Abstract

Prostate cancer is the second leading cause of cancer related deaths for men in the U.S. A common therapy for early stage prostate cancer (after failure of surgery or radiation therapy) is androgen hormone deprivation therapy which blocks the production of androgens that are known to foster the progression of prostate cancer. While initially effective for about 80% of newly diagnosed cases, most prostate cancer patients develop resistance to hormone deprivation therapy within three years and progress to castration resistant prostate cancer (CRPC), and become metastatic. There has been a major focus on the androgen receptor (AR) pathway as the principal therapeutic target for CRPC including recent approved therapies such as abiraterone and enzalutamide. Despite these advances that provide temporary respite, there is still no cure for CRPC. Ultimately, all patients will go on to die from progressive and resistant prostate cancer. Therefore, there is a pressing need to identify the pathways that perpetuate disease progression during effective AR blockade. NF-KB functions as a master transcription factor that activates inflammatory cytokines/chemokines and underpins the synthesis of genes implicated in cell survival and chemo resistance, angiogenesis and localized invasion. The non-canonical NF-KB pathway involves the processing of p100 to p52. Overproduction of p52 has been observed in several solid tumors including breast and prostate cancers. We have recently demonstrated that p52 protein is anti-apoptotic to CaP cells and promotes survival upon treatment with androgen deprivation or with chemotherapeutic agents. p52 interacts with AR and increases AR activation and androgen regulated PSA and NKX3.1 expression. We propose that activation of p52 signaling will activate resistance pathways in the CRPC microenvironment and thus attenuates therapeutic response to anti-androgen therapy. The goals of the application are two folds: to determine the roles of p52 in AR activation and CRPC progression, and to evaluate p52 activation in promoting a microenvironment-wide mechanism of resistance to the novel AR antagonist, enzalutamide.
The specific aims of this proposal are: 1) Determine the functional roles of p52 in CRPC progression. 2) Determine the effects of p52 on modulating treatment response to novel anti-androgen therapeutics in CRPC models. Characterization of these additional resistance-promoting pathways will identify the appropriate complementary approaches that can be used to increase the magnitude and duration of benefit of androgen deprivation therapies such as enzalutamide which will dramatically impact the care of men with CRPC.

Public Health Relevance

Targeting androgen signaling via androgen deprivation therapy has been the mainstream of clinical interventions in prostate cancer. Recent FDA approved new anti- androgen agents such as enzalutamide only slightly improve median overall survival. There is an urgent need to identify the pathways that perpetuate disease progression during effective AR blockade. Identification of these additional resistance pathways will help to design co-targeting strategies to improve the magnitude and duration of benefit of enzalutamide in men with CRPC.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21CA179970-01
Application #
8590098
Study Section
Special Emphasis Panel (ZCA1-GRB-I (M1))
Program Officer
Alley, Michael C
Project Start
2013-09-12
Project End
2015-08-31
Budget Start
2013-09-12
Budget End
2014-08-31
Support Year
1
Fiscal Year
2013
Total Cost
$200,970
Indirect Cost
$70,470

  Institution

Name
University of California Davis
Department
Urology
Type
Schools of Medicine
DUNS #
047120084
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Liu, Chengfei; Lou, Wei; Yang, Joy C et al. (2018) Proteostasis by STUB1/HSP70 complex controls sensitivity to androgen receptor targeted therapy in advanced prostate cancer. Nat Commun 9:4700
Lombard, Alan P; Liu, Liangren; Cucchiara, Vito et al. (2018) Intra versus Inter Cross-resistance Determines Treatment Sequence between Taxane and AR-Targeting Therapies in Advanced Prostate Cancer. Mol Cancer Ther 17:2197-2205
Liu, Chengfei; Armstrong, Cameron M; Lou, Wei et al. (2017) Niclosamide and Bicalutamide Combination Treatment Overcomes Enzalutamide- and Bicalutamide-Resistant Prostate Cancer. Mol Cancer Ther 16:1521-1530
Liu, Chengfei; Armstrong, Cameron M; Lou, Wei et al. (2017) Inhibition of AKR1C3 Activation Overcomes Resistance to Abiraterone in Advanced Prostate Cancer. Mol Cancer Ther 16:35-44
Lombard, Alan P; Liu, Chengfei; Armstrong, Cameron M et al. (2017) ABCB1 Mediates Cabazitaxel-Docetaxel Cross-Resistance in Advanced Prostate Cancer. Mol Cancer Ther 16:2257-2266
Tummala, Ramakumar; Lou, Wei; Gao, Allen C et al. (2017) Quercetin Targets hnRNPA1 to Overcome Enzalutamide Resistance in Prostate Cancer Cells. Mol Cancer Ther 16:2770-2779
Armstrong, Cameron M; Liu, Chengfei; Lou, Wei et al. (2017) MicroRNA-181a promotes docetaxel resistance in prostate cancer cells. Prostate 77:1020-1028
Tummala, Ramakumar; Nadiminty, Nagalakshmi; Lou, Wei et al. (2016) Lin28 induces resistance to anti-androgens via promotion of AR splice variant generation. Prostate 76:445-55
Armstrong, Cameron M; Gao, Allen C (2016) Adaptive pathways and emerging strategies overcoming treatment resistance in castration resistant prostate cancer. Asian J Urol 3:185-194
Liu, Chengfei; Armstrong, Cameron; Zhu, Yezi et al. (2016) Niclosamide enhances abiraterone treatment via inhibition of androgen receptor variants in castration resistant prostate cancer. Oncotarget 7:32210-20

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