; Shin, Dong Yeon; Oh, Hwanhee et al. (2016) MEKK2 mediates an alternative ?-catenin pathway that promotes bone formation. Proc Natl Acad Sci U S A 113:E1226-35
Poulos, Michael G; Ramalingam, Pradeep; Gutkin, Michael C et al. (2016) Endothelial-specific inhibition of NF-?B enhances functional haematopoiesis. Nat Commun 7:13829