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AGILE: a seamless phase I/IIa platform for the rapid evaluation of candidates for COVID-19 treatment: an update to the structured summary of a study protocol for a randomised platform trial letter

AGILE: a seamless phase I/IIa platform for the rapid evaluation of candidates for COVID-19 treatment: an update to the structured summary of a study protocol for a randomised platform trial letter
AGILE: a seamless phase I/IIa platform for the rapid evaluation of candidates for COVID-19 treatment: an update to the structured summary of a study protocol for a randomised platform trial letter

Background: there is an urgent unmet clinical need for the identification of novel therapeutics for the treatment of COVID-19. A number of COVID-19 late phase trial platforms have been developed to investigate (often repurposed) drugs both in the UK and globally (e.g. RECOVERY led by the University of Oxford and SOLIDARITY led by WHO). There is a pressing need to investigate novel candidates within early phase trial platforms, from which promising candidates can feed into established later phase platforms. AGILE grew from a UK-wide collaboration to undertake early stage clinical evaluation of candidates for SARS-CoV-2 infection to accelerate national and global healthcare interventions.

Methods/design: AGILE is a seamless phase I/IIa platform study to establish the optimum dose, determine the activity and safety of each candidate and recommend whether it should be evaluated further. Each candidate is evaluated in its own trial, either as an open label single arm healthy volunteer study or in patients, randomising between candidate and control usually in a 2:1 allocation in favour of the candidate. Each dose is assessed sequentially for safety usually in cohorts of 6 patients. Once a phase II dose has been identified, efficacy is assessed by seamlessly expanding into a larger cohort. AGILE is completely flexible in that the core design in the master protocol can be adapted for each candidate based on prior knowledge of the candidate (i.e. population, primary endpoint and sample size can be amended). This information is detailed in each candidate specific trial protocol of the master protocol.

Discussion: few approved treatments for COVID-19 are available such as dexamethasone, remdesivir and tocilizumab in hospitalised patients. The AGILE platform aims to rapidly identify new efficacious and safe treatments to help end the current global COVID-19 pandemic. We currently have three candidate specific trials within this platform study that are open to recruitment.

Trial registration: EudraCT Number: 2020-001860-27 14 March 2020 ClinicalTrials.gov Identifier: NCT04746183 19 February 2021 ISRCTN reference: 27106947.

COVID-19, Cohort Studies, Humans, Pandemics, SARS-CoV-2, Treatment Outcome
1745-6215
Griffiths, Gareth O.
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FitzGerald, Richard
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Jaki, Thomas
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Corkhill, Andrea
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Reynolds, Helen
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Ewings, Sean
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Condie, Susannah
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Tilt, Emma
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Johnson, Lucy
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Radford, Mike
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Simpson, Catherine
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Saunders, Geoffrey
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Yeats, Sara
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Mozgunov, Pavel
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Tansley-Hancock, Olana
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Martin, Karen
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Downs, Nichola
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Eberhart, Izabela
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Martin, Jonathan W. B.
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Goncalves, Cristiana
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Song, Anna
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Fletcher, Tom
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Byrne, Kelly
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Lalloo, David G.
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Owen, Andrew
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Jacobs, Michael
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Walker, Lauren
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Lyon, Rebecca
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Woods, Christie
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Gibney, Jennifer
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Chiong, Justin
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Chandiwana, Nomathemba
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Jacob, Shevin
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Lamorde, Mohammed
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Orrell, Catherine
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Pirmohamed, Munir
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Khoo, Saye
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AGILE investigators
Griffiths, Gareth O.
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FitzGerald, Richard
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Jaki, Thomas
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Corkhill, Andrea
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Reynolds, Helen
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Ewings, Sean
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Condie, Susannah
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Tilt, Emma
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Johnson, Lucy
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Radford, Mike
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Simpson, Catherine
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Saunders, Geoffrey
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Yeats, Sara
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Mozgunov, Pavel
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Tansley-Hancock, Olana
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Martin, Karen
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Downs, Nichola
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Eberhart, Izabela
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Martin, Jonathan W. B.
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Goncalves, Cristiana
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Song, Anna
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Fletcher, Tom
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Byrne, Kelly
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Lalloo, David G.
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Owen, Andrew
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Jacobs, Michael
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Walker, Lauren
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Lyon, Rebecca
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Woods, Christie
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Gibney, Jennifer
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Chiong, Justin
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Chandiwana, Nomathemba
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Jacob, Shevin
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Lamorde, Mohammed
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Orrell, Catherine
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Pirmohamed, Munir
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Khoo, Saye
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Griffiths, Gareth O., FitzGerald, Richard, Jaki, Thomas, Corkhill, Andrea, Reynolds, Helen, Ewings, Sean and Condie, Susannah , AGILE investigators (2021) AGILE: a seamless phase I/IIa platform for the rapid evaluation of candidates for COVID-19 treatment: an update to the structured summary of a study protocol for a randomised platform trial letter. Trials, 22, [487 (2021)]. (doi:10.1186/s13063-021-05458-4).

Record type: Article

Abstract

Background: there is an urgent unmet clinical need for the identification of novel therapeutics for the treatment of COVID-19. A number of COVID-19 late phase trial platforms have been developed to investigate (often repurposed) drugs both in the UK and globally (e.g. RECOVERY led by the University of Oxford and SOLIDARITY led by WHO). There is a pressing need to investigate novel candidates within early phase trial platforms, from which promising candidates can feed into established later phase platforms. AGILE grew from a UK-wide collaboration to undertake early stage clinical evaluation of candidates for SARS-CoV-2 infection to accelerate national and global healthcare interventions.

Methods/design: AGILE is a seamless phase I/IIa platform study to establish the optimum dose, determine the activity and safety of each candidate and recommend whether it should be evaluated further. Each candidate is evaluated in its own trial, either as an open label single arm healthy volunteer study or in patients, randomising between candidate and control usually in a 2:1 allocation in favour of the candidate. Each dose is assessed sequentially for safety usually in cohorts of 6 patients. Once a phase II dose has been identified, efficacy is assessed by seamlessly expanding into a larger cohort. AGILE is completely flexible in that the core design in the master protocol can be adapted for each candidate based on prior knowledge of the candidate (i.e. population, primary endpoint and sample size can be amended). This information is detailed in each candidate specific trial protocol of the master protocol.

Discussion: few approved treatments for COVID-19 are available such as dexamethasone, remdesivir and tocilizumab in hospitalised patients. The AGILE platform aims to rapidly identify new efficacious and safe treatments to help end the current global COVID-19 pandemic. We currently have three candidate specific trials within this platform study that are open to recruitment.

Trial registration: EudraCT Number: 2020-001860-27 14 March 2020 ClinicalTrials.gov Identifier: NCT04746183 19 February 2021 ISRCTN reference: 27106947.

Text
s13063-021-05458-4 - Version of Record
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More information

Accepted/In Press date: 14 July 2021
Published date: 26 July 2021
Keywords: COVID-19, Cohort Studies, Humans, Pandemics, SARS-CoV-2, Treatment Outcome

Identifiers

Local EPrints ID: 453383
URI: http://eprints.soton.ac.uk/id/eprint/453383
DOI: doi:10.1186/s13063-021-05458-4
ISSN: 1745-6215
PURE UUID: 9ddb8f82-8789-4578-b88d-890728e2d4b4
ORCID for Gareth O. Griffiths: ORCID iD orcid.org/0000-0002-9579-8021
ORCID for Karen Martin: ORCID iD orcid.org/0000-0002-6362-0501

Catalogue record

Date deposited: 13 Jan 2022 18:18
Last modified: 17 Mar 2024 03:36

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Contributors

Author: Gareth O. Griffiths ORCID iD
Author: Richard FitzGerald
Author: Thomas Jaki
Author: Andrea Corkhill
Author: Helen Reynolds
Author: Sean Ewings
Author: Susannah Condie
Author: Emma Tilt
Author: Lucy Johnson
Author: Mike Radford
Author: Catherine Simpson
Author: Geoffrey Saunders
Author: Sara Yeats
Author: Pavel Mozgunov
Author: Olana Tansley-Hancock
Author: Karen Martin ORCID iD
Author: Nichola Downs
Author: Izabela Eberhart
Author: Jonathan W. B. Martin
Author: Cristiana Goncalves
Author: Anna Song
Author: Tom Fletcher
Author: Kelly Byrne
Author: David G. Lalloo
Author: Andrew Owen
Author: Michael Jacobs
Author: Lauren Walker
Author: Rebecca Lyon
Author: Christie Woods
Author: Jennifer Gibney
Author: Justin Chiong
Author: Nomathemba Chandiwana
Author: Shevin Jacob
Author: Mohammed Lamorde
Author: Catherine Orrell
Author: Munir Pirmohamed
Author: Saye Khoo
Corporate Author: AGILE investigators

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