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- W4360853935 abstract "Abstract A novel Influenza A virus (subtype H7N9) emerged in spring 2013 and caused considerable mortality in zoonotically infected patients. To be prepared for potential pandemics, broadly effective and safe vaccines are crucial. Recombinant measles virus (MeV) encoding antigens of foreign pathogens constitutes a promising vector platform to generate novel vaccines. To characterize the efficacy of H7N9 antigens in a prototypic vaccine platform technology, we generated MeVs encoding either neuraminidase (N9) or hemagglutinin (H7). Moraten vaccine strain-derived vaccine candidates were rescued; they replicated with efficiency comparable to that of the measles vaccine, robustly expressed H7 and N9, and were genetically stable over 10 passages. Immunization of MeV-susceptible mice triggered the production of antibodies against H7 and N9, including hemagglutination-inhibiting and neutralizing antibodies induced by MV vac2 -H7(P) and neuraminidase-inhibiting antibodies by MV vac2 -N9(P). Vaccinated mice also developed long-lasting H7- and N9-specific T cells. Both MV vac2 -H7(P) and MV vac2 -N9(P)-vaccinated mice were protected from lethal H7N9 challenge." @default.
- W4360853935 created "2023-03-25" @default.
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- W4360853935 date "2023-03-24" @default.
- W4360853935 modified "2023-10-15" @default.
- W4360853935 title "A protective measles virus-derived vaccine inducing long-lasting immune responses against influenza A virus H7N9" @default.
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- W4360853935 doi "https://doi.org/10.1038/s41541-023-00643-9" @default.
- W4360853935 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36964176" @default.
- W4360853935 hasPublicationYear "2023" @default.
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