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抗组胺药对心脏钾通道及其他通道的阻滞作用。

Blockade of cardiac potassium and other channels by antihistamines.

作者信息

Delpón E, Valenzuela C, Tamargo J

机构信息

Department of Pharmacology, School of Medicine, Universidad Complutense, Madrid, Spain.

出版信息

Drug Saf. 1999;21 Suppl 1:11-8; discussion 81-7. doi: 10.2165/00002018-199921001-00003.

Abstract

The use of terfenadine and astemizole, two long-acting nonsedating histamine H1 receptor antagonists, has been associated with prolongation of the QT interval, development of ventricular arrhythmias, particularly torsade de pointes, and sudden cardiac death. Both drugs block the rapidly activating component of the delayed rectifier channel, I(Kr). At much higher concentrations, they also block several other cardiac channels (Na+, Ca2+, K+). Since many other antihistamines can also block one or other of the cardiac ion currents (e.g. loratadine blocks the human cardiac K+ channel, hKv1.5, with the same potency as terfenadine), these results are also reviewed and their clinical relevance discussed. Because of the proarrhythmic risk, some antihistamines should be taken only at the recommended doses and avoided in patients with liver disease or in those taking medications that inhibit oxidative cytochrome P-450 enzymes. These drugs should also be avoided in those with the congenital long QT syndrome or with secondary forms of delayed repolarisation (hypokalaemia, bradycardia, drug-induced QT prolongation). Identification of predisposing factors could enable physicians to anticipate, and thereby avoid, this potentially lethal complication of antihistamine therapy.

摘要

特非那定和阿司咪唑这两种长效非镇静性组胺H1受体拮抗剂的使用,已与QT间期延长、室性心律失常尤其是尖端扭转型室速的发生以及心源性猝死相关。这两种药物均阻断延迟整流钾通道I(Kr)的快速激活成分。在高得多的浓度下,它们还会阻断其他几种心脏通道(Na+、Ca2+、K+)。由于许多其他抗组胺药也能阻断一种或另一种心脏离子电流(例如氯雷他定阻断人类心脏钾通道hKv1.5的效力与特非那定相同),因此对这些结果也进行了综述并讨论了其临床相关性。由于存在致心律失常风险,一些抗组胺药应仅按推荐剂量服用,肝病患者或正在服用抑制细胞色素P-450氧化酶药物的患者应避免使用。先天性长QT综合征患者或有继发性延迟复极(低钾血症、心动过缓、药物性QT间期延长)的患者也应避免使用这些药物。识别易感因素可使医生能够预测并从而避免抗组胺药治疗这种潜在的致命并发症。

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