Endothelium-dependent Vasorelaxant and Anti-aggregatory Effect and Mechanism of Action of Some Antifibrinogen RGD (Arg-Gly-Asp-containing) Peptides

Abstract

Vasorelaxation caused by some antifibrinogen RGD (Arg‐Gly‐Asp‐containing) peptides and their basic mechanism of action was studied on rabbit isolated thoracic aortic rings preconstricted with 0.25 μM phenylephrine. GRGDS (Gly‐Arg‐Gly‐Asp‐Ser‐OH) and RGDV (Arg‐Gly‐Asp‐Val‐OH) caused dose‐dependent relaxation. RGDS (Arg‐Gly‐Asp‐Ser‐OH) had a biphasic effect (a transient relaxation followed by a contraction) while GRGDS‐[SE] (Gly‐Arg‐Gly‐Asp‐Ser(SO₃)‐OH) did not change the isometric tone of precontracted aortic preparations. GRGDS and RGDV exerted no relaxing effect on endothelium‐denuded blood vessels suggesting that the vascular action of these peptides was entirely dependent on the presence of functionally intact endothelium. L‐N^G‐Nitro‐arginine (30 μM) attenuated the relaxation induced by GRGDS and abolished that induced by RGDV. All of the four RGD congeners inhibited ADP‐induced aggregation of human platelets. These findings indicate that the relaxant effect of RGDV is mediated exclusively by the nitric oxide pathway, but GRGDS could cause, besides nitric oxide release, the release of another substance which is different from nitric oxide. Because the rank order of the vasorelaxant potencies of RGD peptides differed from that found for their anti‐aggregatory activities, a vascular effector mechanism mediated by an RGD‐recognizing structure other than the known glycoprotein IIb/IIIa‐like RGD‐binding site is suggested.