Common and Diverse Features of Cocirculating Type 2 and 3 Recombinant Vaccine-derived Polioviruses Isolated from Patients with Poliomyelitis and Healthy Children

Overview

Journal J Infect Dis

Publisher Oxford University Press

Specialty Infectious Diseases

Date 2012 Mar 30

PMID 22457288

Citations 24

Authors

Marie-Line Joffret

Sophie Jegouic

Mael Bessaud

Jean Balanant

Coralie Tran

Valerie Caro

Barbara Holmblat

Richter Razafindratsimandresy

Jean-Marc Reynes

Mala Rakoto-Andrianarivelo

Francis Delpeyroux

Affiliations

Soon will be listed here.

Abstract

Background: Five cases of poliomyelitis due to type 2 or 3 recombinant vaccine-derived polioviruses (VDPVs) were reported in the Toliara province of Madagascar in 2005.

Methods: We sequenced the genome of the VDPVs isolated from the patients and from 12 healthy children and characterized phenotypic aspects, including pathogenicity, in mice transgenic for the poliovirus receptor.

Results: We identified 6 highly complex mosaic recombinant lineages composed of sequences derived from different vaccine polioviruses and other species C human enteroviruses (HEV-Cs). Most had some recombinant genome features in common and contained nucleotide sequences closely related to certain cocirculating coxsackie A virus isolates. However, they differed in terms of their recombinant characteristics or nucleotide substitutions and phenotypic features. All VDPVs were neurovirulent in mice.

Conclusions: This study confirms the genetic relationship between type 2 and 3 VDPVs, indicating that both types can be involved in a single outbreak of disease. Our results highlight the various ways in which a vaccine-derived poliovirus may become pathogenic in complex viral ecosystems, through frequent recombination events and mutations. Intertypic recombination between cocirculating HEV-Cs (including polioviruses) appears to be a common mechanism of genetic plasticity underlying transverse genetic variability.

Citing Articles

Recombination in Enteroviruses, a Multi-Step Modular Evolutionary Process.

Muslin C, Mac Kain A, Bessaud M, Blondel B, Delpeyroux F Viruses. 2019; 11(9).

PMID: 31540135 PMC: 6784155. DOI: 10.3390/v11090859.

Genetic landscape and macro-evolution of co-circulating Coxsackieviruses A and Vaccine-derived Polioviruses in the Democratic Republic of Congo, 2008-2013.

Sadeuh-Mba S, Kavunga-Membo H, Joffret M, Yogolelo R, Endegue-Zanga M, Bessaud M PLoS Negl Trop Dis. 2019; 13(4):e0007335.

PMID: 31002713 PMC: 6505894. DOI: 10.1371/journal.pntd.0007335.

High Permissiveness for Genetic Exchanges between Enteroviruses of Species A, including Enterovirus 71, Favors Evolution through Intertypic Recombination in Madagascar.

Volle R, Razafindratsimandresy R, Joffret M, Bessaud M, Rabemanantsoa S, Andriamamonjy S J Virol. 2019; 93(6).

PMID: 30602612 PMC: 6401452. DOI: 10.1128/JVI.01667-18.

Pediatric HIV Infection and Decreased Prevalence of OPV Point Mutations Linked to Vaccine-associated Paralytic Poliomyelitis.

Halpern M, Altamirano J, Maldonado Y Clin Infect Dis. 2018; 67(suppl_1):S78-S84.

PMID: 30376083 PMC: 6206102. DOI: 10.1093/cid/ciy635.

Whole Genome Sequencing of Enteroviruses Species A to D by High-Throughput Sequencing: Application for Viral Mixtures.

Joffret M, Polston P, Razafindratsimandresy R, Bessaud M, Heraud J, Delpeyroux F Front Microbiol. 2018; 9:2339.

PMID: 30323802 PMC: 6172331. DOI: 10.3389/fmicb.2018.02339.