Synthesis and Translation of Viral mRNA in Reovirus-Infected Cells: Progress and Remaining Questions

Lemay, Guy

doi:10.3390/v10120671

Cited by 27 publications

(25 citation statements)

References 208 publications

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“…Viral translation also is enhanced by the reovirus σ3 outer-capsid protein [46]. The σ3 protein binds dsRNA during infection, blocking the activation of protein kinase RNA-activated (PKR), an interferon-induced enzyme that is activated by binding to dsRNA [47].…”

Section: Morphology and Functions Of Reovirus Inclusionsmentioning

confidence: 99%

Function, Architecture, and Biogenesis of Reovirus Replication Neoorganelles

Tenorio

Castro

Knowlton

et al. 2019

Viruses

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Most viruses that replicate in the cytoplasm of host cells form neoorganelles that serve as sites of viral genome replication and particle assembly. These highly specialized structures concentrate viral proteins and nucleic acids, prevent the activation of cell-intrinsic defenses, and coordinate the release of progeny particles. Reoviruses are common pathogens of mammals that have been linked to celiac disease and show promise for oncolytic applications. These viruses form nonenveloped, double-shelled virions that contain ten segments of double-stranded RNA. Replication organelles in reovirus-infected cells are nucleated by viral nonstructural proteins µNS and σNS. Both proteins partition the endoplasmic reticulum to form the matrix of these structures. The resultant membranous webs likely serve to anchor viral RNA–protein complexes for the replication of the reovirus genome and the assembly of progeny virions. Ongoing studies of reovirus replication organelles will advance our knowledge about the strategies used by viruses to commandeer host biosynthetic pathways and may expose new targets for therapeutic intervention against diverse families of pathogenic viruses.

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Section: Morphology and Functions Of Reovirus Inclusionsmentioning

confidence: 99%

Function, Architecture, and Biogenesis of Reovirus Replication Neoorganelles

Tenorio

Castro

Knowlton

et al. 2019

Viruses

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“…The outer capsid is then added, coinciding with the arrest of transcriptional activity. For a detailed review on transcription and translation during the viral multiplication cycle, the reader is referred to a recent review [9].…”

Section: Brief Overview Of Reovirus Multiplication Cyclementioning

confidence: 99%

“…This is exerted through the action of interferon-stimulated factors, mainly due to the action of IFIT proteins [15,16,17,18,19]. Interestingly, it has been reported that part of viral mRNA is devoid of a cap structure late in infection, rather harboring a monophosphate end, although the transient presence of a diphosphorylated end is possible [20,21,22] (for a recent review on reovirus mRNA structure and synthesis, see [9]). Finally, in the related rotavirus, it was more recently shown that a fraction of the RNA is not completely capped, and this seems to be responsible for recognition by the sensor RIG-I [23].…”

Section: Reovirus and The Interferon Signaling Networkmentioning

confidence: 99%

How Many Mammalian Reovirus Proteins are involved in the Control of the Interferon Response?

et al. 2019

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As with most viruses, mammalian reovirus can be recognized and attacked by the host-cell interferon response network. Similarly, many viruses have developed resistance mechanisms to counteract the host-cell response at different points of this response. Reflecting the complexity of the interferon signaling pathways as well as the resulting antiviral response, viruses can—and often have—evolved many determinants to interfere with this innate immune response and allow viral replication. In the last few years, it has been evidenced that mammalian reovirus encodes many different determinants that are involved in regulating the induction of the interferon response or in interfering with the action of interferon-stimulated gene products. In this brief review, we present our current understanding of the different reovirus proteins known to be involved, introduce their postulated modes of action, and raise current questions that may lead to further investigations.

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“…Within the cytoplasm, the core is transcriptionally active. The encapsidated RNA-dependent RNA polymerases use each genome segment as a template to produce mRNAs [3]. These mRNAs, which are capped by the viral capping enzymes also present in the particle, are extruded through turrets in the core into the cytoplasm, for translation by host ribosomes.…”

Section: Introductionmentioning

confidence: 99%

Recognition of Reovirus RNAs by the Innate Immune System

Abad

Danthi

2020

Viruses

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Mammalian orthoreovirus (reovirus) is a dsRNA virus, which has long been used as a model system to study host–virus interactions. One of the earliest interactions during virus infection is the detection of the viral genomic material, and the consequent induction of an interferon (IFN) based antiviral response. Similar to the replication of related dsRNA viruses, the genomic material of reovirus is thought to remain protected by viral structural proteins throughout infection. Thus, how innate immune sensor proteins gain access to the viral genomic material, is incompletely understood. This review summarizes currently known information about the innate immune recognition of the reovirus genomic material. Using this information, we propose hypotheses about host detection of reovirus.

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Synthesis and Translation of Viral mRNA in Reovirus-Infected Cells: Progress and Remaining Questions

Cited by 27 publications

References 208 publications

Function, Architecture, and Biogenesis of Reovirus Replication Neoorganelles

Function, Architecture, and Biogenesis of Reovirus Replication Neoorganelles

How Many Mammalian Reovirus Proteins are involved in the Control of the Interferon Response?

Recognition of Reovirus RNAs by the Innate Immune System

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