Please use this identifier to cite or link to this item: https://hdl.handle.net/1959.11/21306
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dc.contributor.authorEvenson, Den
dc.contributor.authorGerber, Priscilla Freitasen
dc.contributor.authorXiao, C Ten
dc.contributor.authorHalbur, P Gen
dc.contributor.authorWang, Cen
dc.contributor.authorTian, Den
dc.contributor.authorNi, Y Yen
dc.contributor.authorMeng, X Jen
dc.contributor.authorOpriessnig, Ten
dc.date.accessioned2017-06-07T13:58:00Z-
dc.date.issued2016-
dc.identifier.citationVaccine, 34(46), p. 5546-5553en
dc.identifier.issn1873-2518en
dc.identifier.issn0264-410Xen
dc.identifier.urihttps://hdl.handle.net/1959.11/21306-
dc.description.abstractCurrent porcine reproductive and respiratory syndrome virus (PRRSV) vaccines sometimes fail to provide adequate immunity to protect pigs from PRRSV-induced disease. This may be due to antigenic differences among PRRSV strains. Rapid production of attenuated farm-specific homologous vaccines is a feasible alternative to commercial vaccines. In this study, attenuation and efficacy of a codon-pair de-optimized candidate vaccine generated by synthetic attenuated virus engineering approach (SAVE5) were tested in a conventional growing pig model. Forty pigs were vaccinated intranasally or intramuscularly with SAVE5 at day 0 (D0). The remaining 28 pigs were sham-vaccinated with saline. At D42, 30 vaccinated and 19 sham-vaccinated pigs were challenged with the homologous PRRSV strain VR2385. The experiment was terminated at D54. The SAVE5 virus was effectively attenuated as evidenced by a low magnitude of SAVE5 viremia for 1-5 consecutive weeks in 35.9% (14/39) of the vaccinated pigs, lack of detectable nasal SAVE5 shedding and failure to transmit the vaccine virus from pig to pig. By D42, all vaccinated pigs with detectable SAVE5 viremia also had detectable anti-PRRSV IgG. Anti-IgG positive vaccinated pigs were protected from subsequent VR2385 challenge as evidenced by lack of VR2385 viremia and nasal shedding, significantly reduced macroscopic and microscopic lung lesions and significantly reduced amount of PRRSV antigen in lungs compared to the non-vaccinated VR2385-challenged positive control pigs. The nasal vaccination route appeared to be more effective in inducing protective immunity in a larger number of pigs compared to the intramuscular route. Vaccinated pigs without detectable SAVE5 viremia did not seroconvert and were fully susceptible to VR2385 challenge. Under the study conditions, the SAVE approach was successful in attenuating PRRSV strain VR2385 and protected against homologous virus challenge. Virus dosage likely needs to be adjusted to induce replication and protection in a higher percentage of vaccinated pigs.en
dc.languageenen
dc.publisherElsevier Ltden
dc.relation.ispartofVaccineen
dc.titleA porcine reproductive and respiratory syndrome virus candidate vaccine based on the synthetic attenuated virus engineering approach is attenuated and effective in protecting against homologous virus challengeen
dc.typeJournal Articleen
dc.identifier.doi10.1016/j.vaccine.2016.09.049en
dc.subject.keywordsVeterinary Epidemiologyen
dc.subject.keywordsVeterinary Virologyen
dc.subject.keywordsVeterinary Immunologyen
local.contributor.firstnameDen
local.contributor.firstnamePriscilla Freitasen
local.contributor.firstnameC Ten
local.contributor.firstnameP Gen
local.contributor.firstnameCen
local.contributor.firstnameDen
local.contributor.firstnameY Yen
local.contributor.firstnameX Jen
local.contributor.firstnameTen
local.subject.for2008070712 Veterinary Virologyen
local.subject.for2008070705 Veterinary Immunologyen
local.subject.for2008070704 Veterinary Epidemiologyen
local.subject.seo2008830308 Pigsen
local.profile.schoolSchool of Environmental and Rural Scienceen
local.profile.emailpgerber2@une.edu.auen
local.output.categoryC1en
local.record.placeauen
local.record.institutionUniversity of New Englanden
local.identifier.epublicationsrecordune-chute-20170602-153733en
local.publisher.placeUnited Kingdomen
local.format.startpage5546en
local.format.endpage5553en
local.identifier.scopusid84992365964en
local.peerreviewedYesen
local.identifier.volume34en
local.identifier.issue46en
local.contributor.lastnameEvensonen
local.contributor.lastnameGerberen
local.contributor.lastnameXiaoen
local.contributor.lastnameHalburen
local.contributor.lastnameWangen
local.contributor.lastnameTianen
local.contributor.lastnameNien
local.contributor.lastnameMengen
local.contributor.lastnameOpriessnigen
dc.identifier.staffune-id:pgerber2en
local.profile.orcid0000-0002-8343-8299en
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.profile.roleauthoren
local.identifier.unepublicationidune:21499en
local.identifier.handlehttps://hdl.handle.net/1959.11/21306en
dc.identifier.academiclevelAcademicen
local.title.maintitleA porcine reproductive and respiratory syndrome virus candidate vaccine based on the synthetic attenuated virus engineering approach is attenuated and effective in protecting against homologous virus challengeen
local.output.categorydescriptionC1 Refereed Article in a Scholarly Journalen
local.search.authorEvenson, Den
local.search.authorGerber, Priscilla Freitasen
local.search.authorXiao, C Ten
local.search.authorHalbur, P Gen
local.search.authorWang, Cen
local.search.authorTian, Den
local.search.authorNi, Y Yen
local.search.authorMeng, X Jen
local.search.authorOpriessnig, Ten
local.uneassociationUnknownen
local.year.published2016en
local.fileurl.closedpublishedhttps://rune.une.edu.au/web/retrieve/851a77f5-f174-434e-a5f5-bc1eaec36f60en
local.subject.for2020300914 Veterinary virologyen
local.subject.for2020300906 Veterinary immunologyen
local.subject.for2020300905 Veterinary epidemiologyen
local.subject.seo2020100410 Pigsen
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