Author
Listed:
- Serban L. Ilca
(University of Oxford)
- Xiaoyu Sun
(University of Helsinki)
- Kamel El Omari
(Harwell Science and Innovation Campus)
- Abhay Kotecha
(University of Oxford
Thermo Fisher Scientific)
- Felix Haas
(Thermo Fisher Scientific)
- Frank DiMaio
(University of Washington)
- Jonathan M. Grimes
(University of Oxford
Harwell Science and Innovation Campus)
- David I. Stuart
(University of Oxford
Harwell Science and Innovation Campus)
- Minna M. Poranen
(University of Helsinki)
- Juha T. Huiskonen
(University of Oxford
University of Helsinki
University of Helsinki)
Abstract
Characterizing the genome of mature virions is pivotal to understanding the highly dynamic processes of virus assembly and infection. Owing to the different cellular fates of DNA and RNA, the life cycles of double-stranded (ds)DNA and dsRNA viruses are dissimilar. In terms of nucleic acid packing, dsDNA viruses, which lack genome segmentation and intra-capsid transcriptional machinery, predominantly display single-spooled genome organizations1–8. Because the release of dsRNA into the cytoplasm triggers host defence mechanisms9, dsRNA viruses retain their genomes within a core particle that contains the enzymes required for RNA replication and transcription10–12. The genomes of dsRNA viruses vary greatly in the degree of segmentation. In members of the Reoviridae family, genomes consist of 10–12 segments and exhibit a non-spooled arrangement mediated by RNA-dependent RNA polymerases11–14. However, whether this arrangement is a general feature of dsRNA viruses remains unknown. Here, using cryo-electron microscopy to resolve the dsRNA genome structure of the tri-segmented bacteriophage ɸ6 of the Cystoviridae family, we show that dsRNA viruses can adopt a dsDNA-like single-spooled genome organization. We find that in this group of viruses, RNA-dependent RNA polymerases do not direct genome ordering, and the dsRNA can adopt multiple conformations. We build a model that encompasses 90% of the genome, and use this to quantify variation in the packing density and to characterize the different liquid crystalline geometries that are exhibited by the tightly compacted nucleic acid. Our results demonstrate that the canonical model for the packing of dsDNA can be extended to dsRNA viruses.
Suggested Citation
Serban L. Ilca & Xiaoyu Sun & Kamel El Omari & Abhay Kotecha & Felix Haas & Frank DiMaio & Jonathan M. Grimes & David I. Stuart & Minna M. Poranen & Juha T. Huiskonen, 2019.
"Multiple liquid crystalline geometries of highly compacted nucleic acid in a dsRNA virus,"
Nature, Nature, vol. 570(7760), pages 252-256, June.
Handle:
RePEc:nat:nature:v:570:y:2019:i:7760:d:10.1038_s41586-019-1229-9
DOI: 10.1038/s41586-019-1229-9
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Citations
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Cited by:
- Eric Gibbs & Emily Klemm & David Seiferth & Arvind Kumar & Serban L. Ilca & Philip C. Biggin & Sudha Chakrapani, 2023.
"Conformational transitions and allosteric modulation in a heteromeric glycine receptor,"
Nature Communications, Nature, vol. 14(1), pages 1-15, December.
- Nejc Kejzar & Elina Laanto & Ilona Rissanen & Vahid Abrishami & Muniyandi Selvaraj & Sylvain Moineau & Janne Ravantti & Lotta-Riina Sundberg & Juha T. Huiskonen, 2022.
"Cryo-EM structure of ssDNA bacteriophage ΦCjT23 provides insight into early virus evolution,"
Nature Communications, Nature, vol. 13(1), pages 1-13, December.
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