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Endocrinology, doi:10.1210/en.2004-1211
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Endocrinology Vol. 146, No. 4 1727-1736
Copyright © 2005 by The Endocrine Society

Bone Turnover Mediates Preferential Localization of Prostate Cancer in the Skeleton

Abraham Schneider, Linda M. Kalikin, Ana C. Mattos, Evan T. Keller, Matthew J. Allen, Kenneth J. Pienta and Laurie K. McCauley

Department of Periodontics/Prevention/Geriatrics, School of Dentistry (A.S., A.C.M., L.K.M.), Departments of Urology (L.M.K., E.T.K., K.J.P.), Pathology (E.T.K., L.K.M.), and Internal Medicine (Division of Hematology/Oncology), Medical School (K.J.P.), University of Michigan, Ann Arbor, Michigan 48109; and Department of Orthopedic Surgery (M.J.A.), State University of New York Upstate Medical University, Syracuse, New York 13210

Address all correspondence and requests for reprints to: Dr. Laurie K. McCauley, Department of Periodontics/Prevention/Geriatrics, School of Dentistry, Room 3343, University of Michigan, 1011 North University Avenue, Ann Arbor, Michigan 48109-1078. E-mail: mccauley{at}umich.edu.

Bone metastasis is a common untreatable complication associated with prostate cancer. Metastatic cells seed in skeletal sites under active turnover containing dense marrow cellularity. We hypothesized that differences in these skeletal-specific processes are among the critical factors that facilitate the preferential localization of metastatic prostate cancer in bone. To test this, athymic mice were administered PTH to induce bone turnover and increase marrow cellularity daily 1 wk before and after intracardiac inoculation of luciferase-tagged PC-3 cells. Tumor localization was monitored by bioluminescence imaging weekly for 5 wk. At the time of tumor inoculation, PTH-treated mice demonstrated significant increases in serum levels of bone turnover markers such as osteocalcin and tartrate-resistant acid phosphatase 5b and in the number of tartrate-resistant acid phosphatase-positive osteoclasts per millimeter of bone when compared with the other groups. Likewise, PTH treatment stimulated a qualitative increase in marrow cellular proliferation as determined by 5-bromo-2'-deoxyuridine immunostaining. Skeletal metastases formed in the hind limb and craniofacial regions of young mice with no difference between groups. In adult mice, however, bioluminescent signals in the hind limb and craniofacial regions were 3-fold higher in PTH-treated mice vs. controls. Fluorochrome labeling revealed increased bone formation activity in trabecular bone adjacent to tumors. When zoledronic acid, a nitrogen-containing bisphosphonate that inhibits osteoclast-mediated bone resorption, was administered concurrently with PTH, a significant reduction in the incidence of bone tumors was observed. Overall, these studies provide new evidence that skeletal sites rich in marrow cellularity under active turnover offer a more congenial microenvironment to facilitate cancer localization in the skeleton.




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