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      Overexpression of the rabies virus glycoprotein results in enhancement of apoptosis and antiviral immune response.

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          Abstract

          A recombinant rabies virus (RV) carrying two identical glycoprotein (G) genes (SPBNGA-GA) was constructed and used to determine the effect of RV G overexpression on cell viability and immunity. Immunoprecipitation analysis and flow cytometry showed that tissue culture cells infected with SPBNGA-GA produced, on average, twice as much RV G as cells infected with RV carrying only a single RV G gene (SPBNGA). The overexpression of RV G in SPBNGA-GA-infected NA cells was paralleled by a significant increase in caspase 3 activity followed by a marked decrease in mitochondrial respiration, neither of which was observed in SPBNGA-infected cells. Furthermore, fluorescence staining and confocal microscopy revealed an increased extent of apoptosis and markedly reduced neurofilament and F actin in SPBNGA-GA-infected primary neuron cultures compared with neuronal cells infected with SPBNGA, supporting the concept that RV G or motifs of the RV G gene trigger the apoptosis cascade. Mice immunized with SPBNGA-GA showed substantially higher antibody titers against the RV G and against the nucleoprotein than SPBNGA-immunized mice, suggesting that the speed or extent of apoptosis directly determines the magnitude of the antibody response.

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          Author and article information

          Journal
          J Virol
          Journal of virology
          American Society for Microbiology
          0022-538X
          0022-538X
          Apr 2002
          : 76
          : 7
          Affiliations
          [1 ] Department of Microbiology and Immunology, Center for Human Virology, Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA.
          Article
          10.1128/jvi.76.7.3374-3381.2002
          136034
          11884563
          e555eb1c-8558-4a51-bca8-5f27deca5247
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