Imprecise recombinant viruses evolve via a fitness-driven,iterative process of polymerase template-switching events |
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Authors: | Kirsten Bentley,Fadi Ghassan Alnaji,Luke Woodford,Siâ n Jones,Andrew Woodman,David J. Evans |
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Affiliation: | 1. BSRC and School of Biology, University of St Andrews, St Andrews, United Kingdom ; 2. Department of Microbiology, University of Illinois, Champaign-Urbana, Illinois, United States of America ; 3. Department of Biochemistry and Molecular Biology, Pennsylvania State University, Pennsylvania, United States of America ; University of Maryland, UNITED STATES |
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Abstract: | Recombination is a common feature of many positive-strand RNA viruses, playing an important role in virus evolution. However, to date, there is limited understanding of the mechanisms behind the process. Utilising in vitro assays, we have previously shown that the template-switching event of recombination is a random and ubiquitous process that often leads to recombinant viruses with imprecise genomes containing sequence duplications. Subsequently, a process termed resolution, that has yet to be mechanistically studied, removes these duplicated sequences resulting in a virus population of wild type length genomes. Using defined imprecise recombinant viruses together with Oxford Nanopore and Illumina high throughput next generation sequencing technologies we have investigated the process of resolution. We show that genome resolution involves subsequent rounds of template-switching recombination with viral fitness resulting in the survival of a small subset of recombinant genomes. This alters our previously held understanding that recombination and resolution are independent steps of the process, and instead demonstrates that viruses undergo frequent and continuous recombination events over a prolonged period until the fittest viruses, predominantly those with wild type length genomes, dominate the population. |
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