PLoS ONE (Oct 2008)

Robust intrapulmonary CD8 T cell responses and protection with an attenuated N1L deleted vaccinia virus.

  • Anuja Mathew,
  • Joel O'Bryan,
  • William Marshall,
  • Girish J Kotwal,
  • Masanori Terajima,
  • Sharone Green,
  • Alan L Rothman,
  • Francis A Ennis

DOI
https://doi.org/10.1371/journal.pone.0003323
Journal volume & issue
Vol. 3, no. 10
p. e3323

Abstract

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Vaccinia viruses have been used as a model for viral disease and as a protective live vaccine.We investigated the immunogenicity of an attenuated strain of vaccinia virus engineered to inactivate the N1L gene (vGK5). Using the intranasal route, this recombinant virus was 2 logs less virulent compared to the wildtype VACV-WR. Infection by the intranasal, intraperitoneal, and tail scarification routes resulted in the robust induction of cytolytic virus-specific CD8 T cells in the spleens and the lungs. VACV-specific antibodies were also detected in the sera of mice infected 3-5 months prior with the attenuated vGK5 virus. Finally, mice immunized with vGK5 were significantly protected when challenged with a lethal dose of VACV-WR.These results indicate that the attenuated vGK5 virus protects against subsequent infection and suggest that the N1L protein limits the strength of the early antiviral CD8 T cell response following respiratory infection.