π Important role for the transmembrane domain of severe acute respiratory syndrome coronavirus spike protein during entry
The spike protein (S) of severe acute respiratory syndrome coronavirus (SARS-CoV) is responsible for receptor binding and membrane fusion. It contains a highly conserved transmembrane domain that consists of three parts: an N-terminal tryptophan-rich domain, a central domain, and a cysteine-rich C-terminal domain. The cytoplasmic tail of S has previously been shown to be required for assembly. Here, the roles of the transmembrane and cytoplasmic domains of S in the infectivity and membrane fusion activity of SARS-CoV have been studied. SARS-CoV S-pseudotyped retrovirus (SARSpp) was used to measure S-mediated infectivity. In addition, the cell-cell fusion activity of S was monitored by a Renilla luciferase-based cell-cell fusion assay. Svsv-cyt, an S chimera with a cytoplasmic tail derived from vesicular stomatitis virus G protein (VSV-G), and SMHV-TMDCyt, an S chimera with the cytoplasmic and transmembrane domains of mouse hepatitis virus, displayed wild-type-like activity in both assays. SVSV-TMDCyt, a chimera with the cytoplasmic and transmembrane domains of VSV-G, was impaired in the SARSpp and cell-cell fusion assays, showing 3 to 25% activity compared to the wild type, depending on the assay and the cells used. Examination of the oligomeric state of the chimeric S proteins in SARSpp revealed that SVSV-TMDCyt trimers were less stable than wild-type S trimers, possibly explaining the lowered fusogenicity and infectivity. Copyright Β© 2006, American Society for Microbiology.
keywords
π severe acute (1373)
π syndrome coronavirus (1074)
π cell-cell fusion (34)
π spike protein (353)
π hepatitis virus (437)
π mouse hepatitis (371)
π transmembrane domain (51)
π receptor binding (86)
π respiratory syndrome (2004)
π highly conserved (80)
π acute respiratory (1734)
π wild type (34)
π vesicular stomatitis (25)
π membrane fusion (105)
author
π€ Broer, Rene
π€ Boson, Bertrand
π€ Spaan, Willy
π€ Cosset, FranΓ§ois LoΓ―c
π€ Corver, Jeroen
year
β° 2006
journal
π Journal of Virology
issn
π 0022538X
volume
80
number
3
page
1302-1310
citedbycount
28
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