4.7 Article

Synergistic action between inhibition of P2Y12/P2Y1 and P2Y12/thrombin in ADP- and thrombin-induced human platelet activation

Journal

BRITISH JOURNAL OF PHARMACOLOGY
Volume 142, Issue 8, Pages 1325-1331

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/sj.bjp.0705885

Keywords

P2Y(12); P2Y(1); flow cytometry; alpha(llb)beta(3); platelets; thrombin; melagatran; AR-C69931MX; ADP

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1 The objective of this study was to investigate if there is a synergistic effect of a combination of P2Y(12) and P2Y(1) inhibition and P2Y(12) and thrombin inhibition, on ADP- and thrombin-induced platelet activation, respectively. The rationale being that these combinations will cause a concurrent inhibition of both Galpha(q) and Galpha(i) signalling. 2 Blood from healthy volunteers was preincubated with AR-C69931MX, a reversible P2Y(12) antagonist; MRS2179, a reversible P2Y(1) antagonist; or melagatran, a direct reversible thrombin inhibitor; alone or in various combinations prior to activation with ADP or thrombin. Platelet function in whole blood was assessed by flow cytometry using the antibody PAC-1 to estimate the expression of active alpha(IIb)beta(3) (the fibrinogen receptor GPIIb/IIIa). A synergistic effect was evaluated by comparing the concentrations in the different combinations with those of corresponding equipotent concentrations of each single inhibitor alone. The equipotent single concentrations were experimentally obtained from concentration response curves performed in parallel. 3 A synergistic effect regarding inhibition of ADP-induced platelet activation (10 muM) was obtained with different combinations of AR-C69931MX and MRS2179. 4 Inhibition of thrombin-induced platelet activation (2 nM) with combinations of AR-C69931MX and the thrombin inhibitor melagatran did also result in a strong synergistic effect. 5 To our knowledge, this is the first time that data supporting a synergistic effect has been published for the inhibitor combinations described. 6 Whether this synergistic effect in vitro also results in an improved antithrombotic effect in vivo with or without an increased risk of bleeding remains to be studied in well-conducted clinical studies.

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