MicroRNA regulation of prostate cancer desensitization to androgen receptor antagonist drugs during androgen deprivation therapy

Lorch, Robert A.

01 May 2011

The current standard treatment of prostate cancer by androgen deprivation therapy involves using drugs such as bicalutamide (Casodex) to antagonistically block androgen receptors that are normally present within prostate cells. Usually, the therapy is successful in the short run at limiting the growth of prostate cancer. However, in virtually all cases tumors begin to grow aggressively again after several months of treatment and new therapies must be started. The mechanism by which these prostate cells transform from androgen sensitive to androgen independent and anti-androgen resistant is unclear. In this study, we investigated the role of microRNAs, small 15 to 18 nucleotide regulatory RNAs, in regulating the desensitization of prostate cancer cells to the androgen receptor antagonist drug bicalutamide. In order to identify significant microRNAs, quantitative PCR was used to obtain genome-wide microRNA expression levels of 885 human microRNAs at different timepoints for androgen sensitive LNCaP cancer cells treated with bicalutamide and for untreated control cells in tissue culture. Analysis of microRNA expression by clustering analysis and by statistical comparisons of treatment groups resulted in identification of 28 microRNAs that have altered expression in the progression process. In silico target prediction analysis was performed with the microRNAs shown to have altered expression, and a group of genes predicted to be under microRNA regulatory control during cancer progression to resistance was identified. A microRNA expression profile can be useful in developing more effective prognostic and therapeutic tools for prostate cancer.

Molecular Biology

Screening for Anticancer Agents to Inhibit Mitotic Kinases and Proliferation of Metastatic Prostate Cancer Cells

Nguyen, Khoa

01 January 2016

Current treatments for prostate cancer (PCa) are marred with high relapse frequency and development of progressively aggressive cancers; developing new treatment options for PCa remains crucial. In this project, a series of synthetic compounds based on natural products will be screened to identify inhibitors for Aurora-A kinase (Aur-A). Aur-A facilitates centrosome separation and bipolar spindle formation during mitosis. Aur-A is overexpressed in metastatic PCa cells, and is a good candidate for targeted therapies. Compound libraries are designed using natural compounds that contain simple structural elements as starting points for developing drug like libraries. High-throughput screening of these libraries will be used to identify potent antimitotic agents that selectively affect cancer cells but not normal cells. A combination of in vitro protein assays – quantifying protein activity – cell-based assays – measuring cell growth and proliferation – and cell-reporter assays – to determine which metabolic pathway the compound affects – were used to identify potential inhibitors. Through these methods, we have identified several compounds, with special consideration to thiazole piperazine compounds, to successfully inhibit proliferation of metastatic PCa cells.

Aurora-A Kinase

Drug Screening

Prostate Cancer

Lipinski

Metastatic

Cancer Biology

A Novel Drug to Induce Apoptosis in Advanced Prostate Cancer Cells

Sanghvi, Parshva A

01 January 2022

Prostate cancer is one of the leading causes of death for men in America as approximately 1 in 41 men will have prostate cancer. In this research, we focus on enzalutamide-resistant prostate cancer cells as cell resistance to enzalutamide is a prevalent obstacle in treating prostate cancer. We tested a novel compound library at different doses and observed each compound's efficacy in inducing apoptosis in enzalutamide-resistant cells. Furthermore, we analyzed the mechanism by which apoptosis was induced in compounds that showed a high efficacy at lower doses. Overall, we found that Darapladib shows promising results in treating cells that have acquired enzalutamide resistance.

Advanced Prostate Cancer

Novel Compounds

Compound Screening

Cancer Biology

Expression of Oncogenic Antigen 519 (OA-519) in Prostate Cancer Is a Potential Prognostic Indicator

Shurbaji, M. S., Kuhajda, F. P., Pasternack, G. R., Thurmond, T. S.

01 May 1992

Predicting the prognosis of patients with prostate cancer is a clinically important problem. Previous studies have indicated that the expression of haptoglobin-related protein epitopes in samples of breast cancer in early stages was associated with earlier relapses and higher risk for tumor recurrence. Oncogenic antigen 519 (OA-519) is the new marker designation for molecules expressing haptoglobin-related protein epitopes. The objective of this immunohistochemical study was to examine OA-519 expression in prostate cancer samples and its relationship to the established prognostic indicators of tumor grade, tumor volume, and clinical stage. Forty-two consecutive tissue samples of prostate adenocarcinoma were examined using an affinity- purified anti-OA-519 antibody. Twenty specimens (48%) tested positive, whereas 22 (52%) tested negative. No staining was observed in normal or hyperplastic prostate tissue. Staining occurred in 6 of 9 (67%) grade III, 14 of 23 (61%) grade II, and in none of 10 (0%) grade I cases (I vs. II and/or III: Fisher exact test, P < 0.006). Twenty-three of the 42 samples were transurethral resection specimens with cancer; 11 (48%) of these tested positive. The mean percentage of tissue chips with tumor, a measure of tumor volume, was significantly higher in the positive group (57%) than in the negative group (15%) (P = 0.004). The proportion of positively stained cases increased with advancing clinical stage, with 25% of Stage A cases expressing OA-519, and 46%, 67%, and 64% of Stages B, C, and D, respectively, expressing OA-519. OA-519 expression correlates with higher tumor grades, larger tumors, and possibly with advanced stage, and thus, it is potentially of prognostic value in prostate cancer.

haptoglobin-related protein

immunohistochemistry

OA- 519

prognosis

prostate adenocarcinoma

Pathology

ON-LINE RE-OPTIMIZATION OF PROSTATE IMRT PLAN FOR ADAPTIVE RADIATION THERAPY – A FEASIBILITY STUDY AND IMPLEMENTATION

Thongphiew, Danthai

January 2008

No description available.

Dose

Registration

PROSTATE

IMRT

MLC

RADIATION THERAPY

dose distribution

Implications for XMRV Infections in Prostate Cancer

Hong, Seunghee

23 January 2010

No description available.

Molecular Biology

Virology

XMRV

SEVI

XPR1

prostate cancer

IL-8

Targeting Prostate Cancer by Small Molecules

Zhang, Jian

January 2011

No description available.

Cellular Biology

prostate cancer

androgen receptor

AR

drug discovery

Human Prostate Cancer Cell Apoptosis Induced by Interferon-γ and Double-Stranded RNA and Studies on the Biological Roles of Transmembrane and Coiled-Coil Domains 1

Tan, Haiyan

23 August 2010

No description available.

Molecular Biology

Interferon

Double-stranded RNA

Prostate cancer

Apoptosis

TMCO1

Evaluating XMRV As An Indicator Of Prostate Cancer Risk

Barton, Maria

12 July 2011

No description available.

Biomedical Research

Prostate cancer

XMRV

envelope protein

amplicon

Mechanisms Underlying the Link Between Obesity and Neoplastic Progression

Liu, Jehnan

20 May 2010

No description available.

Biomedical Research

CEACAM1

prostate

PTEN

obesity

high fat

cancer

PIN