Runx2 association with progression of prostate cancer in patients: mechanisms mediating bone osteolysis and osteoblastic metastatic lesions

被引:0
|
作者
J Akech
J J Wixted
K Bedard
M van der Deen
S Hussain
T A Guise
A J van Wijnen
J L Stein
L R Languino
D C Altieri
J Pratap
E Keller
G S Stein
J B Lian
机构
[1] The Cancer Center Prostate Cancer Discovery and Development Program,Department of Cell Biology
[2] University of Massachusetts Medical School,Department of Orthopedic Surgery and Rehabilitation
[3] University of Massachusetts Medical School,Department of Internal Medicine
[4] University of Massachusetts Medical School,Department of Cancer Biology
[5] Endocrinology and Metabolism,Department of Urology
[6] Indiana University School of Medicine,undefined
[7] University of Massachusetts Medical School,undefined
[8] University of Michigan School of Medicine,undefined
来源
Oncogene | 2010年 / 29卷
关键词
Runx2; bone metastasis; prostate cancer tissue arrays;
D O I
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中图分类号
学科分类号
摘要
Runx2, a bone-specific transcriptional regulator, is abnormally expressed in highly metastatic prostate cancer cells. Here, we identified the functional activities of Runx2 in facilitating tumor growth and osteolysis. Our studies show that negligible Runx2 is found in normal prostate epithelial and non-metastatic LNCaP prostate cancer cells. In the intra-tibial metastasis model, high Runx2 levels are associated with development of large tumors, increased expression of metastasis-related genes (MMP9, MMP13, VEGF, Osteopontin) and secreted bone-resorbing factors (PTHrP, IL8) promoting osteolytic disease. Runx2 siRNA treatment of PC3 cells decreased cell migration and invasion through Matrigel in vitro, and in vivo shRunx2 expression in PC3 cells blocked their ability to survive in the bone microenvironment. Mechanisms of Runx2 function were identified in co-culture studies showing that PC3 cells promote osteoclastogenesis and inhibit osteoblast activity. The clinical significance of these findings is supported by human tissue microarray studies of prostate tumors at stages of cancer progression, in which Runx2 is expressed in both adenocarcinomas and metastatic tumors. Together these findings indicate that Runx2 is a key regulator of events associated with prostate cancer metastatic bone disease.
引用
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页码:811 / 821
页数:10
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