A Spread-Deficient Cytomegalovirus for Assessment of First-Target Cells in Vaccination

Author:

Mohr Christian Andreas1,Arapovic Jurica2,Mühlbach Hermine1,Panzer Marc3,Weyn Annelies1,Dölken Lars1,Krmpotic Astrid2,Voehringer David3,Ruzsics Zsolt1,Koszinowski Ulrich1,Sacher Torsten1

Affiliation:

1. Max von Pettenkofer Institute, Ludwig Maximilians University, Pettenkoferstrasse 9a, D-80336 Munich, Germany

2. Department of Histology and Embryology, University of Rijeka, Brace Branchetta St. No. 20, HR-51 000 Rijeka, Croatia

3. Institute for Immunology, Ludwig Maximilians University, Goethestrasse 29-31, D-80336 Munich, Germany

Abstract

ABSTRACT Human cytomegalovirus (HCMV) is a human pathogen that causes severe disease primarily in the immunocompromised or immunologically immature individual. To date, no vaccine is available. We describe use of a spread-deficient murine CMV (MCMV) as a novel approach for betaherpesvirus vaccination. To generate a spread-deficient MCMV, the conserved, essential gene M94 was deleted. Immunization with MCMV-Δ M94 is apathogenic and protective against wild-type challenge even in highly susceptible IFNαβR −/− mice. MCMV-Δ M94 was able to induce a robust CD4 + and CD8 + T-cell response as well as a neutralizing antibody response comparable to that induced by wild-type infection. Endothelial cells were identified as activators of CD8 + T cells in vivo . Thus, the vaccination with a spread-deficient betaherpesvirus is a safe and protective strategy and allows the linkage between cell tropism and immunogenicity. Furthermore, genomes of MCMV- ΔM94 were present in lungs 12 months after infection, revealing first-target cells as sites of genome maintenance.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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