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Research Article

A nonstructural viral protein expressed by a recombinant vaccinia virus protects against lethal cytomegalovirus infection.

S Jonjić, M del Val, G M Keil, M J Reddehase, U H Koszinowski
S Jonjić
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M del Val
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G M Keil
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M J Reddehase
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U H Koszinowski
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ABSTRACT

The nonstructural immediate-early protein pp89 of murine cytomegalovirus (MCMV) is the first viral protein synthesized after infection and has a regulatory function in viral gene expression. Despite its localization in the nucleus of infected cells, pp89 is also the dominant antigen recognized by MCMV-specific cytolytic T lymphocytes. The recombinant vaccinia virus MCMV-ieI-VAC, which expresses pp89, was used to study the capacity of this protein to induce protective immunity in BALB/c mice. Vaccination with MCMV-ieI-VAC induced a long-lasting immunity that protected mice against challenge with a lethal dose of MCMV but did not prevent infection and morbidity. In vivo depletion of CD8+ T lymphocytes before challenge completely abrogated the protective immunity. CD8+ T lymphocytes derived from MCMV-ieI-VAC-primed donors and adoptively transferred into sublethally irradiated and MCMV-infected recipients were found to limit viral replication in host tissues, whereas CD4+ T lymphocytes and pp89-specific antiserum had no protective effect. The data demonstrate for the first time that a single nonstructural viral protein can confer protection against a lethal cytolytic infection and that this immunity is entirely mediated by the CD8+ subpopulation of T lymphocytes.

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A nonstructural viral protein expressed by a recombinant vaccinia virus protects against lethal cytomegalovirus infection.
S Jonjić, M del Val, G M Keil, M J Reddehase, U H Koszinowski
Journal of Virology May 1988, 62 (5) 1653-1658; DOI:

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A nonstructural viral protein expressed by a recombinant vaccinia virus protects against lethal cytomegalovirus infection.
S Jonjić, M del Val, G M Keil, M J Reddehase, U H Koszinowski
Journal of Virology May 1988, 62 (5) 1653-1658; DOI:
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