Demonstration of Ac-Arg-Gly-Asp-Ser-NH2 as an Antiaggregatory Agent in the Dog by Intracoronary Administration

Abstract

This study compared the anti-platelet effect of Ac-RGDS-NH₂ which is a peptide fragment from fibrinogen to Ac-RGES-NH₂ in which the aspartic acid (D) of Ac-RGDS-NH₂ has been replaced by glutamic acid (E). When Ac-RGDS-NH₂ was infused intracoronary at concentrations of 100–400 mM, acute platelet dependent thrombus formation in the dog coronary artery was inhibited. However, infusion of Ac-RGES-NH₂ intracoronary at similar concentrations to Ac-RGDS-NH₂ failed to inhibit platelet dependent thrombus formation in the dog. Ac-RGDS-NH₂ and Ac-RGES-NH₂ were also tested for their ability to inhibit collagen-induced platelet aggregation in vitro. Ac-RGDS-NH₂ elicited concentration-dependent inhibition of collagen-induced aggregation with no effect of Ac-RGES-NHz otr collagen-induced platelet aggregation. Thus, Ac-RGDS-NH₂ is an effective antiplatelet agent after intracoronary administration in the dog and also inhibits collagen-induced platelet aggregation in vitro. Ac-RGDS-NH₂ is a specific inhibitor of platelet aggregation as replacement of the aspartic acid in Ac-RGDS-NH₂ with glutamic acid results in complete loss of biological activity.