Abstract

A successful virus infection involves entry into the cell; uncoating, expression and replication of the genome; assembly and release of infectious virus particles; and defense against specific and non- specific host immune mechanisms. Combined genetic, biochemical, electron microscopic, and immunological approaches are being used to investigate these complex processes. Two genetic approaches have been developed and applied to the study of vaccinia virus assembly. For essential genes, the elements of the E coli lac operon were used to construct inducer-dependent conditional lethal mutants of vaccinia virus. Repression of the D13L gene, which encodes a 65,000 Dalton protein, prevented the formation of the immature spicule-coated viral envelope and mimiced the action of the drug rifampicin. Repression of the F18R gene allowed virion morphogenesis to proceed up to the stage of differentiation of the virion core. The second approach, gene knock-out, was used to investigate the function of the outer viral envelope and the release of virions from cells. Deletion of the viral gene encoding the VP37 envelope protein did not affect the formation of intracellular infectious virus but prevented the membrane wrapping of virions and their fusion with the plasma membrane. Evidence was obtained for an additional post-budding step in virion release. With some strains of vaccinia virus, enveloped virions remain attached to the surface of cells but can be released with trypsin treatment. To evade the host immune system, vaccinia virus encodes a variety of proteins. We demonstrated that the complement control protein (VCP), the secreted product of the C2IL gene, is able to prevent complement- enhanced antibody-mediated neutralization of infectious virus. These data demonstrated that VCP blocks the alternative, as well as the classical, pathway of complement activation. A mutant virus containing a knock-out deletion of the C2IL gene was highly attenuated when injected into the skin of animals. The basis for the interferon- resistance of vaccinia virus was investigated. The product of the K3L gene was found to inhibit the double-stranded RNA activated protein kinase and to thereby prevent the interferon induced phosphorylation of the alpha subunit of eukaryotic initiation factor 2. Evidence against the possibility that vaccinia inhibits host protein synthesis by degrading or causing the underphosphorylation of components of the cap- binding translation initiation factor complex eIF-4F was obtained.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000539-05
Application #
3790798
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
5
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
National Institute of Allergy and Infectious Diseases
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Wagenaar, Timothy R; Moss, Bernard (2009) Expression of the A56 and K2 proteins is sufficient to inhibit vaccinia virus entry and cell fusion. J Virol 83:1546-54
Resch, Wolfgang; Weisberg, Andrea S; Moss, Bernard (2009) Expression of the highly conserved vaccinia virus E6 protein is required for virion morphogenesis. Virology 386:478-85
Wagenaar, Timothy R; Ojeda, Suany; Moss, Bernard (2008) Vaccinia virus A56/K2 fusion regulatory protein interacts with the A16 and G9 subunits of the entry fusion complex. J Virol 82:5153-60
Nelson, Gretchen E; Wagenaar, Timothy R; Moss, Bernard (2008) A conserved sequence within the H2 subunit of the vaccinia virus entry/fusion complex is important for interaction with the A28 subunit and infectivity. J Virol 82:6244-50
Townsley, Alan C; Moss, Bernard (2007) Two distinct low-pH steps promote entry of vaccinia virus. J Virol 81:8613-20
Resch, Wolfgang; Hixson, Kim K; Moore, Ronald J et al. (2007) Protein composition of the vaccinia virus mature virion. Virology 358:233-47
Husain, Matloob; Weisberg, Andrea S; Moss, Bernard (2007) Sequence-independent targeting of transmembrane proteins synthesized within vaccinia virus factories to nascent viral membranes. J Virol 81:2646-55
Wagenaar, Timothy R; Moss, Bernard (2007) Association of vaccinia virus fusion regulatory proteins with the multicomponent entry/fusion complex. J Virol 81:6286-93
Husain, Matloob; Weisberg, Andrea S; Moss, Bernard (2007) Resistance of a vaccinia virus A34R deletion mutant to spontaneous rupture of the outer membrane of progeny virions on the surface of infected cells. Virology 366:424-32
Charity, James C; Katz, Ehud; Moss, Bernard (2007) Amino acid substitutions at multiple sites within the vaccinia virus D13 scaffold protein confer resistance to rifampicin. Virology 359:227-32

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