Key Amino Acids of M1-41 and M2-27 Determine Growth and Pathogenicity of Chimeric H17 Bat Influenza Virus in Cells and in Mice

Jianmei Yang; Pei Zhang; Min Huang; Shuyuan Qiao; Qinfang Liu; Hongjun Chen; Qiaoyang Teng; Xuesong Li; Zhifei Zhang; Dawei Yan; Haiwei Sun; Zejun Li

doi:10.1128/JVI.01019-21

Key Amino Acids of M1-41 and M2-27 Determine Growth and Pathogenicity of Chimeric H17 Bat Influenza Virus in Cells and in Mice

J Virol. 2021 Sep 9;95(19):e0101921. doi: 10.1128/JVI.01019-21. Epub 2021 Sep 9.

Authors

Jianmei Yang^{1

2}, Pei Zhang¹, Min Huang¹, Shuyuan Qiao¹, Qinfang Liu^{1

2}, Hongjun Chen¹, Qiaoyang Teng^{1

2}, Xuesong Li^{1

2}, Zhifei Zhang², Dawei Yan^{1

2}, Haiwei Sun¹, Zejun Li^{1

2}

Affiliations

¹ Shanghai Veterinary Research Institutegrid.464410.3, Chinese Academy of Agricultural Sciences, Shanghai, China.
² Animal Influenza and Emerging Avian Viral Diseases Innovation Team, Shanghai, China.

Abstract

Based on our previous studies, we show that the M gene is critical for the replication and pathogenicity of the chimeric H17 bat influenza virus (Bat09:mH1mN1) by replacing the bat M gene with those from human and swine influenza A viruses. However, the key amino acids of the M1 and/or M2 proteins that are responsible for virus replication and pathogenicity remain unknown. In this study, replacement of the PR8 M gene with the Eurasian avian-like M gene from the A/California/04/2009 pandemic H1N1 virus significantly decreased viral replication in both mammalian and avian cells in the background of the chimeric H17 bat influenza virus. Further studies revealed that M1 was more crucial for viral growth and pathogenicity than M2 and that the amino acid residues M1-41V and M2-27A were responsible for these characteristics in cells and in mice. These key residues of the M1 and M2 proteins identified in this study might be important for influenza virus surveillance and could be used to produce live attenuated vaccines in the future. IMPORTANCE The M1 and M2 proteins influence the morphology, replication, virulence, and transmissibility of influenza viruses. Although a few key residues in the M1 and M2 proteins have been identified, whether other residues of the M1 and M2 proteins are involved in viral replication and pathogenicity remains to be discovered. In the background of the chimeric H17 bat influenza virus, the Eurasian avian-like M gene from the A/California/04/2009 virus significantly decreased viral growth in mammalian and avian cells. Further study showed that M1 was implicated more than M2 in viral growth and pathogenicity in vitro and in vivo and that the key amino acid residues M1-41V and M2-27A were responsible for these characteristics in cells and in mice. These key residues of the M1 and M2 proteins could be used for influenza virus surveillance and live attenuated vaccine applications in the future. These findings provide important contributions to knowledge of the genetic basis of the virulence of influenza viruses.

Keywords: M1; M2; chimeric bat influenza virus; key amino acids; pathogenicity; viral growth.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amino Acids / metabolism
Animals
Cell Line
Chiroptera
Genes, Viral
Humans
Influenza A Virus, H1N1 Subtype / genetics*
Lung / virology
Mice
Orthomyxoviridae / genetics
Orthomyxoviridae / growth & development*
Orthomyxoviridae / pathogenicity*
Orthomyxoviridae Infections / virology*
Reassortant Viruses / genetics
Reassortant Viruses / growth & development
Reassortant Viruses / pathogenicity
Turbinates / virology
Viral Matrix Proteins / chemistry
Viral Matrix Proteins / genetics
Viral Matrix Proteins / metabolism*
Virulence
Virus Replication

Substances

Amino Acids
M1 protein, Influenza A virus
M2 protein, Influenza A virus
Viral Matrix Proteins

Abstract

Publication types

MeSH terms

Substances

Grants and funding