Journal
CANCER
Volume 97, Issue 3, Pages 779-784Publisher
WILEY
DOI: 10.1002/cncr.11129
Keywords
osteoblast; endothelin; bone metastasis; breast cancer; prostate cancer
Categories
Funding
- NCI NIH HHS [CA69158, CA40035] Funding Source: Medline
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BACKGROUND. Certain solid tumors metastasize to bone and cause an osteoblastic response. The mechanisms by which turner cells stimulate this new bone formation are not completely understood. METHODS. The authors identified three breast cancer lines that cause osteoblastic metastases in female nude mice and provided evidence that tumor-produced endothelin-1 (ET-1) mediates the osteoblastic response. RESULTS. Tumor conditioned media, as well as exogenous ET-1, stimulated osteoblast proliferation and new bone formation in cultures of mouse calvariae. These effects were blocked by antagonists of the endothelin A (ETA), but not ETB, receptors. Mice inoculated with the ZR-75-1 breast cancer line and treated with a selective ETA receptor antagonist (ABT-627) had significantly fewer osteoblastic bone metastases and less tumor burden compared with untreated mice. In contrast, there was no effect of ABT-627 on osteolytic bone metastases caused by ET-1-negative breast cancer, MDA-MB-231. ABT-627 had no effect on growth in vitro or at the orthotopic site of ZR-75-1 or MDA-MB-231 cells. CONCLUSIONS. Collectively, the data suggested that tumor-produced ET-1 mediates osteoblastic bone metastases by stimulating osteoblast proliferation and new bone formation. ETA receptor blockade may be useful for prevention and the treatment of osteoblastic bone metastases due to breast or prostate cancer. (C) 2003 American Cancer Society.
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