Epidemiological studies and clinical observations suggest that persistent chronic inflammation is important in prostate carcinogenesis. The chronic inflammatory lesions frequently observed in prostate tissue biopsies and radical prostatectomy specimens are consequence to the aging process and precursor to prostate cancer development. These findings are supported by the reports that long-term use of anti-oxidant decreases the risk of prostate cancer. Members of the FOX family group 'O'control important network of genes that influence cell proliferation, inflammation, repair DNA damage, and oxidants/antioxidants balance. In the absence of growth signal, the FOXO family members remain transcriptionally active in the nucleus. Upon stimulus via PI3K-Akt pathway, FOXO proteins are phosphorylated and translocates to the cytoplasm, abrogating its transcriptional activity. We have recently demonstrated (Submitted in the Late- Breaking Session at the Annual Meeting of American Association for Cancer Research, 2008 and as preliminary data in the proposal) deregulation and redistribution of FOXO proteins in the cellular compartments in human prostate cancer cell lines and tissues. Furthermore, levels of FOXO3A were significantly higher in the cytosolic fraction than the nucleus as a function of age and disease progression. Hyperactivation of Akt causes increased Foxo3a binding with 14-3-3 and its accumulation in the cytoplasm of TRAMP mice prostates, compared to non-transgenic littermates at 20-28 weeks of age. This decreased Foxo3a levels correlated with downregulation of the basal levels of p21/WAF1, MnSOD and Cu/ZnSOD in the prostates of TRAMP mice thereby shifting the oxidants/antioxidants balance towards increased oxidative stress and cancer progression. Based on these interesting findings we suggest FOXO signaling pathway as a key molecular target for the development of preventive strategies against prostate cancer. The present proposal capitalizes on these novel findings and is designed to investigate the cancer preventive potential of apigenin, a plant flavonoid present in common fruits and vegetables, by targeting FOXO signaling pathway. This proposal will employ TRAMP model which is an appropriate animal model to test our working hypothesis as it mimics progressive forms of human prostatic disease. Validation of this hypothesis may have implications for prostate cancer in humans.

Public Health Relevance

Our long-term goal is to develop apigenin, a plant flavonoid present in common fruits and vegetables, as preventive agent for prostate cancer. Recent studies suggest a plausible link between aging, inflammation and prostate cancer. In fact, men approaching to sixties and seventies observe a sharp rise in the incidence of prostate cancer. The age-related increase in intraprostatic inflammatory lesions is considered as a significant risk factor in the development prostate cancer. Supportive evidence suggests long-term use of antioxidants decrease the risk of prostate cancer. Some of the genes play dominant role in regulating oxidant/antioxidant balance;one of such is transcription factor Forkhead box O (FOXO) that is critical in modulating the expression of genes involved in cell growth, proliferation, differentiation, DNA damage repair, and longevity. Deregulation of FOXO family members has been implicated in the pathogenesis of several human malignancies. Our recent studies (Submitted in the Late- Breaking Session at the Annual Meeting of American Association for Cancer Research, 2008 and preliminary data in the proposal) have shown that deregulation and redistribution of FOXO3A in the sub-cellular compartments in various human prostate cancer cell lines; transgenic adenocarcinoma of the mouse prostate (TRAMP) model and human prostate cancer specimens correlates with disease progression. Based on these interesting findings, we suggest FOXO-signaling pathway as a key molecular target for the development of preventive strategies against prostate cancer. The present proposal capitalizes on these novel findings and will investigate the cancer preventive potential of apigenin by targeting FOXO transcription pathway employing TRAMP model which emulates human prostatic disease.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Small Research Grants (R03)
Project #
5R03CA137667-02
Application #
7894678
Study Section
Special Emphasis Panel (ZCA1-SRLB-F (M1))
Program Officer
Kim, Young S
Project Start
2009-07-16
Project End
2012-06-30
Budget Start
2010-07-01
Budget End
2012-06-30
Support Year
2
Fiscal Year
2010
Total Cost
$78,500
Indirect Cost
Name
Case Western Reserve University
Department
Urology
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106
Shukla, Sanjeev; Bhaskaran, Natarajan; Babcook, Melissa A et al. (2014) Apigenin inhibits prostate cancer progression in TRAMP mice via targeting PI3K/Akt/FoxO pathway. Carcinogenesis 35:452-60
Shukla, Sanjeev; MacLennan, Gregory T; Fu, Pingfu et al. (2012) Apigenin attenuates insulin-like growth factor-I signaling in an autochthonous mouse prostate cancer model. Pharm Res 29:1506-17
Shukla, Sanjeev; Gupta, Sanjay (2010) Apigenin: a promising molecule for cancer prevention. Pharm Res 27:962-78