Abstract

Coxsackievirus A8 (CV-A8) is one of the pathogens associated with hand, foot and mouth disease (HFMD) and herpangina (HA), occasionally leading to severe neurological disorders such as acute flaccid paralysis (AFP). Only one study aimed at CV-A8 has been published to date, and only 12 whole-genome sequences are publicly available. In this study, complete genome sequences from 11 CV-A8 strains isolated from HFMD patients in extensive regions from China between 2013 and 2018 were determined, and all sequences from GenBank were retrieved. A phylogenetic analysis based on a total of 34 complete VP1 sequences of CV-A8 revealed five genotypes: A, B, C, D and E. The newly emerging genotype E presented a highly phylogenetic divergence compared with the other genotypes and was composed of the majority of the strains sequenced in this study. Markov chain Monte Carlo (MCMC) analysis revealed that genotype E has been evolving for nearly a century and somehow arose in approximately 2010. The Bayesian skyline plot showed that the population size of CV-A8 has experienced three dynamic fluctuations since 2001. Amino acid residues of VP1100N, 103Y, 240T and 241V, which were embedded in the potential capsid loops of genotype E, might enhance genotype E adaption to the human hosts. The CV-A8 whole genomes displayed significant intra-genotypic genetic diversity in the non-capsid region, and a total of six recombinant lineages were detected. The Chinese viruses from genotype E might have emerged recently from recombining with European CV-A6 strains. CV-A8 is a less important HFMD pathogen, and the capsid gene diversity and non-capsid recombination variety observed in CV-A8 strains indicated that the constant generation of deleterious genomes and a constant selection pressure against these deleterious mutations is still ongoing within CV-A8 quasispecies. It is possible that CV-A8 could become an important pathogen in the HFMD spectrum in the future. Further surveillance of CV-A8 is greatly needed.

Highlights

  • Human enteroviruses (EVs) are genetically diverse RNA viruses belonging to the genus Enterovirus and family Picornaviridae

  • As millions of HFMD-related cases and repeated HFMD outbreaks across China were reported in the past decade, an extensive three-level HFMD surveillance laboratory network including one national lab, 31 provincial labs and 331 prefectural labs was established in China since

  • Eleven Coxsackievirus A8 (CV-A8) strains isolated since 2008 from China were contributed by this study

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Summary

Introduction

Human enteroviruses (EVs) are genetically diverse RNA viruses belonging to the genus Enterovirus and family Picornaviridae. There are currently over 100 designated human EVs that are classified into. Viruses 2020, 12, 1061 four species: EV-A to -D. The EV-A species currently consists of 25 serotypes, including coxsackievirus. Similar to all EVs, CV-A8 is a small, non-enveloped, single stranded, positive-sense. The genome, which has approximately 7400 nucleotides (nt), contains a long open reading frame (ORF) flanked by a 50 -untranslated region (UTR) and a 30 -UTR. The ORF can be translated into a 2,189-amino acid-long polyprotein and cleaved into the three polyprotein precursors P1, P2, and P3, which encode the structural proteins VP4, VP2, VP3, and VP1, and the nonstructural proteins

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