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Abstract
Binding of ligands, including RGD-containing peptides, to the platelet fibrinogen receptor, integrin alpha beta has been reported to cause outside-in signals, which result in clustering of occupied receptors and changes in conformation of the receptor and its cytoplasmic tails. Thus, the peptides that are usually used as inhibitors may function as partial agonists. Binding of ligand, fibrinogen or polymerizing fibrin, to platelets with activated alpha beta causes decreases in phosphatidylinositol 4,5-bisphosphate (PIP ), which may affect actin organization. IIb 3 Whether or not binding to unactivated platelets of the peptide RGDS, the fibrinogen gamma -chain C-terminal dodecapeptide (H12), or a high affinity RGD mimetic SC-54701B affects phosphoinositide metabolism was tested. Although incubation of RGDS (230 mu M), dodecapeptide (400 mu M) or SC-54701B (10 mu M) with platelets for 2 min caused trends towards decreases in PIP , no significant decreases were found. As a positive control, 2 SC-54701B was shown to inhibit the decrease in PIP in ADP-stimulated platelets at concentrations consistent 2 with the reported IC of 0.12 mu M. Thus, binding of peptides or the high affinity RGD mimetic does not 50 generate a sufficient signal to affect the signalling pathway that is involved phosphoinositide metabolism. IIb 3 2