Hyperphosphorylation of the Rotavirus NSP5 Protein Is Independent of Serine 67 or NSP2, and the Intrinsic Insolubility of NSP5 Is Regulated by Cellular Phosphatases

A, Sen; Agresti, Darin; Mackow, Erich R.

doi:10.1128/jvi.80.4.1807-1816.2006

Cited by 19 publications

(16 citation statements)

References 46 publications

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“…2). Although the positions and mechanisms of phosphorylational modification of the NSP5 protein are still unclear, NSP5 is known to be activated by complex hyperphospholyration of serine residues among RVAs (Poncet et al, 1997;Afrikanova et al, 1998;Eichwald et al, 2002Eichwald et al, , 2004bSen et al, 2006;Bar-magen et al, 2007;Sotelo et al, 2010). While this Table 2 NSP5 sequence identities (%) in nucleotide (upper right) and amino acids (lower left) among genotypes grouped by phylogenetic analysis.…”

Section: Discussionmentioning

confidence: 96%

“…NSP5 has a high number of serine and threonine residues and various posttranslational modifications, like O-glycosylation and polyphosphorylation (Welch et al, 1989;Gonzalez and Burrone, 1991). Although there are some reports on the phosphorylational modification mechanisms of NSP5 protein involving autokinase and cellular kinases, the role of NSP5 phosphorylation is still unclear and elusive (Afrikanova et al, 1998;Eichwald et al, 2002Eichwald et al, , 2004bSen et al, 2006;Bar-Magen et al, 2007). NSP5 also binds to ssRNA and dsRNA without sequence specificity (Vende et al, 2002).…”

Section: Introductionmentioning

confidence: 97%

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Phylogenetic analysis of nonstructural protein 5 (NSP5) gene sequences in porcine rotavirus B strains

Suzuki

Soma

Miyazaki

et al. 2012

Infection, Genetics and Evolution

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Section: Discussionmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 97%

Phylogenetic analysis of nonstructural protein 5 (NSP5) gene sequences in porcine rotavirus B strains

Suzuki

Soma

Miyazaki

et al. 2012

Infection, Genetics and Evolution

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“…Interestingly, the phosphatase PPM1A, which negatively regulates host stress response pathways and antiviral defense mechanisms (84,85), is upregulated and is also localized to the VM in rotavirus-infected cells. The enhanced viral protein expression and progeny virus yield in cells in which PPM1A protein expression is downregulated by siRNA suggest that its phosphatase activity is detrimental to virus growth (86). The PP2C family phosphatases play important roles in several cellular processes, including nuclear transport, and their activities are regulated by posttranslational modifications, such as phosphorylation and N-myristoylation (87)(88)(89)(90).…”

Section: Fig 10mentioning

confidence: 99%

Rotavirus Induces Formation of Remodeled Stress Granules and P Bodies and Their Sequestration in Viroplasms To Promote Progeny Virus Production

Dhillon

Rao

2018

J Virol

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Rotavirus replicates in unique virus-induced cytoplasmic inclusion bodies called viroplasms (VMs), the composition and structure of which have yet to be understood. Based on the analysis of a few proteins, earlier studies reported that rotavirus infection inhibits stress granule (SG) formation and disrupts P bodies (PBs). However, the recent demonstration that rotavirus infection induces cytoplasmic relocalization and colocalization with VMs of several nuclear hnRNPs and AU-rich element-binding proteins (ARE-BPs), which are known components of SGs and PBs, suggested the possibility of rotavirus-induced remodeling of SGs and PBs, prompting us to analyze a large number of the SG and PB components to understand the status of SGs and PBs in rotavirus-infected cells. Here we demonstrate that rotavirus infection induces molecular triage by selective exclusion of a few proteins of SGs (G3BP1 and ZBP1) and PBs (DDX6, EDC4, and Pan3) and sequestration of the remodeled/atypical cellular organelles, containing the majority of their components, in the VM. The punctate SG and PB structures are seen at about 4 h postinfection (hpi), coinciding with the appearance of small VMs, many of which fuse to form mature large VMs with progression of infection. By use of small interfering RNA (siRNA)-mediated knockdown and/or ectopic overexpression, the majority of the SG and PB components, except for ADAR1, were observed to inhibit viral protein expression and virus growth. In conclusion, this study demonstrates that VMs are highly complex supramolecular structures and that rotavirus employs a novel strategy of sequestration in the VM and harnessing of the remodeled cellular RNA recycling bins to promote its growth.IMPORTANCE Rotavirus is known to replicate in specialized virus-induced cytoplasmic inclusion bodies called viroplasms (VMs), but the composition and structure of VMs are not yet understood. Here we demonstrate that rotavirus interferes with normal SG and PB assembly but promotes formation of atypical SG-PB structures by selective exclusion of a few components and employs a novel strategy of sequestration of the remodeled SG-PB granules in the VMs to promote virus growth by modulating their negative influence on virus infection. Rotavirus VMs appear to be complex supramolecular structures formed by the union of the triad of viral replication complexes and remodeled SGs and PBs, as well as other host factors, and designed to promote productive virus infection. These observations have implications for the planning of future research with the aim of understanding the structure of the VM, the mechanism of morphogenesis of the virus, and the detailed roles of host proteins in rotavirus biology.

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“…12 Cellular kinases, such as casein kinase I and II, have also been reported to phosphorylate NSP5. [13][14][15] Moreover, the interaction of NSP2 with NSP5 has been shown to stimulate NSP5 phosphorylation. 16 The role of NSP5 phosphorylation is still elusive, even though it was suggested to be involved in regulating the fate of mRNA between translation and replication 1 7 and in RNA selective encapsidation.…”

Section: Introductionmentioning

confidence: 98%

Structural Organisation of the Rotavirus Nonstructural Protein NSP5

Martin¹,

Ouldali²,

Menetrey³

et al. 2011

Journal of Molecular Biology

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Hyperphosphorylation of the Rotavirus NSP5 Protein Is Independent of Serine 67 or NSP2, and the Intrinsic Insolubility of NSP5 Is Regulated by Cellular Phosphatases

Cited by 19 publications

References 46 publications

Phylogenetic analysis of nonstructural protein 5 (NSP5) gene sequences in porcine rotavirus B strains

Phylogenetic analysis of nonstructural protein 5 (NSP5) gene sequences in porcine rotavirus B strains

Rotavirus Induces Formation of Remodeled Stress Granules and P Bodies and Their Sequestration in Viroplasms To Promote Progeny Virus Production

Structural Organisation of the Rotavirus Nonstructural Protein NSP5

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