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LSECtin interacts with filovirus glycoproteins and the spike protein of SARS coronavirus |
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| Authors: | Gramberg Thomas Hofmann Heike Möller Peggy Lalor Patricia F Marzi Andrea Geier Martina Krumbiegel Mandy Winkler Thomas Kirchhoff Frank Adams David H Becker Stephan Münch Jan Pöhlmann Stefan |
| Affiliation: | Institute for Clinical and Molecular Virology, University Erlangen-Nürnberg, Germany. |
| Abstract: | Cellular attachment factors like the C-type lectins DC-SIGN and DC-SIGNR (collectively referred to as DC-SIGN/R) can augment viral infection and might promote viral dissemination in and between hosts. The lectin LSECtin is encoded in the same chromosomal locus as DC-SIGN/R and is coexpressed with DC-SIGNR on sinusoidal endothelial cells in liver and lymphnodes. Here, we show that LSECtin enhances infection driven by filovirus glycoproteins (GP) and the S protein of SARS coronavirus, but does not interact with human immunodeficiency virus type-1 and hepatitis C virus envelope proteins. Ligand binding to LSECtin was inhibited by EGTA but not by mannan, suggesting that LSECtin unlike DC-SIGN/R does not recognize high-mannose glycans on viral GPs. Finally, we demonstrate that LSECtin is N-linked glycosylated and that glycosylation is required for cell surface expression. In summary, we identified LSECtin as an attachment factor that in conjunction with DC-SIGNR might concentrate viral pathogens in liver and lymph nodes. |
| Keywords: | Ebolavirus SARS coronavirus Human immunodeficiency virus Hepatitis C virus LSECtin DC-SIGN DC-SIGNR Attachment factor Receptor Glycoprotein |
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