4.6 Article

The Importance of Intergenic Recombination in Norovirus GII.3 Evolution

Journal

JOURNAL OF VIROLOGY
Volume 87, Issue 7, Pages 3687-3698

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/JVI.03056-12

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Funding

  1. Victorian Government's Operational Infrastructure Support Program
  2. Intramural Research Program of the NIH, NIAID

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Norovirus genotype II.3 (GII.3) strains are a major cause of sporadic gastroenteritis. Intergenic recombination between the capsid and RNA-dependent RNA polymerase (RdRp) genes is common and results in the acquisition of an alternative RdRp genotype. This study aimed to explore the evolution of the GII. 3 capsid gene, focusing on the influence of intergenic recombination. The capsid genes from six GII. 3 norovirus strains, collected from Australian children between 2001 and 2010, were sequenced and aligned with 66 GII. 3 capsid sequences from GenBank, spanning 1975 to 2010. The GII. 3 capsid gene evolved at a rate of 4.16 x 10(-3) to 6.97 x 10(-3) nucleotide substitutions/site/year from 1975 to 2010 and clustered into five temporally sequential lineages. Clustering of the GII. 3 capsid gene sequences was associated with intergenic recombination and switches between RdRp genotypes GII.3, GII.a, GII.b, GII.12, and an undefined ancestral RdRp. Comparison of the substitution rate of the GII. 3 and GII.b RdRps suggested that RdRp switching allows a higher evolutionary rate, leading to increased genetic diversity and adaptability. Alignment of GII. 3 capsid sequences revealed 36 lineage-specific conserved amino acid substitutions, four of which were under positive selection. Many conserved substitutions were within predicted antibody binding regions and close to host attachment factor binding sites. In conclusion, evolution of GII. 3 noroviruses was primarily driven by intergenic recombination. The acquisition of new RdRps may lead to a faster mutation rate and increased genetic diversity, improving overall GII. 3 fitness.

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