2012
DOI: 10.1016/j.jviromet.2011.11.021
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Addition of exogenous polypeptides on the mammalian reovirus outer capsid using reverse genetics

Abstract: Addition of exogenous peptide sequences on viral capsids is a powerful approach to study the process of viral infection or to retarget viruses toward defined cell types. Until recently, it was not possible to manipulate the genome of mammalian reovirus and this was an obstacle to the addition of exogenous sequence tags onto the capsid of a replicating virus. This obstacle has now been overcome by the advent of the plasmid-based reverse genetics system. In the present study, reverse genetics was used to introdu… Show more

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Cited by 22 publications
(18 citation statements)
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“…Cells were grown in MEM for suspension culture with 10% fetal bovine serum, proline (20μg/ml) and β-mercaptoethanol (50μM) and antibodies were recovered, as previously described (Brochu-Lafontaine and Lemay, 2012). The polyclonal antiserum directed against the carboxyl-terminal head domain of σ1 was produced originally in the laboratory of Dr. Terence Dermody (Vanderbilt University, Tennessee) and was a generous gift from Dr. Earl Brown (University of Ottawa).…”
Section: Antibodiesmentioning
confidence: 99%
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“…Cells were grown in MEM for suspension culture with 10% fetal bovine serum, proline (20μg/ml) and β-mercaptoethanol (50μM) and antibodies were recovered, as previously described (Brochu-Lafontaine and Lemay, 2012). The polyclonal antiserum directed against the carboxyl-terminal head domain of σ1 was produced originally in the laboratory of Dr. Terence Dermody (Vanderbilt University, Tennessee) and was a generous gift from Dr. Earl Brown (University of Ottawa).…”
Section: Antibodiesmentioning
confidence: 99%
“…Infected cells were recovered by scraping in a small volume of medium and processed for immunoblotting, as previously described (Brochu-Lafontaine and Lemay, 2012). Images were obtained using either autoradiography on Kodak BioMax Light films or on a Typhoon Trio™ imager (GE Healthcare Life Sciences).…”
Section: Immunoblottingmentioning
confidence: 99%
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“…Both replicating and nonreplicating recombinant viruses have also been recovered with fluorescent proteins iLOV and UnaG independently expressed downstream of the N-terminal half of viral spike protein 1 ( 1-N), as well as a fusion of 1-N with UnaG, which could infect cells but was unable to replicate in the absence of wild-type MRV (19,20). In addition, recombinant reoviruses in which small protein-coding sequences (6His, hemagglutinin [HA] tag, and 3HA tag) were added to the 1 protein have been recovered (21). However, there is currently no other published evidence of a replicating, recombinant virus in which NS or other viral proteins have been successfully tagged with fluorescent or other tags.…”
mentioning
confidence: 99%