Xenoestrogen action in breast cancer: impact on ER-dependent transcription and mitogenesis

被引:0
作者
J.K. Hess-Wilson
J. Boldison
K.E. Weaver
K.E. Knudsen
机构
[1] University of Cincinnati College of Medicine,Department of Cell Biology
[2] University of Cincinnati College of Medicine,Center for Environmental Genetics
[3] University of Cincinnati College of Medicine,Department of Cell Biology
来源
Breast Cancer Research and Treatment | 2006年 / 96卷
关键词
breast cancer; bisphenol A; co-activators; coumestrol; estrogen receptor; ER-; xenoestrogens;
D O I
暂无
中图分类号
学科分类号
摘要
Several estrogen mimics (xenoestrogens) inappropriately activate the estrogen receptor (ER) in the absence of endogenous ligand. Given the importance of the ER in breast cancer growth and regulation, delineating the impact of these agents under conditions related to tumor treatment is of significant importance. We examined the effect of two prevalent xenoestrogens (bisphenol A and coumestrol) on ER activation and ER-dependent mitogenesis in breast cancer cells. We show that the ability of these agents to induce mitogenesis was restricted to conditions of estrogen depletion, and that these agents failed to cooperate with estradiol to induce MCF-7 breast cancer cell growth. These observations are consistent with the impact of each agent specifically on exogenous ER activation as monitored in HeLa cells, wherein the xenoestrogens activated the receptor in the absence of estradiol but failed to cooperate with estrogen. Tamoxifen blocked bisphenol A and coumestrol-mediated ER activation, indicating that exposure to these agents is unlikely to disrupt such therapeutic intervention. The response of tumor-derived ER alleles to these xenoestrogens was also examined. Although the xenoestrogens failed to alter ER-Y537S function, the ER-D351Y mutant demonstrated an enhanced response to bisphenol A. Moreover, tamoxifen enhanced the agonistic effects of xenoestrogens on ER-D351Y. Lastly, we examined the impact of ER co-activator overexpression on xenoestrogen response. Bisphenol A and coumestrol exhibited differential responses to co-activators with regard to ER activation. However, when using mitogenesis as an endpoint, these co-activators were insufficient to provide a significant growth advantage. Combined, these data demonstrate that bisphenol A and coumestrol can impact ER activity and ER-dependent proliferation in breast cancer cells, but the influence of these agents is restricted to conditions of estrogen depletion, selective mutation of the ER, and expression of specific co-activators.
引用
收藏
页码:279 / 292
页数:13
相关论文
共 433 条
  • [1] Jemal A(2004)Cancer statistics, 2004 CA Cancer J Clin 54 8-29
  • [2] Tiwari RC(2002)Recent trends in breast cancer incidence and mortality Environ Mol Mutagen 39 82-8
  • [3] Murray T(2001)Epidemiology of breast cancer Lancet Oncol 2 133-40
  • [4] Ghafoor A(2004)The effect of environment on breast cancer risk Breast Cancer Res Treat 84 273-88
  • [5] Samuels A(1983)Biological significance of aromatase activity in human breast tumors J Clin Endocrinol Metab 57 1125-8
  • [6] Ward E(1996)Hormonal carcinogenesis and environmental influences: background and overview Prog Clin Biol Res 394 3-23
  • [7] Feuer EJ(1997)Recent developments on the avoidable causes of breast cancer Ann N Y Acad Sci 837 513-23
  • [8] Thun MJ(2004)Estrogens and their receptors in breast cancer progression: a dual role in cancer proliferation and invasion Crit Rev Oncol Hematol 51 55-67
  • [9] Lacey JV(2004)The molecular determinants of estrogen receptor pharmacology Maturitas 48 7-12
  • [10] Devesa SS(2002)Molecular determinants for the tissue specificity of SERMs Science 295 2465-8
12345678910