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[心脏病诊断与治疗干预中血小板功能的改变]

[Modification of thrombocyte function in diagnostic and therapeutic interventions in cardiology].

作者信息

Darius H, Beisiegel B, Erbel R, Rupprecht H J, Hafner G, Pop T, Treese N, Meyer J

机构信息

II. Medizinische Klinik und Poliklinik, Johannes Gutenberg-Universität, Mainz.

出版信息

Z Kardiol. 1991;80 Suppl 5:65-70.

PMID:1776338
Abstract

In patients with coronary heart disease platelet activity may be pathologically increased. Administration of platelet inhibitor drugs is an established treatment principle. The interactions between platelet activation, platelet inhibitor drugs like acetylsalicylic acid (ASA) or molsidomine and the endogenous fibrinolysis were studied in three trials. Platelet aggregation and thromboxane synthesis are dose- dependently inhibited after oral intake of ASA (0, 10, 30, 100 or 500 mg/d) Additional intake of the antianginal agent and nitric oxide donator Molsidomine (8 mg) results in a synergistic platelet inhibitor effect characterized by a significantly delayed aggregation response. In a group of patients with coronary artery stenoses platelet activity was markedly enhanced, when compared to healthy individuals. During physical exercise platelet activity was even further enhanced and plasma t-PA-activity was increased by a factor of 2.2. The stimulation of the endogenous fibrinolytic system was markedly reduced when compared to healthy subjects. Following successful coronary angioplasty 393 patients were randomized to receive either molsidomine (2 x 8 mg/d) or ASA (1 x 500 mg/d) plus nifedipine (3 x 20 mg/d). Coronary angiography performed after the 6 month treatment period revealed a restenosis rate of 29% in the molsidomine group and of 33% in patients treated with ASA + nifedipine. This difference was not statistically significant.

摘要

在冠心病患者中,血小板活性可能会病理性升高。给予血小板抑制剂药物是既定的治疗原则。在三项试验中研究了血小板活化、血小板抑制剂药物如乙酰水杨酸(ASA)或吗多明与内源性纤维蛋白溶解之间的相互作用。口服ASA(0、10、30、100或500mg/d)后,血小板聚集和血栓素合成呈剂量依赖性抑制。额外摄入抗心绞痛药物和一氧化氮供体吗多明(8mg)会产生协同的血小板抑制作用,其特征为聚集反应明显延迟。与健康个体相比,一组冠状动脉狭窄患者的血小板活性明显增强。在体育锻炼期间,血小板活性进一步增强,血浆组织型纤溶酶原激活物(t-PA)活性增加了2.2倍。与健康受试者相比,内源性纤维蛋白溶解系统的刺激明显减少。在成功进行冠状动脉血管成形术后,393例患者被随机分为接受吗多明(2×8mg/d)或ASA(1×500mg/d)加硝苯地平(3×20mg/d)治疗。治疗6个月后进行的冠状动脉造影显示,吗多明组的再狭窄率为29%。接受ASA+硝苯地平治疗的患者再狭窄率为33%。这一差异无统计学意义。

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