| Literature DB >> 32645335 |
David W Hawman1, Elaine Haddock2, Kimberly Meade-White2, Glenn Nardone3, Friederike Feldmann2, Patrick W Hanley2, Jamie Lovaglio2, Dana Scott2, Takashi Komeno4, Nozomi Nakajima4, Yousuke Furuta4, Brian B Gowen5, Heinz Feldmann6.
Abstract
Crimean-Congo hemorrhagic fever virus (CCHFV) is a widely distributed hemorrhagic fever virus found throughout Eastern Europe, Africa, the Middle East and Asia. It is spread through bites from infected ticks, animal husbandry and can also be acquired in the healthcare setting during care of infected patients. In humans, CCHFV can cause a sudden onset of a non-specific febrile illness that can rapidly progress to severe hemorrhagic manifestations. Currently, there is no widely available vaccine and although ribavirin has been suggested for the treatment of CCHFV, clinical efficacy in both animal models and humans is inconsistent suggesting more potent antivirals are needed for CCHFV. Favipiravir is approved in Japan for the treatment of influenza virus infections and has shown promise against other highly pathogenic RNA viruses including CCHFV with demonstrated efficacy in the type I interferon deficient mouse model. In this report we utilized the cynomolgus macaque model to evaluate the efficacy of once- and twice-daily favipiravir treatment against CCHFV infection. We found that favipiravir treatment suppressed viremia and viral shedding when treatment was initiated 24 h post-infection and viral burdens in key tissues trended lower in favipiravir-treated animals. Our data indicate that favipiravir has efficacy against CCHFV in vivo in a non-human primate model of infection. Published by Elsevier B.V.Entities:
Keywords: Antiviral; Crimean-Congo hemorrhagic Fever; Favipiravir; Macaques
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Year: 2020 PMID: 32645335 DOI: 10.1016/j.antiviral.2020.104858
Source DB: PubMed Journal: Antiviral Res ISSN: 0166-3542 Impact factor: 5.970