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dc.contributor.authorIanevski, Aleksandr
dc.contributor.authorYao, Rouan
dc.contributor.authorLysvand, Hilde
dc.contributor.authorGrødeland, Gunnveig
dc.contributor.authorLegrand, Nicolas
dc.contributor.authorOksenych, Valentyn
dc.contributor.authorZusinaite, Eva
dc.contributor.authorTenson, Tanel
dc.contributor.authorBjørås, Magnar
dc.contributor.authorKainov, Denis E.
dc.date.accessioned2022-03-04T09:09:43Z
dc.date.available2022-03-04T09:09:43Z
dc.date.created2021-09-20T14:53:16Z
dc.date.issued2021
dc.identifier.citationViruses. 2021, 13:1768 (9), 1-8.en_US
dc.identifier.issn1999-4915
dc.identifier.urihttps://hdl.handle.net/11250/2983016
dc.description.abstractSARS-CoV-2 and its vaccine/immune-escaping variants continue to pose a serious threat to public health due to a paucity of effective, rapidly deployable, and widely available treatments. Here, we address these challenges by combining Pegasys (IFNα) and nafamostat to effectively suppress SARS-CoV-2 infection in cell culture and hamsters. Our results indicate that Serpin E1 is an important mediator of the antiviral activity of IFNα and that both Serpin E1 and nafamostat can target the same cellular factor TMPRSS2, which plays a critical role in viral replication. The low doses of the drugs in combination may have several clinical advantages, including fewer adverse events and improved patient outcome. Thus, our study may provide a proactive solution for the ongoing pandemic and potential future coronavirus outbreaks, which is still urgently required in many parts of the world.en_US
dc.language.isoengen_US
dc.publisherMDPIen_US
dc.rightsNavngivelse 4.0 Internasjonal*
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/deed.no*
dc.titleNafamostat–interferon-α combination suppresses sars-cov-2 infection in vitro and in vivo by cooperatively targeting host TMPRSS2en_US
dc.typePeer revieweden_US
dc.typeJournal articleen_US
dc.description.versionpublishedVersionen_US
dc.source.pagenumber1-8en_US
dc.source.volume13:1768en_US
dc.source.journalVirusesen_US
dc.source.issue9en_US
dc.identifier.doi10.3390/v13091768
dc.identifier.cristin1936163
cristin.ispublishedtrue
cristin.fulltextoriginal
cristin.qualitycode1


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