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Efficient influenza B virus propagation due to deficient interferon-induced antiviral activity in MDCK cells
Authors:Frensing Timo  Seitz Claudius  Heynisch Bjoern  Patzina Corinna  Kochs Georg  Reichl Udo
Affiliation:a Bioprocess Engineering, Max Planck Institute for Dynamics of Complex Technical Systems Magdeburg, Sandtorstr. 1, D-39106 Magdeburg, Germany
b Chair of Bioprocess Engineering, Institute for Process Engineering, Otto von Guericke University Magdeburg, Universitätsplatz 2, D-39106 Magdeburg, Germany
c Department of Virology, University of Freiburg, Hermann-Herder-Str. 11, D-79104 Freiburg, Germany
Abstract:Influenza B virus infections are mainly restricted to humans, which is partially caused by the inability of influenza B virus NS1 protein to counteract the innate immune response of other species. However, for cell culture-based influenza vaccine production non-human cells, such as Madin-Darby canine kidney (MDCK) cells, are commonly used. Therefore, the impact of cellular pathogen defence mechanisms on influenza B virus propagation in MDCK cells was analysed in this study. Activation of the cellular antiviral defence by interferon stimulation slowed down influenza B virus replication at early time points but after 48 h the same virus titres were reached in stimulated and control cells. Furthermore, suppression of the antiviral host defence by transient expression of a viral antagonist, the rabies virus phosphoprotein, could not increase influenza B virus replication. Finally, canine Myxovirus resistance (Mx) proteins showed no antiviral activity in an influenza B virus-specific minireplicon assay in contrast to the murine Mx1 protein. Taken together, these results indicate that an insufficient antiviral defence in MDCK cells promotes efficient influenza B virus replication favouring the use of MDCK cells in influenza vaccine production.
Keywords:Influenza B virus   Cell culture-based vaccine production   Myxovirus resistance proteins   Interferon signalling   MDCK cells
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