Evaluation of lesions and viral antigen distribution in domestic pigs inoculated intranasally with African swine fever virus Ken05/Tk1 (genotype X)
Evaluation of lesions and viral antigen distribution in domestic pigs inoculated intranasally with African swine fever virus Ken05/Tk1 (genotype X)
The understanding of the pathogenic mechanisms and the clinicopathological forms caused by currently circulating African swine fever virus (ASFV) isolates is incomplete. So far, most of the studies have been focused on isolates classified within genotypes I and II, the only genotypes that have circulated outside of Africa. However, less is known about the clinical presentations and lesions induced by isolates belonging to the other twenty-two genotypes. Therefore, the early clinicopathological identification of disease outbreaks caused by isolates belonging to, as yet, not well-characterised ASFV genotypes may be compromised, which might cause a delay in the implementation of control measures to halt the virus spread. To improve the pathological characterisation of disease caused by diverse isolates, we have refined the macroscopic and histopathological evaluation protocols to standardise the scoring of lesions. Domestic pigs were inoculated intranasally with different doses (high, medium and low) of ASFV isolate Ken05/Tk1 (genotype X). To complement previous studies, the distribution and severity of macroscopic and histopathological lesions, along with the amount and distribution of viral antigen in tissues, were characterised by applying the new scoring protocols. The intranasal inoculation of domestic pigs with high doses of the Ken05/Tk1 isolate induced acute forms of ASF in most of the animals. Inoculation with medium doses mainly induced acute forms of disease. A less severe but longer clinical course, typical of subacute forms, characterised by the presence of more widespread and severe haemorrhages and oedema, was observed in one pig inoculated with the medium dose. The severity of vascular lesions (haemorrhages and oedema) induced by high and medium doses was not associated with the amount of virus antigen detected in tissues, therefore these might be attributed to indirect mechanisms not evaluated in the present study. The absence of clinical signs, lesions and detectable levels of virus genome or antigen in blood from the animals inoculated with the lowest dose ruled out the existence of possible asymptomatic carriers or persistently infected pigs, at least for the 21 days period of the study. The results corroborate the moderate virulence of the Ken05/Tk1 isolate, as well as its capacity to induce both the acute and, occasionally, subacute forms of ASF when high and medium doses were administered intranasally.
Sánchez-Cordón, Pedro J.
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Floyd, Tobias
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Hicks, Daniel
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Crooke, Helen R.
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McCleary, Stephen
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McCarthy, Ronan R.
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Strong, Rebecca
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Dixon, Linda K.
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Neimanis, Aleksija
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Wikström-Lassa, Emil
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Gavier-Widén, Dolores
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Núñez, Alejandro
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18 June 2021
Sánchez-Cordón, Pedro J.
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Floyd, Tobias
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Hicks, Daniel
53470617-5cf3-42c6-a580-5f7eff85e7b2
Crooke, Helen R.
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McCleary, Stephen
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McCarthy, Ronan R.
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Strong, Rebecca
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Dixon, Linda K.
5c43e34f-e597-48da-ba5c-c4ef3ff6dbeb
Neimanis, Aleksija
ff2b1775-5367-4b31-8ab9-ed410268d8bf
Wikström-Lassa, Emil
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Gavier-Widén, Dolores
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Núñez, Alejandro
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Sánchez-Cordón, Pedro J., Floyd, Tobias, Hicks, Daniel, Crooke, Helen R., McCleary, Stephen, McCarthy, Ronan R., Strong, Rebecca, Dixon, Linda K., Neimanis, Aleksija, Wikström-Lassa, Emil, Gavier-Widén, Dolores and Núñez, Alejandro
(2021)
Evaluation of lesions and viral antigen distribution in domestic pigs inoculated intranasally with African swine fever virus Ken05/Tk1 (genotype X).
Pathogens, 10 (6), [768].
(doi:10.3390/pathogens10060768).
Abstract
The understanding of the pathogenic mechanisms and the clinicopathological forms caused by currently circulating African swine fever virus (ASFV) isolates is incomplete. So far, most of the studies have been focused on isolates classified within genotypes I and II, the only genotypes that have circulated outside of Africa. However, less is known about the clinical presentations and lesions induced by isolates belonging to the other twenty-two genotypes. Therefore, the early clinicopathological identification of disease outbreaks caused by isolates belonging to, as yet, not well-characterised ASFV genotypes may be compromised, which might cause a delay in the implementation of control measures to halt the virus spread. To improve the pathological characterisation of disease caused by diverse isolates, we have refined the macroscopic and histopathological evaluation protocols to standardise the scoring of lesions. Domestic pigs were inoculated intranasally with different doses (high, medium and low) of ASFV isolate Ken05/Tk1 (genotype X). To complement previous studies, the distribution and severity of macroscopic and histopathological lesions, along with the amount and distribution of viral antigen in tissues, were characterised by applying the new scoring protocols. The intranasal inoculation of domestic pigs with high doses of the Ken05/Tk1 isolate induced acute forms of ASF in most of the animals. Inoculation with medium doses mainly induced acute forms of disease. A less severe but longer clinical course, typical of subacute forms, characterised by the presence of more widespread and severe haemorrhages and oedema, was observed in one pig inoculated with the medium dose. The severity of vascular lesions (haemorrhages and oedema) induced by high and medium doses was not associated with the amount of virus antigen detected in tissues, therefore these might be attributed to indirect mechanisms not evaluated in the present study. The absence of clinical signs, lesions and detectable levels of virus genome or antigen in blood from the animals inoculated with the lowest dose ruled out the existence of possible asymptomatic carriers or persistently infected pigs, at least for the 21 days period of the study. The results corroborate the moderate virulence of the Ken05/Tk1 isolate, as well as its capacity to induce both the acute and, occasionally, subacute forms of ASF when high and medium doses were administered intranasally.
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pathogens-10-00768-v3
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Accepted/In Press date: 16 June 2021
Published date: 18 June 2021
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Local EPrints ID: 506441
URI: http://eprints.soton.ac.uk/id/eprint/506441
ISSN: 2076-0817
PURE UUID: 12a7433b-0c53-4406-96fe-4e3c73817a34
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Date deposited: 07 Nov 2025 17:33
Last modified: 08 Nov 2025 03:19
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Author:
Pedro J. Sánchez-Cordón
Author:
Tobias Floyd
Author:
Daniel Hicks
Author:
Helen R. Crooke
Author:
Stephen McCleary
Author:
Ronan R. McCarthy
Author:
Rebecca Strong
Author:
Linda K. Dixon
Author:
Aleksija Neimanis
Author:
Emil Wikström-Lassa
Author:
Dolores Gavier-Widén
Author:
Alejandro Núñez
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