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Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs

Over the last 15 years, FMDV serotype A viruses in South-East Asia (A/ASIA/SEA-97 lineage) have diverged into several clusters. Variants from Thailand in 2011-2013 have caused vaccine failures and returned poor r(1)-values (<0.30) to A(22) Iraq 64 (A22) and A Malaysia 97 (A May) vaccine strains....

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Autores principales: Horsington, Jacquelyn, Singanallur Balasubramanian, Nagendrakumar, Nfon, Charles K., Bittner, Hilary, Vosloo, Wilna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9649919/
https://www.ncbi.nlm.nih.gov/pubmed/36387399
http://dx.doi.org/10.3389/fvets.2022.1027556
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author Horsington, Jacquelyn
Singanallur Balasubramanian, Nagendrakumar
Nfon, Charles K.
Bittner, Hilary
Vosloo, Wilna
author_facet Horsington, Jacquelyn
Singanallur Balasubramanian, Nagendrakumar
Nfon, Charles K.
Bittner, Hilary
Vosloo, Wilna
author_sort Horsington, Jacquelyn
collection PubMed
description Over the last 15 years, FMDV serotype A viruses in South-East Asia (A/ASIA/SEA-97 lineage) have diverged into several clusters. Variants from Thailand in 2011-2013 have caused vaccine failures and returned poor r(1)-values (<0.30) to A(22) Iraq 64 (A22) and A Malaysia 97 (A May) vaccine strains. We investigated the protective ability of monovalent and bivalent A Malaysia 97 and A22 Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs. Pigs were challenged with a variant of A/Asia/SEA-97 lineage either 21- or 7- days post-vaccination (V21 or V7) using the heal-bulb challenge. Only one in five pigs were protected in the V21 monovalent vaccine groups. Less severe clinical signs were observed in the A22 IRQ group compared to the A MAY 97 group. In the V21 combination group, 4 out of 5 pigs were protected and viraemia was significantly reduced compared to the monovalent V21 groups. V7 vaccine groups were not protected. The neutralising antibody response was below the detection limit in all groups on the challenge day, showing a poor correlation with protection. There was no evidence that the pigs protected from systemic disease had protective antibody responses sooner than other pigs in the study, implying other immune mechanisms might play a role in protecting these animals. FMDV was detected in the nasal and oral swab samples between 1 and 6 dpc. Viral loads were lower in the nasal swab samples from the V21 combination group than the other groups, but there was no difference in the oral swab samples. Since all unvaccinated controls were euthanised by 6-day post-challenge for ethical reasons, the ‘area under the curve (AUC)' method was used to compare the viraemia and virus excretion in different groups. We recommend that for the A/Asia/SEA97 variants, a combination vaccine with A Malaysia 97 and A22 Iraq 64 vaccine strains would be ideal compared to monovalent vaccines.
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spelling pubmed-96499192022-11-15 Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs Horsington, Jacquelyn Singanallur Balasubramanian, Nagendrakumar Nfon, Charles K. Bittner, Hilary Vosloo, Wilna Front Vet Sci Veterinary Science Over the last 15 years, FMDV serotype A viruses in South-East Asia (A/ASIA/SEA-97 lineage) have diverged into several clusters. Variants from Thailand in 2011-2013 have caused vaccine failures and returned poor r(1)-values (<0.30) to A(22) Iraq 64 (A22) and A Malaysia 97 (A May) vaccine strains. We investigated the protective ability of monovalent and bivalent A Malaysia 97 and A22 Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs. Pigs were challenged with a variant of A/Asia/SEA-97 lineage either 21- or 7- days post-vaccination (V21 or V7) using the heal-bulb challenge. Only one in five pigs were protected in the V21 monovalent vaccine groups. Less severe clinical signs were observed in the A22 IRQ group compared to the A MAY 97 group. In the V21 combination group, 4 out of 5 pigs were protected and viraemia was significantly reduced compared to the monovalent V21 groups. V7 vaccine groups were not protected. The neutralising antibody response was below the detection limit in all groups on the challenge day, showing a poor correlation with protection. There was no evidence that the pigs protected from systemic disease had protective antibody responses sooner than other pigs in the study, implying other immune mechanisms might play a role in protecting these animals. FMDV was detected in the nasal and oral swab samples between 1 and 6 dpc. Viral loads were lower in the nasal swab samples from the V21 combination group than the other groups, but there was no difference in the oral swab samples. Since all unvaccinated controls were euthanised by 6-day post-challenge for ethical reasons, the ‘area under the curve (AUC)' method was used to compare the viraemia and virus excretion in different groups. We recommend that for the A/Asia/SEA97 variants, a combination vaccine with A Malaysia 97 and A22 Iraq 64 vaccine strains would be ideal compared to monovalent vaccines. Frontiers Media S.A. 2022-10-28 /pmc/articles/PMC9649919/ /pubmed/36387399 http://dx.doi.org/10.3389/fvets.2022.1027556 Text en Copyright © 2022 Horsington, Singanallur Balasubramanian, Nfon, Bittner and Vosloo. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Veterinary Science
Horsington, Jacquelyn
Singanallur Balasubramanian, Nagendrakumar
Nfon, Charles K.
Bittner, Hilary
Vosloo, Wilna
Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs
title Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs
title_full Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs
title_fullStr Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs
title_full_unstemmed Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs
title_short Investigation into the protective ability of monovalent and bivalent A Malaysia 97 and A(22) Iraq 64 vaccine strains against infection with an A/Asia/SEA-97 variant in pigs
title_sort investigation into the protective ability of monovalent and bivalent a malaysia 97 and a(22) iraq 64 vaccine strains against infection with an a/asia/sea-97 variant in pigs
topic Veterinary Science
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9649919/
https://www.ncbi.nlm.nih.gov/pubmed/36387399
http://dx.doi.org/10.3389/fvets.2022.1027556
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