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Reports
Functional analyses of the cancer stem cell-like properties of human endometrial tumor initiating cells
Anne M. Friel, Petra A. Sergent, Christine Patnaude, Paul P. Szotek, Esther Oliva, David T. Scadden, Michael V. Seiden, Rosemary Foster and Bo R. Rueda
volume 7 | issue 2
15 January 2008Pages: 242 - 249
This is an open-access article
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Recent data suggest that rare stem cell populations with the capacity to self renew and drive tumor formation are a feature of solid tumors. Several investigators have identified putative stem cells from solid tumors and cancer cell lines following isolation of a side population (SP) defined by dye exclusion. We investigated this parameter in our efforts to identify an endometrial cancer (EnCa) stem cell population. Multiple EnCa cell lines were assessed and verapamil sensitive SP and non-SP cells were isolated from two human EnCa cell lines. The functional significance of the SP and non-SP derived from AN3CA was evaluated in vitro and in vivo. SP cells proliferated at a significantly slower rate than the non-SP fraction, and a larger proportion of the SP cells were in G1 phase of the cell cycle as compared to the non-SP fraction. The SP fraction was more resistant to the chemotherapeutic agent paclitaxel. The SP comprised ~0.02% of the initial AN3CA cell population and this proportion of SP cells was maintained within the larger heterogeneous population following repeated passages of purified SP cells. These findings suggest that SP cells derived from the AN3CA cell line have the stem cell properties of low proliferative activity, chemoresistance, and self-renewal. We also tested relative tumor formation activity of the SP and non-SP fractions. Only the SP fraction was tumorigenic. Additionally, we identified SP fractions in primary EnCa. Together these results are consistent with the hypothesis that EnCa contain a subpopulation of tumor initiating cells with stem like properties.
Authors
Anne M. Friel
Massachusetts General Hospital; Boston, MA
Petra A. Sergent
Massachusetts General Hospital; Boston, MA
Christine Patnaude
Massachusetts General Hospital; Boston, MA
Paul P. Szotek
Massachusetts General Hospital; Boston, MA
Esther Oliva
Massachusetts General Hospital; Boston, MA
David T. Scadden
Massachusetts General Hospital; Boston, MA
Michael V. Seiden
Massachusetts General Hospital; Boston, MA
Rosemary Foster
Massachusetts General Hospital; Boston, MA
Bo R. Rueda
Massachusetts General Hospital; Boston, MA
This is an open-access article
If the document does not open, please right-click on the link (control-click on a Macintosh) and select the option to save the file to disk.




