Our aim was to determine whether the newly described P2X1 antagonist NF449 [4,4′,4″,4‴-(carbonylbis(imino-5,1,3- benzenetriylbis(carbonylimino)))tetrakis-benzene-1,3-disulfonic acid octasodium salt] could selectively antagonize the platelet P2X1 receptor and how it affected platelet function. NF449 inhibited α,β- methyleneadenosine 5′-triphosphate-induced shape change (IC50 = 83 ± 13 nM; n = 3) and calcium influx (pA2 = 7.2 ± 0.1; n = 3) (pIC50 = 6.95) in washed human platelets treated with apyrase to prevent desensitization of the P2X1 receptor. NF449 also antagonized the calcium rise mediated by the P2Y1 receptor, but with lower potency (IC50 = 5.8 ± 2.2 μM; n = 3). In contrast, it was a very weak antagonist of the P2Y12-mediated inhibition of adenylyl cyclase activity. Selective blockade of the P2X1 receptor with NF449 led to reduced collagen-induced aggregation, confirming a role of this receptor in platelet activation induced by collagen. Intravenous injection of 10 mg/kg NF449 into mice resulted in selective inhibition of the P2X 1 receptor and decreased intravascular platelet aggregation in a model of systemic thromboembolism (35 ± 4 versus 51 ± 3%) (P = 0.0061; n = 10) but without prolongation of the bleeding time (106 ± 16 versus 78 ± 7 s; n = 10) (N.S.; P = 0.1209). At a higher dose (50 mg/kg), NF449 inhibited the three platelet P2 receptors. This led to a further reduction in platelet consumption compared with mice injected with saline (13 ± 4 versus 42 ± 3%) (P = 0.0002; n = 5). NF449 also reduced dose-dependently the size of thrombi formed after laser-induced injury of mesenteric arterioles. Overall, our results indicate that NF449 constitutes a new tool to investigate the functions of the P2X1 receptor and could be a starting compound in the search for new antithrombotic drugs targeting the platelet P2 receptors. Copyright
Inhibition of platelet functions and thrombosis through selective or nonselective inhibition of the platelet P2 receptors with increasing doses of NF449 [4,4',4'',4'''-(carbonylbis(imino-5,1,3-benzenetriylbis-(carbonylimino)))tetrakis -benzene-1,3-disulfonic acid octasodium salt] / B. Hechler, S. Magnenat, M.L. Zighetti, M.U. Kassack, H. Ullmann, J.P. Cazenave, R. Evans, M. Cattaneo, C. Gachet. - In: JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS. - ISSN 0022-3565. - 314:1(2005 Jul), pp. 232-243.
Inhibition of platelet functions and thrombosis through selective or nonselective inhibition of the platelet P2 receptors with increasing doses of NF449 [4,4',4'',4'''-(carbonylbis(imino-5,1,3-benzenetriylbis-(carbonylimino)))tetrakis -benzene-1,3-disulfonic acid octasodium salt]
M. CattaneoPenultimo
;
2005
Abstract
Our aim was to determine whether the newly described P2X1 antagonist NF449 [4,4′,4″,4‴-(carbonylbis(imino-5,1,3- benzenetriylbis(carbonylimino)))tetrakis-benzene-1,3-disulfonic acid octasodium salt] could selectively antagonize the platelet P2X1 receptor and how it affected platelet function. NF449 inhibited α,β- methyleneadenosine 5′-triphosphate-induced shape change (IC50 = 83 ± 13 nM; n = 3) and calcium influx (pA2 = 7.2 ± 0.1; n = 3) (pIC50 = 6.95) in washed human platelets treated with apyrase to prevent desensitization of the P2X1 receptor. NF449 also antagonized the calcium rise mediated by the P2Y1 receptor, but with lower potency (IC50 = 5.8 ± 2.2 μM; n = 3). In contrast, it was a very weak antagonist of the P2Y12-mediated inhibition of adenylyl cyclase activity. Selective blockade of the P2X1 receptor with NF449 led to reduced collagen-induced aggregation, confirming a role of this receptor in platelet activation induced by collagen. Intravenous injection of 10 mg/kg NF449 into mice resulted in selective inhibition of the P2X 1 receptor and decreased intravascular platelet aggregation in a model of systemic thromboembolism (35 ± 4 versus 51 ± 3%) (P = 0.0061; n = 10) but without prolongation of the bleeding time (106 ± 16 versus 78 ± 7 s; n = 10) (N.S.; P = 0.1209). At a higher dose (50 mg/kg), NF449 inhibited the three platelet P2 receptors. This led to a further reduction in platelet consumption compared with mice injected with saline (13 ± 4 versus 42 ± 3%) (P = 0.0002; n = 5). NF449 also reduced dose-dependently the size of thrombi formed after laser-induced injury of mesenteric arterioles. Overall, our results indicate that NF449 constitutes a new tool to investigate the functions of the P2X1 receptor and could be a starting compound in the search for new antithrombotic drugs targeting the platelet P2 receptors. Copyright
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