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QT间期延长药物:其致心律失常风险的机制及临床相关性

QT-interval prolonging drugs: mechanisms and clinical relevance of their arrhythmogenic hazards.

作者信息

Zehender M, Hohnloser S, Just H

机构信息

Innere Medizin III, Universität Freiburg, FRG.

出版信息

Cardiovasc Drugs Ther. 1991 Apr;5(2):515-30. doi: 10.1007/BF03029779.

Abstract

The antiarrhythmic principle of drug-induced QT-interval prolongation is well known. However, with the widespread use of the presently known and new Class III antiarrhythmic agents under investigation, and the growing number of agents not primarily designed as antiarrhythmic drugs that potentially cause QT prolongation, we have also become aware of the proarrhythmic hazards associated with many of these agents. The proarrhythmic risk differs markedly from one agent to another and interferes with many individual clinical variables (e.g., hypokalemia, sinus bradycardia). This paper summarizes the present data on the proarrhythmic risk of drug-induced QT prolongation, including the value and problems of the rate-corrected QT interval, the mechanisms involved in the genesis of proarrhythmia, and the clinical cofactors that facilitate the occurrence of proarrhythmic events. In addition, an extensive database provides information on the known proarrhythmic risk of all currently used QT-prolonging agents.

摘要

药物诱导的QT间期延长的抗心律失常原理是众所周知的。然而,随着目前已知的和正在研究的新型III类抗心律失常药物的广泛使用,以及越来越多并非主要设计为抗心律失常药物但可能导致QT延长的药物的出现,我们也已经意识到与这些药物中的许多药物相关的促心律失常风险。不同药物的促心律失常风险差异显著,并且受到许多个体临床变量(如低钾血症、窦性心动过缓)的影响。本文总结了目前关于药物诱导的QT延长的促心律失常风险的数据,包括校正心率的QT间期的价值和问题、促心律失常发生的机制以及促进促心律失常事件发生的临床辅助因素。此外,一个广泛的数据库提供了关于所有目前使用的QT延长药物已知促心律失常风险的信息。

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