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A first step towards a global nomogram to predict disease progression for men on active surveillance
BACKGROUND: Signs of disease progression (28%) and conversion to active treatment without evidence of disease progression (13%) are the main reasons for discontinuation of active surveillance (AS) in men with localised prostate cancer (PCa). We aimed to develop a nomogram to predict disease progress...
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Formato: | Online Artículo Texto |
Lenguaje: | English |
Publicado: |
AME Publishing Company
2021
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Materias: | |
Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8039580/ https://www.ncbi.nlm.nih.gov/pubmed/33850745 http://dx.doi.org/10.21037/tau-20-1082 |
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author | Van Hemelrijck, Mieke Ji, Xinge Helleman, Jozien Roobol, Monique J. Nieboer, Daan Bangma, Chris Frydenberg, Mark Rannikko, Antti Lee, Lui Shiong Gnanapragasam, Vincent Kattan, Michael W. Trock, Bruce Ehdaie, Behfar Carroll, Peter Filson, Christopher Kim, Jeri Logothetis, Christopher Morgan, Todd Klotz, Laurence Pickles, Tom Hyndman, Eric Moore, Caroline Gnanapragasam, Vincent Van Hemelrijck, Mieke Dasgupta, Prokar Bangma, Chris Roobol, Monique Villers, Arnauld Rannikko, Antti Valdagni, Riccardo Perry, Antoinette Hugosson, Jonas Rubio-Briones, Jose Bjartell, Anders Hefermehl, Lukas Shiong, Lee Lui Frydenberg, Mark Kakehi, Yoshiyuki Chung, Mikio Sugimoto Byung Ha van der Kwast, Theo Obbink, Henk van der Linden, Wim Hulsen, Tim de Jonge, Cees Kattan, Mike Xinge, Ji Muir, Kenneth Lophatananon, Artitaya Fahey, Michael Steyerberg, Ewout Nieboer, Daan Zhang, Liying Guo, Wei Benfante, Nicole Cowan, Janet Patil, Dattatraya Tolosa, Emily Kim, Tae-Kyung Mamedov, Alexandre LaPointe, Vincent Crump, Trafford Stavrinides, Vasilis Kimberly-Duffell, Jenna Santaolalla, Aida Nieboer, Daan Olivier, Jonathan Rancati, Tiziana Ahlgren, Helén Mascarós, Juanma Löfgren, Annica Lehmann, Kurt Lin, Catherine Han Hirama, Hiromi Lee, Kwang Suk Jenster, Guido Auvinen, Anssi Bjartell, Anders Haider, Masoom van Bochove, Kees Carter, Ballentine Gledhill, Sam Buzza, Mark Kouspou, Michelle Bangma, Chris Roobol, Monique Bruinsma, Sophie Helleman, Jozien |
author_facet | Van Hemelrijck, Mieke Ji, Xinge Helleman, Jozien Roobol, Monique J. Nieboer, Daan Bangma, Chris Frydenberg, Mark Rannikko, Antti Lee, Lui Shiong Gnanapragasam, Vincent Kattan, Michael W. Trock, Bruce Ehdaie, Behfar Carroll, Peter Filson, Christopher Kim, Jeri Logothetis, Christopher Morgan, Todd Klotz, Laurence Pickles, Tom Hyndman, Eric Moore, Caroline Gnanapragasam, Vincent Van Hemelrijck, Mieke Dasgupta, Prokar Bangma, Chris Roobol, Monique Villers, Arnauld Rannikko, Antti Valdagni, Riccardo Perry, Antoinette Hugosson, Jonas Rubio-Briones, Jose Bjartell, Anders Hefermehl, Lukas Shiong, Lee Lui Frydenberg, Mark Kakehi, Yoshiyuki Chung, Mikio Sugimoto Byung Ha van der Kwast, Theo Obbink, Henk van der Linden, Wim Hulsen, Tim de Jonge, Cees Kattan, Mike Xinge, Ji Muir, Kenneth Lophatananon, Artitaya Fahey, Michael Steyerberg, Ewout Nieboer, Daan Zhang, Liying Guo, Wei Benfante, Nicole Cowan, Janet Patil, Dattatraya Tolosa, Emily Kim, Tae-Kyung Mamedov, Alexandre LaPointe, Vincent Crump, Trafford Stavrinides, Vasilis Kimberly-Duffell, Jenna Santaolalla, Aida Nieboer, Daan Olivier, Jonathan Rancati, Tiziana Ahlgren, Helén Mascarós, Juanma Löfgren, Annica Lehmann, Kurt Lin, Catherine Han Hirama, Hiromi Lee, Kwang Suk Jenster, Guido Auvinen, Anssi Bjartell, Anders Haider, Masoom van Bochove, Kees Carter, Ballentine Gledhill, Sam Buzza, Mark Kouspou, Michelle Bangma, Chris Roobol, Monique Bruinsma, Sophie Helleman, Jozien |
author_sort | Van Hemelrijck, Mieke |
collection | PubMed |
description | BACKGROUND: Signs of disease progression (28%) and conversion to active treatment without evidence of disease progression (13%) are the main reasons for discontinuation of active surveillance (AS) in men with localised prostate cancer (PCa). We aimed to develop a nomogram to predict disease progression in these patients. METHODS: As a first step in the development of a nomogram, using data from Movembers’ GAP3 Consortium (n=14,380), we assessed heterogeneity between centres in terms of risk of disease progression. We started with assessment of baseline hazards for disease progression based on grouping of centres according to follow-up protocols [high: yearly; intermediate: ~2 yearly; and low: at year 1, 4 & 7 (i.e., PRIAS)]. We conducted cause-specific random effect Cox proportional hazards regression to estimate risk of disease progression by centre in each group. RESULTS: Disease progression rates varied substantially between centres [median hazard ratio (MHR): 2.5]. After adjustment for various clinical factors (age, year of diagnosis, Gleason grade group, number of positive cores and PSA), substantial heterogeneity in disease progression remained between centres. CONCLUSIONS: When combining worldwide data on AS, we noted unexplained differences of disease progression rate even after adjustment for various clinical factors. This suggests that when developing a global nomogram, local adjustments for differences in risk of disease progression and competing outcomes such as conversion to active treatment need to be considered. |
format | Online Article Text |
id | pubmed-8039580 |
institution | National Center for Biotechnology Information |
language | English |
publishDate | 2021 |
publisher | AME Publishing Company |
record_format | MEDLINE/PubMed |
spelling | pubmed-80395802021-04-12 A first step towards a global nomogram to predict disease progression for men on active surveillance Van Hemelrijck, Mieke Ji, Xinge Helleman, Jozien Roobol, Monique J. Nieboer, Daan Bangma, Chris Frydenberg, Mark Rannikko, Antti Lee, Lui Shiong Gnanapragasam, Vincent Kattan, Michael W. Trock, Bruce Ehdaie, Behfar Carroll, Peter Filson, Christopher Kim, Jeri Logothetis, Christopher Morgan, Todd Klotz, Laurence Pickles, Tom Hyndman, Eric Moore, Caroline Gnanapragasam, Vincent Van Hemelrijck, Mieke Dasgupta, Prokar Bangma, Chris Roobol, Monique Villers, Arnauld Rannikko, Antti Valdagni, Riccardo Perry, Antoinette Hugosson, Jonas Rubio-Briones, Jose Bjartell, Anders Hefermehl, Lukas Shiong, Lee Lui Frydenberg, Mark Kakehi, Yoshiyuki Chung, Mikio Sugimoto Byung Ha van der Kwast, Theo Obbink, Henk van der Linden, Wim Hulsen, Tim de Jonge, Cees Kattan, Mike Xinge, Ji Muir, Kenneth Lophatananon, Artitaya Fahey, Michael Steyerberg, Ewout Nieboer, Daan Zhang, Liying Guo, Wei Benfante, Nicole Cowan, Janet Patil, Dattatraya Tolosa, Emily Kim, Tae-Kyung Mamedov, Alexandre LaPointe, Vincent Crump, Trafford Stavrinides, Vasilis Kimberly-Duffell, Jenna Santaolalla, Aida Nieboer, Daan Olivier, Jonathan Rancati, Tiziana Ahlgren, Helén Mascarós, Juanma Löfgren, Annica Lehmann, Kurt Lin, Catherine Han Hirama, Hiromi Lee, Kwang Suk Jenster, Guido Auvinen, Anssi Bjartell, Anders Haider, Masoom van Bochove, Kees Carter, Ballentine Gledhill, Sam Buzza, Mark Kouspou, Michelle Bangma, Chris Roobol, Monique Bruinsma, Sophie Helleman, Jozien Transl Androl Urol Original Article BACKGROUND: Signs of disease progression (28%) and conversion to active treatment without evidence of disease progression (13%) are the main reasons for discontinuation of active surveillance (AS) in men with localised prostate cancer (PCa). We aimed to develop a nomogram to predict disease progression in these patients. METHODS: As a first step in the development of a nomogram, using data from Movembers’ GAP3 Consortium (n=14,380), we assessed heterogeneity between centres in terms of risk of disease progression. We started with assessment of baseline hazards for disease progression based on grouping of centres according to follow-up protocols [high: yearly; intermediate: ~2 yearly; and low: at year 1, 4 & 7 (i.e., PRIAS)]. We conducted cause-specific random effect Cox proportional hazards regression to estimate risk of disease progression by centre in each group. RESULTS: Disease progression rates varied substantially between centres [median hazard ratio (MHR): 2.5]. After adjustment for various clinical factors (age, year of diagnosis, Gleason grade group, number of positive cores and PSA), substantial heterogeneity in disease progression remained between centres. CONCLUSIONS: When combining worldwide data on AS, we noted unexplained differences of disease progression rate even after adjustment for various clinical factors. This suggests that when developing a global nomogram, local adjustments for differences in risk of disease progression and competing outcomes such as conversion to active treatment need to be considered. AME Publishing Company 2021-03 /pmc/articles/PMC8039580/ /pubmed/33850745 http://dx.doi.org/10.21037/tau-20-1082 Text en 2021 Translational Andrology and Urology. All rights reserved. https://creativecommons.org/licenses/by-nc-nd/4.0/Open Access Statement: This is an Open Access article distributed in accordance with the Creative Commons Attribution-NonCommercial-NoDerivs 4.0 International License (CC BY-NC-ND 4.0), which permits the non-commercial replication and distribution of the article with the strict proviso that no changes or edits are made and the original work is properly cited (including links to both the formal publication through the relevant DOI and the license). See: https://creativecommons.org/licenses/by-nc-nd/4.0 (https://creativecommons.org/licenses/by-nc-nd/4.0/) . |
spellingShingle | Original Article Van Hemelrijck, Mieke Ji, Xinge Helleman, Jozien Roobol, Monique J. Nieboer, Daan Bangma, Chris Frydenberg, Mark Rannikko, Antti Lee, Lui Shiong Gnanapragasam, Vincent Kattan, Michael W. Trock, Bruce Ehdaie, Behfar Carroll, Peter Filson, Christopher Kim, Jeri Logothetis, Christopher Morgan, Todd Klotz, Laurence Pickles, Tom Hyndman, Eric Moore, Caroline Gnanapragasam, Vincent Van Hemelrijck, Mieke Dasgupta, Prokar Bangma, Chris Roobol, Monique Villers, Arnauld Rannikko, Antti Valdagni, Riccardo Perry, Antoinette Hugosson, Jonas Rubio-Briones, Jose Bjartell, Anders Hefermehl, Lukas Shiong, Lee Lui Frydenberg, Mark Kakehi, Yoshiyuki Chung, Mikio Sugimoto Byung Ha van der Kwast, Theo Obbink, Henk van der Linden, Wim Hulsen, Tim de Jonge, Cees Kattan, Mike Xinge, Ji Muir, Kenneth Lophatananon, Artitaya Fahey, Michael Steyerberg, Ewout Nieboer, Daan Zhang, Liying Guo, Wei Benfante, Nicole Cowan, Janet Patil, Dattatraya Tolosa, Emily Kim, Tae-Kyung Mamedov, Alexandre LaPointe, Vincent Crump, Trafford Stavrinides, Vasilis Kimberly-Duffell, Jenna Santaolalla, Aida Nieboer, Daan Olivier, Jonathan Rancati, Tiziana Ahlgren, Helén Mascarós, Juanma Löfgren, Annica Lehmann, Kurt Lin, Catherine Han Hirama, Hiromi Lee, Kwang Suk Jenster, Guido Auvinen, Anssi Bjartell, Anders Haider, Masoom van Bochove, Kees Carter, Ballentine Gledhill, Sam Buzza, Mark Kouspou, Michelle Bangma, Chris Roobol, Monique Bruinsma, Sophie Helleman, Jozien A first step towards a global nomogram to predict disease progression for men on active surveillance |
title | A first step towards a global nomogram to predict disease progression for men on active surveillance |
title_full | A first step towards a global nomogram to predict disease progression for men on active surveillance |
title_fullStr | A first step towards a global nomogram to predict disease progression for men on active surveillance |
title_full_unstemmed | A first step towards a global nomogram to predict disease progression for men on active surveillance |
title_short | A first step towards a global nomogram to predict disease progression for men on active surveillance |
title_sort | first step towards a global nomogram to predict disease progression for men on active surveillance |
topic | Original Article |
url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8039580/ https://www.ncbi.nlm.nih.gov/pubmed/33850745 http://dx.doi.org/10.21037/tau-20-1082 |
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firststeptowardsaglobalnomogramtopredictdiseaseprogressionformenonactivesurveillance |