TY - JOUR
T1 - Caveolin-1-deficient mice have an increased mammary stem cell population with upregulation of Wnt/β-catenin signaling
AU - Sotgia, Federica
AU - Williams, Terence M.
AU - Cohen, Alex W.
AU - Minetti, Carlo
AU - Pestell, Richard G.
AU - Lisanti, Michael P.
N1 - Funding Information:
This work was supported by grants from National Institutes of Health (NIH), and the American Heart Association, as well as Hirschl/ Weil-Caulier Career Scientist Award (all to M.P.L.). T.M.W. was supported by a National Institutes of Health Medical Scientist Training Program Grant (T32-GM07288).
PY - 2005/12
Y1 - 2005/12
N2 - Here, we show that a caveolin-1 (Cav-1) deficiency leads to an amplification of the adult mammary stem cell population, both in vivo and in vitro. First, the expression of two stem cell markers, Sca-1 and Keratin 6, is dramatically increased in the hyperplastic mammary ducts of Cav-1 deficient mice, suggesting that loss of Cav-1 induces the accumulation of a progenitor cell population in the mammary gland. To independently validate these results, we reconstituted mammary acini formation in vitro via a 3D Matrigel assay system - using primary cultures of mammary epithelial cells derived from WT and Cav-1 deficient mice. We show that Cav-1 null 3D epithelial structures display an intense increase in the expression of three stem cell markers, i.e., Sca-1, keratin 6 and keratin 5. Overall, we observed a 2-to-3 fold increase in the number of Cav-1 KO acini that are positive for a given stem cell marker. Also, we show that such amplification of progenitor cells has functional consequences, as demonstrated by the abnormal presence of myoepithelial cells in the hyperplastic lesions of Cav-1 deficient mammary glands. Finally, we provide evidence that hyper-activation of Wnt/β-catenin signaling may constitute one of the down-stream mechanisms leading to mammary stem cell accumulation. The longevity and slow-dividing properties of mammary stem cells facilitates the accumulation of genetic alterations, and renders these progenitor cells the likely precursors of malignant derivatives. As such, we propose that loss of Cav-1 induces the accumulation of mammary stem cells, and that this event may be an initiating factor during mammary tumorigenesis.
AB - Here, we show that a caveolin-1 (Cav-1) deficiency leads to an amplification of the adult mammary stem cell population, both in vivo and in vitro. First, the expression of two stem cell markers, Sca-1 and Keratin 6, is dramatically increased in the hyperplastic mammary ducts of Cav-1 deficient mice, suggesting that loss of Cav-1 induces the accumulation of a progenitor cell population in the mammary gland. To independently validate these results, we reconstituted mammary acini formation in vitro via a 3D Matrigel assay system - using primary cultures of mammary epithelial cells derived from WT and Cav-1 deficient mice. We show that Cav-1 null 3D epithelial structures display an intense increase in the expression of three stem cell markers, i.e., Sca-1, keratin 6 and keratin 5. Overall, we observed a 2-to-3 fold increase in the number of Cav-1 KO acini that are positive for a given stem cell marker. Also, we show that such amplification of progenitor cells has functional consequences, as demonstrated by the abnormal presence of myoepithelial cells in the hyperplastic lesions of Cav-1 deficient mammary glands. Finally, we provide evidence that hyper-activation of Wnt/β-catenin signaling may constitute one of the down-stream mechanisms leading to mammary stem cell accumulation. The longevity and slow-dividing properties of mammary stem cells facilitates the accumulation of genetic alterations, and renders these progenitor cells the likely precursors of malignant derivatives. As such, we propose that loss of Cav-1 induces the accumulation of mammary stem cells, and that this event may be an initiating factor during mammary tumorigenesis.
KW - Acini formation
KW - Animal models
KW - Caveolae
KW - Caveolin-1
KW - Keratin 6
KW - Mammary progenitor cells
KW - Sca-1
KW - Stem cells
KW - β-Catenin
UR - http://www.scopus.com/inward/record.url?scp=29244451080&partnerID=8YFLogxK
U2 - 10.4161/cc.4.12.2198
DO - 10.4161/cc.4.12.2198
M3 - Article
C2 - 16294019
AN - SCOPUS:29244451080
SN - 1538-4101
VL - 4
SP - 1808
EP - 1816
JO - Cell Cycle
JF - Cell Cycle
IS - 12
ER -