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Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice

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dc.contributor.author O’Kennedy, Martha M
dc.contributor.author Roth, Robyn
dc.contributor.author Ebersohn, K
dc.contributor.author Du Plessis, LH
dc.contributor.author Mamputha, Sipho
dc.contributor.author Rutkowska, Daria A
dc.contributor.author Du Preez, Ilse
dc.contributor.author Verschoor, JA
dc.contributor.author Lemmer, Yolandy
dc.date.accessioned 2024-09-13T09:29:53Z
dc.date.available 2024-09-13T09:29:53Z
dc.date.issued 2024-04
dc.identifier.citation O’Kennedy, Martha M, Roth, R., Ebersohn, K., Du Plessis, L., Mamputha, S., Rutkowska, D.A., Du Preez, I. & Verschoor, J. et al. 2024. Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice. <i>Plos One, 19(4).</i> http://hdl.handle.net/10204/13756 en_ZA
dc.identifier.issn 1932-6203
dc.identifier.uri https://doi.org/10.1371/journal.pone.0301340
dc.identifier.uri http://hdl.handle.net/10204/13756
dc.description.abstract A safe, highly immunogenic multivalent vaccine to protect against all nine serotypes of African horse sickness virus (AHSV), will revolutionise the AHS vaccine industry in endemic countries and beyond. Plant-produced AHS virus-like particles (VLPs) and soluble viral protein 2 (VP2) vaccine candidates were developed that have the potential to protect against all nine serotypes but can equally well be formulated as mono- and bi-valent formulations for localised outbreaks of specific serotypes. In the first interferon a/ß receptor knock-out (IFNAR-/-) mice trial conducted, a nine-serotype (nonavalent) vaccine administered as two pentavalent (5 µg per serotype) vaccines (VLP/VP2 combination or exclusively VP2), were directly compared to the commercially available AHS live attenuated vaccine. In a follow up trial, mice were vaccinated with an adjuvanted nine-serotype multivalent VP2 vaccine in a prime boost strategy and resulted in the desired neutralising antibody titres of 1:320, previously demonstrated to confer protective immunity in IFNAR-/- mice. In addition, the plant-produced VP2 vaccine performed favourably when compared to the commercial vaccine. Here we provide compelling data for a nonavalent VP2-based vaccine candidate, with the VP2 from each serotype being antigenically distinguishable based on LC-MS/MS and ELISA data. This is the first preclinical trial demonstrating the ability of an adjuvanted nonavalent cocktail of soluble, plant-expressed AHS VP2 proteins administered in a prime-boost strategy eliciting high antibody titres against all 9 AHSV serotypes. Furthermore, elevated T helper cells 2 (Th2) and Th1, indicative of humoral and cell-mediated memory T cell immune responses, respectively, were detected in mouse serum collected 14 days after the multivalent prime-boost vaccination. Both Th2 and Th1 may play a role to confer protective immunity. These preclinical immunogenicity studies paved the way to test the safety and protective efficacy of the plant-produced nonavalent VP2 vaccine candidate in the target animals, horses. en_US
dc.format Fulltext en_US
dc.language.iso en en_US
dc.relation.uri https://journals.plos.org/plosone/article?id=10.1371/journal.pone.0301340 en_US
dc.source Plos One, 19(4) en_US
dc.subject Immunogenic multivalent vaccine en_US
dc.subject African Horse Sickness virus en_US
dc.subject AHSV en_US
dc.subject Plant-produced AHS virus-like particles en_US
dc.subject Soluble viral protein 2 en_US
dc.subject VP2 en_US
dc.title Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice en_US
dc.type Article en_US
dc.description.pages 18 en_US
dc.description.note Copyright: © 2024 O’Kennedy et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. en_US
dc.description.cluster Chemicals en_US
dc.description.cluster Advanced Agriculture & Food en_US
dc.description.impactarea BT: Technology Demonstration en_US
dc.description.impactarea Aquaculture and Veterinary en_US
dc.description.impactarea BT: Bioprocessing en_US
dc.identifier.apacitation O’Kennedy, Martha M, Roth, R., Ebersohn, K., Du Plessis, L., Mamputha, S., Rutkowska, D. A., ... Lemmer, Y. (2024). Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice. <i>Plos One, 19(4)</i>, http://hdl.handle.net/10204/13756 en_ZA
dc.identifier.chicagocitation O’Kennedy, Martha M, Robyn Roth, K Ebersohn, LH Du Plessis, Sipho Mamputha, Daria A Rutkowska, Ilse Du Preez, JA Verschoor, and Yolandy Lemmer "Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice." <i>Plos One, 19(4)</i> (2024) http://hdl.handle.net/10204/13756 en_ZA
dc.identifier.vancouvercitation O’Kennedy, Martha M, Roth R, Ebersohn K, Du Plessis L, Mamputha S, Rutkowska DA, et al. Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice. Plos One, 19(4). 2024; http://hdl.handle.net/10204/13756. en_ZA
dc.identifier.ris TY - Article AU - O’Kennedy, Martha M AU - Roth, Robyn AU - Ebersohn, K AU - Du Plessis, LH AU - Mamputha, Sipho AU - Rutkowska, Daria A AU - Du Preez, Ilse AU - Verschoor, JA AU - Lemmer, Yolandy AB - A safe, highly immunogenic multivalent vaccine to protect against all nine serotypes of African horse sickness virus (AHSV), will revolutionise the AHS vaccine industry in endemic countries and beyond. Plant-produced AHS virus-like particles (VLPs) and soluble viral protein 2 (VP2) vaccine candidates were developed that have the potential to protect against all nine serotypes but can equally well be formulated as mono- and bi-valent formulations for localised outbreaks of specific serotypes. In the first interferon a/ß receptor knock-out (IFNAR-/-) mice trial conducted, a nine-serotype (nonavalent) vaccine administered as two pentavalent (5 µg per serotype) vaccines (VLP/VP2 combination or exclusively VP2), were directly compared to the commercially available AHS live attenuated vaccine. In a follow up trial, mice were vaccinated with an adjuvanted nine-serotype multivalent VP2 vaccine in a prime boost strategy and resulted in the desired neutralising antibody titres of 1:320, previously demonstrated to confer protective immunity in IFNAR-/- mice. In addition, the plant-produced VP2 vaccine performed favourably when compared to the commercial vaccine. Here we provide compelling data for a nonavalent VP2-based vaccine candidate, with the VP2 from each serotype being antigenically distinguishable based on LC-MS/MS and ELISA data. This is the first preclinical trial demonstrating the ability of an adjuvanted nonavalent cocktail of soluble, plant-expressed AHS VP2 proteins administered in a prime-boost strategy eliciting high antibody titres against all 9 AHSV serotypes. Furthermore, elevated T helper cells 2 (Th2) and Th1, indicative of humoral and cell-mediated memory T cell immune responses, respectively, were detected in mouse serum collected 14 days after the multivalent prime-boost vaccination. Both Th2 and Th1 may play a role to confer protective immunity. These preclinical immunogenicity studies paved the way to test the safety and protective efficacy of the plant-produced nonavalent VP2 vaccine candidate in the target animals, horses. DA - 2024-04 DB - ResearchSpace DP - CSIR J1 - Plos One, 19(4) KW - Immunogenic multivalent vaccine KW - African Horse Sickness virus KW - AHSV KW - Plant-produced AHS virus-like particles KW - Soluble viral protein 2 KW - VP2 LK - https://researchspace.csir.co.za PY - 2024 SM - 1932-6203 T1 - Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice TI - Immunogenic profile of a plant-produced nonavalent African horse sickness viral protein 2 (VP2) vaccine in IFNAR-/-mice UR - http://hdl.handle.net/10204/13756 ER - en_ZA
dc.identifier.worklist 28073 en_US


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