Fig. 1.
Fig. 1. Substitution of IIb amino acid residue D224 results in a loss of ligand binding function. FACS histograms depicting the binding of the IIbβ3complex-specific MoAb D57, the activation-independent ligand mimetic MoAb OPG2, or the ligand mimetic MoAb PAC1 to CHO cells transfected with wild-type IIbβ3 or IIbD224Vβ3. (A) MoAb D57 staining of cells transfected with IIbβ3 (shaded histogram) or IIbD224Vβ3 (open histogram). Untransfected CHO cells are depicted by the dotted histogram. (B) MoAb OPG2 staining of the IIbβ3 (shaded histogram) or IIbD224Vβ3 (open histogram) transfected cells. Untransfected CHO cells are depicted by the dotted histogram. Cells expressing wild-type IIbβ3 (C) or IIbD224Vβ3 (D) were activated by incubation with 4 μmol/L anti-LIBS6 for 30 minutes followed by the addition of MoAb PAC1 (IgM). Cells were washed, stained with fluorescein-conjugated goat antimouse IgM for 30 minutes, and analyzed by FACS. The binding of PAC1was analyzed in the presence (open histogram) and absence (shaded histogram) of the competitve inhibitor Ro43-5054.

Substitution of IIb amino acid residue D224 results in a loss of ligand binding function. FACS histograms depicting the binding of the IIbβ3complex-specific MoAb D57, the activation-independent ligand mimetic MoAb OPG2, or the ligand mimetic MoAb PAC1 to CHO cells transfected with wild-type IIbβ3 or IIbD224Vβ3. (A) MoAb D57 staining of cells transfected with IIbβ3 (shaded histogram) or IIbD224Vβ3 (open histogram). Untransfected CHO cells are depicted by the dotted histogram. (B) MoAb OPG2 staining of the IIbβ3 (shaded histogram) or IIbD224Vβ3 (open histogram) transfected cells. Untransfected CHO cells are depicted by the dotted histogram. Cells expressing wild-type IIbβ3 (C) or IIbD224Vβ3 (D) were activated by incubation with 4 μmol/L anti-LIBS6 for 30 minutes followed by the addition of MoAb PAC1 (IgM). Cells were washed, stained with fluorescein-conjugated goat antimouse IgM for 30 minutes, and analyzed by FACS. The binding of PAC1was analyzed in the presence (open histogram) and absence (shaded histogram) of the competitve inhibitor Ro43-5054.

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