Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)

BACKGROUND: There is an active debate about the role that endpoints other than overall survival (OS) should play in the drug approval process. Yet the term ‘surrogate endpoint’ implies that OS is the only critical metric for regulatory approval of cancer treatments. We systematically analyzed the re...

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Detalles Bibliográficos
Autores principales: Brooks, Neon, Campone, Mario, Paddock, Silvia, Shortenhaus, Scott, Grainger, David, Zummo, Jacqueline, Thomas, Samuel, Li, Rose
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioExcel Publishing Ltd 2017
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5699106/
https://www.ncbi.nlm.nih.gov/pubmed/29167693
http://dx.doi.org/10.7573/dic.212507
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author Brooks, Neon
Campone, Mario
Paddock, Silvia
Shortenhaus, Scott
Grainger, David
Zummo, Jacqueline
Thomas, Samuel
Li, Rose
author_facet Brooks, Neon
Campone, Mario
Paddock, Silvia
Shortenhaus, Scott
Grainger, David
Zummo, Jacqueline
Thomas, Samuel
Li, Rose
author_sort Brooks, Neon
collection PubMed
description BACKGROUND: There is an active debate about the role that endpoints other than overall survival (OS) should play in the drug approval process. Yet the term ‘surrogate endpoint’ implies that OS is the only critical metric for regulatory approval of cancer treatments. We systematically analyzed the relationship between U.S. Food and Drug Administration (FDA) approval and publication of OS evidence to understand better the risks and benefits of delaying approval until OS evidence is available. SCOPE: Using the PACE Continuous Innovation Indicators (CII) platform, we analyzed the effects of cancer type, treatment goal, and year of approval on the lag time between FDA approval and publication of first significant OS finding for 53 treatments approved between 1952 and 2016 for 10 cancer types (n = 71 approved indications). FINDINGS: Greater than 59% of treatments were approved before significant OS data for the approved indication were published. Of the drugs in the sample, 31% had lags between approval and first published OS evidence of 4 years or longer. The average number of years between approval and first OS evidence varied by cancer type and did not reliably predict the eventual amount of OS evidence accumulated. CONCLUSIONS: Striking the right balance between early access and minimizing risk is a central challenge for regulators worldwide. We illustrate that endpoints other than OS have long helped to provide timely access to new medicines, including many current standards of care. We found that many critical drugs are approved many years before OS data are published, and that OS may not be the most appropriate endpoint in some treatment contexts. Our examination of approved treatments without significant OS data suggests contexts where OS may not be the most relevant endpoint and highlights the importance of using a wide variety of fit-for-purpose evidence types in the approval process.
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spelling pubmed-56991062017-11-22 Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII) Brooks, Neon Campone, Mario Paddock, Silvia Shortenhaus, Scott Grainger, David Zummo, Jacqueline Thomas, Samuel Li, Rose Drugs Context Original Research BACKGROUND: There is an active debate about the role that endpoints other than overall survival (OS) should play in the drug approval process. Yet the term ‘surrogate endpoint’ implies that OS is the only critical metric for regulatory approval of cancer treatments. We systematically analyzed the relationship between U.S. Food and Drug Administration (FDA) approval and publication of OS evidence to understand better the risks and benefits of delaying approval until OS evidence is available. SCOPE: Using the PACE Continuous Innovation Indicators (CII) platform, we analyzed the effects of cancer type, treatment goal, and year of approval on the lag time between FDA approval and publication of first significant OS finding for 53 treatments approved between 1952 and 2016 for 10 cancer types (n = 71 approved indications). FINDINGS: Greater than 59% of treatments were approved before significant OS data for the approved indication were published. Of the drugs in the sample, 31% had lags between approval and first published OS evidence of 4 years or longer. The average number of years between approval and first OS evidence varied by cancer type and did not reliably predict the eventual amount of OS evidence accumulated. CONCLUSIONS: Striking the right balance between early access and minimizing risk is a central challenge for regulators worldwide. We illustrate that endpoints other than OS have long helped to provide timely access to new medicines, including many current standards of care. We found that many critical drugs are approved many years before OS data are published, and that OS may not be the most appropriate endpoint in some treatment contexts. Our examination of approved treatments without significant OS data suggests contexts where OS may not be the most relevant endpoint and highlights the importance of using a wide variety of fit-for-purpose evidence types in the approval process. BioExcel Publishing Ltd 2017-11-15 /pmc/articles/PMC5699106/ /pubmed/29167693 http://dx.doi.org/10.7573/dic.212507 Text en Copyright © 2017 Brooks N, Campone M, Paddock S, Shortenhaus S, Grainger D, Zummo J, Thomas S, Li R Distributed under the terms of the Creative Commons License Deed CC BY NC ND 4.0, which allows anyone to copy, distribute, and transmit the article provided it is properly attributed in the manner specified below. No commercial use without permission.
spellingShingle Original Research
Brooks, Neon
Campone, Mario
Paddock, Silvia
Shortenhaus, Scott
Grainger, David
Zummo, Jacqueline
Thomas, Samuel
Li, Rose
Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)
title Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)
title_full Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)
title_fullStr Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)
title_full_unstemmed Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)
title_short Approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the PACE Continuous Innovation Indicators™ (CII)
title_sort approving cancer treatments based on endpoints other than overall survival: an analysis of historical data using the pace continuous innovation indicators™ (cii)
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5699106/
https://www.ncbi.nlm.nih.gov/pubmed/29167693
http://dx.doi.org/10.7573/dic.212507
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