T135I substitution in the nonstructural protein 2C enhances foot-and-mouth disease virus replication

Tiangang Yuan; Haiwei Wang; Chen Li; Decheng Yang; Guohui Zhou; Li Yu

doi:10.1007/s11262-017-1480-9

T135I substitution in the nonstructural protein 2C enhances foot-and-mouth disease virus replication

Virus Genes. 2017 Dec;53(6):840-847. doi: 10.1007/s11262-017-1480-9. Epub 2017 Jun 20.

Authors

Tiangang Yuan¹, Haiwei Wang², Chen Li¹, Decheng Yang¹, Guohui Zhou¹, Li Yu³

Affiliations

¹ Division of Livestock Infectious Diseases, State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, No. 678 Haping Road, Xiangfang District, Harbin, 150069, People's Republic of China.
² Division of Livestock Infectious Diseases, State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, No. 678 Haping Road, Xiangfang District, Harbin, 150069, People's Republic of China. whw3791@163.com.
³ Division of Livestock Infectious Diseases, State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, No. 678 Haping Road, Xiangfang District, Harbin, 150069, People's Republic of China. liyu@hvri.ac.cn.

PMID: 28634750
DOI: 10.1007/s11262-017-1480-9

Abstract

The foot-and-mouth disease virus (FMDV) nonstructural protein 3A plays an important role in viral replication, virulence, and host range. It has been shown that deletions of 10 or 19-20 amino acids in the C-terminal half of 3A attenuate serotype O and C FMDVs, which replicate poorly in bovine cells but normally in porcine-derived cells, and the C-terminal half of 3A is not essential for serotype Asia1 FMDV replication in BHK-21 cells. In this study, we constructed a 3A deletion FMDV mutant based on a serotype O FMDV, the wild-type virus O/YS/CHA/05, with a 60-amino acid deletion in the 3A protein sequence, between residues 84 and 143. The rescued virus O/YS/CHA/05-Δ3A exhibited slower growth kinetics and formed smaller plaques compared to O/YS/CHA/05 in both BHK-21 and IBRS-2 cells, indicating that the 60-amino acid deletion in the 3A protein impaired FMDV replication. After 14 passages in BHK-21 cells, the replication capacity of the passaged virus O/YS/CHA/05-Δ3A-P14 returned to a level similar to the wild-type virus, suggesting that amino acid substitutions responsible for the enhanced replication capacity occurred in the genome of O/YS/CHA/05-Δ3A-P14. By sequence analysis, two amino acid substitutions, P153L in VP1 and T135I in 2C, were found in the O/YS/CHA/05-Δ3A-P14 genome compared to the O/YS/CHA/05-Δ3A genome. Subsequently, the amino acid substitutions VP1 P153L and 2C T135I were separately introduced into O/YS/CHA/05-Δ3A to rescue mutant viruses for examining their growth kinetics. Results showed that the 2C T135I instead of the VP1 P153L enhanced the virus replication capacity. The 2C T135I substitution also improved the replication of the wild-type virus, indicating that the effect of 2C T135I substitution on FMDV replication is not associated with the 3A deletion. Furthermore, our results showed that the T135I substitution in the nonstructural protein 2C enhanced O/YS/CHA/05 replication through promoting viral RNA synthesis.

Keywords: Foot-and-mouth disease virus; Mutations and growth kinetics; RNA synthesis; Virus replication.

MeSH terms

Amino Acid Substitution / genetics
Animals
Cell Line
Cricetinae
DNA Replication / genetics
Foot-and-Mouth Disease / virology
Foot-and-Mouth Disease Virus / genetics*
Host Specificity / genetics
Sequence Deletion / genetics
Swine
Viral Nonstructural Proteins / genetics*
Viral Proteins / genetics*
Virulence / genetics
Virus Replication / genetics*

Substances

Viral Nonstructural Proteins
Viral Proteins

Abstract

MeSH terms

Substances

Grants and funding