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Induction of cell-cell fusion by ectromelia virus is not inhibited by its fusion inhibitory complex

Authors :
Paula Schnider
Tomer Israely
Pinhas Fuchs
Boaz Politi
Shlomo Lustig
Nir Paran
Sharon Melamed
Galia Maik-Rachline
Noam Erez
Source :
Virology Journal, Virology Journal, Vol 6, Iss 1, p 151 (2009)
Publication Year :
2009
Publisher :
BioMed Central, 2009.

Abstract

Background Ectromelia virus, a member of the Orthopox genus, is the causative agent of the highly infectious mousepox disease. Previous studies have shown that different poxviruses induce cell-cell fusion which is manifested by the formation of multinucleated-giant cells (polykaryocytes). This phenomenon has been widely studied with vaccinia virus in conditions which require artificial acidification of the medium. Results We show that Ectromelia virus induces cell-cell fusion under neutral pH conditions and requires the presence of a sufficient amount of viral particles on the plasma membrane of infected cells. This could be achieved by infection with a replicating virus and its propagation in infected cells (fusion "from within") or by infection with a high amount of virus particles per cell (fusion "from without"). Inhibition of virus maturation or inhibition of virus transport on microtubules towards the plasma membrane resulted in a complete inhibition of syncytia formation. We show that in contrast to vaccinia virus, Ectromelia virus induces cell-cell fusion irrespectively of its hemagglutination properties and cell-surface expression of the orthologs of the fusion inhibitory complex, A56 and K2. Additionally, cell-cell fusion was also detected in mice lungs following lethal respiratory infection. Conclusion Ectromelia virus induces spontaneous cell-cell fusion in-vitro and in-vivo although expressing an A56/K2 fusion inhibitory complex. This syncytia formation property cannot be attributed to the 37 amino acid deletion in ECTV A56.

Details

Language :
English
ISSN :
1743422X
Volume :
6
Database :
OpenAIRE
Journal :
Virology Journal
Accession number :
edsair.doi.dedup.....1ef84d51b09b4b242eeee53d887cc27d