Action of AD6 (8-monochloro-3-beta-diethylaminoethyl-4-methyl-7-ethoxycarbonylmethoxy coumarin) on human platelets in vitro

Abstract

The action of AD₆ was tested in vitro on human platelets by measuring beta-thromboglobulin (BTG), platelet factor 4 (PF₄) and thromboxane B₂ (TXB₂) release as well as aggregation. BTG and PF₄ release from blood anticoagulated with sodium citrate was inhibited by AD₆ during a 3 h incubation. Platelet rich plasma (PRP) was stimulated with ADP, collagen, sodium arachidonate, PAF, A23187 and epinephrine, while resuspended washed platelets (WP) were stimulated by thrombin. AD₆ (5–100 μM) inhibited dose dependently aggregation, BTG, PF₄ and TXB₂ release induced by threshold concentration of all the tested aggregating agents; however AD₆ action could be overcome by increasing the concentration of the stimulating agents. After cyclo-oxygenase blockade by acetylsalicylic acid (ASA), PRP was stimulated by a supramaximal concentration of PAF. Under these circumstances we could observe a reversible aggregation and a partial release of BTG and PF₄, AD₆ was able to further reduce aggregation and release. Cyclic AMP accumulation induced in WP by prostacyclin was not modified by AD₆ (100 μM), while theophylline greatly potentiated prostacyclin action. We conclude that AD₆ is an inhibitor of platelet activation in vitro. Its mode of action is different from cyclo-oxygenase blockade and provides inhibition of platelet activation by a number of different stimuli.