Abstract

The p53 tumor suppressor plays a central role in controlling cell cycle progression and apoptosis and is anattractive cancer therapeutic target because its tumor suppressor activity can be stimulated to eradicatetumor cells. Recent studies have suggested that stimulation of the p53 activity may be a powerful strategy forthe treatment of the majority of hormone-refractory prostate cancer. In p53 wild-type cancer cells, the p53activity is effectively inhibited by its endogenous inhibitor, the human murine double minute 2 (MDM2) oncoproteinby multiple mechanisms. A new therapeutic approach to stimulation of the activity of p53 is throughnhjbition of its interaction with the MDM2 protein using non-peptide small-molecule MDM2 inhibitors. Designof non-peptide small-molecule inhibitors of the MDM2-p53 interaction is being intensely pursed as a newcancer therapeutic strategy. In the last two years, with the support of the University of Michigan SPOREgrant, we have designed and developed a class of highly potent, non-peptide, orally available, smallmoleculeinhibitors of MDM2. Based upon our promising in vitro and in vivo results, we are advancing ourmost promising lead compound into human clinical trials as a new therapy for the treatment of humancancer. Our long-term transitional goal in this SPORE renewal project is to develop a highly potent andpromising small-molecule inhibitor of the MDM2-p53 interaction (hereafter called MDM2 inhibitor) as a newtherapy for the treatment of advanced human prostate cancer. Toward this goal, we will carry out thefollowing specific Aims:
Aim 1 : Determination of the in vitro activity, specificity and molecular mechanism of action of our potentMDM2 inhibitors in a panel of prostate cancer cell lines and normal cells.
Aim 2 : Determination of the in vivo antitumor activity and molecular mechanism of action of our potent MDM2inhibitors in animal models of human prostate cancer and examination of any toxicity to animals.
Aim 3 : Performance of a Phase II clinical trial of our clinical lead compound in prostate cancer patients withandrogen-independent disease.Successfully carried out, this SPORE project will pave the way for the development of an entirely new classof molecularly targeted anti-cancer therapy for the treatment of advanced prostate cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
2P50CA069568-11
Application #
7468644
Study Section
Special Emphasis Panel (ZCA1-RPRB-M (J1))
Project Start
2008-06-01
Project End
2013-05-31
Budget Start
2008-06-01
Budget End
2009-05-31
Support Year
11
Fiscal Year
2008
Total Cost
$278,234
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Rye, Morten Beck; Bertilsson, Helena; Andersen, Maria K et al. (2018) Cholesterol synthesis pathway genes in prostate cancer are transcriptionally downregulated when tissue confounding is minimized. BMC Cancer 18:478
Xie, Yuanyuan; Cao, Zhen; Wong, Elissa Wp et al. (2018) COP1/DET1/ETS axis regulates ERK transcriptome and sensitivity to MAPK inhibitors. J Clin Invest 128:1442-1457
Singhal, Udit; Wang, Yugang; Henderson, James et al. (2018) Multigene Profiling of CTCs in mCRPC Identifies a Clinically Relevant Prognostic Signature. Mol Cancer Res 16:643-654
Wang, Xiaoju; Qiao, Yuanyuan; Asangani, Irfan A et al. (2017) Development of Peptidomimetic Inhibitors of the ERG Gene Fusion Product in Prostate Cancer. Cancer Cell 31:532-548.e7
Blattner, Mirjam; Liu, Deli; Robinson, Brian D et al. (2017) SPOP Mutation Drives Prostate Tumorigenesis In Vivo through Coordinate Regulation of PI3K/mTOR and AR Signaling. Cancer Cell 31:436-451
Dai, Xiangpeng; Gan, Wenjian; Li, Xiaoning et al. (2017) Prostate cancer-associated SPOP mutations confer resistance to BET inhibitors through stabilization of BRD4. Nat Med 23:1063-1071
Lin, Ke-Chih; Torga, Gonzalo; Wu, Amy et al. (2017) Epithelial and mesenchymal prostate cancer cell population dynamics on a complex drug landscape. Converg Sci Phys Oncol 3:
Piert, Morand; Montgomery, Jeffrey; Kunju, Lakshmi Priya et al. (2016) 18F-Choline PET/MRI: The Additional Value of PET for MRI-Guided Transrectal Prostate Biopsies. J Nucl Med 57:1065-70
Van Allen, Eliezer M; Robinson, Dan; Morrissey, Colm et al. (2016) A comparative assessment of clinical whole exome and transcriptome profiling across sequencing centers: implications for precision cancer medicine. Oncotarget 7:52888-52899
Mehra, Rohit; Udager, Aaron M; Ahearn, Thomas U et al. (2016) Overexpression of the Long Non-coding RNA SChLAP1 Independently Predicts Lethal Prostate Cancer. Eur Urol 70:549-552

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