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We are analyzing https://www.nature.com/articles/1209327.

Title:
Highly purified CD44+ prostate cancer cells from xenograft human tumors are enriched in tumorigenic and metastatic progenitor cells | Oncogene
Description:
CD44 is a multifunctional protein involved in cell adhesion and signaling. The role of CD44 in prostate cancer (PCa) development and progression is controversial with studies showing both tumor-promoting and tumor-inhibiting effects. Most of these studies have used bulk-cultured PCa cells or PCa tissues to carry out correlative or overexpression experiments. The key experiment using prospectively purified cells has not been carried out. Here we use FACS to obtain homogeneous CD44+ and CD44− tumor cell populations from multiple PCa cell cultures as well as four xenograft tumors to compare their in vitro and in vivo tumor-associated properties. Our results reveal that the CD44+ PCa cells are more proliferative, clonogenic, tumorigenic, and metastatic than the isogenic CD44− PCa cells. Subsequent molecular studies demonstrate that the CD44+ PCa cells possess certain intrinsic properties of progenitor cells. First, BrdU pulse-chase experiments reveal that CD44+ cells colocalize with a population of intermediate label-retaining cells. Second, CD44+ PCa cells express higher mRNA levels of several ‘stemness’ genes including Oct-3/4, Bmi, β-catenin, and SMO. Third, CD44+ PCa cells can generate CD44− cells in vitro and in vivo. Fourth, CD44+ PCa cells, which are AR−, can differentiate into AR+ tumor cells. Finally, a very small percentage of CD44+ PCa cells appear to undergo asymmetric cell division in clonal analyses. Altogether, our results suggest that the CD44+ PCa cell population is enriched in tumorigenic and metastatic progenitor cells.
Website Age:
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Keywords {🔍}

cells, cancer, prostate, nature, article, pca, tang, cell, access, oncogene, progenitor, res, content, cookies, information, pdf, van, privacy, bhatia, tumor, open, usa, figure, data, tumorigenic, metastatic, patrawala, calhoun, schneiderbroussard, zhou, experiments, sci, yang, lab, pathol, liu, author, research, advertising, journal, subscribe, purified, xenograft, human, tumors, enriched, chandra, claypool, development, studies,

Topics {✒️}

nature portfolio science park-research division permissions reprints privacy policy nature 432 nature advertising social media intermediate label-retaining cells bulk-cultured pca cells metastatic progenitor cells stem cells ar+ tumor cells prospectively purified cells cd44+ pca cells personal data cd44+ cells colocalize generate cd44− cells progenitor cells author correspondence springerlink instant access development data protection permissions prostate cancer foundation targeted therapy prostate tumor experiments american cancer society national cancer institute obtain homogeneous cd44+ privacy tumor-inhibiting effects issue learn assoc cancer res explore content subscription content xenograft human tumors prostate cancer european economic area multifunctional protein involved institutional subscriptions read ccsg-5 p30 ca166672 immunotherapeutic platform based accepting optional cookies journals search log van der kwast animal facility core article purchase 1-deficient mice results cell sci 114

Schema {🗺️}

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      headline:Highly purified CD44+ prostate cancer cells from xenograft human tumors are enriched in tumorigenic and metastatic progenitor cells
      description:CD44 is a multifunctional protein involved in cell adhesion and signaling. The role of CD44 in prostate cancer (PCa) development and progression is controversial with studies showing both tumor-promoting and tumor-inhibiting effects. Most of these studies have used bulk-cultured PCa cells or PCa tissues to carry out correlative or overexpression experiments. The key experiment using prospectively purified cells has not been carried out. Here we use FACS to obtain homogeneous CD44+ and CD44− tumor cell populations from multiple PCa cell cultures as well as four xenograft tumors to compare their in vitro and in vivo tumor-associated properties. Our results reveal that the CD44+ PCa cells are more proliferative, clonogenic, tumorigenic, and metastatic than the isogenic CD44− PCa cells. Subsequent molecular studies demonstrate that the CD44+ PCa cells possess certain intrinsic properties of progenitor cells. First, BrdU pulse-chase experiments reveal that CD44+ cells colocalize with a population of intermediate label-retaining cells. Second, CD44+ PCa cells express higher mRNA levels of several ‘stemness’ genes including Oct-3/4, Bmi, β-catenin, and SMO. Third, CD44+ PCa cells can generate CD44− cells in vitro and in vivo. Fourth, CD44+ PCa cells, which are AR−, can differentiate into AR+ tumor cells. Finally, a very small percentage of CD44+ PCa cells appear to undergo asymmetric cell division in clonal analyses. Altogether, our results suggest that the CD44+ PCa cell population is enriched in tumorigenic and metastatic progenitor cells.
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         cancer stem cells
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         Cell Biology
         Human Genetics
         Oncology
         Apoptosis
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      affiliation:
            name:The University of Texas MD Anderson Cancer Center
            address:
               name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
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            type:Organization
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      affiliation:
            name:The University of Texas MD Anderson Cancer Center
            address:
               name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
               type:PostalAddress
            type:Organization
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      affiliation:
            name:The University of Texas MD Anderson Cancer Center
            address:
               name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
               type:PostalAddress
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            name:National Cancer Institute, NIH
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               name:Dermatology Branch, National Cancer Institute, NIH, Bethesda, USA
               type:PostalAddress
            type:Organization
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      affiliation:
            name:The University of Texas MD Anderson Cancer Center
            address:
               name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
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            type:Organization
      name:L Coghlan
      affiliation:
            name:The University of Texas MD Anderson Cancer Center
            address:
               name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
               type:PostalAddress
            type:Organization
      name:D G Tang
      affiliation:
            name:The University of Texas MD Anderson Cancer Center
            address:
               name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
               type:PostalAddress
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            name:Program in Environmental & Molecular Carcinogenesis, Graduate School of Biomedical Sciences (GSBS)
            address:
               name:Program in Environmental & Molecular Carcinogenesis, Graduate School of Biomedical Sciences (GSBS), Houston, USA
               type:PostalAddress
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      email:[email protected]
PostalAddress:
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Dermatology Branch, National Cancer Institute, NIH, Bethesda, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Department of Carcinogenesis, Science Park-Research Division, The University of Texas MD Anderson Cancer Center, Smithville, USA
      name:Program in Environmental & Molecular Carcinogenesis, Graduate School of Biomedical Sciences (GSBS), Houston, USA
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