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Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism

The formation of a protective protein container is an essential step in the life-cycle of most viruses. In the case of single-stranded (ss)RNA viruses, this step occurs in parallel with genome packaging in a co-assembly process. Previously, it had been thought that this process can be explained enti...

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Autores principales: Stockley, Peter G., Twarock, Reidun, Bakker, Saskia E., Barker, Amy M., Borodavka, Alexander, Dykeman, Eric, Ford, Robert J., Pearson, Arwen R., Phillips, Simon E. V., Ranson, Neil A., Tuma, Roman
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Netherlands 2013
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3662417/
https://www.ncbi.nlm.nih.gov/pubmed/23704797
http://dx.doi.org/10.1007/s10867-013-9313-0
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author Stockley, Peter G.
Twarock, Reidun
Bakker, Saskia E.
Barker, Amy M.
Borodavka, Alexander
Dykeman, Eric
Ford, Robert J.
Pearson, Arwen R.
Phillips, Simon E. V.
Ranson, Neil A.
Tuma, Roman
author_facet Stockley, Peter G.
Twarock, Reidun
Bakker, Saskia E.
Barker, Amy M.
Borodavka, Alexander
Dykeman, Eric
Ford, Robert J.
Pearson, Arwen R.
Phillips, Simon E. V.
Ranson, Neil A.
Tuma, Roman
author_sort Stockley, Peter G.
collection PubMed
description The formation of a protective protein container is an essential step in the life-cycle of most viruses. In the case of single-stranded (ss)RNA viruses, this step occurs in parallel with genome packaging in a co-assembly process. Previously, it had been thought that this process can be explained entirely by electrostatics. Inspired by recent single-molecule fluorescence experiments that recapitulate the RNA packaging specificity seen in vivo for two model viruses, we present an alternative theory, which recognizes the important cooperative roles played by RNA–coat protein interactions, at sites we have termed packaging signals. The hypothesis is that multiple copies of packaging signals, repeated according to capsid symmetry, aid formation of the required capsid protein conformers at defined positions, resulting in significantly enhanced assembly efficiency. The precise mechanistic roles of packaging signal interactions may vary between viruses, as we have demonstrated for MS2 and STNV. We quantify the impact of packaging signals on capsid assembly efficiency using a dodecahedral model system, showing that heterogeneous affinity distributions of packaging signals for capsid protein out-compete those of homogeneous affinities. These insights pave the way to a new anti-viral therapy, reducing capsid assembly efficiency by targeting of the vital roles of the packaging signals, and opens up new avenues for the efficient construction of protein nanocontainers in bionanotechnology.
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spelling pubmed-36624172013-05-23 Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism Stockley, Peter G. Twarock, Reidun Bakker, Saskia E. Barker, Amy M. Borodavka, Alexander Dykeman, Eric Ford, Robert J. Pearson, Arwen R. Phillips, Simon E. V. Ranson, Neil A. Tuma, Roman J Biol Phys Original Paper The formation of a protective protein container is an essential step in the life-cycle of most viruses. In the case of single-stranded (ss)RNA viruses, this step occurs in parallel with genome packaging in a co-assembly process. Previously, it had been thought that this process can be explained entirely by electrostatics. Inspired by recent single-molecule fluorescence experiments that recapitulate the RNA packaging specificity seen in vivo for two model viruses, we present an alternative theory, which recognizes the important cooperative roles played by RNA–coat protein interactions, at sites we have termed packaging signals. The hypothesis is that multiple copies of packaging signals, repeated according to capsid symmetry, aid formation of the required capsid protein conformers at defined positions, resulting in significantly enhanced assembly efficiency. The precise mechanistic roles of packaging signal interactions may vary between viruses, as we have demonstrated for MS2 and STNV. We quantify the impact of packaging signals on capsid assembly efficiency using a dodecahedral model system, showing that heterogeneous affinity distributions of packaging signals for capsid protein out-compete those of homogeneous affinities. These insights pave the way to a new anti-viral therapy, reducing capsid assembly efficiency by targeting of the vital roles of the packaging signals, and opens up new avenues for the efficient construction of protein nanocontainers in bionanotechnology. Springer Netherlands 2013-04-12 2013-03 /pmc/articles/PMC3662417/ /pubmed/23704797 http://dx.doi.org/10.1007/s10867-013-9313-0 Text en © The Author(s) 2013 https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License which permits any use, distribution, and reproduction in any medium, provided the original author(s) and the source are credited.
spellingShingle Original Paper
Stockley, Peter G.
Twarock, Reidun
Bakker, Saskia E.
Barker, Amy M.
Borodavka, Alexander
Dykeman, Eric
Ford, Robert J.
Pearson, Arwen R.
Phillips, Simon E. V.
Ranson, Neil A.
Tuma, Roman
Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism
title Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism
title_full Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism
title_fullStr Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism
title_full_unstemmed Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism
title_short Packaging signals in single-stranded RNA viruses: nature’s alternative to a purely electrostatic assembly mechanism
title_sort packaging signals in single-stranded rna viruses: nature’s alternative to a purely electrostatic assembly mechanism
topic Original Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3662417/
https://www.ncbi.nlm.nih.gov/pubmed/23704797
http://dx.doi.org/10.1007/s10867-013-9313-0
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