๐ Monitoring of s protein maturation in the endoplasmic reticulum by calnexin is important for the infectivity of severe acute respiratory syndrome coronavirus
Severe acute respiratory syndrome coronavirus (SARS-CoV) is the etiological agent of SARS, a fatal pulmonary disorder with no effective treatment. We found that SARS-CoV spike glycoprotein (S protein), a key molecule for viral entry, binds to calnexin, a molecular chaperone in the endoplasmic reticulum (ER), but not to calreticulin, a homolog of calnexin. Calnexin bound to most truncated mutants of S protein, and S protein bound to all mutants of calnexin. Pseudotyped virus carrying S protein (S-pseudovirus)produced by human cells that were treated with small interfering RNA (siRNA) for calnexin expression (calnexin siRNAtreated ells) showed significantly lower infectivity than S-pseudoviruses produced by untreated and control siRNA-treated cells. S-pseudovirus produced by calnexin siRNA-treated cells contained S protein modified with N-glycan side chains differently from other two S proteins and consisted of two kinds of viral particles: those of normal density with little S protein and those of high density with abundant S protein. Treatment with peptide-N-glycosidase F (PNGase F), which removes all types of N-glycan side chains from glycoproteins, eliminated the infectivity of S-pseudovirus. S-pseudovirus and SARS-CoV produced in the presence of ฮฑ-glucosidase inhibitors, which disrupt the interaction between calnexin and its substrates, showed significantly lower infectivity than each virus produced in the absence of those compounds. In S-pseudovirus, the incorporation of S protein into viral particles was obviously inhibited. In SARS-CoV, viral production was obviously inhibited. These findings demonstrated that calnexin strictly monitors the maturation of S protein by its direct binding, resulting in conferring infectivity on SARS-CoV. ยฉ 2012, American Society for Microbiology.
keywords
๐ syndrome coronavirus (1074)
๐ endoplasmic reticulum (78)
๐ etiological agent (62)
๐ viral particles (45)
๐ spike glycoprotein (99)
๐ respiratory syndrome (2004)
๐ acute respiratory (1734)
๐ viral entry (91)
author
๐ค Fukushi, Masaya
๐ค Yoshinaka, Yoshiyuki
๐ค Matsuoka, Yusuke
๐ค Hatakeyama, Seisuke
๐ค Ishizaka, Yukihito
๐ค Kirikae, Teruo
๐ค Sasazuki, Takehiko
๐ค Miyoshi-Akiyama, Tohru
year
โฐ 2012
journal
๐ Journal of Virology
issn
๐ 0022538X 10985514
volume
86
number
21
page
11745-11753
citedbycount
14
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