Abstract

Osteoblastic metastases represent a significant clinical problem for patients with cancer. They occur almost always in prostate cancer and frequently in other common malignancies such as breast cancer. The pathophysiology underlying osteoblastic metastases is unknown due to lack of a reproducible animal model of this disease. During this Program Project, we have developed an in vivo model of osteoblastic bone metastases which is reproducible and allows investigation into the pathophysiology of this disease. The human tumor cells which cause osteoblastic metastases in this model produce large amounts of endothelin-1 (ET-1), a stimulator of osteoblast growth, which recently has been linked to prostate cancer osteoblastic metastases. This project will characterize the new model, critically test the role of ET-1 in the genesis of osteoblastic metastases and identify other factors responsible for osteoblastic lesions. The following hypotheses will be tested: 1) The human breast cancer cell line, ZR-75-1, mediates osteoblastic metastases by the secretion of a soluble factor or factors which locally stimulate osteoblast proliferation and new bone formation. 2) Tumor- produced ET-1 is a local mediator of osteoblastic metastases caused by prostate and breast cancer. Blocking the effects of tumor-produced ET-1 or decreasing its production will inhibit the development and progression of osteoblastic bone metastases. 3) The relative ratio of tumor-produced osteoblast-stimulating factors to osteoclast-stimulating factors in a given tumor will determine the tumor phenotype in bone. 4) The bone microenvironment enhances tumor production of ET-1 and other osteoblast-stimulating factors, relative to non bone sites. The following specific aims are proposed: 1) To investigate the role of ET-1 in osteoblastic metastasis. The effect of ET-1 on new bone formation will be studied in vitro and in vivo and the relative importance of endothelin receptor A(ETA) and receptor B (ETB) in mediating the effects of endothelin on osteoblast function and osteoblastic bone metastases will be investigated. 2) To determine if tumor production of osteoblastic factors is induced in the bone microenvironment compared with nonbone sites. Molecular techniques will be applied to the bone metastases model to determine which osteoblast-stimulating factors are produced by the ZR-75-1 cells in the bone microenvironment and if ET-1 is the predominant factor.
The aim will also determine if tumor production of osteoblast-stimulating factors are enhanced in the bone microenvironment relative to nonbone sites.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA040035-14
Application #
6314026
Study Section
Project Start
2000-05-09
Project End
2001-04-30
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
14
Fiscal Year
2000
Total Cost
$181,514
Indirect Cost

  Institution

Name
University of Texas Health Science Center San Antonio
Department
Type
DUNS #
800772162
City
San Antonio
State
TX
Country
United States
Zip Code
78229

  Publications

Arnold Egloff, Shanna A; Du, Liping; Loomans, Holli A et al. (2017) Shed urinary ALCAM is an independent prognostic biomarker of three-year overall survival after cystectomy in patients with bladder cancer. Oncotarget 8:722-741
Arnold, Shanna A; Loomans, Holli A; Ketova, Tatiana et al. (2016) Urinary oncofetal ED-A fibronectin correlates with poor prognosis in patients with bladder cancer. Clin Exp Metastasis 33:29-44
Preston Campbell, J; Mulcrone, P; Masood, S K et al. (2015) TRIzol and Alu qPCR-based quantification of metastatic seeding within the skeleton. Sci Rep 5:12635
Sharma, Ramaswamy; Williams, Paul J; Gupta, Anjana et al. (2015) A dominant-negative F-box deleted mutant of E3 ubiquitin ligase, ?-TrCP1/FWD1, markedly reduces myeloma cell growth and survival in mice. Oncotarget 6:21589-602
Seeley, Erin H; Wilson, Kevin J; Yankeelov, Thomas E et al. (2014) Co-registration of multi-modality imaging allows for comprehensive analysis of tumor-induced bone disease. Bone 61:208-16
Johnson, Rachelle W; Merkel, Alyssa R; Page, Jonathan M et al. (2014) Wnt signaling induces gene expression of factors associated with bone destruction in lung and breast cancer. Clin Exp Metastasis 31:945-59
Ding, Hao; Nyman, Jeffry S; Sterling, Julie A et al. (2014) Development of Raman spectral markers to assess metastatic bone in breast cancer. J Biomed Opt 19:111606
Hansen, Amanda G; Arnold, Shanna A; Jiang, Ming et al. (2014) ALCAM/CD166 is a TGF-?-responsive marker and functional regulator of prostate cancer metastasis to bone. Cancer Res 74:1404-15
Bi, Xiaohong; Sterling, Julie A; Merkel, Alyssa R et al. (2013) Prostate cancer metastases alter bone mineral and matrix composition independent of effects on bone architecture in mice--a quantitative study using microCT and Raman spectroscopy. Bone 56:454-60
Waning, David L; Mohammad, Khalid S; Guise, Theresa A (2013) Cancer-associated osteoclast differentiation takes a good look in the miR(NA)ror. Cancer Cell 24:407-9

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