nardulli@life.illinois.edu
513 Burrill Hall
Office: (217) 244-5679
Lab: (217) 244-6143
Fax: (217) 333-1133
Mail to:
Department of Molecular and Integrative Physiology
524 Burrill Hall
407 S. Goodwin Ave
Urbana, IL 61801
Ann M Nardulli
Professor of Molecular and Integrative Physiology
Education
B.S. 1970 Northern Illinois University
M.S. 1984 University of Illinois
PhD. 1987 University of Illinois
Postdoc. 1987-92 University of Illinois
Teaching Interests
Regulation of estrogen-responsive genes
The estrogen receptor mediates the effects of estrogens and antiestrogens in target cells by binding of the receptor to specific DNA sequences present in target genes. This interaction of the estrogen receptor with DNA plays a critical role in development and maintenance of reproductive, cardiovascular, neural, and skeletal cells. Although the receptor-DNA interaction is of paramount importance in the regulation of estrogen-responsive genes, the mechanism by which this interaction leads to changes in gene expression is not well understood.
Our laboratory uses in vitro and in vivo assays to examine the interaction of the estrogen receptor with DNA in order to define mechanisms involved in regulating estrogen-responsive genes. We have demonstrated that the ability of the estrogen receptor to activate transcription is related to its ability to induce directed DNA bending suggesting that DNA bending may facilitate receptor-protein contacts required for transcription activation. We have also demonstrated that the conformation of the estrogen receptor is different when bound to slightly different recognition sequences in DNA. Our findings support the idea that the estrogen receptor is comprised of a large repertoire of functional surfaces that can be formed and serve as contact points for other cellular proteins. The presentation of these functional surfaces and the selection of receptor-associated proteins, which is dictated by a unique DNA sequence, may provide the regulatory versatility required for differential expression of multiple estrogen-responsive genes in a single cell. Taken together, our studies imply that receptor-DNA interaction is a dynamic process involving conformational changes in both receptor and DNA.
Using newly developed, highly sensitive molecular biology techniques, we are examining endogenous, estrogen-responsive genes in intact human breast cancer cells to define how chromatin structure plays a role in estrogen- and antiestrogen- regulated gene transcripion. Understanding the mechanisms by which estrogen agonists and antagonists modulate gene expression is particularly important in light of the fact that these compounds are widely used in hormone replacement therapy and in breast cancer treatment and prevention.
Representative Publications
Schultz-Norton, J.R., McDonald, W.H., Yates J.R., and Nardulli, A.M. 2006. Protein disculfide isomerase serves as a molecular chaperone to maintain estrogen receptor alpha structure and function. Mol Endocrinol, 20(9):1982–95. [Abstract]
Schultz, J.R., Petz, L.N., and Nardulli, A.M. 2005. Cell and ligand specific regulation of promoters containing activator protein 1 and Sp1 sites by estrogen receptors alpha and beta. J Biol Chem, 280(1):347–54. [Abstract]
Loven, M.A., Davis, R.E., Muster, N., Yates, J.R., and Nardulli, A.M. 2004. A novel estrogen receptor alpha associated protein alters receptor DNA interactions and represses receptor mediated transcription. Mol Endocrinol., 18(11):2649–59. [Abstract]
Likhite, V.S., Cass, E.I., Anderson, S.D., Yates, J.R., and Nardulli, A.M. 2004. Interaction of estrogen receptor alpha with 3-methyladenine DNA glycosylase modulates transcription and DNA repair. J Biol Chem, 279(16):16875–82. [Abstract]
Petz, L.N., Ziegler, Y.S., Schultz, J.R., and Nardulli, A.M. 2004. Fos and Jun inhibit estrogen-induced transcription of the human progesterone receptor gene through an activator protein-1 site. Mol Endocrinol, 18(3):521–32. [Abstract]
Petz, L.N., Ziegler, Y.S., Schultz, J.R., Kim, H., Kemper, J., and Nardulli, A.M. 2004. Differential regulation of the human progesterone receptor gene by an estrogen response element half site and Sp1 sites. J Steroid Biochem Mol Biol, 88(2):113–22. [Abstract]
Schultz, J.R., Petz, L.N., and Nardulli, A.M. 2003. Estrogen receptor alpha and Sp1 regulate progesterone receptor gene expression. Mol Cell Endocrinol, 201(1–2):165–75. [Abstract]
Loven, M., Muster, N., Yates, J.R., and Nardulli, A.M. 2003. A novel estrogen receptor alpha associated protein, template activating factor I beta, inhibits acetylation and transactivation. Mol Endocrinol, 17(1):67–78. [Abstract]