TY - JOUR
T1 - Cyclooxygenase-2 expression in primary breast cancers predicts dissemination of cancer cells to the bone marrow
AU - Lucci, Anthony
AU - Krishnamurthy, Savitri
AU - Singh, Balraj
AU - Bedrosian, Isabelle
AU - Meric-Bernstam, Funda
AU - Reuben, James
AU - Broglio, Kristine
AU - Mosalpuria, Kailash
AU - Lodhi, Ashutosh
AU - Vincent, Laura
AU - Cristofanilli, Massimo
N1 - Funding Information:
Acknowledgements These studies were supported in part by the grants DK067682 (AL) and CA16672 (Core) from the National Institutes of Health and DAMD17-03-1-0669 (AL) from the United States Army Medical Research and Material Command. We thank Gabriel Hortobagyi for helpful comments on the manuscript.
PY - 2009/9
Y1 - 2009/9
N2 - Purpose: Cyclooxygenase-2 (COX2) plays a role in breast cancer progression at various stages starting from pre-malignant phenotype to clinical metastasis. Breast cancer metastasizes commonly to the bone and preclinical studies suggest an involvement of COX2 in this process. Detection of disseminated tumor cells in the bone marrow of patients at the time of surgery correlates with the subsequent development of clinical bone metastasis. Therefore, to investigate whether COX2 is important for breast cancer metastasis in humans, we analyzed COX2 protein expression by immunostaining of primary tumors from 112 operable stages I, II, or III patients and determined its correlation with bone marrow micrometastasis (BMM). Methods: We detected COX2 protein in primary tumors by immunostaining with a monoclonal antibody, and tumor cells present in the bone marrow by immunostaining for epithelial cytokeratins and by morphological criteria. Results: COX2 expression in primary breast cancer correlated with BMM in a highly statistically significant manner (P = 0.006). Our statistical analyses of correlations of the COX2 positivity in primary tumor with other clinically relevant indicators revealed that COX2 positivity correlates with high nuclear grade (P = 0.0004). Furthermore, we were able to detect COX2 protein in BMM by immunostaining. Conclusions: These studies indicate that COX2 produced in primary breast cancer cells may be vital to the initial development of BMM that may subsequently lead to osteolytic bone metastases in patients with breast cancer, and that COX2 inhibitors may be useful in halting this process.
AB - Purpose: Cyclooxygenase-2 (COX2) plays a role in breast cancer progression at various stages starting from pre-malignant phenotype to clinical metastasis. Breast cancer metastasizes commonly to the bone and preclinical studies suggest an involvement of COX2 in this process. Detection of disseminated tumor cells in the bone marrow of patients at the time of surgery correlates with the subsequent development of clinical bone metastasis. Therefore, to investigate whether COX2 is important for breast cancer metastasis in humans, we analyzed COX2 protein expression by immunostaining of primary tumors from 112 operable stages I, II, or III patients and determined its correlation with bone marrow micrometastasis (BMM). Methods: We detected COX2 protein in primary tumors by immunostaining with a monoclonal antibody, and tumor cells present in the bone marrow by immunostaining for epithelial cytokeratins and by morphological criteria. Results: COX2 expression in primary breast cancer correlated with BMM in a highly statistically significant manner (P = 0.006). Our statistical analyses of correlations of the COX2 positivity in primary tumor with other clinically relevant indicators revealed that COX2 positivity correlates with high nuclear grade (P = 0.0004). Furthermore, we were able to detect COX2 protein in BMM by immunostaining. Conclusions: These studies indicate that COX2 produced in primary breast cancer cells may be vital to the initial development of BMM that may subsequently lead to osteolytic bone metastases in patients with breast cancer, and that COX2 inhibitors may be useful in halting this process.
KW - Bone marrow micrometastasis
KW - Breast cancer
KW - COX2
KW - Disseminated tumor cells
KW - Minimal residual disease
UR - http://www.scopus.com/inward/record.url?scp=69049112248&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=69049112248&partnerID=8YFLogxK
U2 - 10.1007/s10549-008-0135-x
DO - 10.1007/s10549-008-0135-x
M3 - Article
C2 - 18663571
AN - SCOPUS:69049112248
SN - 0167-6806
VL - 117
SP - 61
EP - 68
JO - Breast Cancer Research and Treatment
JF - Breast Cancer Research and Treatment
IS - 1
ER -