Abstract

The genomes of plus-strand RNA viruses contain many regulatory sequences and structures that direct different viral processes. The traditional view of these RNA elements are as local structures present in non-coding regions. However, this view is changing due to the discovery of regulatory elements in coding regions and functional long-range intra-genomic base pairing interactions. The ∼4.8 kb long RNA genome of the tombusvirus tomato bushy stunt virus (TBSV) contains these types of structural features, including six different functional long-distance interactions. We hypothesized that to achieve these multiple interactions this viral genome must utilize a large-scale organizational strategy and, accordingly, we sought to assess the global conformation of the entire TBSV genome. Atomic force micrographs of the genome indicated a mostly condensed structure composed of interconnected protrusions extending from a central hub. This configuration was consistent with the genomic secondary structure model generated using high-throughput selective 2′-hydroxyl acylation analysed by primer extension (i.e. SHAPE), which predicted different sized RNA domains originating from a central region. Known RNA elements were identified in both domain and inter-domain regions, and novel structural features were predicted and functionally confirmed. Interestingly, only two of the six long-range interactions known to form were present in the structural model. However, for those interactions that did not form, complementary partner sequences were positioned relatively close to each other in the structure, suggesting that the secondary structure level of viral genome structure could provide a basic scaffold for the formation of different long-range interactions. The higher-order structural model for the TBSV RNA genome provides a snapshot of the complex framework that allows multiple functional components to operate in concert within a confined context.

Highlights

  • Many viruses possess RNA genomes, and those with singlestranded plus-sense RNA genomes represent an important subgroup that includes many pathogenic plant, animal, and human viruses

  • What was evident from the atomic force microscopy (AFM) analysis was the general conservation of a global organization consisting of irregular extensions emanating from a central core (Figure 2). Some variation from this overall arrangement was evident, but the level of compactness and the presence of multiple tethered substructures were typically maintained. These results suggest that the tomato bushy stunt virus (TBSV) genome assumes a mostly condensed structure that is composed of interconnected domain-like protrusions extending from a central hub

  • The current structural model provides a context to begin to understand the organization of local structures and long-range RNA-RNA interactions within the TBSV genome

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Summary

Introduction

Many viruses possess RNA genomes, and those with singlestranded plus-sense RNA genomes represent an important subgroup that includes many pathogenic plant, animal, and human viruses. Many viruses use this strategy by situating their REs terminally in 59- and 39-untranslated regions (UTRs) or/and internally within inter-cistronic regions [1,3] One drawback to this approach is that the size and/or location of the non-coding regions can be limiting. One strategy used by many RNA viruses to deal with suboptimally positioned REs is to reorganize their relative location within the genome via intramolecular long-range RNA-RNA interactions [4]. This tactic is employed by a number of different plant viruses to mediate translation of viral proteins from their uncapped and nonpolyadenylated genomes.

Author Summary
Conclusion and perspective
Findings
Materials and Methods
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