Fig. 4.
Fig. 4. Tetramerization of peptides results in high-affinity binding. / Competition studies of synthetic peptides with TM11-PO (2 nM) for P-selectin binding were performed in an ELISA. (A) Competition of TM11 (▪) with TM11-PO resulted in an IC50 of 2 μM. A 200-fold increase in affinity was observed when TM11 was presented as a tetramer, (TM11)4, by conjugation of TM11-biotin to streptavidin (▴, IC50 = 10 nM). (B) The IC50 of monomeric TM31 (▪, 19 μM) was 300-fold lower than that of tetrameric TM31 (▴, IC50 = 61 nM). Values represent means of triplicate experiments ± variation.

Tetramerization of peptides results in high-affinity binding.

Competition studies of synthetic peptides with TM11-PO (2 nM) for P-selectin binding were performed in an ELISA. (A) Competition of TM11 (▪) with TM11-PO resulted in an IC50 of 2 μM. A 200-fold increase in affinity was observed when TM11 was presented as a tetramer, (TM11)4, by conjugation of TM11-biotin to streptavidin (▴, IC50 = 10 nM). (B) The IC50 of monomeric TM31 (▪, 19 μM) was 300-fold lower than that of tetrameric TM31 (▴, IC50 = 61 nM). Values represent means of triplicate experiments ± variation.

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