A Multi-Institutional Evaluation of Active Surveillance for Low Risk Prostate Cancer

Eggener, Scott E.; Mueller, Alex; Berglund, Ryan K.; Ayyathurai, Rajnikanth; Soloway, Cindy; Soloway, Mark S.; Abouassaly, Robert; Klein, Eric A.; Jones, Steven J.; Zappavigna, Christopher; Goldenberg, Larry; Scardino, Peter T.; Eastham, James A.; Guillonneau, Bertrand

doi:10.1016/j.juro.2012.11.023

Cited by 73 publications

(75 citation statements)

References 21 publications

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“…This is consistent with data from Europe [20] and the USA [22]: in these studies, the distribution to RP, RT, HT and 'other' therapies was 48.0, 45.2, 1.5 and 5.3%, respectively, and 60.5, 30, 7 and 2.5%, respectively. By contrast, Klotz et al [28] found the use of RT was predominant at 67% (RP, 26%; HT, 7%).…”

Section: Totalsupporting

confidence: 91%

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Active surveillance in localized prostate cancer: comparison of incidental tumours (T1a/b) and tumours diagnosed by core needle biopsy (T1c/T2a): results from the HAROW study

Herden

Wille

Weißbach³

2015

BJU International

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ObjectiveTo conduct a comparative prospective analysis of patients with incidental T1a/T1b prostate cancer (IPCa) and those with prostate cancer (PCa) diagnosed by core needle biopsy, treated by active surveillance (AS), with regard to inclusion criteria, progression and switch to deferred treatment. Patients and MethodsThe HAROW study is an observational outcomes research study on the management of localized PCa. Treating urologists reported clinical variables and information on therapy and clinical course of disease at 6-month intervals. With respect to therapy, only recommendations were made; the final decision on the therapeutic method rested with the treating physician. ResultsOut of 2 957 patients included in the HAROW study, 447 chose AS. The median follow-up was 28.3 months. T1a, T1b, T1c and T2a disease were diagnosed in 81, 18, 292 and 56 patients, respectively. Patients in the IPCa group had lower prostate-specific antigen (PSA) levels (4.2 vs 6.1 ng/mL) and more comorbidities than those diagnosed by core needle biospy. The IPCa group also had fewer re-biopsies (25.3 vs 43.2%) and fewer changes to invasive treatment (12.1 vs 25.9%). No significant differences were found with respect to the criteria for discontinuation, subsequent therapies and histological findings after radical prostatectomy. ConclusionUrologists are highly inclined to use AS as a therapeutic option in IPCa. More patients with IPCa than those diagnosed after core needle biopsy continued on AS, which was also associated with the indication for a re-biopsy being less stringently observed.

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Section: Totalsupporting

confidence: 91%

“…Most clinical studies mention T1c and T2a tumours almost exclusively. T1a/b cancer is either not included in the reports, not specified separately or represented only sparingly [20][21][22], e.g. 4.8% in the report by Klotz et al [8].…”

Section: Discussionmentioning

confidence: 99%

Active surveillance in localized prostate cancer: comparison of incidental tumours (T1a/b) and tumours diagnosed by core needle biopsy (T1c/T2a): results from the HAROW study

Herden

Wille

Weißbach³

2015

BJU International

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“…10,11,19,24 Fewer cohorts reportedly have a median followup of beyond 5 years. 5e7 Our results extend the median followup previously reported in this cohort from 3.6 to 5 years and include more than 200 men with followup beyond 7.5 years.…”

Section: Discussionmentioning

confidence: 99%

Extended Followup and Risk Factors for Disease Reclassification in a Large Active Surveillance Cohort for Localized Prostate Cancer

et al. 2015

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“…27 Along with clinical TNM stage and preoperative PSA value, Gleason score based on biopsy is among the most important factors in treatment decision making for prostate cancer. 13,[17][18][19][20] The AJCC 6th and 7th editions both state that prostate cancers should be microscopically diagnosed. Therefore, theoretically nearly every case should have Gleason patterns (SSF7) and/or scores (SSF8) recorded.…”

Section: Discussionmentioning

confidence: 99%

“…24 Several studies have explored the value of using the number of positive biopsy cores to enhance prediction of clinically insignificant disease or recurrence, with mixed results. 13,30 Inclusion of the number of positive and negative cores enhanced the predictive accuracy of a preoperative nomogram predicting the 10-year probability of prostate cancer recurrence after radical prostatectomy. 31 The AJCC 7th edition recommended as clinically significant collecting both the number of cores positive for cancer (SSF12) and the number of cores examined (SSF13).…”

Section: Discussionmentioning

confidence: 99%

Prostate cancer collaborative stage data items—their definitions, quality, usage, and clinical implications: A review of SEER data for 2004‐2010

Howlader

Chen

Ries

et al. 2014

Cancer

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BACKGROUND: Version 2 of the Collaborative Stage Data Collection System (CSv2) became effective with cases diagnosed in 2010. This report focuses on the CSv2 components required to derive the American Joint Committee on Cancer (AJCC) stage for prostate cancer and on the site-specific factors for prostate cancer captured in CSv2. The report also highlights differences between the AJCC 6th and 7th editions for classifying prostate cancer stage. METHODS: Data from 18 Surveillance, Epidemiology, and End Results (SEER) Program population-based registries (SEER-18) were analyzed for the years 2004-2010, which included 400,591 prostate cancer cases. RESULTS: CSv2 provides specificity with regard to the Gleason grading system by distinguishing between clinical and pathologic patterns and scores. The AJCC 7th edition incorporates prostate-specific antigen values into staging, subdivides stage II into IIA and IIB, and reclassifies extraprostatic invasion with microscopic bladder neck invasion from T4 in the 6th edition to T3a; this latter change affected the AJCC stage of 283 cases in 2010. Of the 44,578 prostate cancer cases diagnosed in 2010 that would have been classified as stage II in the AJCC 6th edition, 32.7%, 27.5%, and 39.8% are classified as stages I, IIA, and IIB, respectively, in the 7th edition. CONCLUSIONS: CSv2 provides more information than was previously available to researchers using SEER prostate data.

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A Multi-Institutional Evaluation of Active Surveillance for Low Risk Prostate Cancer

Cited by 73 publications

References 21 publications

Active surveillance in localized prostate cancer: comparison of incidental tumours (T1a/b) and tumours diagnosed by core needle biopsy (T1c/T2a): results from the HAROW study

Active surveillance in localized prostate cancer: comparison of incidental tumours (T1a/b) and tumours diagnosed by core needle biopsy (T1c/T2a): results from the HAROW study

Extended Followup and Risk Factors for Disease Reclassification in a Large Active Surveillance Cohort for Localized Prostate Cancer

Prostate cancer collaborative stage data items—their definitions, quality, usage, and clinical implications: A review of SEER data for 2004‐2010

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