๐ Entry from the cell surface of severe acute respiratory syndrome coronavirus with cleaved S protein as revealed by pseudotype virus bearing cleaved S protein
Severe acute respiratory syndrome (SARS) coronavirus (SARS-CoV) is known to take an endosomal pathway for cell entry; however, it is thought to enter directly from the cell surface when a receptor-bound virion spike (S) protein is affected by trypsin, which induces cleavage of the S protein and activates its fusion potential. This suggests that SARS-CoV bearing a cleaved form of the S protein can enter cells directly from the cell surface without trypsin treatment. To explore this possibility, we introduced a furin-like cleavage sequence in the S protein at amino acids 798 to 801 and found that the mutated S protein was cleaved and induced cell fusion without trypsin treatment when expressed on the cell surface. Furthermore, a pseudotype virus bearing a cleaved S protein was revealed to infect cells in the presence of a lysosomotropic agent as well as a protease inhibitor, both of which are known to block SARS-CoV infection via an endosome, whereas the infection of pseudotypes with an uncleaved, wild-type S protein was blocked by these agents. A heptad repeat peptide, derived from a SARS-CoV S protein that is known to efficiently block infections from the cell surface, blocked the infection by a pseudotype with a cleaved S protein but not that with an uncleaved S protein. Those results indicate that SARS-CoV with a cleaved S protein is able to enter cells directly from the cell surface and agree with the previous observation of the protease-mediated cell surface entry of SARS-CoV. Copyright ยฉ 2008, American Society for Microbiology.
keywords
๐ amino acid (454)
๐ cell surface (110)
๐ heptad repeat (55)
๐ respiratory syndrome (2004)
๐ acute respiratory (1734)
๐ amino acids (205)
๐ results indicate (178)
author
๐ค Watanabe, Rie
๐ค Matsuyama, Shutoku
๐ค Shirato, Kazuya
๐ค Maejima, Masami
๐ค Fukushi, Shuetsu
๐ค Morikawa, Shigeru
๐ค Taguchi, Fumihiro
year
โฐ 2008
journal
๐ Journal of Virology
issn
๐ 0022538X
volume
82
number
23
page
11985-11991
citedbycount
36
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