Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O

The presence of sequence divergence through adaptive mutations in the major capsid protein VP1, and also in VP0 (VP4 and VP2) and VP3, of foot-and-mouth disease virus (FMDV) is relevant to a broad range of viral characteristics. To explore the potential role of isolate-specific residues in the VP0 a...

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Autores principales: Bai, Xing-Wen, Bao, Hui-Fang, Li, Ping-Hua, Ma, Xue-Qing, Sun, Pu, Bai, Qi-Feng, Zhang, Meng, Yuan, Hong, Chen, Dong-Dong, Li, Kun, Chen, Ying-Li, Cao, Yi-Mei, Fu, Yuan-Fang, Zhang, Jing, Li, Dong, Lu, Zeng-Jun, Liu, Zai-Xin, Luo, Jian-Xun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2019
Materias:
Virus-Cell Interactions
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6430551/
https://www.ncbi.nlm.nih.gov/pubmed/30700601
http://dx.doi.org/10.1128/JVI.02278-18
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author Bai, Xing-Wen
Bao, Hui-Fang
Li, Ping-Hua
Ma, Xue-Qing
Sun, Pu
Bai, Qi-Feng
Zhang, Meng
Yuan, Hong
Chen, Dong-Dong
Li, Kun
Chen, Ying-Li
Cao, Yi-Mei
Fu, Yuan-Fang
Zhang, Jing
Li, Dong
Lu, Zeng-Jun
Liu, Zai-Xin
Luo, Jian-Xun
author_facet Bai, Xing-Wen
Bao, Hui-Fang
Li, Ping-Hua
Ma, Xue-Qing
Sun, Pu
Bai, Qi-Feng
Zhang, Meng
Yuan, Hong
Chen, Dong-Dong
Li, Kun
Chen, Ying-Li
Cao, Yi-Mei
Fu, Yuan-Fang
Zhang, Jing
Li, Dong
Lu, Zeng-Jun
Liu, Zai-Xin
Luo, Jian-Xun
author_sort Bai, Xing-Wen
collection PubMed
description The presence of sequence divergence through adaptive mutations in the major capsid protein VP1, and also in VP0 (VP4 and VP2) and VP3, of foot-and-mouth disease virus (FMDV) is relevant to a broad range of viral characteristics. To explore the potential role of isolate-specific residues in the VP0 and VP3 coding regions of PanAsia-1 strains in genetic and phenotypic properties of FMDV, a series of recombinant full-length genomic clones were constructed using Cathay topotype infectious cDNA as the original backbone. The deleterious and compensatory effects of individual amino acid substitutions at positions 4008 and 3060 and in several different domains of VP2 illustrated that the chain-based spatial interaction patterns of VP1, VP2, and VP3 (VP1-3), as well as between the internal VP4 and the three external capsid proteins of FMDV, might contribute to the assembly of eventually viable viruses. The Y2079H site-directed mutants dramatically induced a decrease in plaque size on BHK-21 cells and viral pathogenicity in suckling mice. Remarkably, the 2079H-encoding viruses displayed a moderate increase in acid sensitivity correlated with NH(4)Cl resistance compared to the Y2079-encoding viruses. Interestingly, none of all the 16 rescued viruses were able to infect heparan sulfate-expressing CHO-K1 cells. However, viral infection in BHK-21 cells was facilitated by utilizing non-integrin-dependent, heparin-sensitive receptor(s) and replacements of four uncharged amino acids at position 3174 in VP3 of FMDV had no apparent influence on heparin affinity. These results provide particular insights into the correlation of evolutionary biology with genetic diversity in adapting populations of FMDV. IMPORTANCE The sequence variation within the capsid proteins occurs frequently in the infection of susceptible tissue cultures, reflecting the high levels of genetic diversity of FMDV. A systematic study for the functional significance of isolate-specific residues in VP0 and VP3 of FMDV PanAsia-1 strains suggested that the interaction of amino acid side chains between the N terminus of VP4 and several potential domains of VP1-3 had cascading effects on the viability and developmental characteristics of progeny viruses. Y2079H in VP0 of the indicated FMDVs could affect plaque size and pathogenicity, as well as acid sensitivity correlated with NH(4)Cl resistance, whereas there was no inevitable correlation in viral plaque and acid-sensitive phenotypes. The high affinity of non-integrin-dependent FMDVs for heparin might be explained by the differences in structures of heparan sulfate proteoglycans on the surfaces of different cell lines. These results may contribute to our understanding of the distinct phenotypic properties of FMDV in vitro and in vivo.
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spelling pubmed-64305512019-04-12 Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O Bai, Xing-Wen Bao, Hui-Fang Li, Ping-Hua Ma, Xue-Qing Sun, Pu Bai, Qi-Feng Zhang, Meng Yuan, Hong Chen, Dong-Dong Li, Kun Chen, Ying-Li Cao, Yi-Mei Fu, Yuan-Fang Zhang, Jing Li, Dong Lu, Zeng-Jun Liu, Zai-Xin Luo, Jian-Xun J Virol Virus-Cell Interactions The presence of sequence divergence through adaptive mutations in the major capsid protein VP1, and also in VP0 (VP4 and VP2) and VP3, of foot-and-mouth disease virus (FMDV) is relevant to a broad range of viral characteristics. To explore the potential role of isolate-specific residues in the VP0 and VP3 coding regions of PanAsia-1 strains in genetic and phenotypic properties of FMDV, a series of recombinant full-length genomic clones were constructed using Cathay topotype infectious cDNA as the original backbone. The deleterious and compensatory effects of individual amino acid substitutions at positions 4008 and 3060 and in several different domains of VP2 illustrated that the chain-based spatial interaction patterns of VP1, VP2, and VP3 (VP1-3), as well as between the internal VP4 and the three external capsid proteins of FMDV, might contribute to the assembly of eventually viable viruses. The Y2079H site-directed mutants dramatically induced a decrease in plaque size on BHK-21 cells and viral pathogenicity in suckling mice. Remarkably, the 2079H-encoding viruses displayed a moderate increase in acid sensitivity correlated with NH(4)Cl resistance compared to the Y2079-encoding viruses. Interestingly, none of all the 16 rescued viruses were able to infect heparan sulfate-expressing CHO-K1 cells. However, viral infection in BHK-21 cells was facilitated by utilizing non-integrin-dependent, heparin-sensitive receptor(s) and replacements of four uncharged amino acids at position 3174 in VP3 of FMDV had no apparent influence on heparin affinity. These results provide particular insights into the correlation of evolutionary biology with genetic diversity in adapting populations of FMDV. IMPORTANCE The sequence variation within the capsid proteins occurs frequently in the infection of susceptible tissue cultures, reflecting the high levels of genetic diversity of FMDV. A systematic study for the functional significance of isolate-specific residues in VP0 and VP3 of FMDV PanAsia-1 strains suggested that the interaction of amino acid side chains between the N terminus of VP4 and several potential domains of VP1-3 had cascading effects on the viability and developmental characteristics of progeny viruses. Y2079H in VP0 of the indicated FMDVs could affect plaque size and pathogenicity, as well as acid sensitivity correlated with NH(4)Cl resistance, whereas there was no inevitable correlation in viral plaque and acid-sensitive phenotypes. The high affinity of non-integrin-dependent FMDVs for heparin might be explained by the differences in structures of heparan sulfate proteoglycans on the surfaces of different cell lines. These results may contribute to our understanding of the distinct phenotypic properties of FMDV in vitro and in vivo. American Society for Microbiology 2019-03-21 /pmc/articles/PMC6430551/ /pubmed/30700601 http://dx.doi.org/10.1128/JVI.02278-18 Text en Copyright © 2019 Bai 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 Virus-Cell Interactions
Bai, Xing-Wen
Bao, Hui-Fang
Li, Ping-Hua
Ma, Xue-Qing
Sun, Pu
Bai, Qi-Feng
Zhang, Meng
Yuan, Hong
Chen, Dong-Dong
Li, Kun
Chen, Ying-Li
Cao, Yi-Mei
Fu, Yuan-Fang
Zhang, Jing
Li, Dong
Lu, Zeng-Jun
Liu, Zai-Xin
Luo, Jian-Xun
Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O
title Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O
title_full Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O
title_fullStr Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O
title_full_unstemmed Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O
title_short Engineering Responses to Amino Acid Substitutions in the VP0- and VP3-Coding Regions of PanAsia-1 Strains of Foot-and-Mouth Disease Virus Serotype O
title_sort engineering responses to amino acid substitutions in the vp0- and vp3-coding regions of panasia-1 strains of foot-and-mouth disease virus serotype o
topic Virus-Cell Interactions
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6430551/
https://www.ncbi.nlm.nih.gov/pubmed/30700601
http://dx.doi.org/10.1128/JVI.02278-18
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