三环类抗抑郁药物中毒:心血管毒性。

H K Ruben Thanacoody, Simon H L Thomas
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引用次数: 154

摘要

三环抗抑郁药仍然是致命药物中毒的常见原因,因为它们的心血管毒性表现为心电图异常、心律失常和低血压。服用过量的多舒平和阿米替林似乎毒性特别大。毒性的主要机制是阻断心脏钠通道,增加心脏动作电位和不应期的持续时间,延迟房室传导。心电图改变包括PR、QRS和QT间期延长,非特异性ST段和T波改变,房室传导阻滞,QRS复合物正面40 ms末端矢量右轴偏移(T 40 ms轴)和Brugada模式(V1-V3导联ST段倾斜抬高伴右束支传导阻滞)。QRS持续时间和t40ms轴的最大变化通常在摄入后12小时内出现,但可能需要长达一周的时间才能消退。窦性心动过速是最常见的心律失常,由于抗胆碱能活性和三环抗抑郁药抑制去甲肾上腺素的摄取,但也可能发生缓速性心律失常(由于房室传导阻滞)和速速性心律失常(室上性和室性)。点扭转不常见。由于α -肾上腺素能阻断,心肌收缩力降低和全身血管阻力降低共同导致低血压。三环类抗抑郁药中毒通常在摄入后24小时内发生危及生命的心律失常和死亡。迅速恶化是常见的。表现时的意识水平是严重并发症最敏感的临床预测指标。尽管QRS持续时间>100 ms和向右t40 ms轴似乎比血浆三环药物浓度更好地预测心血管毒性,但它们在预测并发症方面最多只能具有中等的敏感性和特异性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tricyclic antidepressant poisoning : cardiovascular toxicity.

Tricyclic antidepressants remain a common cause of fatal drug poisoning as a result of their cardiovascular toxicity manifested by ECG abnormalities, arrhythmias and hypotension. Dosulepin and amitriptyline appear to be particularly toxic in overdose. The principal mechanism of toxicity is cardiac sodium channel blockade, which increases the duration of the cardiac action potential and refractory period and delays atrioventricular conduction. Electrocardiographic changes include prolongation of the PR, QRS and QT intervals, nonspecific ST segment and T wave changes, atrioventricular block, right axis deviation of the terminal 40 ms vector of the QRS complex in the frontal plane (T 40 ms axis) and the Brugada pattern (downsloping ST segment elevation in leads V1-V3 in association with right bundle branch block). Maximal changes in the QRS duration and the T 40 ms axis are usually present within 12 hours of ingestion but may take up to a week to resolve. Sinus tachycardia is the most common arrhythmia due to anticholinergic activity and inhibition of norepinephrine uptake by tricyclic antidepressants but bradyarrhythmias (due to atrioventricular block) and tachyarrhythmias (supraventricular and ventricular) may occur. Torsade de pointes occurs uncommonly. Hypotension results from a combination of reduced myocardial contractility and reduced systemic vascular resistance due to alpha-adrenergic blockade. Life-threatening arrhythmias and death due to tricyclic antidepressant poisoning usually occurs within 24 hours of ingestion. Rapid deterioration is common. Level of consciousness at presentation is the most sensitive clinical predictor of serious complications. Although a QRS duration >100 ms and a rightward T 40 ms axis appear to be better predictors of cardiovascular toxicity than the plasma tricyclic drug concentration, they have at best moderate sensitivity and specificity for predicting complications.

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