Report of the first seven agents in the I-SPY COVID trial: a phase 2, open label, adaptive platform randomised controlled trial. (April 2023)
- Record Type:
- Journal Article
- Title:
- Report of the first seven agents in the I-SPY COVID trial: a phase 2, open label, adaptive platform randomised controlled trial. (April 2023)
- Main Title:
- Report of the first seven agents in the I-SPY COVID trial: a phase 2, open label, adaptive platform randomised controlled trial
- Authors:
- Files, D. Clark
Aggarwal, Neil
Albertson, Timothy
Auld, Sara
Beitler, Jeremy R.
Berger, Paul
Burnham, Ellen L.
Calfee, Carolyn S.
Cobb, Nathan
Crippa, Alessio
Discacciati, Andrea
Eklund, Martin
Esserman, Laura
Friedman, Eliot
Gandotra, Sheetal
Khan, Kashif
Koff, Jonathan
Kumar, Santhi
Liu, Kathleen D.
Martin, Thomas R.
Matthay, Michael A.
Meyer, Nuala J.
Obermiller, Timothy
Robinson, Philip
Russell, Derek
Thomas, Karl
Wong, Se Fum
Wunderink, Richard G.
Wurfel, Mark M.
Yen, Albert
Youssef, Fady A.
Darmanian, Anita
Dzierba, Amy L.
Garcia, Ivan
Gosek, Katarzyna
Madahar, Purnema
Mittel, Aaron M.
Muir, Justin
Rosen, Amanda
Schicchi, John
Serra, Alexis L.
Wahab, Romina
Gibbs, Kevin W.
Landreth, Leigha
LaRose, Mary
Parks, Lisa
Wynn, Adina
Ittner, Caroline A.G.
Mangalmurti, Nilman S.
Reilly, John P.
Harris, Donna
Methukupally, Abhishek
Patel, Siddharth
Boerger, Lindsie
Kazianis, John
Higgins, Carrie
McKeehan, Jeff
Daniel, Brian
Fields, Scott
Hurst-Hopf, James
Jauregui, Alejandra
Brown Swigart, Lamorna
Blevins, Daniel
Nguyen, Catherine
Suarez, Alexis
Tanios, Maged A.
Sarafian, Farjad
Shah, Usman
Adelman, Max
Creel-Bulos, Christina
Detelich, Joshua
Harris, Gavin
Nugent, Katherine
Spainhour, Christina
Yang, Philip
Haczku, Angela
Hardy, Erin
Harper, Richart
Morrissey, Brian
Sandrock, Christian
Budinger, G. R. Scott
Donnelly, Helen K.
Singer, Benjamin D.
Moskowitz, Ari
Coleman, Melissa
Levitt, Joseph
Lu, Ruixiao
Henderson, Paul
Asare, Adam
Dunn, Imogene
Botello Barragan, Alejandro
… (more) - Abstract:
- Summary: Background: An urgent need exists to rapidly screen potential therapeutics for severe COVID-19 or other emerging pathogens associated with high morbidity and mortality. Methods: Using an adaptive platform design created to rapidly evaluate investigational agents, hospitalised patients with severe COVID-19 requiring ≥6 L/min oxygen were randomised to either a backbone regimen of dexamethasone and remdesivir alone (controls) or backbone plus one open-label investigational agent. Patients were enrolled to the arms described between July 30, 2020 and June 11, 2021 in 20 medical centres in the United States. The platform contained up to four potentially available investigational agents and controls available for randomisation during a single time-period. The two primary endpoints were time-to-recovery (<6 L/min oxygen for two consecutive days) and mortality. Data were evaluated biweekly in comparison to pre-specified criteria for graduation (i.e., likely efficacy), futility, and safety, with an adaptive sample size of 40–125 individuals per agent and a Bayesian analytical approach. Criteria were designed to achieve rapid screening of agents and to identify large benefit signals. Concurrently enrolled controls were used for all analyses. https://clinicaltrials.gov/ct2/show/NCT04488081 . Findings: The first 7 agents evaluated were cenicriviroc (CCR2/5 antagonist; n = 92), icatibant (bradykinin antagonist; n = 96), apremilast (PDE4 inhibitor; n = 67), celecoxib/famotidineSummary: Background: An urgent need exists to rapidly screen potential therapeutics for severe COVID-19 or other emerging pathogens associated with high morbidity and mortality. Methods: Using an adaptive platform design created to rapidly evaluate investigational agents, hospitalised patients with severe COVID-19 requiring ≥6 L/min oxygen were randomised to either a backbone regimen of dexamethasone and remdesivir alone (controls) or backbone plus one open-label investigational agent. Patients were enrolled to the arms described between July 30, 2020 and June 11, 2021 in 20 medical centres in the United States. The platform contained up to four potentially available investigational agents and controls available for randomisation during a single time-period. The two primary endpoints were time-to-recovery (<6 L/min oxygen for two consecutive days) and mortality. Data were evaluated biweekly in comparison to pre-specified criteria for graduation (i.e., likely efficacy), futility, and safety, with an adaptive sample size of 40–125 individuals per agent and a Bayesian analytical approach. Criteria were designed to achieve rapid screening of agents and to identify large benefit signals. Concurrently enrolled controls were used for all analyses. https://clinicaltrials.gov/ct2/show/NCT04488081 . Findings: The first 7 agents evaluated were cenicriviroc (CCR2/5 antagonist; n = 92), icatibant (bradykinin antagonist; n = 96), apremilast (PDE4 inhibitor; n = 67), celecoxib/famotidine (COX2/histamine blockade; n = 30), IC14 (anti-CD14; n = 67), dornase alfa (inhaled DNase; n = 39) and razuprotafib (Tie2 agonist; n = 22). Razuprotafib was dropped from the trial due to feasibility issues. In the modified intention-to-treat analyses, no agent met pre-specified efficacy/graduation endpoints with posterior probabilities for the hazard ratios [HRs] for recovery ≤1.5 between 0.99 and 1.00. The data monitoring committee stopped Celecoxib/Famotidine for potential harm (median posterior HR for recovery 0.5, 95% credible interval [CrI] 0.28–0.90; median posterior HR for death 1.67, 95% CrI 0.79–3.58). Interpretation: None of the first 7 agents to enter the trial met the prespecified criteria for a large efficacy signal. Celecoxib/Famotidine was stopped early for potential harm. Adaptive platform trials may provide a useful approach to rapidly screen multiple agents during a pandemic. Funding: Quantum Leap Healthcare Collaborative is the trial sponsor. Funding for this trial has come from: the COVID R&D Consortium, Allergan, Amgen Inc., Takeda Pharmaceutical Company, Implicit Bioscience, Johnson & Johnson, Pfizer Inc., Roche /Genentech, Apotex Inc., FAST Grant from Emergent Venture George Mason University, The DoD Defense Threat Reduction Agency (DTRA), The Department of Health and Human Services Biomedical Advanced Research and Development Authority (BARDA), and The Grove Foundation . Effort sponsored by the U.S. Government under Other Transaction number W15QKN-16-9-1002 between the MCDC, and the Government. … (more)
- Is Part Of:
- EClinicalMedicine. Volume 58(2023)
- Journal:
- EClinicalMedicine
- Issue:
- Volume 58(2023)
- Issue Display:
- Volume 58, Issue 2023 (2023)
- Year:
- 2023
- Volume:
- 58
- Issue:
- 2023
- Issue Sort Value:
- 2023-0058-2023-0000
- Page Start:
- Page End:
- Publication Date:
- 2023-04
- Subjects:
- SARS-CoV-2 -- Respiratory insufficiency -- Clinical trial -- Acute lung injury
Medicine -- Research -- Periodicals
Medical policy -- Periodicals
Clinical Medicine
Health Policy
Public Health
Medical policy
Medicine -- Research
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613 - Journal URLs:
- https://www.sciencedirect.com/science/journal/25895370 ↗
http://www.sciencedirect.com/ ↗ - DOI:
- 10.1016/j.eclinm.2023.101889 ↗
- Languages:
- English
- ISSNs:
- 2589-5370
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- Legaldeposit
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