Trial design and objectives for castration-resistant prostate cancer: Updated recommendations from the prostate cancer clinical trials working group 3

Howard I. Scher; Michael J. Morris; Walter M. Stadler; Celestia Higano; Ethan Basch; Karim Fizazi; Emmanuel S. Antonarakis; Tomasz M. Beer; Michael A. Carducci; Kim N. Chi; Paul G. Corn; Johann S. De Bono; Robert Dreicer; Daniel J. George; Elisabeth I. Heath; Maha Hussain; Wm Kevin Kelly; Glenn Liu; Christopher Logothetis; David Nanus; Mark N. Stein; Dana E. Rathkopf; Susan F. Slovin; Charles J. Ryan; Oliver Sartor; Eric J. Small; Matthew Raymond Smith; Cora N. Sternberg; Mary Ellen Taplin; George Wilding; Peter S. Nelson; Lawrence H. Schwartz; Susan Halabi; Philip W. Kantoff; Andrew J. Armstrong

doi:10.1200/JCO.2015.64.2702

Trial design and objectives for castration-resistant prostate cancer: Updated recommendations from the prostate cancer clinical trials working group 3

Howard I. Scher, Michael J. Morris, Walter M. Stadler, Celestia Higano, Ethan Basch, Karim Fizazi, Emmanuel S. Antonarakis, Tomasz M. Beer, Michael A. Carducci, Kim N. Chi, Paul G. Corn, Johann S. De Bono, Robert Dreicer, Daniel J. George, Elisabeth I. Heath, Maha Hussain, Wm Kevin Kelly, Glenn Liu, Christopher Logothetis, David NanusMark N. Stein, Dana E. Rathkopf, Susan F. Slovin, Charles J. Ryan, Oliver Sartor, Eric J. Small, Matthew Raymond Smith, Cora N. Sternberg, Mary Ellen Taplin, George Wilding, Peter S. Nelson, Lawrence H. Schwartz, Susan Halabi, Philip W. Kantoff, Andrew J. Armstrong

Hematology & Medical Oncology

Research output: Contribution to journal › Article › peer-review

1050 Scopus citations

Abstract

Purpose Evolving treatments, disease phenotypes, and biology, together with a changing drug development environment, have created the need to revise castration-resistant prostate cancer (CRPC) clinical trial recommendations to succeed those from prior Prostate Cancer Clinical Trials Working Groups. Methods An international expert committee of prostate cancer clinical investigators (the Prostate Cancer Clinical Trials Working Group 3 [PCWG3]) was reconvened and expanded and met in 2012-2015 to formulate updated criteria on the basis of emerging trial data and validation studies of the Prostate Cancer Clinical Trials Working Group 2 recommendations. Results PCWG3 recommends that baseline patient assessment include tumor histology, detailed records of prior systemic treatments and responses, and a detailed reporting of disease subtypes based on an anatomic pattern of metastatic spread. New recommendations for trial outcome measures include the time to event end point of symptomatic skeletal events, as well as time to first metastasis and time to progression for trials in the nonmetastatic CRPC state. PCWG3 introduces the concept of no longer clinically benefiting to underscore the distinction between first evidence of progression and the clinical need to terminate or change treatment, and the importance of documenting progression in existing lesions as distinct from the development of new lesions. Serial biologic profiling using tumor samples from biopsies, blood-based diagnostics, and/or imaging is also recommended to gain insight into mechanisms of resistance and to identify predictive biomarkers of sensitivity for use in prospective trials. Conclusion PCWG3 moves drug development closer to unmet needs in clinical practice by focusing on disease manifestations most likely to affect prognosis adversely for therapeutics tested in both nonmetastatic and metastatic CRPC populations. Consultation with regulatory authorities is recommended if a trial is intended to seek support for drug approval.

Original language	English (US)
Pages (from-to)	1402-1418
Number of pages	17
Journal	Journal of Clinical Oncology
Volume	34
Issue number	12
DOIs	https://doi.org/10.1200/JCO.2015.64.2702
State	Published - Apr 20 2016

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1200/JCO.2015.64.2702

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Scher, H. I., Morris, M. J., Stadler, W. M., Higano, C., Basch, E., Fizazi, K., Antonarakis, E. S., Beer, T. M., Carducci, M. A., Chi, K. N., Corn, P. G., De Bono, J. S., Dreicer, R., George, D. J., Heath, E. I., Hussain, M., Kelly, W. K., Liu, G., Logothetis, C., ... Armstrong, A. J. (2016). Trial design and objectives for castration-resistant prostate cancer: Updated recommendations from the prostate cancer clinical trials working group 3. Journal of Clinical Oncology, 34(12), 1402-1418. https://doi.org/10.1200/JCO.2015.64.2702

Scher, HI, Morris, MJ, Stadler, WM, Higano, C, Basch, E, Fizazi, K, Antonarakis, ES, Beer, TM, Carducci, MA, Chi, KN, Corn, PG, De Bono, JS, Dreicer, R, George, DJ, Heath, EI, Hussain, M, Kelly, WK, Liu, G, Logothetis, C, Nanus, D, Stein, MN, Rathkopf, DE, Slovin, SF, Ryan, CJ, Sartor, O, Small, EJ, Smith, MR, Sternberg, CN, Taplin, ME, Wilding, G, Nelson, PS, Schwartz, LH, Halabi, S, Kantoff, PW & Armstrong, AJ 2016, 'Trial design and objectives for castration-resistant prostate cancer: Updated recommendations from the prostate cancer clinical trials working group 3', Journal of Clinical Oncology, vol. 34, no. 12, pp. 1402-1418. https://doi.org/10.1200/JCO.2015.64.2702

@article{a2c7b17f10d74793911486a59f574899,

title = "Trial design and objectives for castration-resistant prostate cancer: Updated recommendations from the prostate cancer clinical trials working group 3",

abstract = "Purpose Evolving treatments, disease phenotypes, and biology, together with a changing drug development environment, have created the need to revise castration-resistant prostate cancer (CRPC) clinical trial recommendations to succeed those from prior Prostate Cancer Clinical Trials Working Groups. Methods An international expert committee of prostate cancer clinical investigators (the Prostate Cancer Clinical Trials Working Group 3 [PCWG3]) was reconvened and expanded and met in 2012-2015 to formulate updated criteria on the basis of emerging trial data and validation studies of the Prostate Cancer Clinical Trials Working Group 2 recommendations. Results PCWG3 recommends that baseline patient assessment include tumor histology, detailed records of prior systemic treatments and responses, and a detailed reporting of disease subtypes based on an anatomic pattern of metastatic spread. New recommendations for trial outcome measures include the time to event end point of symptomatic skeletal events, as well as time to first metastasis and time to progression for trials in the nonmetastatic CRPC state. PCWG3 introduces the concept of no longer clinically benefiting to underscore the distinction between first evidence of progression and the clinical need to terminate or change treatment, and the importance of documenting progression in existing lesions as distinct from the development of new lesions. Serial biologic profiling using tumor samples from biopsies, blood-based diagnostics, and/or imaging is also recommended to gain insight into mechanisms of resistance and to identify predictive biomarkers of sensitivity for use in prospective trials. Conclusion PCWG3 moves drug development closer to unmet needs in clinical practice by focusing on disease manifestations most likely to affect prognosis adversely for therapeutics tested in both nonmetastatic and metastatic CRPC populations. Consultation with regulatory authorities is recommended if a trial is intended to seek support for drug approval.",

author = "Scher, {Howard I.} and Morris, {Michael J.} and Stadler, {Walter M.} and Celestia Higano and Ethan Basch and Karim Fizazi and Antonarakis, {Emmanuel S.} and Beer, {Tomasz M.} and Carducci, {Michael A.} and Chi, {Kim N.} and Corn, {Paul G.} and {De Bono}, {Johann S.} and Robert Dreicer and George, {Daniel J.} and Heath, {Elisabeth I.} and Maha Hussain and Kelly, {Wm Kevin} and Glenn Liu and Christopher Logothetis and David Nanus and Stein, {Mark N.} and Rathkopf, {Dana E.} and Slovin, {Susan F.} and Ryan, {Charles J.} and Oliver Sartor and Small, {Eric J.} and Smith, {Matthew Raymond} and Sternberg, {Cora N.} and Taplin, {Mary Ellen} and George Wilding and Nelson, {Peter S.} and Schwartz, {Lawrence H.} and Susan Halabi and Kantoff, {Philip W.} and Armstrong, {Andrew J.}",

note = "Publisher Copyright: {\textcopyright} 2016 by American Society of Clinical Oncology.",

year = "2016",

month = apr,

day = "20",

doi = "10.1200/JCO.2015.64.2702",

language = "English (US)",

volume = "34",

pages = "1402--1418",

journal = "Journal of Clinical Oncology",

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TY - JOUR

T1 - Trial design and objectives for castration-resistant prostate cancer

T2 - Updated recommendations from the prostate cancer clinical trials working group 3

AU - Scher, Howard I.

AU - Morris, Michael J.

AU - Stadler, Walter M.

AU - Higano, Celestia

AU - Basch, Ethan

AU - Fizazi, Karim

AU - Antonarakis, Emmanuel S.

AU - Beer, Tomasz M.

AU - Carducci, Michael A.

AU - Chi, Kim N.

AU - Corn, Paul G.

AU - De Bono, Johann S.

AU - Dreicer, Robert

AU - George, Daniel J.

AU - Heath, Elisabeth I.

AU - Hussain, Maha

AU - Kelly, Wm Kevin

AU - Liu, Glenn

AU - Logothetis, Christopher

AU - Nanus, David

AU - Stein, Mark N.

AU - Rathkopf, Dana E.

AU - Slovin, Susan F.

AU - Ryan, Charles J.

AU - Sartor, Oliver

AU - Small, Eric J.

AU - Smith, Matthew Raymond

AU - Sternberg, Cora N.

AU - Taplin, Mary Ellen

AU - Wilding, George

AU - Nelson, Peter S.

AU - Schwartz, Lawrence H.

AU - Halabi, Susan

AU - Kantoff, Philip W.

AU - Armstrong, Andrew J.

PY - 2016/4/20

Y1 - 2016/4/20

N2 - Purpose Evolving treatments, disease phenotypes, and biology, together with a changing drug development environment, have created the need to revise castration-resistant prostate cancer (CRPC) clinical trial recommendations to succeed those from prior Prostate Cancer Clinical Trials Working Groups. Methods An international expert committee of prostate cancer clinical investigators (the Prostate Cancer Clinical Trials Working Group 3 [PCWG3]) was reconvened and expanded and met in 2012-2015 to formulate updated criteria on the basis of emerging trial data and validation studies of the Prostate Cancer Clinical Trials Working Group 2 recommendations. Results PCWG3 recommends that baseline patient assessment include tumor histology, detailed records of prior systemic treatments and responses, and a detailed reporting of disease subtypes based on an anatomic pattern of metastatic spread. New recommendations for trial outcome measures include the time to event end point of symptomatic skeletal events, as well as time to first metastasis and time to progression for trials in the nonmetastatic CRPC state. PCWG3 introduces the concept of no longer clinically benefiting to underscore the distinction between first evidence of progression and the clinical need to terminate or change treatment, and the importance of documenting progression in existing lesions as distinct from the development of new lesions. Serial biologic profiling using tumor samples from biopsies, blood-based diagnostics, and/or imaging is also recommended to gain insight into mechanisms of resistance and to identify predictive biomarkers of sensitivity for use in prospective trials. Conclusion PCWG3 moves drug development closer to unmet needs in clinical practice by focusing on disease manifestations most likely to affect prognosis adversely for therapeutics tested in both nonmetastatic and metastatic CRPC populations. Consultation with regulatory authorities is recommended if a trial is intended to seek support for drug approval.

AB - Purpose Evolving treatments, disease phenotypes, and biology, together with a changing drug development environment, have created the need to revise castration-resistant prostate cancer (CRPC) clinical trial recommendations to succeed those from prior Prostate Cancer Clinical Trials Working Groups. Methods An international expert committee of prostate cancer clinical investigators (the Prostate Cancer Clinical Trials Working Group 3 [PCWG3]) was reconvened and expanded and met in 2012-2015 to formulate updated criteria on the basis of emerging trial data and validation studies of the Prostate Cancer Clinical Trials Working Group 2 recommendations. Results PCWG3 recommends that baseline patient assessment include tumor histology, detailed records of prior systemic treatments and responses, and a detailed reporting of disease subtypes based on an anatomic pattern of metastatic spread. New recommendations for trial outcome measures include the time to event end point of symptomatic skeletal events, as well as time to first metastasis and time to progression for trials in the nonmetastatic CRPC state. PCWG3 introduces the concept of no longer clinically benefiting to underscore the distinction between first evidence of progression and the clinical need to terminate or change treatment, and the importance of documenting progression in existing lesions as distinct from the development of new lesions. Serial biologic profiling using tumor samples from biopsies, blood-based diagnostics, and/or imaging is also recommended to gain insight into mechanisms of resistance and to identify predictive biomarkers of sensitivity for use in prospective trials. Conclusion PCWG3 moves drug development closer to unmet needs in clinical practice by focusing on disease manifestations most likely to affect prognosis adversely for therapeutics tested in both nonmetastatic and metastatic CRPC populations. Consultation with regulatory authorities is recommended if a trial is intended to seek support for drug approval.

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Trial design and objectives for castration-resistant prostate cancer: Updated recommendations from the prostate cancer clinical trials working group 3

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