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Paradoxical Effect of Aspirin

机译:阿司匹林的矛盾效应

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Low-dose aspirin is an important therapeutic option in the secondary prevention of myocardial infarction (MI) and ischemic stroke, basedon its unique cost-effectiveness and widespread availability. In addition, based on the results of a number of large studies, aspirin is also widely used in the primary prevention of MI. This paper provides an update of the available data to offer greater clarity regarding the risks of aspirin with respect to hemorrhagic stroke. In the secondary prevention of cardiovascular, cerebrovascular, and ischemic events, the evidence supports that the benefits of aspirin treatment significantly outweigh the risk of a major hemorrhage. When considering whether aspirin is appropriate, the absolute therapeutic cardiovascular benefits of aspirin must be balanced with the possible risks associated with its use, being hemorrhagic stroke. Regarding these clinical facts, normal, COX 1 −/−, and COX 2 −/− mice were treated with a wide range of doses of aspirin and studied by induced hemorrhagic time. The results outlined three major conclusions: high doses of aspirin induce hemorrhage, while low doses of aspirin do not. In the absence of COX 1, ultra low doses of aspirin produce an antihemorrhagic effect not observed with intermediate doses. The absence of COX 2 induced a hemorrhagic effect that needs further research, probably originated in compensatory phenomena.
机译:低剂量的阿司匹林基于其独特的成本效益和广泛的可利用性,在二级预防心肌梗塞(MI)和缺血性中风方面是重要的治疗选择。此外,根据许多大型研究的结果,阿司匹林还被广泛用于MI的一级预防。本文提供了可用数据的更新,以更清晰地了解阿司匹林在出血性中风方面的风险。在心血管,脑血管和缺血事件的二级预防中,有证据表明阿司匹林治疗的益处大大超过了发生大出血的风险。在考虑阿司匹林是否合适时,必须权衡阿司匹林对心血管的绝对治疗益处和与出血有关的可能风险,例如出血性中风。关于这些临床事实,对正常,COX 1-/-和COX 2-/-小鼠用各种剂量的阿司匹林治疗,并通过诱发的出血时间进行研究。结果概述了三个主要结论:大剂量阿司匹林可引起出血,而小剂量阿司匹林则不会。在没有COX 1的情况下,超低剂量的阿司匹林可产生中等剂量未观察到的抗出血性作用。缺乏COX 2会引起出血效应,需要进一步研究,可能是由于代偿现象。

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