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Mucosally-administered human-simian immunodeficiency virus DNA and fowlpoxvirus-based recombinant vaccines reduce acute phase viral replication in macaques following vaginal challenge with CCR5-tropic SHIVSF162P3

dc.contributor.authorKent, Stephen Jen_AU
dc.contributor.authorDale, C Janeen_AU
dc.contributor.authorStratov, Ivanen_AU
dc.contributor.authorDe Rose, Roberten_AU
dc.contributor.authorChea, Socheataen_AU
dc.contributor.authorMontefiori, David Cen_AU
dc.contributor.authorThomson, Scotten_AU
dc.contributor.authorRamshaw, Ianen_AU
dc.contributor.authorCoupar, Barbara E Hen_AU
dc.contributor.authorBoyle, David Ben_AU
dc.contributor.authorLaw, Matthew Gen_AU
dc.contributor.authorWilson, Kim Men_AU
dc.contributor.authorRamsay, Alistairen_AU
dc.contributor.authorRanasinghe, Charanien_AU
dc.date.accessioned2015-12-13T23:00:13Z
dc.date.issued2005
dc.date.updated2015-12-12T07:32:40Z
dc.description.abstractFurther advances are required in understanding protection from AIDS by T cell immunity across mucosal sites of virus transmission. We analysed a set of multigenic HIV and SHIV DNA and Fowlpoxvirus (FPV) prime and boost vaccines for immunogenicity and protective efficacy in outbred pigtail macaques when delivered via mucosal surfaces (intranasally or intrarectally). Intranasally delivered DNA, even when adjuvanted and given as a fine droplet spray, was neither immunogenic nor protective in macaques. Some protection from acute infection with a pathogenic vaginal SHIVSF162P3 challenge was, however, observed with a regimen involving intramuscular DNA vaccine priming followed by either intranasally or intrarectally delivered rFPV boosting. Interestingly, animals boosted with rFPV vaccine via either of these mucosal routes had poor circulating T cell responses prior to challenge with SHIV compared to those boosted via the intramuscular route. Nevertheless, the mucosally-vaccinated animals generated equivalent anamnestic mucosal and systemic SHIV-specific CD4 and CD8 T cell responses following SHIV administration, with significant reduction in acute plasma viremia against this vaginal challenge. Our data suggest strategies for effective priming of partial immunity to mucosal HIV-1 exposure utilizing systemic prime and mucosal boost vaccination strategies.
dc.identifier.issn0264-410X
dc.identifier.urihttp://hdl.handle.net/1885/84023
dc.publisherElsevier
dc.sourceVaccine
dc.subjectKeywords: recombinant vaccine; Simian immunodeficiency virus vaccine; virus DNA; animal experiment; animal model; article; comparative study; controlled study; drug efficacy; exposure; Fowlpox virus; Human immunodeficiency virus; immunity; immunogenicity; Macaca; n DNA; Macaque; Mucosal immunology; Prime/Boost; Recombinant fowlpox virus; Vaccine
dc.titleMucosally-administered human-simian immunodeficiency virus DNA and fowlpoxvirus-based recombinant vaccines reduce acute phase viral replication in macaques following vaginal challenge with CCR5-tropic SHIVSF162P3
dc.typeJournal article
local.bibliographicCitation.lastpage5021
local.bibliographicCitation.startpage5009
local.contributor.affiliationKent, Stephen J, University of Melbourne
local.contributor.affiliationDale, C Jane, University of Melbourne
local.contributor.affiliationRanasinghe, Charani, University of Newcastle
local.contributor.affiliationStratov, Ivan, University of Melbourne
local.contributor.affiliationDe Rose, Robert, University of Melbourne
local.contributor.affiliationChea, Socheata, University of Melbourne
local.contributor.affiliationMontefiori, David C, Duke University
local.contributor.affiliationThomson, Scott, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationRamshaw, Ian, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationCoupar, Barbara E H, Duke University
local.contributor.affiliationBoyle, David B, CSIRO Division of Livestock Industries
local.contributor.affiliationLaw, Matthew G, University of New South Wales
local.contributor.affiliationWilson, Kim M, St Vincent's Institute of Medical Research
local.contributor.affiliationRamsay, Alistair, University of Newcastle
local.contributor.authoruidThomson, Scott, u9711363
local.contributor.authoruidRamshaw, Ian, u8202754
local.description.embargo2037-12-31
local.description.notesImported from ARIES
local.description.refereedYes
local.identifier.absfor110799 - Immunology not elsewhere classified
local.identifier.ariespublicationMigratedxPub12289
local.identifier.citationvolume23
local.identifier.doi10.1016/j.vaccine.2005.05.032
local.identifier.scopusID2-s2.0-23844532213
local.type.statusPublished Versionen_AU

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