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Thiol/disulfide exchange is required for membrane fusion directed by the Newcastle disease virus fusion protein
UMass Chan Affiliations
Department of Molecular Genetics and MicrobiologyMorningside Graduate School of Biomedical Sciences
Document Type
Journal ArticlePublication Date
2006-12-08
Metadata
Show full item recordAbstract
Newcastle disease virus (NDV), an avian paramyxovirus, initiates infection with attachment of the viral hemagglutinin-neuraminidase (HN) protein to sialic acid-containing receptors, followed by fusion of viral and cell membranes, which is mediated by the fusion (F) protein. Like all class 1 viral fusion proteins, the paramyxovirus F protein is thought to undergo dramatic conformational changes upon activation. How the F protein accomplishes extensive conformational rearrangements is unclear. Since several viral fusion proteins undergo disulfide bond rearrangement during entry, we asked if similar rearrangements occur in NDV proteins during entry. We found that inhibitors of cell surface thiol/disulfide isomerase activity--5'5-dithio-bis(2-nitrobenzoic acid) (DTNB), bacitracin, and anti-protein disulfide isomerase antibody--inhibited cell-cell fusion and virus entry but had no effect on cell viability, glycoprotein surface expression, or HN protein attachment or neuraminidase activities. These inhibitors altered the conformation of surface-expressed F protein, as detected by conformation-sensitive antibodies. Using biotin maleimide (MPB), a reagent that binds to free thiols, free thiols were detected on surface-expressed F protein, but not HN protein. The inhibitors DTNB and bacitracin blocked the detection of these free thiols. Furthermore, MPB binding inhibited cell-cell fusion. Taken together, our results suggest that one or several disulfide bonds in cell surface F protein are reduced by the protein disulfide isomerase family of isomerases and that F protein exists as a mixture of oxidized and reduced forms. In the presence of HN protein, only the reduced form may proceed to refold into additional intermediates, leading to the fusion of membranes.Source
J Virol. 2007 Mar;81(5):2328-39. Epub 2006 Dec 6. Link to article on publisher's siteDOI
10.1128/JVI.01940-06Permanent Link to this Item
http://hdl.handle.net/20.500.14038/33914PubMed ID
17151113Related Resources
Link to article in PubMedae974a485f413a2113503eed53cd6c53
10.1128/JVI.01940-06