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      H7N9 Live Attenuated Influenza Vaccine Is Highly Immunogenic, Prevents Virus Replication, and Protects Against Severe Bronchopneumonia in Ferrets

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          Abstract

          Avian influenza viruses continue to cross the species barrier, and if such viruses become transmissible among humans, it would pose a great threat to public health. Since its emergence in China in 2013, H7N9 has caused considerable morbidity and mortality. In the absence of a universal influenza vaccine, preparedness includes development of subtype-specific vaccines. In this study, we developed and evaluated in ferrets an intranasal live attenuated influenza vaccine (LAIV) against H7N9 based on the A/Leningrad/134/17/57 (H2N2) cold-adapted master donor virus. We demonstrate that the LAIV is attenuated and safe in ferrets and induces high hemagglutination- and neuraminidase-inhibiting and virus-neutralizing titers. The antibodies against hemagglutinin were also cross-reactive with divergent H7 strains. To assess efficacy, we used an intratracheal challenge ferret model in which an acute severe viral pneumonia is induced that closely resembles viral pneumonia observed in severe human cases. A single- and two-dose strategy provided complete protection against severe pneumonia and prevented virus replication. The protective effect of the two-dose strategy appeared better than the single dose only on the microscopic level in the lungs. We observed, however, an increased lymphocytic infiltration after challenge in single-vaccinated animals and hypothesize that this a side effect of the model.

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          Author and article information

          Journal
          Mol Ther
          Mol. Ther
          Molecular Therapy
          Nature Publishing Group
          1525-0016
          1525-0024
          May 2016
          22 January 2016
          01 March 2016
          : 24
          : 5
          : 991-1002
          Affiliations
          [1 ] Centre for Infectious Disease Control, National Institute of Public Health and the Environment (RIVM) , Bilthoven, the Netherlands
          [2 ] Department of Virology, Institute of Experimental Medicine , Saint Petersburg, Russia
          [3 ] Department of Virology, Central Veterinary Institute of Wageningen UR , Lelystad, the Netherlands
          [4 ] Microscope Consultancy , Weesp, the Netherlands
          [5 ]Current address: BioNovion , Oss, the Netherlands
          [6 ]Current address: Genmab , Utrecht, the Netherlands
          Author notes
          [* ]Centre for Infectious Disease Control, National Institute of Public Health and the Environment (RIVM), 3720 BA, Bilthoven, the Netherlands. E-mail: jorgen.de.jonge@ 123456rivm.nl
          Article
          PMC4881767 PMC4881767 4881767 mt201623
          10.1038/mt.2016.23
          4881767
          26796670
          f214e708-290d-4f1b-9103-be3840a4451c
          Copyright © 2016 American Society of Gene & Cell Therapy
          History
          : 02 October 2015
          : 22 December 2015
          Categories
          Original Article

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