Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza

BACKGROUND: The pharmacokinetics and appropriate dose regimens of favipiravir are unknown in hospitalized influenza patients; such data are also needed to determine dosage selection for favipiravir trials in COVID-19. METHODS: In this dose-escalating study, favipiravir pharmacokinetics and tolerabil...

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Autores principales: Wang, Yeming, Zhong, Wu, Salam, Alex, Tarning, Joel, Zhan, Qingyuan, Huang, Jian-an, Weng, Heng, Bai, Changqing, Ren, Yanhong, Yamada, Koichi, Wang, Dayan, Guo, Qiang, Fang, Qiongqiong, Tsutomu, Sakurai, Zou, Xiaohui, Li, Haibo, Gillesen, Annelies, Castle, Lyndsey, Chen, Cheng, Li, Hongyan, Zhen, Jing, Lu, Binghuai, Duan, Jun, Guo, Liping, Jiang, Jinfang, Cao, Ruiyuan, Fan, Guohui, Li, Jintong, Hayden, Frederick G., Wang, Chen, Horby, Peter, Cao, Bin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7689521/
https://www.ncbi.nlm.nih.gov/pubmed/33232871
http://dx.doi.org/10.1016/j.ebiom.2020.103125
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author Wang, Yeming
Zhong, Wu
Salam, Alex
Tarning, Joel
Zhan, Qingyuan
Huang, Jian-an
Weng, Heng
Bai, Changqing
Ren, Yanhong
Yamada, Koichi
Wang, Dayan
Guo, Qiang
Fang, Qiongqiong
Tsutomu, Sakurai
Zou, Xiaohui
Li, Haibo
Gillesen, Annelies
Castle, Lyndsey
Chen, Cheng
Li, Hongyan
Zhen, Jing
Lu, Binghuai
Duan, Jun
Guo, Liping
Jiang, Jinfang
Cao, Ruiyuan
Fan, Guohui
Li, Jintong
Hayden, Frederick G.
Wang, Chen
Horby, Peter
Cao, Bin
author_facet Wang, Yeming
Zhong, Wu
Salam, Alex
Tarning, Joel
Zhan, Qingyuan
Huang, Jian-an
Weng, Heng
Bai, Changqing
Ren, Yanhong
Yamada, Koichi
Wang, Dayan
Guo, Qiang
Fang, Qiongqiong
Tsutomu, Sakurai
Zou, Xiaohui
Li, Haibo
Gillesen, Annelies
Castle, Lyndsey
Chen, Cheng
Li, Hongyan
Zhen, Jing
Lu, Binghuai
Duan, Jun
Guo, Liping
Jiang, Jinfang
Cao, Ruiyuan
Fan, Guohui
Li, Jintong
Hayden, Frederick G.
Wang, Chen
Horby, Peter
Cao, Bin
author_sort Wang, Yeming
collection PubMed
description BACKGROUND: The pharmacokinetics and appropriate dose regimens of favipiravir are unknown in hospitalized influenza patients; such data are also needed to determine dosage selection for favipiravir trials in COVID-19. METHODS: In this dose-escalating study, favipiravir pharmacokinetics and tolerability were assessed in critically ill influenza patients. Participants received one of two dosing regimens; Japan licensed dose (1600 mg BID on day 1 and 600 mg BID on the following days) and the higher dose (1800 mg/800 mg BID) trialed in uncomplicated influenza. The primary pharmacokinetic endpoint was the proportion of patients with a minimum observed plasma trough concentration (C(trough)) ≥20 mg/L at all measured time points after the second dose. RESULTS: Sixteen patients were enrolled into the low dose group and 19 patients into the high dose group of the study. Favipiravir C(trough) decreased significantly over time in both groups (p <0.01). Relative to day 2 (48 hrs), concentrations were 91.7% and 90.3% lower in the 1600/600 mg group and 79.3% and 89.5% lower in the 1800/800 mg group at day 7 and 10, respectively. In contrast, oseltamivir concentrations did not change significantly over time. A 2-compartment disposition model with first-order absorption and elimination described the observed favipiravir concentration-time data well. Modeling demonstrated that less than 50% of patients achieved C(trough) ≥20 mg/L for >80% of the duration of treatment of the two dose regimens evaluated (18.8% and 42.1% of patients for low and high dose regimen, respectively). Increasing the favipravir dosage predicted a higher proportion of patients reaching this threshold of 20 mg/L, suggesting that dosing regimens of ≥3600/2600 mg might be required for adequate concentrations. The two dosing regimens were well-tolerated in critical ill patients with influenza. CONCLUSION: The two dosing regimens proposed for uncomplicated influenza did not achieve our pre-defined treatment threshold.
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spelling pubmed-76895212020-12-07 Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza Wang, Yeming Zhong, Wu Salam, Alex Tarning, Joel Zhan, Qingyuan Huang, Jian-an Weng, Heng Bai, Changqing Ren, Yanhong Yamada, Koichi Wang, Dayan Guo, Qiang Fang, Qiongqiong Tsutomu, Sakurai Zou, Xiaohui Li, Haibo Gillesen, Annelies Castle, Lyndsey Chen, Cheng Li, Hongyan Zhen, Jing Lu, Binghuai Duan, Jun Guo, Liping Jiang, Jinfang Cao, Ruiyuan Fan, Guohui Li, Jintong Hayden, Frederick G. Wang, Chen Horby, Peter Cao, Bin EBioMedicine Research Paper BACKGROUND: The pharmacokinetics and appropriate dose regimens of favipiravir are unknown in hospitalized influenza patients; such data are also needed to determine dosage selection for favipiravir trials in COVID-19. METHODS: In this dose-escalating study, favipiravir pharmacokinetics and tolerability were assessed in critically ill influenza patients. Participants received one of two dosing regimens; Japan licensed dose (1600 mg BID on day 1 and 600 mg BID on the following days) and the higher dose (1800 mg/800 mg BID) trialed in uncomplicated influenza. The primary pharmacokinetic endpoint was the proportion of patients with a minimum observed plasma trough concentration (C(trough)) ≥20 mg/L at all measured time points after the second dose. RESULTS: Sixteen patients were enrolled into the low dose group and 19 patients into the high dose group of the study. Favipiravir C(trough) decreased significantly over time in both groups (p <0.01). Relative to day 2 (48 hrs), concentrations were 91.7% and 90.3% lower in the 1600/600 mg group and 79.3% and 89.5% lower in the 1800/800 mg group at day 7 and 10, respectively. In contrast, oseltamivir concentrations did not change significantly over time. A 2-compartment disposition model with first-order absorption and elimination described the observed favipiravir concentration-time data well. Modeling demonstrated that less than 50% of patients achieved C(trough) ≥20 mg/L for >80% of the duration of treatment of the two dose regimens evaluated (18.8% and 42.1% of patients for low and high dose regimen, respectively). Increasing the favipravir dosage predicted a higher proportion of patients reaching this threshold of 20 mg/L, suggesting that dosing regimens of ≥3600/2600 mg might be required for adequate concentrations. The two dosing regimens were well-tolerated in critical ill patients with influenza. CONCLUSION: The two dosing regimens proposed for uncomplicated influenza did not achieve our pre-defined treatment threshold. Elsevier 2020-11-22 /pmc/articles/PMC7689521/ /pubmed/33232871 http://dx.doi.org/10.1016/j.ebiom.2020.103125 Text en © 2020 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Wang, Yeming
Zhong, Wu
Salam, Alex
Tarning, Joel
Zhan, Qingyuan
Huang, Jian-an
Weng, Heng
Bai, Changqing
Ren, Yanhong
Yamada, Koichi
Wang, Dayan
Guo, Qiang
Fang, Qiongqiong
Tsutomu, Sakurai
Zou, Xiaohui
Li, Haibo
Gillesen, Annelies
Castle, Lyndsey
Chen, Cheng
Li, Hongyan
Zhen, Jing
Lu, Binghuai
Duan, Jun
Guo, Liping
Jiang, Jinfang
Cao, Ruiyuan
Fan, Guohui
Li, Jintong
Hayden, Frederick G.
Wang, Chen
Horby, Peter
Cao, Bin
Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza
title Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza
title_full Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza
title_fullStr Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza
title_full_unstemmed Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza
title_short Phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (T-705) in combination with oseltamivir in patients with severe influenza
title_sort phase 2a, open-label, dose-escalating, multi-center pharmacokinetic study of favipiravir (t-705) in combination with oseltamivir in patients with severe influenza
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7689521/
https://www.ncbi.nlm.nih.gov/pubmed/33232871
http://dx.doi.org/10.1016/j.ebiom.2020.103125
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