Literature DB >> 22703025

Comprehensive analysis of post-diagnostic prostate-specific antigen kinetics as predictor of a prostate cancer progression in active surveillance patients.

Viacheslav Iremashvili1, Murugesan Manoharan, Soum D Lokeshwar, Daniel L Rosenberg, David Pan, Mark S Soloway.   

Abstract

UNLABELLED: WHAT'S KNOWN ON THE SUBJECT? AND WHAT DOES THE STUDY ADD?: A significant proportion of patients diagnosed with prostate cancer do not require immediate treatment and could be managed by active surveillance, which usually includes serial measurements of prostate-specific antigen (PSA) levels and regular biopsies. The rate of rise in PSA levels, which could be calculated as PSA velocity or PSA doubling time, was previously suggested to be associated with the biological aggressiveness of prostate cancer. Although these parameters are obvious candidates for predicting tumour progression in active surveillance patients, earlier studies that examined this topic provided conflicting results. Our analysis showed that PSA velocity and PSA doubling time calculated at different time-points, by different methods, over different intervals, and in different sub-groups of active surveillance patients provide little if any prognostic information. Although we found some significant associations between PSA velocity and the risk of progression as determined by biopsy, the actual clinical significance of this association was small. Furthermore, PSA velocity did not add to the predictive accuracy of total PSA.
OBJECTIVE: To study whether prostate-specific antigen (PSA) velocity (PSAV) and PSA doubling time (PSADT) are associated with biopsy progression in patients managed by active surveillance. PATIENTS AND METHODS: Our inclusion criteria for active surveillance are biopsy Gleason sum <7, two or fewer positive biopsy cores, ≤20% tumour present in any core, and clinical stage T1-T2a. Changes in any of these parameters during the follow-up that went beyond these limits are considered to be progression. This study included 250 patients who had at least one surveillance biopsy, an available PSA measured no earlier than 3 months before diagnosis, and at least one PSA measurement before each surveillance biopsy. We evaluated the association between PSA kinetics and progression at successive surveillance biopsies in different sub-groups of patients by calculating the area under the curve (AUC) as well as sensitivity and specificity of different thresholds.
RESULTS: Over a median follow-up of 3.0 years, the disease of 64 (26%) patients progressed. PSADT was not associated with biopsy progression, whereas PSAV was only weakly associated with progression in certain sub-groups. However, incorporation of PSAV in models including total PSA resulted in a moderate increase in AUC only when the entire cohort was analysed. In other sub-groups the predictive accuracy of total PSA was not significantly improved by adding PSAV.
CONCLUSIONS: Our findings confirm that PSA kinetics should not be used in decision-making in patients with low-risk prostate cancer managed by active surveillance. Regular surveillance biopsies should remain as the principal method of monitoring cancer progression in these men.
© 2012 The Authors. BJU International © 2012 BJU International.

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Year:  2012        PMID: 22703025     DOI: 10.1111/j.1464-410X.2012.11295.x

Source DB:  PubMed          Journal:  BJU Int        ISSN: 1464-4096            Impact factor:   5.588


  11 in total

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2.  Prostate cancer: active surveillance in African American men.

Authors:  Judd W Moul
Journal:  Nat Rev Urol       Date:  2013-05-07       Impact factor: 14.432

3.  Predictive role of free prostate-specific antigen in a prospective active surveillance program (PRIAS).

Authors:  Hanna Vasarainen; Jolanda Salman; Heidi Salminen; Riccardo Valdagni; Tom Pickles; Chris Bangma; Monique J Roobol; Antti Rannikko
Journal:  World J Urol       Date:  2015-03-31       Impact factor: 4.226

Review 4.  Active surveillance for prostate cancer: current evidence and contemporary state of practice.

Authors:  Jeffrey J Tosoian; H Ballentine Carter; Abbey Lepor; Stacy Loeb
Journal:  Nat Rev Urol       Date:  2016-03-08       Impact factor: 14.432

5.  Prostate specific antigen velocity risk count predicts biopsy reclassification for men with very low risk prostate cancer.

Authors:  Hiten D Patel; Zhaoyong Feng; Patricia Landis; Bruce J Trock; Jonathan I Epstein; H Ballentine Carter
Journal:  J Urol       Date:  2013-09-20       Impact factor: 7.450

6.  [Active surveillance for low-risk prostate cancer].

Authors:  Annika Herlemann; Christian G Stief
Journal:  Urologe A       Date:  2016-02       Impact factor: 0.639

7.  Seventh Joint Meeting of K-J-CaP and CaPSURE: extending the global initiative to improve prostate cancer management.

Authors:  Hideyuki Akaza; Choung Soo Kim; Peter Carroll; In Young Choi; Byung Ha Chung; Matthew R Cooperberg; Yoshihiko Hirao; Shiro Hinotsu; Shigeo Horie; Ji Youl Lee; Mikio Namiki; Chi-Fai Ng; Mizuki Onozawa; Seiichiro Ozono; Satoru Ueno; Rainy Umbas; Dingwei Ye; Gang Zhu
Journal:  Prostate Int       Date:  2014-06-30

Review 8.  Biomarkers for prostate cancer: present challenges and future opportunities.

Authors:  Pranav Sharma; Kamran Zargar-Shoshtari; Julio M Pow-Sang
Journal:  Future Sci OA       Date:  2015-12-17

9.  Low-risk prostate cancer selected for active surveillance with negative MRI at entry: can repeat biopsies at 1 year be avoided? A pilot study.

Authors:  Jonathan Olivier; Veeru Kasivisvanathan; Elodie Drumez; Jean-Christophe Fantoni; Xavier Leroy; Philippe Puech; Arnauld Villers
Journal:  World J Urol       Date:  2018-07-23       Impact factor: 4.226

Review 10.  Green tea extract for prevention of prostate cancer progression in patients on active surveillance.

Authors:  Nagi B Kumar; Shohreh I Dickinson; Michael J Schell; Brandon J Manley; Michael A Poch; Julio Pow-Sang
Journal:  Oncotarget       Date:  2018-12-28
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