Abstract

Accurate characterization of prostate cancer remains a major problem in the clinical management of individual prostate cancer patients and in monitoring clinical trials of emerging therapies. High Resolution - Magic Angle Spinning (HR-MAS) spectroscopy is a non-destructive ex vivo technique that can provide a full chemical analysis of intact prostate tissues prior to a complete histopathologic, immunohistochemical and genetic analysis of the exact same tissue. In this project we will use the high specificity of combined in vivo MRI/MRSI for identifying prostate cancer to target prostate biopsy and surgical tissues in 250 patients prior to therapy and 125 patients demonstrating biochemical failure (rising PSA) and MRI/MRSI evidence of recurrent disease after hormone deprivation therapy for subsequent ex-vivo analyses. The goal of this proposal is to establish a database correlating metabolic profiles associated with specific prostate tissue types, grades of prostate cancer, and response to hormone deprivation therapy and to begin correlating pre-therapy metabolic profiles with gene expression profiles. Using this correlative data we wish to test the following hypotheses: (1) That distinctive metabolic profiles can be associated with the following pathologic prostate tissue types predominatly glandular and stromal healthy peripheral zone tissues, predominatly glandular and stromal benign prostatic hyperplasia, cancers of increasing Gleason score, prostatic intraepithelial neoplasia (PIN), prostatic inflammatory atrophy (PIA) and prostatitis. (2) The dramatic decreases in prostate citrate levels with prostate cancer evolution, progression, and in response to hormone deprivation therapy are associated with changes in morphology (reduction in glandular tissue), prostatic Zn concentration, and/or expression of key Kreb cycle enzymes. (3) Elevated concentrations of phospholipid metabolites (glycerophosphocholine, phosphocholine and choline) in prostate cancer prior to and after therapy are associated with changes in morphology (increased malignant epithelial cell density) and/or changes in cellular proliferation and apoptosis. (4) The dramatic decrease in prostatic spermine concentration with prostate cancer evolution, progression and in response to hormone deprivation therapy is associated with changes in its secretion (reduction in glandular tissue), and/or changes in cellular proliferation and apoptosis. (5) That distinctive metabolic profiles can be associated with the over- and/or under-expression of specific genes categorized by the following pathologic criteria, predominatly stromal versus predominatly glandular healthy tissue, healthy tissue versus prostate cancer, and cancer having Gleason Score equal to or less than 6 versus cancer having a Gleason Score equal to or greater than 7. This work should result in improved interpretation of patient MRSI data, and provide data on how HR-MAS metabolic profiles can compliment the pathologic and genetic assessment of prostate cancer prior to and after hormone deprivation therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA102751-03
Application #
7169829
Study Section
Medical Imaging Study Section (MEDI)
Program Officer
Farahani, Keyvan
Project Start
2005-01-25
Project End
2009-12-31
Budget Start
2007-01-01
Budget End
2007-12-31
Support Year
3
Fiscal Year
2007
Total Cost
$250,049
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Radiation-Diagnostic/Oncology
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Keshari, K R; Tsachres, H; Iman, R et al. (2011) Correlation of phospholipid metabolites with prostate cancer pathologic grade, proliferative status and surgical stage - impact of tissue environment. NMR Biomed 24:691-9
Costello, Leslie C; Franklin, Renty B; Zou, Jing et al. (2011) Human prostate cancer ZIP1/zinc/citrate genetic/metabolic relationship in the TRAMP prostate cancer animal model. Cancer Biol Ther 12:1078-84
Santos, Carissa F; Kurhanewicz, John; Tabatabai, Z Laura et al. (2010) Metabolic, pathologic, and genetic analysis of prostate tissues: quantitative evaluation of histopathologic and mRNA integrity after HR-MAS spectroscopy. NMR Biomed 23:391-8
Ratiney, Helene; Albers, Mark J; Rabeson, Herald et al. (2010) Semi-parametric time-domain quantification of HR-MAS data from prostate tissue. NMR Biomed 23:1146-57
Albers, Mark J; Butler, Thomas N; Rahwa, Iman et al. (2009) Evaluation of the ERETIC method as an improved quantitative reference for 1H HR-MAS spectroscopy of prostate tissue. Magn Reson Med 61:525-32
Levin, Yakir S; Albers, Mark J; Butler, Thomas N et al. (2009) Methods for metabolic evaluation of prostate cancer cells using proton and (13)C HR-MAS spectroscopy and [3-(13)C] pyruvate as a metabolic substrate. Magn Reson Med 62:1091-8
Kurhanewicz, John; Vigneron, Daniel B (2008) Advances in MR spectroscopy of the prostate. Magn Reson Imaging Clin N Am 16:697-710, ix-x
Tessem, May-Britt; Swanson, Mark G; Keshari, Kayvan R et al. (2008) Evaluation of lactate and alanine as metabolic biomarkers of prostate cancer using 1H HR-MAS spectroscopy of biopsy tissues. Magn Reson Med 60:510-6
Swanson, Mark G; Keshari, Kayvan R; Tabatabai, Z Laura et al. (2008) Quantification of choline- and ethanolamine-containing metabolites in human prostate tissues using 1H HR-MAS total correlation spectroscopy. Magn Reson Med 60:33-40