Adaptive platform trials: definition, design, conduct and reporting considerations

Derek C. Angus; Brian M. Alexander; Scott Berry; Meredith Buxton; Roger Lewis; Melissa Paoloni; Steven A. R. Webb; Steven Arnold; Anna Barker; Donald A. Berry; Marc J. M. Bonten; Mary Brophy; Christopher Butler; Timothy F. Cloughesy; Lennie P. G. Derde; Laura J. Esserman; Ryan Ferguson; Louis Fiore; Sarah C. Gaffey; J. Michael Gaziano; Kathy Giusti; Herman Goossens; Stephane Heritier; Bradley Hyman; Michael Krams; Kay Larholt; Lisa M. LaVange; Philip Lavori; Andrew W. Lo; Alex John London; Victoria Manax; Colin McArthur; Genevieve O'Neill; Giovanni Parmigiani; Jane Perlmutter; Elizabeth A. Petzold; Craig Ritchie; Kathryn M. Rowan; Christopher W. Seymour; Nathan, I Shapiro; Diane M. Simeone; Bradley Smith; Bradley Spellberg; Ariel Dora Stern; Lorenzo Trippa; Mark Trusheim; Kert Viele; Patrick Y. Wen; Janet Woodcock

doi:10.1038/s41573-019-0034-3

Adaptive platform trials: definition, design, conduct and reporting considerations

Derek C. Angus
, Brian M. Alexander
, Scott Berry
, Meredith Buxton
, Roger Lewis
, Melissa Paoloni
, Steven A. R. Webb
, Steven Arnold
, Anna Barker
, Donald A. Berry
, Marc J. M. Bonten
, Mary Brophy
, Christopher Butler
, Timothy F. Cloughesy
, Lennie P. G. Derde
, Laura J. Esserman
, Ryan Ferguson
, Louis Fiore
, Sarah C. Gaffey
, J. Michael Gaziano

Kathy Giusti, Herman Goossens, Stephane Heritier, Bradley Hyman, Michael Krams, Kay Larholt, Lisa M. LaVange, Philip Lavori, Andrew W. Lo, Alex John London, Victoria Manax, Colin McArthur, Genevieve O'Neill, Giovanni Parmigiani, Jane Perlmutter, Elizabeth A. Petzold, Craig Ritchie, Kathryn M. Rowan, Christopher W. Seymour, Nathan, I Shapiro, Diane M. Simeone, Bradley Smith, Bradley Spellberg, Ariel Dora Stern, Lorenzo Trippa, Mark Trusheim, Kert Viele, Patrick Y. Wen, Janet Woodcock

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

Abstract

Researchers, clinicians, policymakers and patients are increasingly interested in questions about therapeutic interventions that are difficult or costly to answer with traditional, free-standing, parallel-group randomized controlled trials (RCTs). Examples include scenarios in which there is a desire to compare multiple interventions, to generate separate effect estimates across subgroups of patients with distinct but related conditions or clinical features, or to minimize downtime between trials. In response, researchers have proposed new RCT designs such as adaptive platform trials (APTs), which are able to study multiple interventions in a disease or condition in a perpetual manner, with interventions entering and leaving the platform on the basis of a predefined decision algorithm. APTs offer innovations that could reshape clinical trials, and several APTs are now funded in various disease areas. With the aim of facilitating the use of APTs, here we review common features and issues that arise with such trials, and offer recommendations to promote best practices in their design, conduct, oversight and reporting.

Original language	English
Pages (from-to)	797-807
Number of pages	11
Journal	Nature Reviews Drug Discovery
Volume	18
Issue number	10
DOIs	https://doi.org/10.1038/s41573-019-0034-3
Publication status	Published - Oct 2019

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Angus, D. C., Alexander, B. M., Berry, S., Buxton, M., Lewis, R., Paoloni, M., Webb, S. A. R., Arnold, S., Barker, A., Berry, D. A., Bonten, M. J. M., Brophy, M., Butler, C., Cloughesy, T. F., Derde, L. P. G., Esserman, L. J., Ferguson, R., Fiore, L., Gaffey, S. C., ... Woodcock, J. (2019). Adaptive platform trials: definition, design, conduct and reporting considerations. Nature Reviews Drug Discovery, 18(10), 797-807. https://doi.org/10.1038/s41573-019-0034-3

@article{330ede87de6f4d6591a4eea7b7129bf1,

title = "Adaptive platform trials: definition, design, conduct and reporting considerations",

abstract = "Researchers, clinicians, policymakers and patients are increasingly interested in questions about therapeutic interventions that are difficult or costly to answer with traditional, free-standing, parallel-group randomized controlled trials (RCTs). Examples include scenarios in which there is a desire to compare multiple interventions, to generate separate effect estimates across subgroups of patients with distinct but related conditions or clinical features, or to minimize downtime between trials. In response, researchers have proposed new RCT designs such as adaptive platform trials (APTs), which are able to study multiple interventions in a disease or condition in a perpetual manner, with interventions entering and leaving the platform on the basis of a predefined decision algorithm. APTs offer innovations that could reshape clinical trials, and several APTs are now funded in various disease areas. With the aim of facilitating the use of APTs, here we review common features and issues that arise with such trials, and offer recommendations to promote best practices in their design, conduct, oversight and reporting.",

author = "Angus, \{Derek C.\} and Alexander, \{Brian M.\} and Scott Berry and Meredith Buxton and Roger Lewis and Melissa Paoloni and Webb, \{Steven A. R.\} and Steven Arnold and Anna Barker and Berry, \{Donald A.\} and Bonten, \{Marc J. M.\} and Mary Brophy and Christopher Butler and Cloughesy, \{Timothy F.\} and Derde, \{Lennie P. G.\} and Esserman, \{Laura J.\} and Ryan Ferguson and Louis Fiore and Gaffey, \{Sarah C.\} and Gaziano, \{J. Michael\} and Kathy Giusti and Herman Goossens and Stephane Heritier and Bradley Hyman and Michael Krams and Kay Larholt and LaVange, \{Lisa M.\} and Philip Lavori and Lo, \{Andrew W.\} and London, \{Alex John\} and Victoria Manax and Colin McArthur and Genevieve O'Neill and Giovanni Parmigiani and Jane Perlmutter and Petzold, \{Elizabeth A.\} and Craig Ritchie and Rowan, \{Kathryn M.\} and Seymour, \{Christopher W.\} and Shapiro, \{Nathan, I\} and Simeone, \{Diane M.\} and Bradley Smith and Bradley Spellberg and Stern, \{Ariel Dora\} and Lorenzo Trippa and Mark Trusheim and Kert Viele and Wen, \{Patrick Y.\} and Janet Woodcock",

note = "Funding Information: APTs do not lend themselves to traditional funding models. National Institutes of Health grants, for example, typically require known trial sizes and timelines to calculate and distribute budgets. A trial design intended to enrol perpetually, with an unclear — and theoretically unbounded — number of enrollees, does not fit this paradigm. Similarly, APTs that test multiple experimental interventions must overcome the financial and legal hurdles that arise when approaching multiple pharmaceutical companies to participate in a single trial. In this scenario, the APT sponsor would interact with industry by offering various financial terms to participate in the trial. For smaller trials without registration potential, this might take the form of investigator-initiated studies through the usual channels. For larger trials with potential for registration, more significant financing is required. This may take the form of a fee-for-service arrangement whereby industry partners pay a per-patient or per-arm cost to participate (a form of {\textquoteleft}pay-to-play{\textquoteright}). I-SPY 2 was initially funded through federal support and donations, but has now evolved to a pay-to-play model. REMAP-CAP has thus far focused on comparative effectiveness questions and is funded by government grants from multiple countries. GBM AGILE is funded via donations and a pay-to-play model. Publisher Copyright: {\textcopyright} 2019, Springer Nature Limited.",

year = "2019",

month = oct,

doi = "10.1038/s41573-019-0034-3",

language = "English",

volume = "18",

pages = "797--807",

journal = "Nature Reviews Drug Discovery",

issn = "1474-1776",

publisher = "Nature Research",

number = "10",

}

Angus, DC, Alexander, BM, Berry, S, Buxton, M, Lewis, R, Paoloni, M, Webb, SAR, Arnold, S, Barker, A, Berry, DA, Bonten, MJM, Brophy, M, Butler, C, Cloughesy, TF, Derde, LPG, Esserman, LJ, Ferguson, R, Fiore, L, Gaffey, SC, Gaziano, JM, Giusti, K, Goossens, H, Heritier, S, Hyman, B, Krams, M, Larholt, K, LaVange, LM, Lavori, P, Lo, AW, London, AJ, Manax, V, McArthur, C, O'Neill, G, Parmigiani, G, Perlmutter, J, Petzold, EA, Ritchie, C, Rowan, KM, Seymour, CW, Shapiro, NI, Simeone, DM, Smith, B, Spellberg, B, Stern, AD, Trippa, L, Trusheim, M, Viele, K, Wen, PY & Woodcock, J 2019, 'Adaptive platform trials: definition, design, conduct and reporting considerations', Nature Reviews Drug Discovery, vol. 18, no. 10, pp. 797-807. https://doi.org/10.1038/s41573-019-0034-3

TY - JOUR

T1 - Adaptive platform trials: definition, design, conduct and reporting considerations

AU - Angus, Derek C.

AU - Alexander, Brian M.

AU - Berry, Scott

AU - Buxton, Meredith

AU - Lewis, Roger

AU - Paoloni, Melissa

AU - Webb, Steven A. R.

AU - Arnold, Steven

AU - Barker, Anna

AU - Berry, Donald A.

AU - Bonten, Marc J. M.

AU - Brophy, Mary

AU - Butler, Christopher

AU - Cloughesy, Timothy F.

AU - Derde, Lennie P. G.

AU - Esserman, Laura J.

AU - Ferguson, Ryan

AU - Fiore, Louis

AU - Gaffey, Sarah C.

AU - Gaziano, J. Michael

AU - Giusti, Kathy

AU - Goossens, Herman

AU - Heritier, Stephane

AU - Hyman, Bradley

AU - Krams, Michael

AU - Larholt, Kay

AU - LaVange, Lisa M.

AU - Lavori, Philip

AU - Lo, Andrew W.

AU - London, Alex John

AU - Manax, Victoria

AU - McArthur, Colin

AU - O'Neill, Genevieve

AU - Parmigiani, Giovanni

AU - Perlmutter, Jane

AU - Petzold, Elizabeth A.

AU - Ritchie, Craig

AU - Rowan, Kathryn M.

AU - Seymour, Christopher W.

AU - Shapiro, Nathan, I

AU - Simeone, Diane M.

AU - Smith, Bradley

AU - Spellberg, Bradley

AU - Stern, Ariel Dora

AU - Trippa, Lorenzo

AU - Trusheim, Mark

AU - Viele, Kert

AU - Wen, Patrick Y.

AU - Woodcock, Janet

N1 - Funding Information: APTs do not lend themselves to traditional funding models. National Institutes of Health grants, for example, typically require known trial sizes and timelines to calculate and distribute budgets. A trial design intended to enrol perpetually, with an unclear — and theoretically unbounded — number of enrollees, does not fit this paradigm. Similarly, APTs that test multiple experimental interventions must overcome the financial and legal hurdles that arise when approaching multiple pharmaceutical companies to participate in a single trial. In this scenario, the APT sponsor would interact with industry by offering various financial terms to participate in the trial. For smaller trials without registration potential, this might take the form of investigator-initiated studies through the usual channels. For larger trials with potential for registration, more significant financing is required. This may take the form of a fee-for-service arrangement whereby industry partners pay a per-patient or per-arm cost to participate (a form of ‘pay-to-play’). I-SPY 2 was initially funded through federal support and donations, but has now evolved to a pay-to-play model. REMAP-CAP has thus far focused on comparative effectiveness questions and is funded by government grants from multiple countries. GBM AGILE is funded via donations and a pay-to-play model. Publisher Copyright: © 2019, Springer Nature Limited.

PY - 2019/10

Y1 - 2019/10

N2 - Researchers, clinicians, policymakers and patients are increasingly interested in questions about therapeutic interventions that are difficult or costly to answer with traditional, free-standing, parallel-group randomized controlled trials (RCTs). Examples include scenarios in which there is a desire to compare multiple interventions, to generate separate effect estimates across subgroups of patients with distinct but related conditions or clinical features, or to minimize downtime between trials. In response, researchers have proposed new RCT designs such as adaptive platform trials (APTs), which are able to study multiple interventions in a disease or condition in a perpetual manner, with interventions entering and leaving the platform on the basis of a predefined decision algorithm. APTs offer innovations that could reshape clinical trials, and several APTs are now funded in various disease areas. With the aim of facilitating the use of APTs, here we review common features and issues that arise with such trials, and offer recommendations to promote best practices in their design, conduct, oversight and reporting.

AB - Researchers, clinicians, policymakers and patients are increasingly interested in questions about therapeutic interventions that are difficult or costly to answer with traditional, free-standing, parallel-group randomized controlled trials (RCTs). Examples include scenarios in which there is a desire to compare multiple interventions, to generate separate effect estimates across subgroups of patients with distinct but related conditions or clinical features, or to minimize downtime between trials. In response, researchers have proposed new RCT designs such as adaptive platform trials (APTs), which are able to study multiple interventions in a disease or condition in a perpetual manner, with interventions entering and leaving the platform on the basis of a predefined decision algorithm. APTs offer innovations that could reshape clinical trials, and several APTs are now funded in various disease areas. With the aim of facilitating the use of APTs, here we review common features and issues that arise with such trials, and offer recommendations to promote best practices in their design, conduct, oversight and reporting.

UR - https://www.scopus.com/pages/publications/85072790580

U2 - 10.1038/s41573-019-0034-3

DO - 10.1038/s41573-019-0034-3

M3 - Article

SN - 1474-1776

VL - 18

SP - 797

EP - 807

JO - Nature Reviews Drug Discovery

JF - Nature Reviews Drug Discovery

IS - 10

ER -

Adaptive platform trials: definition, design, conduct and reporting considerations

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