Publication | Open Access
DC-SIGN and DC-SIGNR Interact with the Glycoprotein of Marburg Virus and the S Protein of Severe Acute Respiratory Syndrome Coronavirus
396
Citations
59
References
2004
Year
Virus StructureDc-signr InteractMolecular VirologyRespiratory DiseasesMedicineFilovirus InfectionImmunologyViral PathogenesisPathologyVirologyS ProteinAntiviral ResponseVirus-host InteractionViral Structural ProteinLectins Dc-signMarburg VirusCovid-19
The lectins DC-SIGN and DC-SIGNR can augment viral infection; however, the range of pathogens interacting with these attachment factors is incompletely defined. Here we show that DC-SIGN and DC-SIGNR enhance infection mediated by the glycoprotein (GP) of Marburg virus (MARV) and the S protein of severe acute respiratory syndrome coronavirus and might promote viral dissemination. SIGNR1, a murine DC-SIGN homologue, also enhanced infection driven by MARV and Ebola virus GP and could be targeted to assess the role of attachment factors in filovirus infection in vivo.
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