Publication | Open Access
Coxsackieviruses B1, B3, and B5 use decay accelerating factor as a receptor for cell attachment
287
Citations
32
References
1995
Year
Cell Surface MoleculesViral ReplicationMolecular VirologyMedicineViral Polymerase MechanismPathogenesisViral PathogenesisImmunologyVirologyCell AttachmentReceptor BindingVirus-host InteractionViral Structural ProteinCoxsackieviruses B1Cell BiologyViral GeneticsVirus Tissue Tropism
Receptor binding and subsequent cell-mediated internalization or disassembly are the initial steps in virus replication. Cell surface molecules that participate in this process are the primary determinants of virus tissue tropism. Monoclonal antibody blockade, immunoprecipitation, and DNA transfection were used to identify decay accelerating factor as a major cell attachment receptor for coxsackieviruses B1, B3, and B5. However, expression of human decay acceleration factor on the surface of nonpermissive murine fibroblasts led only to virus attachment without subsequent replication, and it was concluded that an additional cellular cofactor(s) is required to facilitate cell entry and subsequent replication.
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