Evolutionary Dynamics and Temporal/Geographical Correlates of Recombination in the Human Enterovirus Echovirus Types 9, 11, and 30

Author:

McWilliam Leitch E. C.1,Cabrerizo M.2,Cardosa J.3,Harvala H.4,Ivanova O. E.5,Kroes A. C. M.6,Lukashev A.5,Muir P.7,Odoom J.8,Roivainen M.9,Susi P.10,Trallero G.2,Evans D. J.11,Simmonds P.1

Affiliation:

1. Centre for Infectious Diseases, University of Edinburgh, Summerhall, Edinburgh EH9 1QH, United Kingdom

2. Enterovirus Laboratory, National Centre for Microbiology, Carlos III Institute of Health, Majadahonda, Madrid, Spain

3. Institute of Health and Community Medicine, University Sarawak Malaysia, Sarawak, Malaysia

4. Specialist Virology Centre, Royal Infirmary of Edinburgh, Edinburgh, United Kingdom

5. M. P. Chumakov Institute of Poliomyelitis and Viral Encephalitides, Moscow, Russia

6. Department of Medical Microbiology, Leiden University Medical Centre, Leiden, Netherlands

7. HPA South West Regional Laboratory, Bristol, United Kingdom

8. Department of Virology, Noguchi Memorial Institute for Medical Research, University of Ghana, Legon, Accra, Ghana

9. Intestinal Viruses Unit, National Institute for Health and Welfare, Helsinki, Finland

10. Department of Virology, University of Turku, Turku, Finland

11. Department of Biological Sciences, University of Warwick, Warwick, United Kingdom

Abstract

ABSTRACT The relationship between virus evolution and recombination in species B human enteroviruses was investigated through large-scale genetic analysis of echovirus type 9 (E9) and E11 isolates ( n = 85 and 116) from 16 European, African, and Asian countries between 1995 and 2008. Cluster 1 E9 isolates and genotype D5 and A E11 isolates showed evidence of frequent recombination between the VP1 and 3Dpol regions, the latter falling into 23 (E9) and 43 (E11) clades interspersed phylogenetically with 46 3Dpol clades of E30 and with those of other species B serotypes. Remarkably, only 2 of the 112 3Dpol clades were shared by more than one serotype (E11 and E30), demonstrating an extremely large and genetically heterogeneous recombination pool of species B nonstructural-region variants. The likelihood of recombination increased with geographical separation and time, and both were correlated with VP1 divergence, whose substitution rates allowed recombination half-lives of 1.3, 9.8, and 3.1 years, respectively, for E9, E11, and E30 to be calculated. These marked differences in recombination dynamics matched epidemiological patterns of periodic epidemic cycles of 2 to 3 (E9) and 5 to 6 (E30) years and the longer-term endemic pattern of E11 infections. Phylotemporal analysis using a Bayesian Markov chain Monte Carlo method, which placed recombination events within the evolutionary reconstruction of VP1, showed a close relationship with VP1 lineage expansion, with defined recombination events that correlated with their epidemiological periodicity. Whether recombination events contribute directly to changes in transmissibility that drive epidemic behavior or occur stochastically during periodic population bottlenecks is an unresolved issue vital to future understanding of enterovirus molecular epidemiology and pathogenesis.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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