Please use this identifier to cite or link to this item: https://hdl.handle.net/1959.11/51340
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dc.contributor.authorMcNeilly, Celiaen
dc.contributor.authorCosh, Samanthaen
dc.contributor.authorVu, Thereseen
dc.contributor.authorNichols, Jemmaen
dc.contributor.authorHenningham, Annaen
dc.contributor.authorHofmann, Andreasen
dc.contributor.authorFane, Anneen
dc.contributor.authorSmeesters, Pierre Ren
dc.contributor.authorRush, Catherine Men
dc.contributor.authorHafner, Louise Men
dc.contributor.authorKetheesan, Natkunamen
dc.contributor.authorSriprakash, Kadaba Sen
dc.contributor.authorMcMillan, David Jen
dc.date.accessioned2022-03-21T03:28:00Z-
dc.date.available2022-03-21T03:28:00Z-
dc.date.issued2016-06-16-
dc.identifier.citationPLoS One, 11(6), p. 1-17en
dc.identifier.issn1932-6203en
dc.identifier.urihttps://hdl.handle.net/1959.11/51340-
dc.description.abstract<p> The C-terminal region of the M-protein of Streptococcus pyogenes is a major target for vaccine development. The major feature is the C-repeat region, consisting of 35-42 amino acid repeat units that display high but not perfect identity. SV1 is a S. pyogenes vaccine candidate that incorporates five 14mer amino acid sequences (called J14<sub>i</sub> variants) from differing C-repeat units in a single recombinant construct. Here we show that the J14<sub>i</sub> variants chosen for inclusion in SV1 are the most common variants in a dataset of 176 unique M-proteins. Murine antibodies raised against SV1 were shown to bind to each of the J14<sub>i</sub> variants present in SV1, as well as variants not present in the vaccine. Antibodies raised to the individual J14<sub>i</sub> variants were also shown to bind to multiple but different combinations of J14<sub>i</sub> variants, supporting the underlying rationale for the design of SV1. A Lewis Rat Model of valvulitis was then used to assess the capacity of SV1 to induce deleterious immune response associated with rheumatic heart disease. In this model, both SV1 and the M5 positive control protein were immunogenic. Neither of these antibodies were cross-reactive with cardiac myosin or collagen. Splenic T cells from SV1/CFA and SV1/alum immunized rats did not proliferate in response to cardiac myosin or collagen. Subsequent histological examination of heart tissue showed that 4 of 5 mice from the M5/CFA group had valvulitis and inflammatory cell infiltration into valvular tissue, whereas mice immunised with SV1/CFA, SV1/alum showed no sign of valvulitis. These results suggest that SV1 is a safe vaccine candidate that will elicit antibodies that recognise the vast majority of circulating GAS M-types. </p>en
dc.languageenen
dc.publisherPublic Library of Scienceen
dc.relation.ispartofPLoS Oneen
dc.relation.isversionofe0156639en
dc.rightsAttribution 4.0 International*
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/*
dc.titlePredicted Coverage and Immuno-Safety of a Recombinant C-Repeat Region Based Streptococcus pyogenes Vaccine Candidateen
dc.typeJournal Articleen
dc.identifier.doi10.1371/journal.pone.0156639en
dc.identifier.pmid27310707en
dcterms.accessRightsUNE Greenen
local.contributor.firstnameCeliaen
local.contributor.firstnameSamanthaen
local.contributor.firstnameThereseen
local.contributor.firstnameJemmaen
local.contributor.firstnameAnnaen
local.contributor.firstnameAndreasen
local.contributor.firstnameAnneen
local.contributor.firstnamePierre Ren
local.contributor.firstnameCatherine Men
local.contributor.firstnameLouise Men
local.contributor.firstnameNatkunamen
local.contributor.firstnameKadaba Sen
local.contributor.firstnameDavid Jen
local.profile.schoolSchool of Science and Technologyen
local.profile.emailnkethees@une.edu.auen
local.output.categoryC1en
local.record.placeauen
local.record.institutionUniversity of New Englanden
local.publisher.placeUnited States of Americaen
local.format.startpage1en
local.format.endpage17en
local.identifier.scopusid84976319629en
local.peerreviewedYesen
local.identifier.volume11en
local.identifier.issue6en
local.access.fulltextYesen
local.contributor.lastnameMcNeillyen
local.contributor.lastnameCoshen
local.contributor.lastnameVuen
local.contributor.lastnameNicholsen
local.contributor.lastnameHenninghamen
local.contributor.lastnameHofmannen
local.contributor.lastnameFaneen
local.contributor.lastnameSmeestersen
local.contributor.lastnameRushen
local.contributor.lastnameHafneren
local.contributor.lastnameKetheesanen
local.contributor.lastnameSriprakashen
local.contributor.lastnameMcMillanen
dc.identifier.staffune-id:nketheesen
local.profile.orcid0000-0002-4870-706Xen
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local.identifier.unepublicationidune:1959.11/51340en
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
dc.identifier.academiclevelAcademicen
local.title.maintitlePredicted Coverage and Immuno-Safety of a Recombinant C-Repeat Region Based Streptococcus pyogenes Vaccine Candidateen
local.relation.fundingsourcenoteNational Health and Medical Research Council of Australia and National Heart Foundationen
local.output.categorydescriptionC1 Refereed Article in a Scholarly Journalen
local.search.authorMcNeilly, Celiaen
local.search.authorCosh, Samanthaen
local.search.authorVu, Thereseen
local.search.authorNichols, Jemmaen
local.search.authorHenningham, Annaen
local.search.authorHofmann, Andreasen
local.search.authorFane, Anneen
local.search.authorSmeesters, Pierre Ren
local.search.authorRush, Catherine Men
local.search.authorHafner, Louise Men
local.search.authorKetheesan, Natkunamen
local.search.authorSriprakash, Kadaba Sen
local.search.authorMcMillan, David Jen
local.open.fileurlhttps://rune.une.edu.au/web/retrieve/26671c67-e9b6-4162-ae4a-1a518c85117aen
local.uneassociationNoen
local.atsiresearchNoen
local.sensitive.culturalNoen
local.identifier.wosid000378029800010en
local.year.published2016en
local.fileurl.openhttps://rune.une.edu.au/web/retrieve/26671c67-e9b6-4162-ae4a-1a518c85117aen
local.fileurl.openpublishedhttps://rune.une.edu.au/web/retrieve/26671c67-e9b6-4162-ae4a-1a518c85117aen
local.subject.for2020320211 Infectious diseasesen
local.subject.for2020320701 Medical bacteriologyen
local.subject.seo2020240801 Human biological preventativesen
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School of Science and Technology
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