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Research Project:
DEVELOPMENT OF METHODS FOR RAPID CONTROL OF CLASSICAL SWINE FEVER (CSF)
Project Number: 1940-32000-050-00
Project Type:
Appropriated
Start Date: Mar 28, 2007
End Date: Feb 28, 2012
Objective:
Develop effective CSFV marker vaccines and companion diagnostic tests capable of differentiating vaccinated from infected animals.
Examine innate local immune mechanisms mediating early protection in vaccinated pigs and mechanisms of delivery for rapid mucosal immunity.
Approach:
Development of a novel live-attenuated CSF marker vaccine requires knowledge of the genetic basis of viral virulence. Using reverse genetics, it is possible to systematically evaluate the role of specific viral proteins or virus virulence, and use this information to engineer recombinant LAVs. Our strategy is to introduce modifications in our CSFV infectious clone. The first objective will be achieved by introducing specific mutations on the CSFV envelope glycoprotein and determine their effect on virus virulence. We hypothesize that positive and negative virus antigenic markers will induce unique antibody responses in vaccinated animals, thus showing differentiation in ELISA tests. Serological tests will be developed to differentiate experimentally vaccinated from CSFV wildtype infected animals. The approach to achieving the second objective consists in identifying and characterizing the tissues and cells infected with attenuated and virulent strains. This will provide information on the mechanisms inducing early protection after LAV administration. A comparison will be conducted of the tissue and cell types affected during early stages of infection with attenuated and virulent strains. Analysis will be done on the profiles of locally produced pro-inflammatory chemical mediators and host gene activation during infection with attenuated and virulent strains. We also postulate that oral administration of the candidate LAV strains will lead to effective protective response in domestic pigs. We will evaluate the delivery of CSFV vaccines by mucosal routes and their effectiveness in early protection of domestic and eventually in feral swine.
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Last Modified: 05/08/2009
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