Optimal dose and safety of intravenous favipiravir in hospitalized patients with COVID-19: a dose-escalating, randomized controlled Phase Ib study
Optimal dose and safety of intravenous favipiravir in hospitalized patients with COVID-19: a dose-escalating, randomized controlled Phase Ib study
AGILE (NCT04746183) is a Phase Ib/IIa platform, evaluating candidates to treat COVID-19. Candidate Specific Trial 6 evaluated the safety and optimal dose of a novel intravenous formulation of favipiravir in a dose-escalating, open-label, randomized, controlled, Bayesian adaptive Phase Ib trial. Hospitalized adults with PCR-confirmed SARS-CoV-2 infection, within 14 days of symptomatic COVID-19 were randomized 2:1 in groups of 6 (n = 4 favipiravir, n = 2 standard of care) to ascending doses of intravenous favipiravir twice daily (b.i.d.) for 7 days or standard of care. Clinical data, safety evaluations, virology and pharmacokinetic samples were collected. The primary outcome was safety. Secondary outcomes included clinical, pharmacokinetic and virological endpoints. Twenty-four participants enrolled between September 10, 2022 and November 1, 2023 [10/24 female; median age 74 years (range 52-93)]. Favipiravir was well tolerated despite a high background rate of unrelated adverse events. No dose limiting toxicities were observed, with a model-predicted dose limiting toxicity risk of 16.8% and probability of unacceptable toxicity of 2.7% at the highest dose level. No serious adverse events were deemed related to favipiravir but an expected association with asymptomatic, transient hyperuricemia was observed. Favipiravir exposures increased disproportionally to dose with significant accumulation in plasma, but with marked variability between participants within each cohort. This novel formulation of favipiravir was safe at sustained high doses that reached pre-specified pharmacokinetic targets in a study group with frailty and complex health profiles. We consider doses up to 2,400 mg b.i.d. to be safe for further evaluation.
1650-1661
Rowland, Tim
3210f781-83d0-41fe-81c3-2106d9088ee9
Fitzgerald, Richard
ee3308c2-16b8-4295-9130-1f52e5f20f59
Dickinson, Laura
2de19256-6a07-4497-81d7-aba38e9420ef
Saunders, Geoff
003d2b6f-fbfd-4247-911c-8b57a83f1fd7
Griffiths, Gareth
7fd300c0-d279-4ff6-842d-aa1f2b9b864d
the AGILE CST-6 Study Group
8 May 2026
Rowland, Tim
3210f781-83d0-41fe-81c3-2106d9088ee9
Fitzgerald, Richard
ee3308c2-16b8-4295-9130-1f52e5f20f59
Dickinson, Laura
2de19256-6a07-4497-81d7-aba38e9420ef
Saunders, Geoff
003d2b6f-fbfd-4247-911c-8b57a83f1fd7
Griffiths, Gareth
7fd300c0-d279-4ff6-842d-aa1f2b9b864d
Rowland, Tim, Fitzgerald, Richard and Challenger, Elizabeth
,
the AGILE CST-6 Study Group
(2026)
Optimal dose and safety of intravenous favipiravir in hospitalized patients with COVID-19: a dose-escalating, randomized controlled Phase Ib study.
Clinical Pharmacology and Therapeutics, 119 (6), .
(doi:10.1002/cpt.70261).
Abstract
AGILE (NCT04746183) is a Phase Ib/IIa platform, evaluating candidates to treat COVID-19. Candidate Specific Trial 6 evaluated the safety and optimal dose of a novel intravenous formulation of favipiravir in a dose-escalating, open-label, randomized, controlled, Bayesian adaptive Phase Ib trial. Hospitalized adults with PCR-confirmed SARS-CoV-2 infection, within 14 days of symptomatic COVID-19 were randomized 2:1 in groups of 6 (n = 4 favipiravir, n = 2 standard of care) to ascending doses of intravenous favipiravir twice daily (b.i.d.) for 7 days or standard of care. Clinical data, safety evaluations, virology and pharmacokinetic samples were collected. The primary outcome was safety. Secondary outcomes included clinical, pharmacokinetic and virological endpoints. Twenty-four participants enrolled between September 10, 2022 and November 1, 2023 [10/24 female; median age 74 years (range 52-93)]. Favipiravir was well tolerated despite a high background rate of unrelated adverse events. No dose limiting toxicities were observed, with a model-predicted dose limiting toxicity risk of 16.8% and probability of unacceptable toxicity of 2.7% at the highest dose level. No serious adverse events were deemed related to favipiravir but an expected association with asymptomatic, transient hyperuricemia was observed. Favipiravir exposures increased disproportionally to dose with significant accumulation in plasma, but with marked variability between participants within each cohort. This novel formulation of favipiravir was safe at sustained high doses that reached pre-specified pharmacokinetic targets in a study group with frailty and complex health profiles. We consider doses up to 2,400 mg b.i.d. to be safe for further evaluation.
Text
Clin Pharma and Therapeutics - 2026 - Rowland - Optimal Dose and Safety of Intravenous Favipiravir in Hospitalized Patients
- Version of Record
More information
Accepted/In Press date: 23 February 2026
e-pub ahead of print date: 18 March 2026
Published date: 8 May 2026
Identifiers
Local EPrints ID: 511862
URI: http://eprints.soton.ac.uk/id/eprint/511862
ISSN: 0009-9236
PURE UUID: bbb26838-cd5d-4d9f-a3ca-6675dffa927f
Catalogue record
Date deposited: 08 Jun 2026 16:44
Last modified: 09 Jun 2026 01:46
Export record
Altmetrics
Contributors
Author:
Tim Rowland
Author:
Richard Fitzgerald
Author:
Elizabeth Challenger
Author:
Laura Dickinson
Author:
Geoff Saunders
Corporate Author: the AGILE CST-6 Study Group
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics
