Favipiravir versus Arbidol for COVID-19: A Randomized Clinical Trial

Chen, Chang; Zhang, Yi; Huang, Jianying; Yin, Ping; Cheng, Zhenshun; Wu, Jiangquan; Chen, Song; Zhang, Yongxi; Chen, Bin; Lü, Mengxin; Luo, Yongwen; Ju, Lingao; Zhang, Jingyi; Wang, Xinghuan

doi:10.1101/2020.03.17.20037432

Cited by 671 publications

(791 citation statements)

References 8 publications

(13 reference statements)

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“…A recent trial for favipirivir, demonstrated some success with an improvement over arbidol from 56% to 71% (p = 0.02) in patients without risk factors (but not critical cases or patients with hypertension and/or diabetes) [38]. The results of compassionate use of remdesivir in severely ill patients was also recently reported, and if confirmed in ongoing randomized, placebo-controlled trials will serve as a further validation of the other candidates presented here [39].…”

Section: Discussionmentioning

(Expert classified)

Prioritisation of potential anti-SARS-CoV-2 drug repurposing opportunities based on ability to achieve adequate plasma and target site concentrations derived from their established human pharmacokinetics

Arshad

Pertinez

Box

et al. 2020

Preprint

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There is a rapidly expanding literature on the in vitro antiviral activity of drugs that may be repurposed for therapy or chemoprophylaxis against SARS-CoV-2. However, this has not been accompanied by a comprehensive evaluation of the ability of these drugs to achieve target plasma and lung concentrations following approved dosing in humans. Moreover, most publications have focussed on 50% maximum effective concentrations (EC50), which may be an insufficiently robust indicator of antiviral activity because of marked differences in the slope of the concentration-response curve between drugs. Accordingly, in vitro anti-SARS-CoV-2 activity data was digitised from all available publications up to 13 th April 2020 and used to recalculate an EC90 value for each drug. EC90 values were then expressed as a ratio to the achievable maximum plasma concentrations (Cmax) reported for each drug after administration of the approved dose to humans (Cmax/EC90 ratio). Only 14 of the 56 analysed drugs achieved a Cmax/EC90 ratio above 1 meaning that plasma Cmax concentrations exceeded those necessary to inhibit 90% of SARS-CoV-2 replication. A more in-depth assessment of the putative agents tested demonstrated that only nitazoxanide, nelfinavir, tipranavir (boosted with ritonavir) and sulfadoxine achieved plasma concentrations above their reported anti-SARS-CoV-2 activity across their entire approved dosing interval at their approved human dose. For all drugs reported, the unbound lung to plasma tissue partition coefficient (KpUlung) was also simulated and used along with reported Cmax and fraction unbound in plasma to derive a lung Cmax/EC50 as a better indicator of potential human efficacy (lung Cmax/EC90 ratio was also calculable for a limited number of drugs). Using this parameter hydroxychloroquine, chloroquine, mefloquine, atazanavir (boosted with ritonavir), tipranavir (boosted with ritonavir), ivermectin, azithromycin and lopinavir (boosted with ritonavir) were all predicted to achieve lung concentrations over 10-fold higher than their reported EC50. This analysis was not possible for nelfinavir because insufficient data were available to calculate KpUlung but nitozoxanide and sulfadoxine were also predicted to exceed their reported EC50 by 3.1-and 1.5-fold in lung, respectively. The antiviral activity data reported to date have been acquired under different laboratory conditions across multiple groups, applying variable levels of stringency. However, this analysis may be used to select potential candidates for further clinical testing, while deprioritising compounds which are unlikely to attain target concentrations for antiviral activity. Future studies should focus on EC90 values and discuss findings in the context of achievable exposures in humans, especially within target compartments such as the lung, in order to maximise the potential for success of proposed human clinical trials.

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Section: Discussionmentioning

(Expert classified)

Prioritisation of potential anti-SARS-CoV-2 drug repurposing opportunities based on ability to achieve adequate plasma and target site concentrations derived from their established human pharmacokinetics

Arshad

Pertinez

Box

et al. 2020

Preprint

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“…The efficacy of chain-terminating nucleotide analogs requires viral RdRps to recognize and successfully incorporate the active form of the inhibitors into the growing RNA strand. Sofosbuvir (2'-F-2'-C-methyluridine monophosphate) is a prodrug which targets HCV ns5b and has been approved for the treatment of chronic HCV infection (16). It acts by binding to the catalytic site of HCV ns5b polymerase (12,16).…”

mentioning

confidence: 99%

“…Sofosbuvir (2'-F-2'-C-methyluridine monophosphate) is a prodrug which targets HCV ns5b and has been approved for the treatment of chronic HCV infection (16). It acts by binding to the catalytic site of HCV ns5b polymerase (12,16). Given that remdesivir and sofosbuvir are both nucleotide analogs and the structural conservation of the catalytic site between COVID-19 virus nsp12 and HCV ns5b polymerase (13, 16) ( fig.…”

mentioning

confidence: 99%

Structure of the RNA-dependent RNA polymerase from COVID-19 virus

Gao

Yan

Huang

et al. 2020

Science

1,373

1,691

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A novel coronavirus (COVID-19 virus) outbreak has caused a global pandemic resulting in tens of thousands of infections and thousands of deaths worldwide. The RNA-dependent RNA polymerase (RdRp, also named nsp12) is the central component of coronaviral replication/transcription machinery and appears to be a primary target for the antiviral drug, remdesivir. We report the cryo-EM structure of COVID-19 virus fulllength nsp12 in complex with cofactors nsp7 and nsp8 at 2.9-Å resolution. In addition to the conserved architecture of the polymerase core of the viral polymerase family, nsp12 possesses a newly identified βhairpin domain at its N terminus. A comparative analysis model shows how remdesivir binds to this polymerase. The structure provides a basis for the design of new antiviral therapeutics targeting viral RdRp.

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“…The results were published on March 20, 2020 which revealed that the 7 day's recovery rate for arbidol group was 55.86% in comparison to 71.43% for favipiravir group (p = 0.0199). Patients with hypertension or diabetes also showed better improvement in case of favipiravir group in comparison to arbidol (15). Currently, three more phase IV clinical trials are planned for arbidol in the treatment of COVID-19.…”

Section: Umifenovirmentioning

confidence: 96%

“…Favipiravir was first developed in Japan by Fujifilm and was subjected to another clinical trial on 340 patients in China recently and resulted in very encouraging results as the patients receiving favipiravir with standard care showed cleared viral load in four days as compared to eleven days in patients receiving standard care only (14). Another multicentre, open labeled, randomized trial in China was conducted to compare the efficacy of favipiravir (1,600 mg × 2 on the first day followed by 600 mg × 2 for 9 days) and umifenovir (200 mg × 3 per day for 10 days) and the results revealed a higher recovery rate and better clinical outcomes in the patients treated with favipiravir at day 7 (15). A phase III trial is ongoing in Japan involving 100 patients and is expected to be completed in June.…”

Section: Favipiravirmentioning

confidence: 99%

Treatment of SARS-CoV-2: How far have we reached?

Ahsan

Javed

Bratty

et al. 2020

DD&T

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The virus severe acute respiratory syndrome-coronavirus-2 (SARS-CoV-2) is currently affecting more than 200 countries and territories worldwide. It has been declared as pandemic by World Health Organization (WHO) and the whole world is suffering from corona virus disease 2019 . Currently, no treatment for SARS-CoV-2 are approved because of lack of evidence, but a number of clinical trials are in process and we are expecting fruitful results very soon. This review focuses on various approaches of treatment and few of the most recent clinical trials carried out in this field.

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Favipiravir versus Arbidol for COVID-19: A Randomized Clinical Trial

Cited by 671 publications

References 8 publications

Prioritisation of potential anti-SARS-CoV-2 drug repurposing opportunities based on ability to achieve adequate plasma and target site concentrations derived from their established human pharmacokinetics

Prioritisation of potential anti-SARS-CoV-2 drug repurposing opportunities based on ability to achieve adequate plasma and target site concentrations derived from their established human pharmacokinetics

Structure of the RNA-dependent RNA polymerase from COVID-19 virus

Treatment of SARS-CoV-2: How far have we reached?

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