Tracking the antigenic evolution of foot-and-mouth disease virus

dc.contributor.authorReeve, Richard
dc.contributor.authorBorley, Daryl W.
dc.contributor.authorMaree, Francois Frederick
dc.contributor.authorUpadhyaya, Sasmita
dc.contributor.authorLukhwareni, Azwidowi
dc.contributor.authorEsterhuysen, Jan J.
dc.contributor.authorHarvey, William T.
dc.contributor.authorBlignaut, Belinda
dc.contributor.authorFry, Elizabeth E.
dc.contributor.authorParida, Satya
dc.contributor.authorPaton, David J.
dc.contributor.authorMahapatra, Mana
dc.date.accessioned2016-08-24T06:54:11Z
dc.date.available2016-08-24T06:54:11Z
dc.date.issued2016-07-22
dc.descriptionS1 Data. VNT serological results for serotype O viruses and antisera.en_ZA
dc.descriptionS2 Data. LPBE serological results for serotype O viruses and antisera.en_ZA
dc.descriptionS3 Data. VNT serological results for serotype SAT1 viruses and antisera.en_ZA
dc.descriptionS1 Table. Foot-and-mouth disease virus details with accession numbers.en_ZA
dc.descriptionS2 Table. Pan-serotypic reference alignment of FMDV. The dataset shows the aligned VP2, VP3 and VP1 proteins of example SAT1 and O isolates used in the study alongside representative isolates from the other five serotypes. The four contiguous surface-exposed structural motifs confirmed as containing antigenic sites on at least four serotypes are highlighted in red–locations are approximate due to structural differences between the serotypes. The RGD cell surface receptor-binding motif, in the centre of the third site, is highlighted in blue.en_ZA
dc.descriptionS3 Table. Residues identified as part of epitopes on structural proteins across the six tested serotypes of FMDV, along with corresponding positions on all serotypes.en_ZA
dc.descriptionS4 Table. SAT1 mar-mutants.en_ZA
dc.description.abstractQuantifying and predicting the antigenic characteristics of a virus is something of a holy grail for infectious disease research because of its central importance to the emergence of new strains, the severity of outbreaks, and vaccine selection. However, these characteristics are defined by a complex interplay of viral and host factors so that phylogenetic measures of viral similarity are often poorly correlated to antigenic relationships. Here, we generate antigenic phylogenies that track the phenotypic evolution of two serotypes of footand- mouth disease virus by combining host serology and viral sequence data to identify sites that are critical to their antigenic evolution. For serotype SAT1, we validate our antigenic phylogeny against monoclonal antibody escape mutants, which match all of the predicted antigenic sites. For serotype O, we validate it against known sites where available, and otherwise directly evaluate the impact on antigenic phenotype of substitutions in predicted sites using reverse genetics and serology. We also highlight a critical and poorly understood problem for vaccine selection by revealing qualitative differences between assays that are often used interchangeably to determine antigenic match between field viruses and vaccine strains. Our approach provides a tool to identify naturally occurring antigenic substitutions, allowing us to track the genetic diversification and associated antigenic evolution of the virus. Despite the hugely important role vaccines have played in enhancing human and animal health, vaccinology remains a conspicuously empirical science. This study advances the field by providing guidance for tuning vaccine strains via site-directed mutagenesis through this high-resolution tracking of antigenic evolution of the virus between rare major shifts in phenotype.en_ZA
dc.description.departmentMicrobiology and Plant Pathologyen_ZA
dc.description.departmentProduction Animal Studiesen_ZA
dc.description.librarianam2016en_ZA
dc.description.sponsorshipThe authors acknowledge the Biotechnology and Biological Sciences Research Council (BBSRC) Institute Strategic Programme on Livestock Viral Diseases at The Pirbright Institute (BB/J004375/1) [RR SP DJP MM] and BBSRC BB/ G529532/1 [DWB MM], BB/F009186/1 [MM] and BBSRC BB/L004828 [RR] and BBSRC / Department for International Development / Scottish Government grants BB/H009302/1 [RR] and BB/H009175/1 [SP FFM RR] (http://www.bbsrc.ac.uk), and Department for Environment, Food and Rural Affairs grant SE2937 (http://www.gov.uk/defra) [MM]. The Food and Agriculture Organisation financially supported the research to determine one-way relationship and antigenic relatedness of SAT1 viruses under grants OSRO/RAF/721/EC and MTF/INT/003/EEC (http:// www.fao.org) [FFM AL JJE BB], and RMRSA (http:// www.rmrdsa.co.za) (Improving detection and characterisation methods for FMDV and ASFV for cattle and pigs in the SADC region) [BB]. Structural studies supported by the UK Medical Research Council grant MR/N00065X/1 [EEF] (http://www.mrc. ac.uk). The work of the Wellcome Trust Centre in Oxford is supported by the Wellcome Trust core award 090532/Z/07/Z [EEF] (http://www.wellcome.ac. uk).en_ZA
dc.description.urihttp://www.plosone.orgen_ZA
dc.identifier.citationReeve R, Borley DW, Maree FF, Upadhyaya S, Lukhwareni A, Esterhuysen JJ, et al. (2016) Tracking the Antigenic Evolution of Foot-and- Mouth Disease Virus. PLoS ONE 11(7): e0159360. DOI: 10.1371/journal.pone.0159360.en_ZA
dc.identifier.issn1932-6203
dc.identifier.other10.1371/journal.pone.0159360
dc.identifier.urihttp://hdl.handle.net/2263/56465
dc.language.isoenen_ZA
dc.publisherPublic Library of Scienceen_ZA
dc.rights© 2016 Reeve et al. This is an open access article distributed under the terms of the Creative Commons Attribution License.en_ZA
dc.subjectSerotype SAT1en_ZA
dc.subjectSerotype Oen_ZA
dc.subjectInfectious diseaseen_ZA
dc.subjectVirusen_ZA
dc.subject.otherVeterinary science articles SDG-01en_ZA
dc.subject.otherVeterinary science articles SDG-02en_ZA
dc.subject.otherSDG-01: No poverty
dc.subject.otherSDG-02: Zero hunger
dc.titleTracking the antigenic evolution of foot-and-mouth disease virusen_ZA
dc.typeArticleen_ZA

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