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糖蛋白IIb/IIIa拮抗剂roxifiban与orbofiban在血栓形成血流模型中抑制血小板反应的疗效比较。

Comparative efficacy between the glycoprotein IIb/IIIa antagonists roxifiban and orbofiban in inhibiting platelet responses in flow models of thrombosis.

作者信息

Mousa Shaker A, Abulencia James P, McCarty Owen J T, Turner Nancy A, Konstantopoulos Konstantinos

机构信息

DuPont Pharmaceuticals Company, 141 & Henry Clay Road, Exp. Station, E400/3470, Wilmington, DE 19880-0400, USA.

出版信息

J Cardiovasc Pharmacol. 2002 Apr;39(4):552-60. doi: 10.1097/00005344-200204000-00011.

Abstract

This study was undertaken to compare the platelet binding characteristics and anti-platelet efficacy of a nonpeptide glycoprotein IIb/IIIa antagonist roxifiban with orbofiban in static and dynamic adhesion and aggregation assays. The results indicate that roxifiban binds with higher affinity to glycoprotein IIb/IIIa receptors and exhibits slower dissociation rates than orbofiban. Furthermore, the platelet inhibitory effects of roxifiban, but not orbofiban, were unaffected by changes in plasma calcium concentrations. Both agents reduced, in a concentration-dependent manner, the size of platelet thrombi deposited onto collagen I upon perfusion of heparinized blood at a shear rate of 1,500/s. At a clinically achievable concentration of 60 nM, roxifiban abrogated the formation of thrombi containing > 20 platelets per thrombus, thereby displaying comparable in vitro efficacy to that achieved by the theoretical maximal abciximab blood concentration (3.5 microg/ml) produced after standard treatment. In contrast, orbofiban, even at 500 nM, was only effective in inhibiting the formation of larger platelet thrombi (> or =150 platelets per thrombus). Pretreatment of surface-anchored platelets with roxifiban (100 nM), but not orbofiban (500 nM), inhibited monocytic THP-1 cell attachment under flow. However, this heterotypic adhesion process was also suppressed when orbofiban (500 nM) was maintained in the perfusion buffer during the entire course of flow experiment. These findings demonstrate roxifiban (unlike orbofiban) is a potent glycoprotein IIb/IIIa antagonist with a long receptor-bound lifetime and prolonged anti-platelet efficacy and may thus be beneficial for the treatment and prevention of acute ischemic syndromes.

摘要

本研究旨在比较非肽糖蛋白IIb/IIIa拮抗剂罗昔非班与奥布非班在静态和动态黏附及聚集试验中的血小板结合特性和抗血小板疗效。结果表明,罗昔非班与糖蛋白IIb/IIIa受体的结合亲和力更高,且与奥布非班相比解离速率更慢。此外,罗昔非班而非奥布非班的血小板抑制作用不受血浆钙浓度变化的影响。在以1500/s的剪切速率灌注肝素化血液时,两种药物均以浓度依赖性方式减少了沉积在I型胶原上的血小板血栓大小。在临床可达到的60 nM浓度下,罗昔非班消除了每个血栓含>20个血小板的血栓形成,从而显示出与标准治疗后产生的理论最大阿昔单抗血药浓度(3.5μg/ml)相当的体外疗效。相比之下,奥布非班即使在500 nM时,也仅对抑制更大的血小板血栓(每个血栓≥150个血小板)形成有效。用罗昔非班(100 nM)而非奥布非班(500 nM)预处理表面锚定的血小板,可在流动条件下抑制单核细胞THP-1细胞黏附。然而,当在整个流动实验过程中将奥布非班(500 nM)维持在灌注缓冲液中时,这种异型黏附过程也受到抑制。这些发现表明,罗昔非班(与奥布非班不同)是一种强效的糖蛋白IIb/IIIa拮抗剂,具有较长的受体结合寿命和延长的抗血小板疗效,因此可能对急性缺血综合征的治疗和预防有益。

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