Author: Niemeyer, Brian F.; Miller, Caitlin M.; Ledesmaâ€Feliciano, Carmen; Morrison, James H.; Jimenezâ€Valdes, Rocio; Clifton, Clarissa; Poeschla, Eric M.; Benam, Kambez H.
Title: Broad antiviral and antiâ€inflammatory efficacy of nafamostat against SARSâ€CoVâ€2 and seasonal coronaviruses in primary human bronchiolar epithelia Cord-id: 9vq5sm0c Document date: 2021_6_30
ID: 9vq5sm0c
Snippet: Antiviral strategies that target host systems needed for SARSâ€CoVâ€2 replication and pathogenesis may have therapeutic potential and help mitigate resistance development. Here, we evaluate nafamostat mesylate, a potent broadâ€spectrum serine protease inhibitor that blocks host protease activation of the viral spike protein. SARSâ€CoVâ€2 is used to infect human polarized mucociliated primary bronchiolar epithelia reconstituted with cells derived from healthy donors, smokers and subjects wit
Document: Antiviral strategies that target host systems needed for SARSâ€CoVâ€2 replication and pathogenesis may have therapeutic potential and help mitigate resistance development. Here, we evaluate nafamostat mesylate, a potent broadâ€spectrum serine protease inhibitor that blocks host protease activation of the viral spike protein. SARSâ€CoVâ€2 is used to infect human polarized mucociliated primary bronchiolar epithelia reconstituted with cells derived from healthy donors, smokers and subjects with chronic obstructive pulmonary disease. Nafamostat markedly inhibits apical shedding of SARSâ€CoVâ€2 from all donors (log(10) reduction). We also observe, for the firstâ€time, antiâ€inflammatory effects of nafamostat on airway epithelia independent of its antiviral effects, suggesting a dual therapeutic advantage in the treatment of COVIDâ€19. Nafamostat also exhibits antiviral properties against the seasonal human coronaviruses 229E and NL6. These findings suggest therapeutic promise for nafamostat in treating SARSâ€CoVâ€2 and other human coronaviruses.
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