Abstract

Antiestrogens (AEs), intriguing compounds that are able to antagonize many of the actions of estrogens, are of particular medical importance because of their efficacy In controlling the growth and spread of hormone-responsive breast and uterine tumors. Our objective is to understand the mechanism by which AEs interact with the estrogen receptor and are effective as estrogen antagonists. Our studies address the question of estrogen antagonist action at two levels: ligand-receptor interaction and receptor-receptor interaction (dimerization).
Our specific aims are to identify the ligand discriminating site in the estrogen receptor through site-directed and random mutagenesis and biocharacter screening, and to investigate the role of receptor dimerization in AE action through the use of bivalent ligands and a dimer contact peptide. Based upon results from our affinity labeling studies, we will prepare a set of mutant estrogen receptors in which carefully controlled substitutions of specific amino acids are made in those regions In the hormone binding domain-E thought to be the most critically involved in distinguishing between estrogen agonists and antagonists, a site we term the ligand discriminating site. Conservative amino acid substitutions will be made, so as to maintain estrogen receptor structure and ligand binding but to change the interaction that the altered domain might have with the basic and polar side chains of AEs. Additional affinity labeling studies using new derivatives of AEs will be conducted to obtain further information on the contact sites between estrogen receptor and the basic side chains of the AEs. In complementary studies, we will use random mutagenesis of selected portions of estrogen receptor cDNA and biocharacter screening in yeast to identify further the residues important in determining agonist/ antagonist character. We will prepare and evaluate the agonist/antagonist potency of bivalent AE and estrogen ligands and their effects on the monomer-dimer equilibrium of receptor. We will also synthesize a dimer contact oligopeptide and determine if it blocks receptor dimerization and alters transactivation. The implications of progress in this area include the development of improved AEs, a greater understanding of the .effectiveness of AEs in treatment of hormone-responsive breast cancer, and elucidation of aspects of ligand character recognition and the regulation of transcription by AEs and estrogens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37CA018119-22
Application #
2700316
Study Section
Special Emphasis Panel (NSS)
Program Officer
Mohla, Suresh
Project Start
1978-12-01
Project End
1999-04-30
Budget Start
1998-05-01
Budget End
1999-04-30
Support Year
22
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Illinois Urbana-Champaign
Department
Physiology
Type
Schools of Arts and Sciences
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820

  Publications

Aghmesheh, Morteza; Saxena, Akshat; Niknam, Farshid (2015) BRCA1 mutation site may be linked with nuclear DNA ploidy in BRCA1-mutated ovarian carcinomas. Asia Pac J Clin Oncol 11:135-41
Kieser, Karen J; Kim, Dong Wook; Carlson, Kathryn E et al. (2010) Characterization of the pharmacophore properties of novel selective estrogen receptor downregulators (SERDs). J Med Chem 53:3320-9
Chambliss, Ken L; Wu, Qian; Oltmann, Sarah et al. (2010) Non-nuclear estrogen receptor alpha signaling promotes cardiovascular protection but not uterine or breast cancer growth in mice. J Clin Invest 120:2319-30
Santollo, Jessica; Katzenellenbogen, Benita S; Katzenellenbogen, John A et al. (2010) Activation of ER? is necessary for estradiol's anorexigenic effect in female rats. Horm Behav 58:872-7
Hartmaier, R J; Walenkamp, M J E; Richter, A S et al. (2009) A case of premature thelarche with no central cause or genetic variants within the estrogen receptor signaling pathway. J Pediatr Endocrinol Metab 22:751-8
Achari, Yamini; Lu, Ting; Katzenellenbogen, Benita S et al. (2009) Distinct roles for AF-1 and -2 of ER-alpha in regulation of MMP-13 promoter activity. Biochim Biophys Acta 1792:211-20
Stossi, Fabio; Madak-Erdogan, Zeynep; Katzenellenbogen, Benita S (2009) Estrogen receptor alpha represses transcription of early target genes via p300 and CtBP1. Mol Cell Biol 29:1749-59
Sengupta, Surojeet; Schiff, Rachel; Katzenellenbogen, Benita S (2009) Post-transcriptional regulation of chemokine receptor CXCR4 by estrogen in HER2 overexpressing, estrogen receptor-positive breast cancer cells. Breast Cancer Res Treat 117:243-51
Madak-Erdogan, Zeynep; Kieser, Karen J; Kim, Sung Hoon et al. (2008) Nuclear and extranuclear pathway inputs in the regulation of global gene expression by estrogen receptors. Mol Endocrinol 22:2116-27
He, Bin; Feng, Qin; Mukherjee, Atish et al. (2008) A repressive role for prohibitin in estrogen signaling. Mol Endocrinol 22:344-60

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