Circulating endothelial progenitor cells correlate to stage in patients with invasive breast cancer

Tumor growth and metastasis is dependent on the formation and assembly of new blood vessels, a process known as neo-angiogenesis. Both pre-existing and circulating vascular cells have been shown to contribute to the assembly of tumor neo-vessels in specific tumors. Mobilization of endothelial progen...

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Veröffentlicht in:Breast cancer research and treatment 2008, Vol.107 (1), p.133-138
Hauptverfasser: Naik, Rakhi P., Jin, David, Chuang, Ellen, Gold, Ellen G., Tousimis, Eleni A., Moore, Anne L., Christos, Paul J., de Dalmas, Tatiana, Donovan, Diana, Rafii, Shahin, Vahdat, Linda T.
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Sprache:eng
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Zusammenfassung:Tumor growth and metastasis is dependent on the formation and assembly of new blood vessels, a process known as neo-angiogenesis. Both pre-existing and circulating vascular cells have been shown to contribute to the assembly of tumor neo-vessels in specific tumors. Mobilization of endothelial progenitor cells (EPCs) from the bone marrow constitutes a crucial step in the formation of de novo blood vessels, and levels of peripheral blood EPCs have been shown to be increased in certain malignant states. However, the role of circulating EPCs in breast cancer is largely unknown. We recruited twenty-five patients with biopsy-proven invasive breast cancer at Weill Cornell Breast Center to participate in a pilot study investigating the correlation of circulating EPCs to extent of disease and initiation of chemotherapy. For each patient, a baseline sample was drawn before systemic treatment, and for seventeen of those patients, a second sample was taken after the first round of chemotherapy. Levels of peripheral blood EPCs, as defined by co-expression of CD133 and VEGFR2, were quantified by flow cytometry. Breast cancer patients with stage III & IV disease had statistically higher levels of circulating EPCs than did patients with stage I & II disease (median = 165,000 EPCs/5 × 10 6 MNCs vs. median = 6,920 EPCs/5 × 10 6 MNCs, respectively, P  
ISSN:0167-6806
1573-7217
DOI:10.1007/s10549-007-9519-6