Abstract

Hypoxia is a key regulatory microenvironmental factor capable of influencing tumor development and progression. Hypoxia is usually considered a global phenomenon, defined as an overall reduced oxygen availability or partial pressure below critical levels. Tumor vasculature, however, is architecturally and functionally abnormal. The tissue oxygenation/blood flow within a tumor is dynamically changing and heterogeneous at the microenvironmental level. Hypoxia has been proposed to functions as a microenvironmental pressure to select for a fraction of hypoxia-resistant cancer cells with an increased ability to survive and progress. Peroxiredoxins(Prxs) are a newly described family of redox-controlling proteins. Two highly homologous members of this protein family, Prx1 and Prx2, have been shown to affect cell survival and increase stress resistance. However, little is known about the effects of Prx elevation in human cancers, their influence on malignant progression and treatment response, or the regulatory mechanisms. Our preliminary studies provide compelling evidences to support the functional relevance of hypoxiaand Prx1 (but not Prx2) in enhancing the AR function, and suppressing apoptotic signaling. In this study, we will systematically investigate """"""""why""""""""and """"""""how"""""""" Prx1 is elevate in prostate cancer cells at the microenvironmentallevel, and study the effect of tissue oxygenation status and Prx1level in modifying the cancer control efficacy of finasteride and selenium. We hypothesize that dynamic changes of tissue oxygenation up-regulate Prx1 expression via redox-sensitive transcription factors, and the dysregulated activation of these transcription factors leads to Prx1 elevation in a subset of prostate cells within a tumor. We also hypothesize that elevated Prx1 confers an aggressive survival phenotype to cells by enhancing AR activity, and reducing oxidative damage and apoptosis. We correspondingly hypothesize that inhibition of Prx1 will increase the AR signaling suppressive and cancer control efficacy of finasteride and selenium. In order to test these hypotheses, four specific aims are proposed.
In Aim 1, we will define the molecular basis of Prx1 up-regulation in prostate cancer cells.
In Aim 2, we will elucidate the mechanisms whereby Prx1 enhances AR function.
In Aim 3 and Aim 4, we will systematically investigate whether and how Prx1 modifies the cancer control efficacy of finasteride and selenium in the context of a hypoxic tumor microenvironment. These studies will provide a sound scientific basis upon which the regulation and function of Prx1 can be elucidated in prostate cancer, enabling the development of novel preventive approaches to inhibit its malignant progression.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA126804-03
Application #
7930595
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
3
Fiscal Year
2009
Total Cost
$304,113
Indirect Cost

  Institution

Name
Roswell Park Cancer Institute Corp
Department
Type
DUNS #
824771034
City
Buffalo
State
NY
Country
United States
Zip Code
14263

  Publications

Ondracek, Rochelle Payne; Kattan, Michael W; Murekeyisoni, Christine et al. (2016) Validation of the Kattan Nomogram for Prostate Cancer Recurrence After Radical Prostatectomy. J Natl Compr Canc Netw 14:1395-1401
Cheng, J; Ondracek, R P; Mehedint, D C et al. (2015) Association of fatty-acid synthase polymorphisms and expression with outcomes after radical prostatectomy. Prostate Cancer Prostatic Dis 18:182-9
Payne Ondracek, Rochelle; Cheng, Jinrong; Gangavarapu, Kalyan J et al. (2015) Impact of devascularization and tissue procurement on cell number and RNA integrity in prostatectomy tissue. Prostate 75:1910-5
Fiandalo, Michael V; Wu, Wenjie; Mohler, James L (2013) The role of intracrine androgen metabolism, androgen receptor and apoptosis in the survival and recurrence of prostate cancer during androgen deprivation therapy. Curr Drug Targets 14:420-40
Chhipa, Rishi Raj; Halim, Danny; Cheng, Jinrong et al. (2013) The direct inhibitory effect of dutasteride or finasteride on androgen receptor activity is cell line specific. Prostate 73:1483-94
Wu, Yue; Godoy, Alejandro; Azzouni, Faris et al. (2013) Prostate cancer cells differ in testosterone accumulation, dihydrotestosterone conversion, and androgen receptor signaling response to steroid 5?-reductase inhibitors. Prostate 73:1470-82
Wu, Yue; Chhipa, Rishi Raj; Zhang, Haitao et al. (2011) The antiandrogenic effect of finasteride against a mutant androgen receptor. Cancer Biol Ther 11:902-9
Chhipa, Rishi Raj; Wu, Yue; Ip, Clement (2011) AMPK-mediated autophagy is a survival mechanism in androgen-dependent prostate cancer cells subjected to androgen deprivation and hypoxia. Cell Signal 23:1466-72
Zhang, Haitao; Fang, Jian; Yao, Dian et al. (2010) Activation of FOXO1 is critical for the anticancer effect of methylseleninic acid in prostate cancer cells. Prostate 70:1265-73
Cheng, Jinrong; Wu, Yue; Mohler, James L et al. (2010) The transcriptomics of de novo androgen biosynthesis in prostate cancer cells following androgen reduction. Cancer Biol Ther 9:1033-42

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