Abstract

It has been determined that the overall conformation of nuclear receptors is influenced by the nature of the ligand to which they bind and that the resulting differences in conformation enable the differential recruitment of cofactors. Despite these accepted concepts, it still remains to be determined (a) which receptor surfaces are responsible for each biological activity and (b) how these surfaces function mechanistically. I have identified one such surface, a unique stretch of proline residues located towards the N-terminus of AR, that is necessary for maximal AR-mediated growth and the regulation of select androgen target genes. The long-term goal of the candidate is to develop novel therapeutic approaches for endocrine maladies. The primary goal of this proposal is to use a combination of bioinformatics and molecular biology to define the specific role(s) of the AR polyproline domain and two identified proteins that interact with this specific surface. These goals will be achieved using the superb research environment at Duke University Medical Center within both the Department of Pharmacology and Cancer Biology and the Duke Institute of Genome Sciences and Policy. To accomplish these goals the following specific aims are proposed:
Aim 1 : Determine the role of the polyproline domain within AR in androgen-regulated biological processes.
Aim 2 : Identify and validate the specific signaling pathways elicited by AR and its polyproline domain that drive cellular effects such as growth, migration, and actin reorganization.
Aim 3 : Evaluate the impact of genetic modification of the AR polyproline domain and its cofactors, SH3YL1 and Lyn kinase, on the activity of selective androgen receptor modulators (SARMs). This work will provide a definitive assessment of the role of the polyproline domain in AR biology and advance our basic understanding of AR signaling. Insights from this work will facilitate mechanism-based screens for the development of compounds, SARMs, with useful tissue-selective activities.

Public Health Relevance

It is anticipated this project will contribute to the knowledge base needed to develop pharmacological strategies that can selectively modulate androgen-regulated actions. At the conclusion of these studies we will be able to directly link a specific biological process to a particular AR-cofactor interaction. This new information will be invaluable for the future design of AR ligands.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
1K01DK084205-01
Application #
7708419
Study Section
Diabetes, Endocrinology and Metabolic Diseases B Subcommittee (DDK)
Program Officer
Hyde, James F
Project Start
2009-07-01
Project End
2010-06-30
Budget Start
2009-07-01
Budget End
2010-06-30
Support Year
1
Fiscal Year
2009
Total Cost
$105,538
Indirect Cost

  Institution

Name
Duke University
Department
Pharmacology
Type
Schools of Medicine
DUNS #
044387793
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Blessing, Alicia M; Ganesan, Sathya; Rajapakshe, Kimal et al. (2015) Identification of a Novel Coregulator, SH3YL1, That Interacts With the Androgen Receptor N-Terminus. Mol Endocrinol 29:1426-39
Tennakoon, J B; Shi, Y; Han, J J et al. (2014) Androgens regulate prostate cancer cell growth via an AMPK-PGC-1?-mediated metabolic switch. Oncogene 33:5251-61
Augello, Michael A; Burd, Craig J; Birbe, Ruth et al. (2013) Convergence of oncogenic and hormone receptor pathways promotes metastatic phenotypes. J Clin Invest 123:493-508
Shi, Yan; Han, Jenny J; Tennakoon, Jayantha B et al. (2013) Androgens promote prostate cancer cell growth through induction of autophagy. Mol Endocrinol 27:280-95
Bratton, Melyssa R; Frigo, Daniel E; Segar, H Chris et al. (2012) The organochlorine o,p'-DDT plays a role in coactivator-mediated MAPK crosstalk in MCF-7 breast cancer cells. Environ Health Perspect 120:1291-6
Bratton, Melyssa R; Antoon, James W; Duong, Bich N et al. (2012) Gýýo potentiates estrogen receptor ýý activity via the ERK signaling pathway. J Endocrinol 214:45-54
Frigo, Daniel E; Howe, Matthew K; Wittmann, Bryan M et al. (2011) CaM kinase kinase beta-mediated activation of the growth regulatory kinase AMPK is required for androgen-dependent migration of prostate cancer cells. Cancer Res 71:528-37