Abstract

Human breast cancer cell proliferation is regulated by the interaction of a variety of steroid and polypeptide hormones. In particular, treatments designed to reduce the estrogen level or to block estrogen's effects on the tumor with antiestrogens frequently cause tumor regression. A better understanding of the mechanisms by which estrogens and antiestrogens regulate breast cancer cell proliferation would have important clinical implications and might provide clues to new treatment approaches. We therefore propose to use human breast cancer cell lines in vitro and cells growing as tumors in athymic nude mice to study mechanisms by which endocrine manipulation inhibits tumor growth and possibly interfers with simultaneous cytotoxic drug treatment, and how breast cancers eventually escape from endocrine suppression. (1) Studies will be performed to determine whether estrogen deprivation or antiestrogen therapy inhibit growth by a cytostatic mechanism, resulting in accumulation of cells in either G or G1 phase, or by a cytocidal mechanism resulting in cell death. (2) Additional studies of the interaction between the antiestrogen tamoxifen and several cytotoxic agents will be done to clarify mechanisms for the antagonism observed in preliminary studies with melphalan and 5-fluorouracil, drugs used frequently in combination with tamoxifen in the clinic. (3) Finally, the acquired endocrine independence which appears after extended endocrine treatment in cultured cells, in tumors growing in nude mice, and in patients with breast cancer, will be investigated. Initial tumor heterogeneity, loss or alteration of receptors, more distal changes in estrogen-regulated pathways, or changes in the host will be considered. The possibility that altered autocrine growth factor activity is responsible for acquired endocrine independence will be examined, in view of recent data suggesting that polypeptide growth factors secreted by breast cancer cells may mediate the effects of estrogen and may account for the autonomy of hormone-independent tumors. These studies could lead to new strategies to better exploit endocrine responsiveness in breast cancer, to avoid interference between components of combined chemoendocrine therapy, and to prevent or counteract the development of resistance to endocrine therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA030251-08
Application #
3169141
Study Section
Biochemical Endocrinology Study Section (BCE)
Project Start
1981-07-01
Project End
1990-12-31
Budget Start
1988-03-01
Budget End
1988-12-31
Support Year
8
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of Texas Health Science Center San Antonio
Department
Type
Schools of Medicine
DUNS #
800772162
City
San Antonio
State
TX
Country
United States
Zip Code
78229

  Publications

Osborne, C K (1998) Tamoxifen in the treatment of breast cancer. N Engl J Med 339:1609-18
Nicholson, R I; Gee, J M; Bryant, S et al. (1996) Pure antiestrogens. The most important advance in the endocrine therapy of breast cancer since 1896. Ann N Y Acad Sci 784:325-35
Osborne, C K; Coronado-Heinsohn, E B; Hilsenbeck, S G et al. (1995) Comparison of the effects of a pure steroidal antiestrogen with those of tamoxifen in a model of human breast cancer. J Natl Cancer Inst 87:746-50
Maenpaa, J; Wiebe, V; Wurz, G et al. (1994) Reduced tamoxifen accumulation is not associated with stimulated growth in tamoxifen resistance. Cancer Chemother Pharmacol 35:149-52
Osborne, C K; Jarman, M; McCague, R et al. (1994) The importance of tamoxifen metabolism in tamoxifen-stimulated breast tumor growth. Cancer Chemother Pharmacol 34:89-95
Koester, S K; Maenpaa, J U; Wiebe, V J et al. (1994) Flow cytometry: potential utility in monitoring drug effects in breast cancer. Breast Cancer Res Treat 32:57-65
Osborne, C K (1993) Mechanisms for tamoxifen resistance in breast cancer: possible role of tamoxifen metabolism. J Steroid Biochem Mol Biol 47:83-9
Wiebe, V J; Osborne, C K; Fuqua, S A et al. (1993) Tamoxifen resistance in breast cancer. Crit Rev Oncol Hematol 14:173-88
Sipila, P E; Wiebe, V J; Hubbard, G B et al. (1993) Prolonged tamoxifen exposure selects a breast cancer cell clone that is stable in vitro and in vivo. Eur J Cancer 29A:2138-44
Maenpaa, J U; Wurz, G T; Baker, W J et al. (1993) A breast cancer clone selected by tamoxifen has increased growth rate and reduced sensitivity to doxorubicin. Oncol Res 5:461-6

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