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Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever

African swine fever virus (ASFV) causes significant morbidity and mortality in pigs worldwide. The lack of vaccines or therapeutic options warrants urgent further investigation. To this aim, we developed a rationally designed live attenuated ASFV-Δ110-9L/505-7R mutant based on the highly pathogenic...

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Autores principales: Ding, Mingyang, Dang, Wen, Liu, Huanan, Zhang, Keshan, Xu, Fan, Tian, Hong, Huang, Huaguo, Shi, Zhengwang, Sunkang, Yongjie, Qin, Xiaodong, Zhang, Yong, Zheng, Haixue
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9599437/
https://www.ncbi.nlm.nih.gov/pubmed/36197109
http://dx.doi.org/10.1128/jvi.01192-22
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author Ding, Mingyang
Dang, Wen
Liu, Huanan
Zhang, Keshan
Xu, Fan
Tian, Hong
Huang, Huaguo
Shi, Zhengwang
Sunkang, Yongjie
Qin, Xiaodong
Zhang, Yong
Zheng, Haixue
author_facet Ding, Mingyang
Dang, Wen
Liu, Huanan
Zhang, Keshan
Xu, Fan
Tian, Hong
Huang, Huaguo
Shi, Zhengwang
Sunkang, Yongjie
Qin, Xiaodong
Zhang, Yong
Zheng, Haixue
author_sort Ding, Mingyang
collection PubMed
description African swine fever virus (ASFV) causes significant morbidity and mortality in pigs worldwide. The lack of vaccines or therapeutic options warrants urgent further investigation. To this aim, we developed a rationally designed live attenuated ASFV-Δ110-9L/505-7R mutant based on the highly pathogenic Genotype II ASFV CN/GS/2018 backbone by deleting 2 well-characterized interferon inhibitors MGF110-9L and MGF505-7R. The mutant was slightly attenuated in vitro compared to parental ASFV but highly tolerant to genetic modifications even after 30 successive passages in vitro. Groups of 5 pigs were intramuscularly inoculated with increasing doses of the mutant, ranging from 10(3) to 10(6) hemadsorption units (HAD(50)). Thirty-five days later, all groups were challenged with 10(2) HAD(50) of virulent parental ASFV. All the animals were clinically normal and devoid of clinical signs consistent with ASFV at the period of inoculation. In the virulent challenge, 2 animals from 10(3) HAD(50)-inoculated group and 1 animal from 10(4) HAD(50)-inoculated group were unprotected with severe postmortem and histological lesions. The rest of animals survived and manifested with relatively normal clinical appearance accompanied by tangible histological improvements in the extent of tissue damage. Meanwhile, antibody response, as represented by p30-specific antibody titers was positively correlated to protective efficacy, potentializing its usage as an indicator of protection. Moreover, compared to 1 dose, 2 doses provided additional protection, proving that 2 doses were better than 1 dose. The sufficiency in effectiveness supports the claim that our attenuated mutant may be a viable vaccine option with which to fight ASF. IMPORTANCE African swine fever virus (ASFV) is a causative agent of acute viral hemorrhagic disease of domestic swine which is associated with significant economic losses in the pig industry. The lack of vaccines or treatment options requires urgent further investigation. ASFV MGF110-9L and MGF505-7R, 2 well-characterized interferon inhibitors, were associated with viral virulence, host range, and immune modulation. In this study, a recombinant two-gene deletion ASFV mutant with deletion of MGF110-9L and MGF505-7R was constructed. The result showed that the mutant was safe, and also highly resistant to genetic modification even after 30 successive passages. High doses of our mutant (10(5) and 10(6) HAD(50)) provided sterile immunity and complete protection in a virulent challenge. Two doses were superior to 1 dose and provided additional protection. This study develops a new ASFV-specific live attenuated vaccine and may be a viable vaccine option against ASF.
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spelling pubmed-95994372022-10-27 Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever Ding, Mingyang Dang, Wen Liu, Huanan Zhang, Keshan Xu, Fan Tian, Hong Huang, Huaguo Shi, Zhengwang Sunkang, Yongjie Qin, Xiaodong Zhang, Yong Zheng, Haixue J Virol Vaccines and Antiviral Agents African swine fever virus (ASFV) causes significant morbidity and mortality in pigs worldwide. The lack of vaccines or therapeutic options warrants urgent further investigation. To this aim, we developed a rationally designed live attenuated ASFV-Δ110-9L/505-7R mutant based on the highly pathogenic Genotype II ASFV CN/GS/2018 backbone by deleting 2 well-characterized interferon inhibitors MGF110-9L and MGF505-7R. The mutant was slightly attenuated in vitro compared to parental ASFV but highly tolerant to genetic modifications even after 30 successive passages in vitro. Groups of 5 pigs were intramuscularly inoculated with increasing doses of the mutant, ranging from 10(3) to 10(6) hemadsorption units (HAD(50)). Thirty-five days later, all groups were challenged with 10(2) HAD(50) of virulent parental ASFV. All the animals were clinically normal and devoid of clinical signs consistent with ASFV at the period of inoculation. In the virulent challenge, 2 animals from 10(3) HAD(50)-inoculated group and 1 animal from 10(4) HAD(50)-inoculated group were unprotected with severe postmortem and histological lesions. The rest of animals survived and manifested with relatively normal clinical appearance accompanied by tangible histological improvements in the extent of tissue damage. Meanwhile, antibody response, as represented by p30-specific antibody titers was positively correlated to protective efficacy, potentializing its usage as an indicator of protection. Moreover, compared to 1 dose, 2 doses provided additional protection, proving that 2 doses were better than 1 dose. The sufficiency in effectiveness supports the claim that our attenuated mutant may be a viable vaccine option with which to fight ASF. IMPORTANCE African swine fever virus (ASFV) is a causative agent of acute viral hemorrhagic disease of domestic swine which is associated with significant economic losses in the pig industry. The lack of vaccines or treatment options requires urgent further investigation. ASFV MGF110-9L and MGF505-7R, 2 well-characterized interferon inhibitors, were associated with viral virulence, host range, and immune modulation. In this study, a recombinant two-gene deletion ASFV mutant with deletion of MGF110-9L and MGF505-7R was constructed. The result showed that the mutant was safe, and also highly resistant to genetic modification even after 30 successive passages. High doses of our mutant (10(5) and 10(6) HAD(50)) provided sterile immunity and complete protection in a virulent challenge. Two doses were superior to 1 dose and provided additional protection. This study develops a new ASFV-specific live attenuated vaccine and may be a viable vaccine option against ASF. American Society for Microbiology 2022-10-05 /pmc/articles/PMC9599437/ /pubmed/36197109 http://dx.doi.org/10.1128/jvi.01192-22 Text en Copyright © 2022 Ding et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Vaccines and Antiviral Agents
Ding, Mingyang
Dang, Wen
Liu, Huanan
Zhang, Keshan
Xu, Fan
Tian, Hong
Huang, Huaguo
Shi, Zhengwang
Sunkang, Yongjie
Qin, Xiaodong
Zhang, Yong
Zheng, Haixue
Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever
title Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever
title_full Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever
title_fullStr Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever
title_full_unstemmed Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever
title_short Sequential Deletions of Interferon Inhibitors MGF110-9L and MGF505-7R Result in Sterile Immunity against the Eurasia Strain of Africa Swine Fever
title_sort sequential deletions of interferon inhibitors mgf110-9l and mgf505-7r result in sterile immunity against the eurasia strain of africa swine fever
topic Vaccines and Antiviral Agents
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9599437/
https://www.ncbi.nlm.nih.gov/pubmed/36197109
http://dx.doi.org/10.1128/jvi.01192-22
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