Abstract

The majority of men with prostate cancer are now diagnosed with tumors with a low risk of causespecific mortality. Such men are most frequently treated with radical prostatectomy or external beam radiotherapy (EBRT) and are followed by regular serum PSA evaluations thereafter. Most men with a rising PSA post-definitive therapy present several months or years after diagnostic biopsy (in the case of EBRT) or radical prostatectomy (in the case of surgery). Some will have clinically obvious local recurrence, have clinically detectable metastasis, but many will have no other evidence of recurrent prostate cancer other than a rising or detectable PSA. The PSA """"""""doubling time"""""""" has been used by some clinicians to determine which of these men deserve adjuvant hormonal ablation, local radiation therapy, or simple observation. We hypothesize that additional biomarkers will help predict which men with a rising PSA post-definitive therapy would benefit from additional therapy. Since many men present with a rising PSA months or years after receiving their definitive therapy elsewhere, the most important biomarkers will be those that can be performed on a specimen that is contemporaneously and easily available, i.e. serum or plasma. The primary goal of Project 1 is to develop potential serum biomarkers that will assist in the management of patients in this situation. However, predicting the prognosis of men at the time of diagnosis is an important direction of current translational prostate cancer research. The secondary goal of Project 1 is to learn if the alterations in the tissue biomarkers at the time of initial diagnosis are associated with later PSA progression and with further systemic progression. To accomplish these focused goals, Project 1 is designed to carefully utilize the patient population resources of the Mayo Clinic prostate cancer practice and the expertise of Mayo Clinic laboratory and clinical scientists.
Specific Aim 1 will discover tissue biomarkers associated with prostate cancer progression in patients with rising PSA following definitive treatment. Using the data from Specific Aim 1, Specific Aim 2 will develop serum biomarkers that similarly predict prostate cancer progression in patients with rising PSA following definitive treatment. To begin to translate these associations into clinical practice, Specific Aim 3 will conduct a phase II clinical trial to determine the effect of temporary androgen deprivation in men with a rising PSA after primary definitive therapy and determine the interaction of response to androgen ablation with serum and tissue biomarker alterations. This project will generate new biomarker panels that will be used in the clinical management of a large and important population of men with prostate cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Specialized Center (P50)
Project #
5P50CA091956-10
Application #
8128725
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
2013-08-31
Budget Start
2010-09-01
Budget End
2011-08-31
Support Year
10
Fiscal Year
2010
Total Cost
$248,344
Indirect Cost

  Institution

Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905

  Publications

Guerrico, Anatilde Gonzalez; Hillman, David; Karnes, Jeffery et al. (2017) Roles of kallikrein-2 biomarkers (free-hK2 and pro-hK2) for predicting prostate cancer progression-free survival. J Circ Biomark 6:1849454417720151
Hearn, Jason W D; AbuAli, Ghada; Reichard, Chad A et al. (2016) HSD3B1 and resistance to androgen-deprivation therapy in prostate cancer: a retrospective, multicohort study. Lancet Oncol 17:1435-1444
Spratt, Daniel E; Evans, Michael J; Davis, Brian J et al. (2015) Androgen Receptor Upregulation Mediates Radioresistance after Ionizing Radiation. Cancer Res 75:4688-96
Lu, Ji; Lonergan, Peter E; Nacusi, Lucas P et al. (2015) The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells. J Urol 193:690-8
Urban, Matthew W; Wang, Chenyi; Alizad, Azra et al. (2015) Complex background suppression for vibro-acoustography images. Ultrasonics 56:456-72
Cooperberg, Matthew R; Davicioni, Elai; Crisan, Anamaria et al. (2015) Combined value of validated clinical and genomic risk stratification tools for predicting prostate cancer mortality in a high-risk prostatectomy cohort. Eur Urol 67:326-33
Alshalalfa, Mohammed; Crisan, Anamaria; Vergara, Ismael A et al. (2015) Clinical and genomic analysis of metastatic prostate cancer progression with a background of postoperative biochemical recurrence. BJU Int 116:556-67
Loeb, Stacy; Sanda, Martin G; Broyles, Dennis L et al. (2015) The prostate health index selectively identifies clinically significant prostate cancer. J Urol 193:1163-9
Ahmed, Kamran A; Davis, Brian J; Mynderse, Lance A et al. (2014) Comparison of biochemical failure rates between permanent prostate brachytherapy and radical retropubic prostatectomy as a function of posttherapy PSA nadir plus 'X'. Radiat Oncol 9:171
Wu, Qiang; Kohli, Manish; Bergen 3rd, H Robert et al. (2014) Preclinical evaluation of the supercritical extract of azadirachta indica (neem) leaves in vitro and in vivo on inhibition of prostate cancer tumor growth. Mol Cancer Ther 13:1067-77

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