Abstract

. Dr. Williams' immediate career goal is to establish himself in the field of nuclear receptor signaling in cancer, with a longer term goal of establishing a career in cancer research focusing on the cross talk between signal transduction pathways as it pertains to cellular signaling in cancer. In conjunction with his previous experience in receptor tyrosine kinase signaling, the proposed research plan will arm Dr. Williams with a well rounded and comprehensive skill set to launch his career as an independent scientist. In addition to laboratory research, Dr. Williams will participate in research focus groups, with which he'll discuss pertinent scientific issues, and present data regularly. Furthermore, he will present his findings at national and local scientific meetings. Tulane Cancer Center facilities will be at Dr. Williams' disposal, and the expertise of tenured faculty to help guide his research. ? ? Dr. Williams will study the therapeutic, prognostic and mechanistic aspects of ER( phosphorylation at 4 newly identified sites. Preliminary results show a dramatic impact of these sites on transcriptional activity of ER(. This proposal hypothesizes that novel phosphorylation sites identified in ER( (at serines 47, 282, 294, and 559) will impact tamoxifen effects on growth of tamoxifen-sensitive and -resistant breast cancer cells through mechanisms that alter ER( transcriptional activity.
Aim 1 will test the hypothesis that ER( phosphorylation at S47, S282, S294, and S559 regulates ER( transcriptional activity, growth of breast cancer cells in culture, and in vivo tumor formation, Aim 2 will identify the kinase signaling pathways that regulate ER( phosphorylation.
Aim 3 will mechanistically address how ER( phosphorylation at serines S47, S282, S294, S559 regulates ER( activation in response to ligand including ER( dimerization, DNA binding and coregulator recruitment.
Aim 4 will ascertain the clinical significance of ER( phosphorylation at serine 47, 282, 294, and 559 in primary breast tumors (IHC staining). ? ? Relevance. Characterization of novel ER( phosphorylation sites will lead to a better understanding of the mechanisms underlying therapeutic resistance in breast cancer. Furthermore these studies may lead to improved therapeutic regimens for breast cancer patients, by targeting kinases associated with resistance. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Scientist Development Award - Research & Training (K01)
Project #
1K01CA129078-01
Application #
7300013
Study Section
Subcommittee G - Education (NCI)
Program Officer
Ojeifo, John O
Project Start
2007-09-14
Project End
2012-08-31
Budget Start
2007-09-14
Budget End
2008-08-31
Support Year
1
Fiscal Year
2007
Total Cost
$93,018
Indirect Cost

  Institution

Name
Tulane University
Department
Biology
Type
Schools of Medicine
DUNS #
053785812
City
New Orleans
State
LA
Country
United States
Zip Code
70118

  Publications

Llopis, Shawn; Singleton, Brittany; Duplessis, Tamika et al. (2013) Dichotomous roles for the orphan nuclear receptor NURR1 in breast cancer. BMC Cancer 13:139
Williams, Christopher C; Singleton, Brittany A; Llopis, Shawn D et al. (2013) Metformin induces a senescence-associated gene signature in breast cancer cells. J Health Care Poor Underserved 24:93-103
Duplessis, Tamika T; Williams, Christopher C; Hill, Steven M et al. (2011) Phosphorylation of Estrogen Receptor ýý at serine 118 directs recruitment of promoter complexes and gene-specific transcription. Endocrinology 152:2517-26
Skliris, George P; Rowan, Brian G; Al-Dhaheri, Mariam et al. (2009) Immunohistochemical validation of multiple phospho-specific epitopes for estrogen receptor alpha (ERalpha) in tissue microarrays of ERalpha positive human breast carcinomas. Breast Cancer Res Treat 118:443-53
Williams, Christopher C; Basu, Aninda; El-Gharbawy, Abeer et al. (2009) Identification of four novel phosphorylation sites in estrogen receptor alpha: impact on receptor-dependent gene expression and phosphorylation by protein kinase CK2. BMC Biochem 10:36