Location of sequences within rotavirus SA11 glycoprotein VP7 which direct it to the endoplasmic reticulum.

Whitfeld, P L; Tyndall, C; Stirzaker, Clare; Bellamy, A R; Both, Gerald W.

doi:10.1128/mcb.7.7.2491

Cited by 23 publications

(30 citation statements)

References 22 publications

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“…These changes suggest that the function of the hydrophobic HI region (aa 6 to 23) is probably inhibited by glycosylation at aa 20, and that such an inhibition of function has a significant effect on the viability of the virus. The precise role of the H1 region is unknown, although this region can act as a signal peptide for transport to the endoplasmic reticulum (Whitfield et al, 1987).…”

Section: Resultsmentioning

confidence: 99%

Serological and genomic characterization of L338, a novel equine group A rotavirus G serotype

Browning

Chalmers

Fitzgerald

et al. 1991

Journal of General Virology

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A group A rotavirusdesignated L338 was isolated from the faeces of a diarrhoeic foal and was compared to 11 standard G serotype strains of group A rotaviruses by cross-neutralization. It was clearly distinct from serotypes G1 to Gll and thus representative of a novel rotavirus G serotype tentatively designated G13. The nucleic acid sequence of the virion protein 7 (VP7) coding region was determined and the deduced amino acid sequence compared to published sequences. Within VP7 regions A and B, L338 was clearly distinct from serotypes G1 to G12 (excluding G7 which has not been sequenced), but region C was very similar to those of G3 and G8. This further questions the significance of region C in determining serotype specificity of at least three distinct rotavirus G serotypes.

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Section: Resultsmentioning

confidence: 99%

Serological and genomic characterization of L338, a novel equine group A rotavirus G serotype

Browning

Chalmers

Fitzgerald

et al. 1991

Journal of General Virology

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“…The results from the morphogenesis studies and previous deletion experiments [15,19,27] on group A vp 7 indicate that the ER retention signal of vp 7 is structurally dependent rather then sequence dependent. The formation of viroplasms with assembly of single-shelled particles budding into ER cisternae leading to the formation of intermediate, enveloped particles as well as the intriguing metamorphosis of this particle into the mature virus particle within the ER cisternae appear therefore to be features shared with group A rotavirus.…”

Section: Discussionmentioning

confidence: 81%

“…In spite of the lack of amino acid homology between the residues associated with ER retention in vp 7 of groups A and C rotaviruses [ 15,16,19,27], group C rotavirus matures and is retained in the ER. The results from the morphogenesis studies and previous deletion experiments [15,19,27] on group A vp 7 indicate that the ER retention signal of vp 7 is structurally dependent rather then sequence dependent.…”

Section: Discussionmentioning

confidence: 96%

“…The morphological studies were undertaken not only because of the absence of homology between groups A and C rotaviruses within the vp 7 region associated with ER retention [15,16,19,27] but also because a counterpart in group C rotavirus to the trans-ER NS 28 receptor of group A rotavirus not has been recognized [11].…”

Section: Morphogenesis Of Group C Rotavirus In Swine Testicular Cellsmentioning

confidence: 99%

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Biosynthesis and morphogenesis of group C rotavirus in swine testicular cells

Nilsson

Bonsdorff

Svensson

1993

Archives of Virology

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Summary. Polypeptide synthesis and morphogenesis of a group C rotavirus (AmC-1) adapted to a continuous swine testicular cell line was examined. SDS-PAGE analysis of 35 S methionine labeled infected cell lysates revealed 9 viral polypeptides (122, 98, 79, 78, 43, 41, 35, 24, and 20kD). Viral polypeptide synthesis appeared to be maximal at 7-10h post infection. Purified group C virus grown in the presence of trypsin was found to contain seven structural polypeptides (122, 98, 79, 53, 43, 41, and 30kD) by protein blotting and five polypeptides (98, 79, 78, 43, and 41 kD) by immunoprecipitation with a hyperimmune rabbit antisera. Tunicamycin treatment, Concanavalin A binding, protein blotting, endo-H treatment and 2,6 H-mannose labeling suggested that group c rotavirus contains one structural glycoprotein (41 kD) with a corresponding precursor mol. wt. of 37 kD and one not previously identified nonstructural glycoprotein (24 kD) with a corresponding precursor mol. wt. of << 20 kD. Electron microscopy of infected swine testicular cells revealed an assembly process for group C rotavirus similar to group A, with single-shelled particles budding through the rough endoplasmic reticulum with concomitant acquisition of a transient membrane.

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“…The relative reduction of specific immunofluorescence shows the degree of specific inhibition by corresponding and noncorresponding peptide respectively (RER) [26] where it triggers the endogenous budding process. The nonstructural glycosylated membrane protein NS28 seems to guide both the mature singleshelled particles and the cytoplasmic VP4 to the endoplasmic reticulum membrane [15] where NS28 and VP7 lodges [1,3,20,30]. During the budding process, VP7 is added to the intermediate particle.…”

Section: Discussionmentioning

confidence: 99%

Monoclonal antipeptide antibodies recognize epitopes upon VP4 and VP7 of simian rotavirus SA11 in infected MA104 cells

Hansen

Mehnert

Streckert

et al. 1992

Archives of Virology

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To study morphogenetic events of rotavirus SA11-infected MA104 cells with strictly defined reagents we produced monoclonal antibodies against synthetic peptides from both outer capsid proteins VP4 (aa residues 228-241: QNTRNIVPVSIVSR) and VP7 (aa residues 319-326: SAAFYYRV) of simian rotavirus SA11. Two of the selected monoclonal antibodies proved to be reactive with determinants of SA11-infected MA104 rhesus monkey kidney cells, with purified SA11 as well as with the particular peptides used for immunization. The anti-VP4 antibody had a demonstrable neutralizing titer of 200 (50% focus reduction) whereas the anti-VP7 MuMAb revealed no detectable neutralizing activity. In peptide-inhibition experiments, the corresponding peptide inhibited its MuMAb whereas the noncorresponding peptide had no effect on antibody binding to intracellular viral antigen. Localization of VP7 was preceded by VP4 as shown by immunofluorescence microscopy.

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Location of sequences within rotavirus SA11 glycoprotein VP7 which direct it to the endoplasmic reticulum.

Cited by 23 publications

References 22 publications

Serological and genomic characterization of L338, a novel equine group A rotavirus G serotype

Serological and genomic characterization of L338, a novel equine group A rotavirus G serotype

Biosynthesis and morphogenesis of group C rotavirus in swine testicular cells

Monoclonal antipeptide antibodies recognize epitopes upon VP4 and VP7 of simian rotavirus SA11 in infected MA104 cells

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