Abstract

Diethylstilbestrol (DES), a potent synthetic estrogen and reproductive toxicant, has been shown to be extensively metabolized. Some metabolites retain hormonal activity while others are biologically inactive. This assignment of activity is consistent with the receptor binding activity of these compounds. Besides reproductive tract effects, some of these metabolites also elicit neuroendocrine effects by suppressing LH secretion. Two groups of metabolites were found to have poor uterotropic activity although they bound very well to the receptor. Some of these compounds show a variety of differences compared to the intracellular responses of DES, including lack of receptor synthesis, poor nuclear translocation, excessive retention of the receptor complex in the nucleus and the inability to stimulate certain tissue responses such as DNA synthesis, mitosis, and induction of specific enzymes and proteins. Estrogen stimulation of reproductive tract tissue involves a mechanism which includes binding to a receptor with subsequent activation and localization in the nucleus. Nuclear translocation follows a bimodal temporal pattern consistent with the stimulation of certain tissue responses such as DNA synthesis or enzyme induction. Only biologically active compounds induce these nuclear receptor events. This pattern was demonstrated by both ligand binding assays and immunoassay with a monoclonal estrogen receptor antibody. Multiple receptor peaks were also present in other estrogen responsive target tissues such as the rat uterus and MCF-7 cell tumors. Cell cycle kinetic studies of uterine estrogen stimulation show that the second peak occurs at the beginning of S-phase. A major effect of estrogen on uterine cells was to shorten the cell cycle by contracting the G-phase. Characterization of the receptor in mouse uterus has indicated multiple forms which are proteolytic fragments and found in nuclear and cytoplasmic tissue fractions. The protease action results in a receptor form which has lost its ability to bind DNA.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Intramural Research (Z01)
Project #
1Z01ES070065-10
Application #
3965300
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
10
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
U.S. National Inst of Environ Hlth Scis
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Li, Yin; Perera, Lalith; Coons, Laurel A et al. (2018) Differential in Vitro Biological Action, Coregulator Interactions, and Molecular Dynamic Analysis of Bisphenol A (BPA), BPAF, and BPS Ligand-ER? Complexes. Environ Health Perspect 126:017012
Burns, Katherine A; Thomas, Seddon Y; Hamilton, Katherine J et al. (2018) Early Endometriosis in Females Is Directed by Immune-Mediated Estrogen Receptor ? and IL-6 Cross-Talk. Endocrinology 159:103-118
Stefkovich, Megan L; Arao, Yukitomo; Hamilton, Katherine J et al. (2018) Experimental models for evaluating non-genomic estrogen signaling. Steroids 133:34-37
Winuthayanon, Wipawee; Lierz, Sydney L; Delarosa, Karena C et al. (2017) Juxtacrine Activity of Estrogen Receptor ? in Uterine Stromal Cells is Necessary for Estrogen-Induced Epithelial Cell Proliferation. Sci Rep 7:8377
Drew, Brian G; Hamidi, Habib; Zhou, Zhenqi et al. (2015) Estrogen receptor (ER)?-regulated lipocalin 2 expression in adipose tissue links obesity with breast cancer progression. J Biol Chem 290:5566-81
Jayes, Friederike L; Burns, Katherine A; Rodriguez, Karina F et al. (2014) The naturally occurring luteinizing hormone surge is diminished in mice lacking estrogen receptor Beta in the ovary. Biol Reprod 90:24
Ball, Christopher B; Rodriguez, Karina F; Stumpo, Deborah J et al. (2014) The RNA-binding protein, ZFP36L2, influences ovulation and oocyte maturation. PLoS One 9:e97324
Li, Yin; Arao, Yukitomo; Hall, Julie M et al. (2014) Research Resource: STR DNA profile and gene expression comparisons of human BG-1 cells and a BG-1/MCF-7 clonal variant. Mol Endocrinol 28:2072-81
Wall, Emma H; Case, Laure K; Hewitt, Sylvia C et al. (2014) Genetic control of ductal morphology, estrogen-induced ductal growth, and gene expression in female mouse mammary gland. Endocrinology 155:3025-35
Devanathan, Sriram; Whitehead, Timothy; Schweitzer, George G et al. (2014) An animal model with a cardiomyocyte-specific deletion of estrogen receptor alpha: functional, metabolic, and differential network analysis. PLoS One 9:e101900

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