Two non-structural rotavirus proteins, NSP2 and NSP5, form viroplasm-like structures in vivo.

Fabbretti, Elsa; Afrikanova, Ivka; Vascotto, Fulvia; Burrone, Óscar R.

doi:10.1099/0022-1317-80-2-333

Cited by 202 publications

(265 citation statements)

References 21 publications

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“…The formation of viral inclusion bodies, or viroplasms, is a common feature of double-stranded (ds)RNA viruses from the family Reoviridae with genomes composed of 10-12 segments (Brookes et al, 1993;Fabbretti et al, 1999;Fukushi et al, 1962;Petrie et al, 1984;Rhim et al, 1962;Shikata & Kitagawa, 1977;Touris-Otero et al, 2004). These inclusion bodies are mainly composed of viral dsRNA, viral proteins and partially and fully assembled viral particles (Dales et al, 1965;Fabbretti et al, 1999;Isogai et al, 1998;Rhim et al, 1962;Silverstein & Schur, 1970;Touris-Otero et al, 2004;Wei et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

“…These inclusion bodies are mainly composed of viral dsRNA, viral proteins and partially and fully assembled viral particles (Dales et al, 1965;Fabbretti et al, 1999;Isogai et al, 1998;Rhim et al, 1962;Silverstein & Schur, 1970;Touris-Otero et al, 2004;Wei et al, 2006). In addition, the inclusion bodies have been shown to contain microtubules and thinner 'kinky' filaments suggested to be intermediate filaments (Dales, 1963;Dales et al, 1965;Spendlove et al, 1964).…”

Section: Introductionmentioning

confidence: 99%

“…In addition, the inclusion bodies have been shown to contain microtubules and thinner 'kinky' filaments suggested to be intermediate filaments (Dales, 1963;Dales et al, 1965;Spendlove et al, 1964). Although the formation mechanism of these inclusions is largely unknown, they are thought to play an important role in viral infections because they are probable sites of viral genome replication, protein synthesis and virus assembly (Fabbretti et al, 1999;Isogai et al, 1998;Petrie et al, 1984;Rhim et al, 1962;Wei et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

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Rice black streaked dwarf virus P9-1, an α-helical protein, self-interacts and forms viroplasms in vivo

Zhang

Liu

Liu³

et al. 2008

Journal of General Virology

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Replication and assembly of viruses from the family Reoviridae are thought to take place in discrete cytoplasmic inclusion bodies, commonly called viral factories or viroplasms. Rice black streaked dwarf virus (RBSDV) P9-1, a non-structural protein, has been confirmed to accumulate in these intracellular viroplasms in infected plants and insects. However, little is known about its exact function. In this study, P9-1 of RBSDV-Baoding was expressed in Escherichia coli as a Histagged fusion protein and analysed using biochemical and biophysical techniques. Mass spectrometry and circular dichroism spectroscopy studies showed that P9-1 was a thermostable, a-helical protein with a molecular mass of 41.804 kDa. A combination of gel-filtration chromatography, chemical cross-linking and a yeast two-hybrid assay was used to demonstrate that P9-1 had the intrinsic ability to self-interact and form homodimers in vitro and in vivo. Furthermore, when transiently expressed in Arabidopsis protoplasts, P9-1 formed large, discrete viroplasm-like structures in the absence of infection or other RBSDV proteins. Taken together, these results suggest that P9-1 is the minimal viral component required for viroplasm formation and that it plays an important role in the early stages of the virus life cycle by forming intracellular viroplasms that serve as the sites of virus replication and assembly.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Rice black streaked dwarf virus P9-1, an α-helical protein, self-interacts and forms viroplasms in vivo

Zhang

Liu

Liu³

et al. 2008

Journal of General Virology

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“…In addition, in viroplasms, NSP5 interacts with other viral proteins such as NSP2 (Poncet et al, 1997;Afrikanova et al, 1998), VP1 (Afrikanova et al, 1998) and VP2 (Berois et al, 2003). The in vivo interaction with NSP2 leads to NSP5 hyperphosphorylation and the formation of viroplasm-like structures (VLSs) (Afrikanova et al, 1998;Fabbretti et al, 1999). We have recently shown that the hyperphosphorylation is the consequence of a cellular kinase that is activated by NSP5 itself in a process resembling autophosphorylation (Eichwald et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

“…An NSP2-encoding cDNA fragment, obtained by PCR amplification using specific primers to incorporate NcoI and BamHI restriction sites at the N and C termini, respectively, was cloned into pVOTE.1 (Ward et al, 1995) to obtain the construct pVOTE.1/NSP2. Constructs pT 7 v-NSP5, pT 7 v-D1, pT 7 v-D2, pT 7 v-D3, pT 7 v-D4, pT 7 v-DT, pT 7 v-D1/D2 and pT 7 v-D4T have been described previously (Afrikanova et al, 1998;Fabbretti et al, 1999;Eichwald et al, 2002). The internal deletion plasmids pT 7 v-D2/D4T, pT 7 v-D2/D3 and pT 7 v-D3/DT were obtained by PCR using specific internal primers and cloned into KpnI and BamHI restriction sites in pcDNA3 (Invitrogen).…”

Section: Introductionmentioning

confidence: 99%

Characterization of rotavirus NSP2/NSP5 interactions and the dynamics of viroplasm formation

Eichwald

Rodrı́guez

Burrone

2004

Journal of General Virology

123

196

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Viroplasms are discrete structures formed in the cytoplasm of rotavirus-infected cells and constitute the replication machinery of the virus. The non-structural proteins NSP2 and NSP5 localize in viroplasms together with other viral proteins, including the polymerase VP1, VP3 and the main inner-core protein, VP2. NSP2 and NSP5 interact with each other, activating NSP5 hyperphosphorylation and the formation of viroplasm-like structures (VLSs). We have used NSP2 and NSP5 fused to the enhanced green fluorescent protein (EGFP) to investigate the localization of both proteins within viroplasms in virus-infected cells, as well as the dynamics of viroplasm formation. The number of viroplasms was shown first to increase and then to decrease with time post-infection, while the area of each one increased, suggesting the occurrence of fusions. The interaction between NSP2 and a series of NSP5 mutants was investigated using two different assays, a yeast two-hybrid system and an in vivo binding/immunoprecipitation assay. Both methods gave comparable results, indicating that the N-terminal region (33 aa) as well as the C-terminal part (aa 131-198) of NSP5 are required for binding to NSP2. When fused to the N and C terminus of EGFP, respectively, these two regions were able to confer the ability to localize in the viroplasm and to form VLSs with NSP2.

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Regulation of processing bodies: From viruses to cancer epigenetic machinery

Kanakamani

Suresh

Venkatesh

2020

Cell Biology International

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Processing bodies (PBs) are 100–300 nm cytoplasmic messenger ribonucleoprotein particle (mRNP) granules that regulate eukaryotic gene expression. These cytoplasmic compartments harbor messenger RNAs (mRNAs) and several proteins involved in mRNA decay, microRNA silencing, nonsense‐mediated mRNA decay, and splicing. Though membrane‐less, PB structures are maintained by RNA‐protein and protein‐protein interactions. PB proteins have intrinsically disordered regions and low complexity domains, which account for its liquid to liquid phase separation. In addition to being dynamic and actively involved in the exchange of materials with other mRNPs and organelles, they undergo changes on various cellular cues and environmental stresses, including viral infections. Interestingly, several PB proteins are individually implicated in cancer development, and no study has addressed the effects on PB dynamics after epigenetic modifications of cancer‐associated PB genes. In the current review, we summarize modulations undergone by P bodies or P body components upon viral infections. Furthermore, we discuss the selective and widely investigated PB proteins that undergo methylation changes in cancer and their potential as biomarkers.

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Two non-structural rotavirus proteins, NSP2 and NSP5, form viroplasm-like structures in vivo.

Cited by 202 publications

References 21 publications

Rice black streaked dwarf virus P9-1, an α-helical protein, self-interacts and forms viroplasms in vivo

Rice black streaked dwarf virus P9-1, an α-helical protein, self-interacts and forms viroplasms in vivo

Characterization of rotavirus NSP2/NSP5 interactions and the dynamics of viroplasm formation

Regulation of processing bodies: From viruses to cancer epigenetic machinery

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