Abstract

Estrogen action in reproductive tract tissue involves a mechanism which includes interaction with a receptor protein with subsequent activation and localization in the nucleus. After hormone stimulation, nuclear receptor occupancy followed a bimodal temporal pattern consistent with stimulation of certain tissue responses such as DNA synthesis or enzyme induction. The bimodal receptor pattern was evident in other responsive target tissues such as human MCF-7 cell tumors. DNA synthesis in tumors or uteri can be produced with discontinuous stimulation with a weak agonist and occurs at similar times as the two nuclear receptor events. We have purified (approximately 11000-fold) the mouse uterine estrogen receptor by steroid affinity chromatography and have characterized it by ligand affinity labeling as well as immunoblot analysis with a monoclonal antibody. Studies indicate multiple forms which are proteolytic fragments. Proteolytic processing of the receptor involves a two-step reaction. The first involving a nuclear cysteine protease and the second a soluble enzyme preliminarily characterized as a cathepsin protease. Additional biochemical characterization of the estrogen receptor protein with monoclonal antibodies demonstrated a doublet form differing by 1500 MW. This receptor form was specific to the nucleus and not found in the soluble fraction. The proportion of the doublet varied depending on the biological activity of the compound with potent agonists producing a greater amount of the upper band form. The profile of the nuclear doublet changed during estrogen stimulation in which the two components were of equal proportion until the time of the second nuclear peak at which time the proportion changed to be primarily the lower band form. Preliminary data indicate both bands are phosphorylated, the upper to a greater extent suggesting this as the protein modification for doublet formation. Experiments to investigate other processes such as acylation or glycosylation are also under study. Receptor modification may be a signal for cellular processing of the protein or programming for its interaction with specific nuclear responsive sites involved in hormone stimulation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Intramural Research (Z01)
Project #
1Z01ES070065-13
Application #
3918744
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
13
Fiscal Year
1988
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
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
Burns, Katherine A; Li, Yin; Liu, Liwen et al. (2014) Research resource: comparison of gene profiles from wild-type ER? and ER? hinge region mutants. Mol Endocrinol 28:1352-61
Li, Yin; Hamilton, Katherine J; Lai, Anne Y et al. (2014) Diethylstilbestrol (DES)-stimulated hormonal toxicity is mediated by ER? alteration of target gene methylation patterns and epigenetic modifiers (DNMT3A, MBD2, and HDAC2) in the mouse seminal vesicle. Environ Health Perspect 122:262-8
Wall, Emma H; Hewitt, Sylvia C; Case, Laure K et al. (2014) The role of genetics in estrogen responses: a critical piece of an intricate puzzle. FASEB J 28:5042-54

Showing the most recent 10 out of 170 publications