Abstract

Bone formation is a complex process regulated by hormones and by systemic and local growth factors. The goal of this laboratory has been to study the effects of systemic and local growth factors on bone formation. Our recetn efforts have focused on the local regulators of bone growth. We discovered that cultured fetal rat calvariae secrete at least two growth factors; these were originally termed bone-derived growth factor (BDGF) I and II. We have now shown that BDGF-I is a transforming growth factor of the beta class (TGF-beta), has a relative molecular mass (Mr) of 23,000 and stimulates preosteoblastic cell replication. We also showed that BDGF II (presently termed BDGF) is a distinct factor, has a Mr of 11-12,000 and stimulates, simultaneously, bone DNA and collagen synthesis. The biochemical and some of the biological properties of TGF-beta have been characterized but the amino acid sequence and many of the biological effects of BDGF are unknown. Over the next five years we intend to determine the amino acid sequence of BDGF by the use of gas phase sequencing and by establishing the structure of a complementary (c) DNA clone for BDGF. We also plan to investigate the effects of TGF-beta and BDGF on bone formation, examine their interactions with hormones an study their receptors. Our studies will include the development of sensitive and specific assays for TGF-beta and BDGF which will be useful to study the synthesis of these factors by bone cells and its regulation by systemic hormones and growth factors. To complement these experiments, we will examine mRNA expression of TGF-beta and BDGF in bone tissue and cells. For this purpose, we obtained a mouse cDNA clone for TGF-beta and we will develop a rat cDNA clone for BDGF by constructing a bone cell library which will be probed with a labeled synthetic oligonucleotide made in accordance with the structure of BDGF. Our research will provide information about the biochemical and biological properties of bone-derived TGF-beta and BDGF and how these factors interact with hormones and other growth factors which may modulate their synthesis or effects. These studies are valuable because local factors are likely to have an important effect on bone remodelling and mediation of the effects of hormones on bone. Our current understanding of bone cell physiology and metabolic bone disease is limited and this research may provide future diagnostic and therapeutic alternatives for metabolic bone disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR021707-11
Application #
3155211
Study Section
General Medicine B Study Section (GMB)
Project Start
1981-04-01
Project End
1992-03-31
Budget Start
1991-04-01
Budget End
1992-03-31
Support Year
11
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
St. Francis Hospital and Medical Center
Department
Type
DUNS #
City
Hartford
State
CT
Country
United States
Zip Code
06105

  Publications

Yang, Jibing; Velikoff, Miranda; Canalis, Ernesto et al. (2014) Activated alveolar epithelial cells initiate fibrosis through autocrine and paracrine secretion of connective tissue growth factor. Am J Physiol Lung Cell Mol Physiol 306:L786-96
Zanotti, Stefano; Kalajzic, Ivo; Aguila, Hector Leonardo et al. (2014) Sex and genetic factors determine osteoblastic differentiation potential of murine bone marrow stromal cells. PLoS One 9:e86757
He, Qing; Yang, Xuehui; Gong, Yan et al. (2014) Deficiency of Sef is associated with increased postnatal cortical bone mass by regulating Runx2 activity. J Bone Miner Res 29:1217-31
Canalis, Ernesto; Zanotti, Stefano; Smerdel-Ramoya, Anna (2014) Connective tissue growth factor is a target of notch signaling in cells of the osteoblastic lineage. Bone 64:273-80
Canalis, Ernesto (2013) Wnt signalling in osteoporosis: mechanisms and novel therapeutic approaches. Nat Rev Endocrinol 9:575-83
Zanotti, Stefano; Canalis, Ernesto (2012) Nemo-like kinase inhibits osteoblastogenesis by suppressing bone morphogenetic protein and WNT canonical signaling. J Cell Biochem 113:449-56
Zanotti, Stefano; Canalis, Ernesto (2012) Notch regulation of bone development and remodeling and related skeletal disorders. Calcif Tissue Int 90:69-75
Canalis, Ernesto; Brunet, Lisa J; Parker, Kristen et al. (2012) Conditional inactivation of noggin in the postnatal skeleton causes osteopenia. Endocrinology 153:1616-26
Canalis, Ernesto; Parker, Kristen; Zanotti, Stefano (2012) Gremlin1 is required for skeletal development and postnatal skeletal homeostasis. J Cell Physiol 227:269-77
Beamer, Wesley G; Shultz, Kathryn L; Coombs 3rd, Harold F et al. (2011) BMD regulation on mouse distal chromosome 1, candidate genes, and response to ovariectomy or dietary fat. J Bone Miner Res 26:88-99

Showing the most recent 10 out of 114 publications