Abstract

The success of translational research hinges on availability of well characterized human samples as well as model systems. The tissue and animal model core represents a combination and continuation of the previously separate cores. The cores were combined to facilitate the success of our prostate donor program (Warm Autopsy Program), which makes heavy use of both the tissue and animal cores. A multi-disciplinary team including surgeons, pathologists, oncologists, and researchers is needed to collect, maintain and make optimum use of this previous resource. This core resource will continue to procure and store well characterized samples from prostate cancer patients and oversee and prioritize their distribution. The tissue and serum bank now contains a diverse set (over 700 radical prostatectomy patients) of various well characterized tumor grades and stages. These samples were obtained without compromising analysis of specimens for patient care. We also have in place a bank of serum and DNA samples from an African American screening population and are collecting tissue from African American prostate cancer cases. Microdissection of prostate cancer specimens is essential to understanding the genetics of prostate cancer. Laser capture microdissection will be available through this core to provide morphologically well characterized lesional tissues for molecular biologic and genetic studies. The extensive data base that accompanies these well characterized microdissected specimens of lesional tissues is a key component for successful translation research in prostate cancer. We also have the capability for digital microscopic imaging and analysis. The digital imaging is a integral part of the laser capture microdissection. The animal model component of the core will continue to prove the transgenic mouse line (TRAMP mice) which develop prostate cancer due to prostate-specific expression of SV40 T antigen regulated by the pro-basin promoter. This core will also provide the skid mice derived tumor xenograft lines developed from our warm autopsy program. In summary, the key components of the tissue and animal model core include the data base, tissue bank, serum bank, African American serum-DNA-tissue bank, laser capture microdissection facility, digital imaging and image analysis, transgenic mice, and warm autopsy derived xenograft line.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA069568-05
Application #
6203373
Study Section
Project Start
1999-08-09
Project End
2003-07-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
5
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
DUNS #
791277940
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:
Chen, Weiqiang; Allen, Steven G; Reka, Ajaya Kumar et al. (2016) Nanoroughened adhesion-based capture of circulating tumor cells with heterogeneous expression and metastatic characteristics. BMC Cancer 16:614
Hu, Shuhuan; Liu, Guangyu; Chen, Weiqiang et al. (2016) Multiparametric Biomechanical and Biochemical Phenotypic Profiling of Single Cancer Cells Using an Elasticity Microcytometer. Small 12:2300-11
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

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