Reilly I A, FitzGerald G A
Division of Clinical Pharmacology, Vanderbilt University, Nashville.
Drugs. 1988 Feb;35(2):154-76. doi: 10.2165/00003495-198835020-00005.
Although other mechanisms may be contributory, the antithrombotic properties of aspirin derive predominantly from its platelet-inhibitory effects. These are mediated via irreversible acetylation of platelet cyclo-oxygenase with subsequent blockade of platelet thromboxane synthesis. Long term administration of doses of aspirin as low as 20mg daily depresses platelet thromboxane formation by more than 90%; however, higher doses appear to be necessary to prevent thromboxane-dependent platelet activation in vivo. While there is evidence of biochemical selectivity with low doses of aspirin, significant reduction of the platelet-inhibitory eicosenoid, prostacyclin, occurs even at dosages ranging from 20 to 40mg daily. The ability of aspirin to prevent the occurrence or recurrence of vaso-occlusion has been extensively investigated. In the secondary prevention of myocardial infarction 7 placebo-controlled trials involving more than 15,000 patients have been completed. The dose of aspirin varied from 300 to 1500mg daily. Although none of the individual trials produced statistically significant reductions in total or coronary mortality, taken together the results are highly suggestive of a beneficial effect of aspirin. Similarly, 2 recent studies in patients with unstable angina demonstrated a protective effect of aspirin against acute myocardial infarction and death. While each study employed widely different doses of aspirin (324mg and 1250mg daily) similar reductions in mortality were reported. The effects of aspirin on the prevention of coronary artery bypass graft occlusion have been evaluated in 9 trials. Aspirin in doses of 100 to 975mg daily was shown to be of benefit in preventing early (less than 6 months) graft occlusion, particularly when therapy was started within 24 hours of operation. In patients with prosthetic vascular grafts of the lower limbs, aspirin has been shown to reduce platelet deposition, however further controlled trials will be required to establish the patient population most likely to benefit and, as in all these studies, the optimum dose of aspirin to employ. In patients with prosthetic heart valves it is clear that aspirin alone is insufficient to prevent thromboembolic complications and when administered as an adjunct to anticoagulant therapy it is associated with a high incidence of bleeding. In contrast, there is convincing evidence from several studies for the efficacy of aspirin in doses of 990 to 1300mg daily in the prevention of stroke and death in patients with transient ischaemic attacks.(ABSTRACT TRUNCATED AT 400 WORDS)
尽管可能还有其他机制起作用,但阿司匹林的抗血栓特性主要源于其对血小板的抑制作用。这些作用是通过血小板环氧化酶的不可逆乙酰化介导的,随后阻断血小板血栓素的合成。每天服用低至20毫克的阿司匹林,长期给药可使血小板血栓素的生成减少90%以上;然而,似乎需要更高剂量才能在体内防止血栓素依赖性血小板激活。虽然有证据表明低剂量阿司匹林具有生化选择性,但即使每天服用20至40毫克的剂量,血小板抑制性类二十烷酸前列环素也会显著减少。阿司匹林预防血管闭塞发生或复发的能力已得到广泛研究。在心肌梗死的二级预防中,已经完成了7项涉及超过15000名患者的安慰剂对照试验。阿司匹林的剂量从每天300毫克到1500毫克不等。虽然没有一项单独的试验在总死亡率或冠状动脉死亡率方面产生统计学上的显著降低,但综合起来,结果强烈暗示阿司匹林有有益作用。同样,最近两项针对不稳定型心绞痛患者的研究表明,阿司匹林对预防急性心肌梗死和死亡有保护作用。虽然每项研究使用的阿司匹林剂量差异很大(每天324毫克和1250毫克),但报告的死亡率降低情况相似。阿司匹林对预防冠状动脉搭桥移植血管闭塞的作用已在9项试验中进行了评估。每天服用100至975毫克剂量的阿司匹林被证明对预防早期(不到6个月)移植血管闭塞有益,特别是在手术24小时内开始治疗时。在下肢人工血管移植患者中,阿司匹林已被证明可减少血小板沉积,然而,需要进一步的对照试验来确定最可能受益的患者群体,并且与所有这些研究一样,确定使用的最佳阿司匹林剂量。在人工心脏瓣膜患者中,很明显仅用阿司匹林不足以预防血栓栓塞并发症,并且当作为抗凝治疗的辅助药物使用时,它与高出血发生率相关。相比之下,几项研究有令人信服的证据表明,每天服用990至1300毫克剂量的阿司匹林对预防短暂性脑缺血发作患者的中风和死亡有效。(摘要截取自400字)
