Abstract

Estrogen receptor-1 (ER) and progesterone receptor (PR) are ligand-induced transcription factors. Accessory proteins, termed coactivators modulate the transcriptional activation of these factors. It has been shown that coactivators enhance transcription of the target genes and play important roles in diverse pathological processes, such as cancers, inherited genetic diseases, metabolic disorders, and inflammation. Earlier work by our laboratory identified E6-associated protein (E6-AP) as a coactivator of steroid hormone receptors. In an attempt to identify E6-AP-interacting protein(s), we have cloned WW-domain binding protein-2 (WBP-2) and have shown that WBP-2 selectively coactivates the transactivation functions of ER and PR. WBP-2 is a novel polyproline rich (PPXY) motif containing protein. The PPXY motif of WBP-2 has been shown to be involved in transcriptional activation pathways. The PPXY motif interacts with WW-domain containing proteins and form PPXY motif and WW-domain (PPXY-WW) complex and mediates transcription stimulation. The PPXY-WW module has gained prominence in the last decade and many new roles of the PPXY-WW complex in the nucleus, cellular pathways, physiological and pathological processes are just emerging. WW-domains have been observed on several key regulatory proteins like yes associated protein (YAP1) and WW-domain- containing oxidoreductase (WWOX1). YAP1 has been shown to act as transcriptional coactivator for several transcription factors and has also been classified as an oncoprotein, whereas, WWOX1 has been identified as a tumor suppressor. Our preliminary data suggest that oncogenic YAP1 in conjunction with WBP-2 enhances ER and PR signaling. This increased in ER and PR signaling is attenuated by the tumor suppressor WWOX1 but the exact mechanism by which these proteins regulate transcription, cell function, growth and tumorigenesis is largely unknown. In order to understand the mechanism of action of these proteins and their physiological and pathological relevance, we hypothesize that the coactivation functions of oncoprotein YAP1 is dependent on WBP-2 where the WBP-2:YAP1 complex enhances ER and PR transactivation functions resulting in breast tumorigenesis. We further hypothesize that WWOX1 acts as a tumor suppressor by physically blocking the formation of this complex (WBP-2:YAP1) resulting in the attenuation of their coactivation and oncogenic functions. This hypothesis will be test by the following specific aims: A) To determine the role of WW-domain containing proteins, YAP1 and WWOX1 in ER and PR-mediated gene transcription;B) To decipher the mechanism by which WBP-2, YAP1 and WWOX1 regulate ER and PR transactivation functions;and C) To determine the role of WBP-2, YAP1 and WWOX1 in breast tumorigenesis.

Public Health Relevance

Estrogen and progesterone receptors are key regulatory proteins that affect many physiological and pathological processes such as reproduction, metabolism and cancer etc. Coactivators are proteins that regulate the functions of these receptor proteins and are also key players in the development of different types of cancers. Given these facts, the understanding of coactivator biology and their mechanism of action will be useful in developing new therapies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK079217-02
Application #
7752537
Study Section
Molecular and Cellular Endocrinology Study Section (MCE)
Program Officer
Margolis, Ronald N
Project Start
2009-01-01
Project End
2012-11-30
Budget Start
2009-12-01
Budget End
2010-11-30
Support Year
2
Fiscal Year
2010
Total Cost
$360,533
Indirect Cost

  Institution

Name
University of Miami School of Medicine
Department
Biochemistry
Type
Schools of Medicine
DUNS #
052780918
City
Coral Gables
State
FL
Country
United States
Zip Code
33146

  Publications

Abdeen, Suhaib K; Salah, Zaidoun; Khawaled, Saleh et al. (2013) Characterization of WWOX inactivation in murine mammary gland development. J Cell Physiol 228:1391-6
Buffa, Laura; Saeed, Ali M; Nawaz, Zafar (2013) Molecular mechanism of WW-domain binding protein-2 coactivation function in estrogen receptor signaling. IUBMB Life 65:76-84
McDonald, Caleb B; Buffa, Laura; Bar-Mag, Tomer et al. (2012) Biophysical basis of the binding of WWOX tumor suppressor to WBP1 and WBP2 adaptors. J Mol Biol 422:58-74
Tufail, Rozina; Jorda, Mercy; Zhao, Wei et al. (2012) Loss of Yes-associated protein (YAP) expression is associated with estrogen and progesterone receptors negativity in invasive breast carcinomas. Breast Cancer Res Treat 131:743-50
Abdeen, S K; Salah, Z; Maly, B et al. (2011) Wwox inactivation enhances mammary tumorigenesis. Oncogene 30:3900-6
Srinivasan, Sathish; Nawaz, Zafar (2011) E3 ubiquitin protein ligase, E6-associated protein (E6-AP) regulates PI3K-Akt signaling and prostate cell growth. Biochim Biophys Acta 1809:119-27
McDonald, Caleb B; McIntosh, Samantha K N; Mikles, David C et al. (2011) Biophysical analysis of binding of WW domains of the YAP2 transcriptional regulator to PPXY motifs within WBP1 and WBP2 adaptors. Biochemistry 50:9616-27
Drusco, Alessandra; Pekarsky, Yuri; Costinean, Stefan et al. (2011) Common fragile site tumor suppressor genes and corresponding mouse models of cancer. J Biomed Biotechnol 2011:984505
Aqeilan, R I; Calin, G A; Croce, C M (2010) miR-15a and miR-16-1 in cancer: discovery, function and future perspectives. Cell Death Differ 17:215-20