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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Magnitude and time course of platelet inhibition with Aggrenox(R) and Aspirin in patients after ischemic stroke: the AGgrenox versus Aspirin Therapy Evaluation (AGATE) trial.
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Magnitude and time course of platelet inhibition with Aggrenox(R) and Aspirin in patients after ischemic stroke: the AGgrenox versus Aspirin Therapy Evaluation (AGATE) trial.

机译:缺血性卒中患者使用Aggrenox(R)和阿司匹林抑制血小板的大小和时间过程:AGgrenox与阿司匹林治疗评估(AGATE)试验。

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摘要

The European Stroke Prevention Study showed greater stroke prevention for Aggrenox(R) than either for aspirin or dipyridamole alone. To test whether Aggrenox(R) has superior antiplatelet properties to aspirin alone we conducted the AGgrenox versus Aspirin Therapy Evaluation (AGATE) trial. Forty patients with prior ischemic stroke not taking aspirin for at least 30 days were randomized to Aggrenox(R) (2 pills/daily) or aspirin (81 mg plus matching placebo/daily) for 30 days. Platelet function was assessed at baseline, 24 h, and days 3, 7, 15, and 30 by aggregometry, flow cytometry and cartridge-based analyzers. Both Aggrenox(R) and aspirin provided fast and sustained platelet inhibition. Aggrenox(R), however, especially after 15 days, showed significant prolongation of the closure time (P=0.04), diminished expression of platelet/endothelial cell adhesion molecule-1 (PECAM-1) (P=0.01), glycoprotein IIb (GPIIb) antigen (P=0.02), and GPIIb/IIIa activity (P=0.01) by PAC-1 C antibody, CD63 (P=0.03), as well as inhibition of Protease Activated Receptors (PAR-1) associated with intact (SPAN12, P=0.01) and cleaved (WEDE15, P=0.01) thrombin receptors as compared with aspirin. Surprisingly, GPIb expression increased, especially after aspirin. In the randomized trial of small sample size, aspirin and Aggrenox(R) produced fast and sustained platelet inhibition. In 25 of 90 direct comparisons, Aggrenox(R) was superior to aspirin, whereas in 4 of 90, aspirin was superior to Aggrenox(R). In 61 of 90 direct comparisons, aspirin and Aggrenox(R) were equivalent. Aggrenox(R) was associated with a profound reduction of PAR-1 receptors, an observation that may be related to the greater clinical benefit of Aggrenox(R) compared with Aspirin in preventing recurrent stroke.
机译:欧洲中风预防研究表明,与单独使用阿司匹林或潘生丁相比,对Aggrenox(R)的中风预防作用更大。为了测试Aggrenox(R)是否具有比单独使用阿司匹林更好的抗血小板特性,我们进行了AGgrenox与阿司匹林治疗评估(AGATE)试验。 40名先前有缺血性中风的患者至少30天未服用阿司匹林,被随机分配至Aggrenox?(每天2片)或阿司匹林(81 mg加相匹配的安慰剂/每天)30天。通过血凝法,流式细胞术和基于盒的分析仪在基线,24小时以及第3、7、15和30天评估血小板功能。和阿司匹林均可提供快速而持续的血小板抑制作用。然而,尤其是15天后,Aggrenox(R)表现出明显的闭合时间延长(P = 0.04),血小板/内皮细胞粘附分子-1(PECAM-1)(P = 0.01),糖蛋白IIb( PAC-1 C抗体CD63(P = 0.03)对GPIIb)抗原(P = 0.02)和GPIIb / IIIa活性(P = 0.01)的影响,以及对与完整相关的蛋白酶激活受体(PAR-1)的抑制(与阿司匹林相比,SPAN12,P = 0.01)并裂解(WEDE15,P = 0.01)凝血酶受体。出人意料的是,GPIb表达增加,尤其是在阿司匹林后。在小样本量的随机试验中,阿司匹林和Aggrenox产生了快速而持续的血小板抑制作用。在90个直接比较中,有25个优于Aspirn,而在90个中有4个,Aspirin优于Aggrenox。在90个直接比较中的61个中,阿司匹林和Aggrenox相当。 Aggrenox(R)与PAR-1受体的大量减少有关,这一观察结果可能与Aggrenox(R)相比阿司匹林在预防复发性中风方面具有更大的临床益处有关。

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