Vaccination of BALB/c Mice withEscherichia coli-Expressed Vaccinia Virus Proteins A27L, B5R, and D8L Protects Mice from Lethal Vaccinia Virus Challenge
- 1 April 2008
- journal article
- Published by American Society for Microbiology in Journal of Virology
- Vol. 82 (7), 3517-3529
- https://doi.org/10.1128/jvi.01854-07
Abstract
The potential threat of smallpox use in a bioterrorist attack has heightened the need to develop an effective smallpox vaccine for immunization of the general public. Vaccination with the current smallpox vaccine, Dryvax, produces protective immunity but may result in adverse reactions for some vaccinees. A subunit vaccine composed of protective vaccinia virus proteins should avoid the complications arising from live-virus vaccination and thus provide a safer alternative smallpox vaccine. In this study, we assessed the protective efficacy and immunogenicity of a multisubunit vaccine composed of the A27L and D8L proteins from the intracellular mature virus (IMV) form and the B5R protein from the extracellular enveloped virus (EEV) form of vaccinia virus. BALB/c mice were immunized with Escherichia coli-produced A27L, D8L, and B5R proteins in an adjuvant consisting of monophosphoryl lipid A and trehalose dicorynomycolate or in TiterMax Gold adjuvant. Following immunization, mice were either sacrificed for analysis of immune responses or lethally challenged by intranasal inoculation with vaccinia virus strain Western Reserve. We observed that three immunizations either with A27L, D8L, and B5R or with the A27L and B5R proteins alone induced potent neutralizing antibody responses and provided complete protection against lethal vaccinia virus challenge. Several linear B-cell epitopes within the three proteins were recognized by sera from the immunized mice. In addition, protein-specific cellular responses were detected in spleens of immunized mice by a gamma interferon enzyme-linked immunospot assay using peptides derived from each protein. Our data suggest that a subunit vaccine incorporating bacterially expressed IMV- and EEV-specific proteins can be effective in stimulating anti-vaccinia virus immune responses and providing protection against lethal virus challenge.Keywords
This publication has 81 references indexed in Scilit:
- Immunogenicity and protection efficacy of subunit-based smallpox vaccines using variola major antigensVirology, 2008
- A protein-based smallpox vaccine protects mice from vaccinia and ectromelia virus challenges when given as a prime and single boostVaccine, 2007
- Adjuvant-enhanced antibody responses to recombinant proteins correlates with protection of mice and monkeys to orthopoxvirus challengesVaccine, 2007
- Human T-Cell Responses to Vaccinia Virus Envelope ProteinsJournal of Virology, 2006
- Differential efficacy of vaccinia virus envelope proteins administered by DNA immunisation in protection of BALB/c mice from a lethal intranasal poxvirus challengeVaccine, 2004
- Identification of Second-Site Mutations That Enhance Release and Spread of Vaccinia VirusJournal of Virology, 2002
- Assembly of vaccinia virus: role of the intermediate compartment between the endoplasmic reticulum and the Golgi stacks.The Journal of cell biology, 1993
- Peptides Presented to the Immune System by the Murine Class II Major Histocompatibility Complex Molecule I-A dScience, 1992
- Risks and benefits of vaccinia vaccine use in the worldwide smallpox eradication campaignResearch in Virology, 1989
- THE UPTAKE AND DEVELOPMENT OF VACCINIA VIRUS IN STRAIN L CELLS FOLLOWED WITH LABELED VIRAL DEOXYRIBONUCLEIC ACIDThe Journal of cell biology, 1963