Abstract

The vast majority of human breast cancers are initially hormone-dependent with estradiol playing a crucial role in their development and evolution (1). However there is relatively little known about how estrogen activation of the estrogen receptor (ER) results in the initiation or promotion of human breast cancer. We have identified a novel gene that is down regulated by estradiol, Estrogen-Down-regulated Gene 1 (EDG1), in breast epithelial cells. Subsequent studies indicate that EDG1 inhibits ERalpha transcriptional activity. A self-contained tetracycline-regulated retroviral vector system (2) has been used to both positively and negatively regulate the expression of EDG1 in breast cancer cells (MCF7 and MDA-MB-231) and normal breast cells (MCF 10A). Compared to control cells, cells that over express EDG 1 (MCF7-EDG 1, MCF 10-EDG1 and MDA-MB-23 1-EDG1) exhibit decreased growth rate, while cells that have decreased EDG1 expression (MCF7-EDG1AS and MCF10-EDG1AS) have enhanced growth rate. Moreover EDG1 overexpression inhibited anchorage independent growth and estrogen-induced MCF7 proliferation. While we see cross talk between estrogen and EDG1, we propose that EDG1 may also function as a tumor suppressor independent of ERa levels. A mechanistic basis for the growth effect of EDG1 is suggested by the interaction of EDG1 with Integrin beta4-interactor protein (p27/BBP) and the 67 kD laminin receptor (67LR). p27/BBP protein interacts with the cytodomain of beta4 integrin and has been proposed to link beta4 integrin with the cytoskeleton, while 67LR binds to laminins and interacts with the alpha6beta4 integrin multimeric complex. Based on our preliminary findings we hypothesize that the growth inhibitory effects of EDG1 in breast cells have ERalpha-dependent and ERalphs-independent components; and EDG1 helps maintain the balance of signaling events generated through the extracellular matrix that regulates normal breast epithelial cell function. To test our hypothesis we will: (1) characterize EdG1 inhibition of ERalpha transcriptional activity and its role in the growth inhibitory effects of EDG1 (2) examine the role of Integrin-beta4-interactor protein and the 67 kD laminin receptor in EDG1 cellular effects and (3) characterize other phenotypic effects of EDG1 and identification of other downstream effectors of EDG1.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA092440-02
Application #
6624250
Study Section
Reproductive Endocrinology Study Section (REN)
Program Officer
Woodhouse, Elizabeth
Project Start
2002-04-01
Project End
2007-03-31
Budget Start
2003-04-01
Budget End
2004-03-31
Support Year
2
Fiscal Year
2003
Total Cost
$290,700
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Pharmacology
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Vazquez, Edwin J; Berthiaume, Jessica M; Kamath, Vasudeva et al. (2015) Mitochondrial complex I defect and increased fatty acid oxidation enhance protein lysine acetylation in the diabetic heart. Cardiovasc Res 107:453-65
Yeh, I-Ju; Song, Kyung; Wittmann, Bryan M et al. (2014) HEXIM1 plays a critical role in the inhibition of the androgen receptor by anti-androgens. Biochem J 462:315-27
Zhong, Bo; Lama, Rati; Ketchart, Wannarasmi et al. (2014) Lead optimization of HMBA to develop potent HEXIM1 inducers. Bioorg Med Chem Lett 24:1410-3
Yeh, I-Ju; Ogba, Ndiya; Bensigner, Heather et al. (2013) HEXIM1 down-regulates hypoxia-inducible factor-1? protein stability. Biochem J 456:195-204
Ketchart, W; Smith, K M; Krupka, T et al. (2013) Inhibition of metastasis by HEXIM1 through effects on cell invasion and angiogenesis. Oncogene 32:3829-39
Montano, Monica M; Desjardins, Candida L; Doughman, Yong Qui et al. (2013) Inducible re-expression of HEXIM1 causes physiological cardiac hypertrophy in the adult mouse. Cardiovasc Res 99:74-82
Krishnamurthy, Nirmala; Hu, Yanduan; Siedlak, Sandra et al. (2012) Induction of quinone reductase by tamoxifen or DPN protects against mammary tumorigenesis. FASEB J 26:3993-4002
Montano, Monica M; Krishnamurthy, Nirmala; Sripathy, Smitha (2012) TARGETING THE GENOTOXIC EFFECTS OF ESTROGENS. Drug Discov Today Dis Mech 9:e29-e33
Ketchart, W; Ogba, N; Kresak, A et al. (2011) HEXIM1 is a critical determinant of the response to tamoxifen. Oncogene 30:3563-9
Smith, Kerri M; Ketchart, Wannarasmi; Zhou, Xiang et al. (2011) Determination of hexamethylene bisacetamide, an antineoplastic compound, in mouse and human plasma by LC-MS/MS. J Chromatogr B Analyt Technol Biomed Life Sci 879:2206-12

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