Abstract

Steroid receptors are gene regulatory proteins that provide an important model in eukaryotes to study gene transcription regulation. In recognition of the role of sex steroids in mammary cancer, study of progesterone regulated gene expression in T47D human breast cancer cells provides a relevant system with which to investigate regulatory mechanisms. Recently we, and others, have shown that in T47D cells, progestins regulate transcription directed by the mouse mammary tumor virus (MMTV) promoter/enhancer. We will exploit MMTV to investigate the fine structural details of the molecular interaction of human progesterone receptors (PR) with regulatory sequences. Toward this end we will (i) purify progesterone receptors using immunoaffinity methods and monoclonal antibodies that we have developed. PR will be purified in several forms: ligand-bound or unbound, transformed or untransformed, A and B receptors separately or together, complexed with heat shock proteins or free of this association. Heat shock proteins and another potential accessory protein, nuclear factor-one, will also be purified for these studies. These different receptor forms and potential accessory proteins will be employed (ii) to perform a detailed binding analysis with progesterone response elements from mouse mammary tumor virus. We will employ several types of assays including DNA-gel shift assays to quantitate binding affinities and association/dissociation rate constants of the various receptor forms with and without accessory proteins. (iii) A characterized library of mutant receptor recognition sequences will be examined for biological activity in T47D cells using a rapid, sensitive DNA-mediated gene transfer assay and a vector constructed expressly for this purpose. Specific binding parameters of the mutant receptor recognition sequences will be assayed in parallel. The expression and binding data with the mutant elements together will be used to assemble a map of the residues critical for receptor recognition and for hormone response. (iv) The induction by progestins of MMTV-directed gene expression will be utilized in a scheme to select for T47D cell variants resistant to progesterone action. Resistant cells will be characterized for the molecular basis of resistance by use of our anti-receptor monoclonal antibodies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA046938-02
Application #
3190443
Study Section
Biochemical Endocrinology Study Section (BCE)
Project Start
1988-02-01
Project End
1991-01-31
Budget Start
1989-02-01
Budget End
1990-01-31
Support Year
2
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Type
Schools of Medicine
DUNS #
065391526
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Elsarraj, Hanan S; Valdez, Kelli E; Hong, Yan et al. (2017) NEMO, a Transcriptional Target of Estrogen and Progesterone, Is Linked to Tumor Suppressor PML in Breast Cancer. Cancer Res 77:3802-3813
Grimm, Sandra L; Hartig, Sean M; Edwards, Dean P (2016) Progesterone Receptor Signaling Mechanisms. J Mol Biol 428:3831-49
Goswami, Devrishi; Callaway, Celetta; Pascal, Bruce D et al. (2014) Influence of domain interactions on conformational mobility of the progesterone receptor detected by hydrogen/deuterium exchange mass spectrometry. Structure 22:961-73
Balakrishnan, Ilango; Yang, Xiaodong; Brown, Joseph et al. (2014) Genome-wide analysis of miRNA-mRNA interactions in marrow stromal cells. Stem Cells 32:662-73
Simons Jr, S Stoney; Edwards, Dean P; Kumar, Raj (2014) Minireview: dynamic structures of nuclear hormone receptors: new promises and challenges. Mol Endocrinol 28:173-82
Wysoczynski, Christina L; Roemer, Sarah C; Dostal, Vishantie et al. (2013) Reversed-phase ion-pair liquid chromatography method for purification of duplex DNA with single base pair resolution. Nucleic Acids Res 41:e194
Kumar, Raj; Moure, Carmen M; Khan, Shagufta H et al. (2013) Regulation of the structurally dynamic N-terminal domain of progesterone receptor by protein-induced folding. J Biol Chem 288:30285-99
Hill, Krista K; Roemer, Sarah C; Churchill, Mair E A et al. (2012) Structural and functional analysis of domains of the progesterone receptor. Mol Cell Endocrinol 348:418-29
Buser, Adam C; Obr, Alison E; Kabotyanski, Elena B et al. (2011) Progesterone receptor directly inhibits ýý-casein gene transcription in mammary epithelial cells through promoting promoter and enhancer repressive chromatin modifications. Mol Endocrinol 25:955-68
Garza, Anna S; Khan, Shagufta H; Moure, Carmen M et al. (2011) Binding-folding induced regulation of AF1 transactivation domain of the glucocorticoid receptor by a cofactor that binds to its DNA binding domain. PLoS One 6:e25875

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