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急性心肌梗死的大剂量溶栓治疗。

Bolus fibrinolytic therapy in acute myocardial infarction.

作者信息

Llevadot J, Giugliano R P, Antman E M

机构信息

TIMI Study Group, 333 Longwood Ave, Suite 402, Boston, MA 02115, USA.

出版信息

JAMA. 2001 Jul 25;286(4):442-9. doi: 10.1001/jama.286.4.442.

Abstract

CONTEXT

New bolus fibrinolytics derived from the human tissue-type plasminogen activator (tPA) have emerged as a means of dissolution of occlusive thrombosis associated with acute myocardial infarction.

OBJECTIVE

To review the new bolus fibrinolytic drugs derived from tPA: reteplase, lanoteplase, and tenecteplase.

DATA SOURCES

The MEDLINE, EMBASE, and Current Contents databases were searched for articles from 1983 to 2001, using the index terms pharmacokinetics, pharmacodynamics, plasminogen activator, reteplase, lanoteplase, and tenecteplase. Additional data sources included bibliographies of articles identified on MEDLINE, EMBASE, and Current Content, inquiry of experts and pharmaceutical companies, and preliminary data presented at recent national and international cardiology conferences.

STUDY SELECTION

We selected for review studies that evaluated the pharmacokinetics and pharmacodynamics of reteplase, lanoteplase, and tenecteplase, and assessed the effects of these bolus fibrinolytic drugs on the angiographic and immediate and long-term outcomes of patients. Of 138 articles identified, 38 were analyzed.

DATA EXTRACTION

Data quality was determined by publication in the peer-reviewed literature or presentation at an official cardiology society-sponsored meeting.

DATA SYNTHESIS

Tenecteplase and reteplase are comparable with accelerated infusion recombinant tPA in terms of efficacy and safety but more convenient because they are administered by bolus injection. Lanoteplase and heparin bolus plus infusion is as effective as tPA with regard to mortality, but the rate of intracranial hemorrhage is significantly higher.

CONCLUSION

Given the ease of administration and the similar outcomes compared with accelerated infusion recombinant tPA, it is likely that a key component of contemporary reperfusion will include a bolus fibrinolytic.

摘要

背景

源自人组织型纤溶酶原激活剂(tPA)的新型大剂量纤溶药物已成为溶解与急性心肌梗死相关的闭塞性血栓的一种手段。

目的

综述源自tPA的新型大剂量纤溶药物:瑞替普酶、拉诺替普酶和替奈普酶。

数据来源

检索MEDLINE、EMBASE和《现刊目次》数据库1983年至2001年的文章,使用的索引词有药代动力学、药效学、纤溶酶原激活剂、瑞替普酶、拉诺替普酶和替奈普酶。其他数据来源包括MEDLINE、EMBASE和《现刊目次》上所确定文章的参考文献、向专家和制药公司咨询以及在近期国内和国际心脏病学会议上展示的初步数据。

研究选择

我们选择进行综述的研究是那些评估瑞替普酶、拉诺替普酶和替奈普酶的药代动力学和药效学,并评估这些大剂量纤溶药物对患者血管造影以及近期和远期预后影响的研究。在检索到的138篇文章中,分析了38篇。

数据提取

数据质量通过发表于同行评审文献或在官方心脏病学会主办会议上的展示来确定。

数据综合

替奈普酶和瑞替普酶在疗效和安全性方面与加速静脉输注重组tPA相当,但因其通过大剂量注射给药而更为方便。拉诺替普酶与肝素大剂量注射加静脉输注在死亡率方面与tPA一样有效,但颅内出血发生率显著更高。

结论

鉴于给药方便且与加速静脉输注重组tPA相比预后相似,当代再灌注治疗的一个关键组成部分可能将包括一种大剂量纤溶药物。

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