Gleason 6 prostate cancer: Translating biology into population health

Scott E. Eggener; Ketan Badani; Daniel A. Barocas; Glen W. Barrisford; Jed Sian Cheng; Arnold I. Chin; Anthony Corcoran; Jonathan I. Epstein; Arvin K. George; Gopal N. Gupta; Matthew H. Hayn; Eric C. Kauffman; Brian Lane; Michael A. Liss; Moben Mirza; Todd M. Morgan; Kelvin Moses; Kenneth G. Nepple; Mark A. Preston; Soroush Rais-Bahrami; Matthew J. Resnick; M. Minhaj Siddiqui; Jonathan Silberstein; Eric A. Singer; Geoffrey A. Sonn; Preston Sprenkle; Kelly L. Stratton; Jennifer Taylor; Jeffrey Tomaszewski; Matt Tollefson; Andrew Vickers; Wesley M. White; William T. Lowrance

doi:10.1016/j.juro.2015.01.126

Gleason 6 prostate cancer: Translating biology into population health

Scott E. Eggener, Ketan Badani, Daniel A. Barocas, Glen W. Barrisford, Jed Sian Cheng, Arnold I. Chin, Anthony Corcoran, Jonathan I. Epstein, Arvin K. George, Gopal N. Gupta, Matthew H. Hayn, Eric C. Kauffman, Brian Lane, Michael A. Liss, Moben Mirza, Todd M. Morgan, Kelvin Moses, Kenneth G. Nepple, Mark A. Preston, Soroush Rais-BahramiMatthew J. Resnick, M. Minhaj Siddiqui, Jonathan Silberstein, Eric A. Singer, Geoffrey A. Sonn, Preston Sprenkle, Kelly L. Stratton, Jennifer Taylor, Jeffrey Tomaszewski, Matt Tollefson, Andrew Vickers, Wesley M. White, William T. Lowrance

Urology

Research output: Contribution to journal › Review article › peer-review

61 Scopus citations

Abstract

Purpose Gleason 6 (3+3) is the most commonly diagnosed prostate cancer among men with prostate specific antigen screening, the most histologically well differentiated and is associated with the most favorable prognosis. Despite its prevalence, considerable debate exists regarding the genetic features, clinical significance, natural history, metastatic potential and optimal management. Materials and Methods Members of the Young Urologic Oncologists in the Society of Urologic Oncology cooperated in a comprehensive search of the peer reviewed English medical literature on Gleason 6 prostate cancer, specifically focusing on the history of the Gleason scoring system, histological features, clinical characteristics, practice patterns and outcomes. Results The Gleason scoring system was devised in the early 1960s, widely adopted by 1987 and revised in 2005 with a more restrictive definition of Gleason 6 disease. There is near consensus that Gleason 6 meets pathological definitions of cancer, but controversy about whether it meets commonly accepted molecular and genetic criteria of cancer. Multiple clinical series suggest that the metastatic potential of contemporary Gleason 6 disease is negligible but not zero. Population based studies in the U.S. suggest that more than 90% of men newly diagnosed with prostate cancer undergo treatment and are exposed to the risk of morbidity for a cancer unlikely to cause symptoms or decrease life expectancy. Efforts have been proposed to minimize the number of men diagnosed with or treated for Gleason 6 prostate cancer. These include modifications to prostate specific antigen based screening strategies such as targeting high risk populations, decreasing the frequency of screening, recommending screening cessation, incorporating remaining life expectancy estimates, using shared decision making and novel biomarkers, and eliminating prostate specific antigen screening entirely. Large nonrandomized and randomized studies have shown that active surveillance is an effective management strategy for men with Gleason 6 disease. Active surveillance dramatically reduces the number of men undergoing treatment without apparent compromise of cancer related outcomes. Conclusions The definition and clinical relevance of Gleason 6 prostate cancer have changed substantially since its introduction nearly 50 years ago. A high proportion of screen detected cancers are Gleason 6 and the metastatic potential is negligible. Dramatically reducing the diagnosis and treatment of Gleason 6 disease is likely to have a favorable impact on the net benefit of prostate cancer screening.

Original language	English (US)
Pages (from-to)	626-634
Number of pages	9
Journal	Journal of Urology
Volume	194
Issue number	3
DOIs	https://doi.org/10.1016/j.juro.2015.01.126
State	Published - Sep 1 2015

Keywords

early detection of cancer
neoplasm grading
prostatectomy
prostatic neoplasms
watchful waiting

ASJC Scopus subject areas

Urology

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10.1016/j.juro.2015.01.126

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Eggener, S. E., Badani, K., Barocas, D. A., Barrisford, G. W., Cheng, J. S., Chin, A. I., Corcoran, A., Epstein, J. I., George, A. K., Gupta, G. N., Hayn, M. H., Kauffman, E. C., Lane, B., Liss, M. A., Mirza, M., Morgan, T. M., Moses, K., Nepple, K. G., Preston, M. A., ... Lowrance, W. T. (2015). Gleason 6 prostate cancer: Translating biology into population health. Journal of Urology, 194(3), 626-634. https://doi.org/10.1016/j.juro.2015.01.126

Eggener, SE, Badani, K, Barocas, DA, Barrisford, GW, Cheng, JS, Chin, AI, Corcoran, A, Epstein, JI, George, AK, Gupta, GN, Hayn, MH, Kauffman, EC, Lane, B, Liss, MA, Mirza, M, Morgan, TM, Moses, K, Nepple, KG, Preston, MA, Rais-Bahrami, S, Resnick, MJ, Siddiqui, MM, Silberstein, J, Singer, EA, Sonn, GA, Sprenkle, P, Stratton, KL, Taylor, J, Tomaszewski, J, Tollefson, M, Vickers, A, White, WM & Lowrance, WT 2015, 'Gleason 6 prostate cancer: Translating biology into population health', Journal of Urology, vol. 194, no. 3, pp. 626-634. https://doi.org/10.1016/j.juro.2015.01.126

@article{c7acd09677394930b61d47034e7e94e2,

title = "Gleason 6 prostate cancer: Translating biology into population health",

abstract = "Purpose Gleason 6 (3+3) is the most commonly diagnosed prostate cancer among men with prostate specific antigen screening, the most histologically well differentiated and is associated with the most favorable prognosis. Despite its prevalence, considerable debate exists regarding the genetic features, clinical significance, natural history, metastatic potential and optimal management. Materials and Methods Members of the Young Urologic Oncologists in the Society of Urologic Oncology cooperated in a comprehensive search of the peer reviewed English medical literature on Gleason 6 prostate cancer, specifically focusing on the history of the Gleason scoring system, histological features, clinical characteristics, practice patterns and outcomes. Results The Gleason scoring system was devised in the early 1960s, widely adopted by 1987 and revised in 2005 with a more restrictive definition of Gleason 6 disease. There is near consensus that Gleason 6 meets pathological definitions of cancer, but controversy about whether it meets commonly accepted molecular and genetic criteria of cancer. Multiple clinical series suggest that the metastatic potential of contemporary Gleason 6 disease is negligible but not zero. Population based studies in the U.S. suggest that more than 90% of men newly diagnosed with prostate cancer undergo treatment and are exposed to the risk of morbidity for a cancer unlikely to cause symptoms or decrease life expectancy. Efforts have been proposed to minimize the number of men diagnosed with or treated for Gleason 6 prostate cancer. These include modifications to prostate specific antigen based screening strategies such as targeting high risk populations, decreasing the frequency of screening, recommending screening cessation, incorporating remaining life expectancy estimates, using shared decision making and novel biomarkers, and eliminating prostate specific antigen screening entirely. Large nonrandomized and randomized studies have shown that active surveillance is an effective management strategy for men with Gleason 6 disease. Active surveillance dramatically reduces the number of men undergoing treatment without apparent compromise of cancer related outcomes. Conclusions The definition and clinical relevance of Gleason 6 prostate cancer have changed substantially since its introduction nearly 50 years ago. A high proportion of screen detected cancers are Gleason 6 and the metastatic potential is negligible. Dramatically reducing the diagnosis and treatment of Gleason 6 disease is likely to have a favorable impact on the net benefit of prostate cancer screening.",

keywords = "early detection of cancer, neoplasm grading, prostatectomy, prostatic neoplasms, watchful waiting",

author = "Eggener, {Scott E.} and Ketan Badani and Barocas, {Daniel A.} and Barrisford, {Glen W.} and Cheng, {Jed Sian} and Chin, {Arnold I.} and Anthony Corcoran and Epstein, {Jonathan I.} and George, {Arvin K.} and Gupta, {Gopal N.} and Hayn, {Matthew H.} and Kauffman, {Eric C.} and Brian Lane and Liss, {Michael A.} and Moben Mirza and Morgan, {Todd M.} and Kelvin Moses and Nepple, {Kenneth G.} and Preston, {Mark A.} and Soroush Rais-Bahrami and Resnick, {Matthew J.} and Siddiqui, {M. Minhaj} and Jonathan Silberstein and Singer, {Eric A.} and Sonn, {Geoffrey A.} and Preston Sprenkle and Stratton, {Kelly L.} and Jennifer Taylor and Jeffrey Tomaszewski and Matt Tollefson and Andrew Vickers and White, {Wesley M.} and Lowrance, {William T.}",

note = "Publisher Copyright: {\textcopyright} 2015 American Urological Association Education and Research, Inc.",

year = "2015",

month = sep,

day = "1",

doi = "10.1016/j.juro.2015.01.126",

language = "English (US)",

volume = "194",

pages = "626--634",

journal = "Journal of Urology",

issn = "0022-5347",

publisher = "Elsevier Inc.",

number = "3",

}

TY - JOUR

T1 - Gleason 6 prostate cancer

T2 - Translating biology into population health

AU - Eggener, Scott E.

AU - Badani, Ketan

AU - Barocas, Daniel A.

AU - Barrisford, Glen W.

AU - Cheng, Jed Sian

AU - Chin, Arnold I.

AU - Corcoran, Anthony

AU - Epstein, Jonathan I.

AU - George, Arvin K.

AU - Gupta, Gopal N.

AU - Hayn, Matthew H.

AU - Kauffman, Eric C.

AU - Lane, Brian

AU - Liss, Michael A.

AU - Mirza, Moben

AU - Morgan, Todd M.

AU - Moses, Kelvin

AU - Nepple, Kenneth G.

AU - Preston, Mark A.

AU - Rais-Bahrami, Soroush

AU - Resnick, Matthew J.

AU - Siddiqui, M. Minhaj

AU - Silberstein, Jonathan

AU - Singer, Eric A.

AU - Sonn, Geoffrey A.

AU - Sprenkle, Preston

AU - Stratton, Kelly L.

AU - Taylor, Jennifer

AU - Tomaszewski, Jeffrey

AU - Tollefson, Matt

AU - Vickers, Andrew

AU - White, Wesley M.

AU - Lowrance, William T.

PY - 2015/9/1

Y1 - 2015/9/1

N2 - Purpose Gleason 6 (3+3) is the most commonly diagnosed prostate cancer among men with prostate specific antigen screening, the most histologically well differentiated and is associated with the most favorable prognosis. Despite its prevalence, considerable debate exists regarding the genetic features, clinical significance, natural history, metastatic potential and optimal management. Materials and Methods Members of the Young Urologic Oncologists in the Society of Urologic Oncology cooperated in a comprehensive search of the peer reviewed English medical literature on Gleason 6 prostate cancer, specifically focusing on the history of the Gleason scoring system, histological features, clinical characteristics, practice patterns and outcomes. Results The Gleason scoring system was devised in the early 1960s, widely adopted by 1987 and revised in 2005 with a more restrictive definition of Gleason 6 disease. There is near consensus that Gleason 6 meets pathological definitions of cancer, but controversy about whether it meets commonly accepted molecular and genetic criteria of cancer. Multiple clinical series suggest that the metastatic potential of contemporary Gleason 6 disease is negligible but not zero. Population based studies in the U.S. suggest that more than 90% of men newly diagnosed with prostate cancer undergo treatment and are exposed to the risk of morbidity for a cancer unlikely to cause symptoms or decrease life expectancy. Efforts have been proposed to minimize the number of men diagnosed with or treated for Gleason 6 prostate cancer. These include modifications to prostate specific antigen based screening strategies such as targeting high risk populations, decreasing the frequency of screening, recommending screening cessation, incorporating remaining life expectancy estimates, using shared decision making and novel biomarkers, and eliminating prostate specific antigen screening entirely. Large nonrandomized and randomized studies have shown that active surveillance is an effective management strategy for men with Gleason 6 disease. Active surveillance dramatically reduces the number of men undergoing treatment without apparent compromise of cancer related outcomes. Conclusions The definition and clinical relevance of Gleason 6 prostate cancer have changed substantially since its introduction nearly 50 years ago. A high proportion of screen detected cancers are Gleason 6 and the metastatic potential is negligible. Dramatically reducing the diagnosis and treatment of Gleason 6 disease is likely to have a favorable impact on the net benefit of prostate cancer screening.

AB - Purpose Gleason 6 (3+3) is the most commonly diagnosed prostate cancer among men with prostate specific antigen screening, the most histologically well differentiated and is associated with the most favorable prognosis. Despite its prevalence, considerable debate exists regarding the genetic features, clinical significance, natural history, metastatic potential and optimal management. Materials and Methods Members of the Young Urologic Oncologists in the Society of Urologic Oncology cooperated in a comprehensive search of the peer reviewed English medical literature on Gleason 6 prostate cancer, specifically focusing on the history of the Gleason scoring system, histological features, clinical characteristics, practice patterns and outcomes. Results The Gleason scoring system was devised in the early 1960s, widely adopted by 1987 and revised in 2005 with a more restrictive definition of Gleason 6 disease. There is near consensus that Gleason 6 meets pathological definitions of cancer, but controversy about whether it meets commonly accepted molecular and genetic criteria of cancer. Multiple clinical series suggest that the metastatic potential of contemporary Gleason 6 disease is negligible but not zero. Population based studies in the U.S. suggest that more than 90% of men newly diagnosed with prostate cancer undergo treatment and are exposed to the risk of morbidity for a cancer unlikely to cause symptoms or decrease life expectancy. Efforts have been proposed to minimize the number of men diagnosed with or treated for Gleason 6 prostate cancer. These include modifications to prostate specific antigen based screening strategies such as targeting high risk populations, decreasing the frequency of screening, recommending screening cessation, incorporating remaining life expectancy estimates, using shared decision making and novel biomarkers, and eliminating prostate specific antigen screening entirely. Large nonrandomized and randomized studies have shown that active surveillance is an effective management strategy for men with Gleason 6 disease. Active surveillance dramatically reduces the number of men undergoing treatment without apparent compromise of cancer related outcomes. Conclusions The definition and clinical relevance of Gleason 6 prostate cancer have changed substantially since its introduction nearly 50 years ago. A high proportion of screen detected cancers are Gleason 6 and the metastatic potential is negligible. Dramatically reducing the diagnosis and treatment of Gleason 6 disease is likely to have a favorable impact on the net benefit of prostate cancer screening.

KW - early detection of cancer

KW - neoplasm grading

KW - prostatectomy

KW - prostatic neoplasms

KW - watchful waiting

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Gleason 6 prostate cancer: Translating biology into population health

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