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阿司匹林、前列环醇和血小板糖蛋白IIb/IIIa拮抗剂GR144053的抗血小板作用比较,特别提及血小板微聚体的作用。

Comparative antiplatelet effects of aspirin, vapiprost and GR144053, a GPIIb/IIIa antagonist, with a special reference to the role of platelet microaggregates.

作者信息

Matsuno H, Kozawa O, Nagashima S, Kanamaru M, Uematsu T

机构信息

Department of Pharmacology, Gifu University School of Medicine, Japan.

出版信息

Br J Pharmacol. 1999 Jul;127(5):1129-34. doi: 10.1038/sj.bjp.0702651.

Abstract

Microthrombi produced have a potential to form larger thrombi, leading to vascular occlusions. Recently, a new device to easily detect microaggregates using laser-light scattering (LS) has been developed. We adopted this device to comparatively evaluate the inhibitory effects of aspirin (1,3 or 10 mg kg(-1)), vapiprost (0.3, 1 or 3 mg kg(-1)) or GR144053 (0.1, 0.3 or 1 mg kg(-1)) on ex vivo aggregation of hamster platelets in relation to their in vivo antithrombotic effects. A transluminal thrombus was produced in the hamster femoral artery by the photochemical reaction. Each compound was injected i.v. as a bolus 10 min prior to the reaction, showing a dose-dependent antithrombotic effect, i.e. they prolonged the time before the artery occluded. At that time cyclic flow reductions occurred more marked when aspirin or vapiprost was given. At the end of experiments, blood was collected to evaluate the platelet aggregation using both the new LS device and the conventional optical density (OD) method. Many more small aggregates were still formed when the highest dose of aspirin or vapiprost was used as compared with that of GR144053, although suppression of the platelet aggregation using the OD method, prolongation of the occlusion time and the bleeding time were quite similar. In conclusion, a GPIIb/IIIa antagonist markedly suppressed the microthrombi and reduced the cyclic flow reduction. This further indicates the importance of small aggregates as triggers of thrombosis and shows that prevention of their formation may result in improved vascular patency after thrombotic insult.

摘要

所产生的微血栓有可能形成更大的血栓,导致血管阻塞。最近,一种利用激光散射(LS)轻松检测微聚集体的新装置已被开发出来。我们采用该装置来比较评估阿司匹林(1、3或10 mg·kg⁻¹)、前列环素(0.3、1或3 mg·kg⁻¹)或GR144053(0.1、0.3或1 mg·kg⁻¹)对仓鼠血小板体外聚集的抑制作用及其体内抗血栓形成作用。通过光化学反应在仓鼠股动脉中产生腔内血栓。每种化合物在反应前10分钟静脉推注给药,呈现出剂量依赖性抗血栓形成作用,即它们延长了动脉阻塞前的时间。此时,给予阿司匹林或前列环素时,循环血流减少更为明显。实验结束时,采集血液,使用新的激光散射装置和传统的光密度(OD)方法评估血小板聚集。与GR144053相比,使用阿司匹林或前列环素的最高剂量时,仍形成了更多的小聚集体,尽管使用OD方法抑制血小板聚集、延长阻塞时间和出血时间相当相似。总之,一种糖蛋白IIb/IIIa拮抗剂显著抑制了微血栓形成并减少了循环血流减少。这进一步表明小聚集体作为血栓形成触发因素的重要性,并表明预防其形成可能会改善血栓形成损伤后的血管通畅性。

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