Visualizing Viral RNA Packaging Signals in Action

doi:10.1016/j.jmb.2024.168765

Journal of Molecular Biology

Volume 436, Issue 22, 15 November 2024, 168765

https://doi.org/10.1016/j.jmb.2024.168765 Get rights and content

Under a Creative Commons license

Open access

Highlights

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CPs make sequence-specific contacts to putative PSs in only the 5ʹ 2/3^rds of the gRNA.
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Only the positive-sense strand carries PSs, triggering virion assembly at low CP concentrations.
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PSs also trigger association of CPs into trimers non-sequence-specifically.
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Variation in PS-CP affinities along the gRNA regulates release of the 3ʹ end first during infection.
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Viral ssRNA genomes play multiple roles in virion formation and cellular infection.

Abstract

Here we confirm, using genome-scale RNA fragments in assembly competition assays, that multiple sub-sites (Packaging Signals, PSs) across the 5′ two-thirds of the gRNA of Satellite Tobacco Necrosis Virus-1 make sequence-specific contacts to the viral CPs helping to nucleate formation of its T = 1 virus-like particle (VLP). These contacts explain why natural virions only package their positive-sense genomes. Asymmetric cryo-EM reconstructions of these VLPs suggest that interactions occur between amino acid residues in the N-terminal ends of the CP subunits and the gRNA PS loop sequences. The base-paired stems of PSs also act non-sequence-specifically by electrostatically promoting the assembly of CP trimers. Importantly, alterations in PS-CP affinity result in an asymmetric distribution of bound PSs inside VLPs, with fuller occupation of the higher affinity 5′ PS RNAs around one vertex, decreasing to an RNA-free opposite vertex within the VLP shell. This distribution suggests that gRNA folding regulates cytoplasmic genome extrusion so that the weakly bound 3′ end of the gRNA, containing the RNA polymerase binding site, extrudes first. This probably occurs after cation-loss induced swelling of the CP-shell, weakening contacts between CP subunits. These data reveal for the first time in any virus how differential PS folding propensity and CP affinities support the multiple roles genomes play in virion assembly and infection. The high degree of conservation between the CP fold of STNV-1 and those of the CPs of many other viruses suggests that these aspects of genome function will be widely shared.

Graphical abstract

Keywords

virus assembly

genome regulated virus assembly and infection

packaging signals

molecular frustration

Data availability

Data will be made available on request.

Cited by (0)

^†: These authors contributed equally to the manuscript.

^‡: Current address: CPM: Biocomputing Unit, Department of Macromolecular Structures, National Centre for Biotechnology (CNB-CSIC), Darwin, 3 28049, Madrid, Spain.

^§: Current address: Diamond Light Source Ltd., Diamond House, Harwell Science & Innovation Campus, Didcot, Oxfordshire, OX11 0DE, United Kingdom.

^||: Current address: Coriolis Pharma Research GmbH, Fraunhoferstr. 18 b, 82152 Martinsried, Germany.

^¶: Current address: South View, Park Road, Combe, OX29 8NA, United Kingdom.