Abstract

Women with estrogen receptor positive breast cancers frequently respond initially to inhibition of estrogen secretion or action but later relapse. Secondary therapies designed to further lower estrogen levels induce additional remiss ions but progression to a hormone refractory state invariably follows. The mechanisms mediating these secondary responses and later progression are incompletely understood. Based upon our priOr studies, we have develOped an overall hypothesis to explain these observations. We postulate that tumor cells can adapt to conditions of estrogen deprivation by developing enhanced sensitivity to estrogens or to their precursor substrates. Using a model system of long term estrogen withdrawal, we directly demonstrated the ability of cells to develop hypersensitivity to estradiol. The enhanced sensitivity results in two biologic effects: a stimulation of cells at 4 log lower concentrations of estradiol and a paradoxical inhibition with a similar left shift in dose response. Remarkable was the observation that the hypersensitivity phenotype can be induced and then reverted back to basal over a two year period by manipulating the levels of estrogen exposure. The mechanisms involved in development of hypersensitivity are unknown but could be the same as those leading to-progression to a hormone resistant state. The proposed studies are based upon the working hypothesis that ligand independent activation of the estrogen receptor serves to enhance sensitivity to estradiol The resultant increase in cell proliferation may be mediated through the transcription factor c- myb. Enhanced sensitivity to estrogen precursor substrates contributes to this adaptive process. Our investigative strategy involves testing of specific components of this hypothesis using our in vitro model for examining precise biochemical steps, a xenograft system for validation of findings in vivo, and breast tumors from women deprived of estrogen. Firstly, we will examine ligand independent receptor activation. Our strategy is to block specific pathways in order to cause reversion of hypersensitive cells back to a normal state and to induce hypersensitivity in wild type cells by activating steps found to be critical. As biologic endpoints, we will examine estrogen receptor mediated transcription and Cellular growth. We will focus upon involvement of the growth factor, MAP kinase, PKA and PKC pathways as mediators of ligand independent receptor activation. Secondly, we will test the hypothesis that c.myb acts as a downstream mediator of estrogen effects on cell proliferation in long term estradiol deprived and in wild type MCF-7 breast cancer cells. Thirdly, we will test the hypothesis that long term estradiol deprivation enhances sensitivity to estrogen precursors by increasing their enzymatic conversion to active estrogens. These studies will provide insight into the sequential process of progression of tumors from hormone sensitive, to hypersensitive, to hormone independent. We expect our findings to identify potential new therapeutic targets for prevention of tumor progression; to gain insight into new sequential approaches to hormonal therapy, and to provide a back round for the possibility of intermittent hormonal therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA065622-07
Application #
2895198
Study Section
Reproductive Endocrinology Study Section (REN)
Program Officer
Mohla, Suresh
Project Start
1994-08-07
Project End
2000-07-31
Budget Start
1999-08-06
Budget End
2000-07-31
Support Year
7
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Virginia
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
001910777
City
Charlottesville
State
VA
Country
United States
Zip Code
22904

  Publications

Song, Robert X-D; Chen, Yuchai; Zhang, Zhenguo et al. (2010) Estrogen utilization of IGF-1-R and EGF-R to signal in breast cancer cells. J Steroid Biochem Mol Biol 118:219-30
Li, Yan; Wang, Ji-Ping; Santen, Richard J et al. (2010) Estrogen stimulation of cell migration involves multiple signaling pathway interactions. Endocrinology 151:5146-56
Harvey, Jennifer A; Santen, Richard J; Petroni, Gina R et al. (2008) Histologic changes in the breast with menopausal hormone therapy use: correlation with breast density, estrogen receptor, progesterone receptor, and proliferation indices. Menopause 15:67-73
Santen, Richard J; Song, Robert X; Masamura, Shigeru et al. (2008) Adaptation to estradiol deprivation causes up-regulation of growth factor pathways and hypersensitivity to estradiol in breast cancer cells. Adv Exp Med Biol 630:19-34
Sogon, Tetsuya; Masamura, Shigeru; Hayashi, Shin-Ichi et al. (2007) Demethylation of promoter C region of estrogen receptor alpha gene is correlated with its enhanced expression in estrogen-ablation resistant MCF-7 cells. J Steroid Biochem Mol Biol 105:106-14
Yue, Wei; Fan, Ping; Wang, Jiping et al. (2007) Mechanisms of acquired resistance to endocrine therapy in hormone-dependent breast cancer cells. J Steroid Biochem Mol Biol 106:102-10
Song, Robert X-D; Zhang, Zhenguo; Chen, Yucai et al. (2007) Estrogen signaling via a linear pathway involving insulin-like growth factor I receptor, matrix metalloproteinases, and epidermal growth factor receptor to activate mitogen-activated protein kinase in MCF-7 breast cancer cells. Endocrinology 148:4091-101
Song, Robert X-D; Santen, Richard J (2006) Membrane initiated estrogen signaling in breast cancer. Biol Reprod 75:9-16
Song, Robert X-D; Zhang, Zhenguo; Santen, Richard J (2005) Estrogen rapid action via protein complex formation involving ERalpha and Src. Trends Endocrinol Metab 16:347-53
Song, R X-D; Zhang, Z; Mor, G et al. (2005) Down-regulation of Bcl-2 enhances estrogen apoptotic action in long-term estradiol-depleted ER(+) breast cancer cells. Apoptosis 10:667-78

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