Progesterone Stimulates Proliferation and Promotes Cytoplasmic Localization of the Cell Cycle Inhibitor p27 in Steroid Receptor Positive Breast Cancers

被引:0
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作者
Anastasia Kariagina
Jianwei Xie
Ingeborg M. Langohr
Razvan C. Opreanu
Marc D. Basson
Sandra Z. Haslam
机构
[1] Michigan State University,Department of Physiology, College of Human Medicine
[2] Michigan State University,Department of Pathobiology and Diagnostic Investigation, College of Veterinary Medicine
[3] Michigan State University,Department of Surgery, College of Human Medicine
[4] Michigan State University,Department of Physiology
来源
Hormones and Cancer | 2013年 / 4卷
关键词
Proliferate Cell Nuclear Antigen; T47D Cell; T47D Breast Cancer Cell; Progesterone Receptor Isoforms; Mammary Cancer Development;
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摘要
Progestins are reported to increase the risk of more aggressive estrogen receptor positive, progesterone receptor positive (ER+ PR+) breast cancers in postmenopausal women. Using an in vivo rat model of ER+ PR + mammary cancer, we show that tumors arising in the presence of estrogen and progesterone exhibit increased proliferation and decreased nuclear expression of the cell cycle inhibitor p27 compared with tumors growing in the presence of estrogen alone. In human T47D breast cancer cells, progestin increased proliferation and decreased nuclear p27 expression. The decrease of nuclear p27 protein was dependent on activation of Src and PI3K by progesterone receptor isoforms PRA or PRB. Importantly, increased proliferation and decreased nuclear p27 expression were observed in invasive breast carcinoma compared with carcinoma in situ. These results suggest that progesterone specifically regulates intracellular localization of p27 protein and proliferation. Therefore, progesterone-activated pathways can provide useful therapeutic targets for treatment of more aggressive ER+ PR+ breast cancers.
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页码:381 / 390
页数:9
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