Polyacrylamides Bearing Pendant R-Sialoside Groups Strongly Inhibit Agglutination of Erythrocytes by Influenza Virus: The Strong Inhibition Reflects Enhanced Binding through Cooperative Polyvalent Interactions

نویسندگان

  • George B. Sigal
  • Mathai Mammen
  • Georg Dahmann
  • George M. Whitesides
چکیده

An ELISA assay is described for measuring the binding of influenza virus A-X31 to R-sialoside groups that are linked to biotin-labeled polyacrylamides. The efficacy of these polymers in inhibiting the adhesion of influenza virus to erythrocytes (as measured by a hemagglutination assay) was shown to be directly related to the binding affinity of the polymers for the viral surface: the differences in inhibitory efficacy among the polymeric inhibitors and monomeric R-methyl sialoside, among fractions of a polymeric, polyvalent inhibitor with narrow molecular weight ranges, and among polymeric inhibitors prepared by copolymerization or modification of a preformed polymer chain, all correlated with differences in the affinity of the inhibitors for the surface of the virus. The polymeric inhibitors studied had affinities for the viral surface that ranged between 103 and >106 greater than R-methyl sialoside, on the basis of total sialic acid groups in solution. The role of steric stabilization in the mechanism by which these polymers inhibit hemagglutination was investigated. The ability of the polymeric, polyvalent inhibitors to inhibit the binding of a polyclonal antibody to the viral surface suggests that steric stabilization may also be an important effect in this system.

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تاریخ انتشار 1997