π S protein of severe acute respiratory syndrome-associated coronavirus mediates entry into hepatoma cell lines and is targeted by neutralizing antibodies in infected patients
The severe acute respiratory syndrome-associated coronavirus (SARS-CoV) causes severe pneumonia with a fatal outcome in approximately 10% of patients. SAS-CoV is not closely related to other coronaviruses but shares a similar genome organization. Entry of coronaviruses into target cells is mediated by the viral S protein. We functionally analyzed SARS-CoV S using pseudotyped lentiviral particles (pseudotypes). The SARS-CoV S protein was found to be expressed at the cell surface upon transient transfection. Coexpression of SARS-CoV S with human immunodeficiency virus-based reporter constructs yielded viruses that were infectious for a range of cell lines. Most notably, viral pseudotypes harboring SARS-CoV S infected hepatoma cell lines but not T- and B-cell lines. Infection of the hepatoma cell line Huh-7 was also observed with replication-competent SARS-CoV, indicating that hepatocytes might be targeted by SARS-CoV in vivo. Inhibition of vacuolar acidification impaired infection by SARS-CoV S-bearing pseudotypes, indicating that S-mediated entry requires low pH. Finally, infection by SARS-CoV S pseudotypes but not by vesicular stomatitis virus G pseudotypes was efficiently inhibited by a rabbit serum raised against SARS-CoV particles and by sera from SARS patients, demonstrating that SARS-CoV S is a target for neutralizing antibodies and that such antibodies are generated in SARS-CoV-infected patients. Our results show that viral pseudotyping can be employed for the analysis of SARS-CoV S function. Moreover, we provide evidence that SARS-CoV infection might not be limited to lung tissue and can be inhibited by the humoral immune response in infected patients.
keywords
π severe acute (1373)
π closely related (222)
π neutralizing antibodies (122)
π cell lines (125)
π respiratory syndrome-associated (90)
π cell surface (110)
π viral particles (45)
π immune response (314)
π respiratory syndrome (2004)
π acute respiratory (1734)
π cell line (211)
π syndrome-associated coronavirus (88)
π vesicular stomatitis (25)
author
π€ Hofmann, Heike
π€ Hattermann, Kim
π€ Marzi, Andrea
π€ Gramberg, Thomas
π€ Geier, Martina
π€ Krumbiegel, Mandy
π€ Kuate, Seraphin
π€ Γberla, Klaus
π€ Niedrig, Matthias
π€ PΓΆhlmann, Stefan
year
β° 2004
journal
π Journal of Virology
issn
π 0022538X
volume
78
number
12
page
6134-6142
citedbycount
112
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