Inhibition of platelet-mediated, tissue factor-induced thrombin generation by the mouse/human chimeric 7E3 antibody. Potential implications for the effect of c7E3 Fab treatment on acute thrombosis and 'clinical restenosis'.
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机译:抑制小鼠/人嵌合 7E3 抗体产生血小板介导的组织因子诱导的凝血酶生成。c7E3 Fab 治疗对急性血栓形成和“临床再狭窄”影响的潜在影响。
The murine/human chimeric monoclonal antibody fragment (c7E3 Fab) blocks GPIIb/IIIa and alpha v beta 3 receptors, inhibits platelet aggregation, and decreases the frequency of ischemic events after coronary artery angioplasty in patients at high risk of suffering such events. Although inhibition of platelet aggregation is likely to be the major mechanism of c7E3 Fab's effects, since activated platelets facilitate thrombin generation, it is possible that c7E3 Fab also decreases thrombin generation. To test this hypothesis, the effects of c7E3 Fab and other antiplatelet agents were tested in a thrombin generation assay triggered by tissue factor. c7E3 Fab produced dose-dependent inhibition of thrombin generation, reaching a plateau of 45-50 inhibition at concentrations > or = 15 micrograms/ml. It also inhibited thrombin-antithrombin complex formation, prothrombin fragment F1-2 generation, platelet-derived growth factor and platelet factor 4 release, incorporation of thrombin into clots, and microparticle formation. Antibody 6D1, which blocks platelet GPIb binding of von Willebrand factor, had no effect on thrombin generation, whereas antibody 10E5, which blocks GPIIb/IIIa but not alpha v beta 3 receptors decreased thrombin generation by approximately 25. Combining antibody LM609, which blocks alpha v beta 3 receptors, with 10E5 increased the inhibition of thrombin generation to approximately 32-41. The platelets from three patients with Glanzmann thrombasthenia, who lacked GPIIb/IIIa receptors but had normal or increased alpha v beta 3 receptors, supported approximately 21 less thrombin generation than normal platelets. We conclude that thrombin generation initiated by tissue factor in the presence of platelets is significantly inhibited by c7E3 Fab, most likely in part through both GPIIb/IIIa and alpha v beta 3 blockade, and that this effect may contribute to its antithrombotic properties.
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机译:鼠/人嵌合单克隆抗体片段 (c7E3 Fab) 阻断 GPIIb/IIIa 和 α v β 3 受体,抑制血小板聚集,并降低冠状动脉血管成形术后缺血事件的发生率。虽然抑制血小板聚集可能是 c7E3 Fab 作用的主要机制,但由于活化的血小板促进凝血酶的产生,因此 c7E3 Fab 也可能减少凝血酶的产生。为了验证这一假设,在由组织因子触发的凝血酶生成测定中测试了 c7E3 Fab 和其他抗血小板药物的作用。c7E3 Fab 对凝血酶生成产生剂量依赖性抑制,在浓度 > 或 = 15 μg/ml 时达到 45-50% 的抑制平台。它还抑制凝血酶-抗凝血酶复合物的形成、凝血酶原片段 F1-2 的产生、血小板衍生的生长因子和血小板因子 4 的释放、凝血酶掺入凝块和微粒形成。抗体 6D1 阻断血小板 GPIb 与血管性血友病因子结合,对凝血酶生成没有影响,而抗体 10E5 阻断 GPIIb/IIIa,但不阻断 α v β 3 受体,使凝血酶生成减少约 25%。将阻断α v β 3受体的抗体LM609与10E5相结合,将凝血酶生成的抑制作用提高到约32-41%。三名缺乏GPIIb/IIIa受体但α v β 3受体正常或升高的Glanzmann血栓无力患者的血小板比正常血小板少约21%。我们得出结论,c7E3 Fab 显着抑制了在血小板存在下由组织因子引发的凝血酶生成,很可能部分通过 GPIIb/IIIa 和 α v β 3 阻断,并且这种作用可能有助于其抗血栓形成特性。
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