低分子肝素与冠状动脉介入治疗。

Garratt
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引用次数: 0

摘要

25年来,利用细胞培养和动物实验技术进行的基础实验预测,使用低分子量肝素(LMWH)比使用未分离肝素(UFH)具有更好的凝血酶抑制作用。这应该应用于心脏实验室,凝血酶控制对于确保动脉粥样硬化性心脏病患者的安全和最佳治疗性血管成形术至关重要。尽管有很大的兴趣,但很少有有意义的临床研究已经完成,并且在大多数接受选择性或紧急心导管手术的患者中,通过使用低分子肝素而不是UFH来确定实际获益的程度的临床数据有限。在这一点上,现有的数据表明,使用低分子肝素比使用UFH获得的临床优势最小。此外,获得这种适度的优势可能需要在干预前后延长药物治疗的时间。任何益处都可能仅限于冠状动脉介入治疗后不久。另一方面,现有数据表明,尽管在接受低分子肝素治疗的患者中难以测量抗凝血酶的效果,但严重出血应该不是问题,即使与强效血小板抑制剂治疗联合使用也是如此。尽管细胞培养和动物实验表明肝素化合物在限制血管成形术后的内膜增生(从而限制临床再狭窄)方面应该是有效的,但随机临床试验迄今为止未能显示UFH或低分子肝素对再狭窄有任何益处。正在进行的研究将阐明低分子肝素联合强效抗血小板药物作为冠状动脉介入治疗的联合医学辅助手段的使用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Low Molecular Weight Heparin and Coronary Intervention.

For more than 25 years, basic experiments using cell culture and animal experimental techniques have predicted superior thrombin inhibition with use of low molecular weight heparin (LMWH) rather than unfractionated heparin (UFH). This should have application in the cardiac laboratory, where thrombin control is essential to securing a safe and optimal therapeutic angioplasty for patients with atherosclerotic heart disease. Despite much interest, few meaningful clinical studies have been completed and there are limited clinical data to establish the magnitude of benefit actually conferred through use of LMWH rather than UFH among most patients undergoing elective or urgent cardiac catheterization procedures. At this point, the available data suggest minimal clinical advantage is to be gained through the use of LMWH over UFH. Also, obtaining this modest advantage may require an extended period of drug therapy before and after intervention. Any benefit conferred is likely restricted to the period shortly after coronary intervention. On the other hand, available data suggest that serious bleeding should not be problematic despite difficulties measuring that antithrombin effect among patients receiving LMWH, even when it is combined with potent platelet inhibitor therapy. Although cell culture and animal experiments suggest that heparin compounds should be effective in limiting intimal hyperplasia (and therefore clinical restenosis) after angioplasty, randomized clinical trials have failed thus far to show any restenosis benefit for either UFH or LMWH. Ongoing studies will clarify the use of combining LMWH with potent antiplatelet agents as combined medical adjuncts to coronary intervention.

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