Genomic RNA folding mediates assembly of human parechovirus

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作者
Shabih Shakeel
Eric C. Dykeman
Simon J. White
Ari Ora
Joseph J.B. Cockburn
Sarah J. Butcher
Peter G. Stockley
Reidun Twarock
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[1] University of Helsinki,Institute of Biotechnology and Department of Biosciences
[2] University of York,Departments of Mathematics and Biology and York Centre for Complex Systems Analysis
[3] University of Leeds,Astbury Centre for Structural Molecular Biology
[4] Aalto University,Department of Applied Physics and Department of Biotechnology and Chemical Technology
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Assembly of the major viral pathogens of the Picornaviridae family is poorly understood. Human parechovirus 1 is an example of such viruses that contains 60 short regions of ordered RNA density making identical contacts with the protein shell. We show here via a combination of RNA-based systematic evolution of ligands by exponential enrichment, bioinformatics analysis and reverse genetics that these RNA segments are bound to the coat proteins in a sequence-specific manner. Disruption of either the RNA coat protein recognition motif or its contact amino acid residues is deleterious for viral assembly. The data are consistent with RNA packaging signals playing essential roles in virion assembly. Their binding sites on the coat proteins are evolutionarily conserved across the Parechovirus genus, suggesting that they represent potential broad-spectrum anti-viral targets.
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