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药物诱导的QT间期延长和尖端扭转型室速:QT列线图的评估

Drug-induced QT prolongation and torsades de pointes: evaluation of a QT nomogram.

作者信息

Chan A, Isbister G K, Kirkpatrick C M J, Dufful S B

机构信息

School of Pharmacy, University of Queensland, Brisbane, Australia.

出版信息

QJM. 2007 Oct;100(10):609-15. doi: 10.1093/qjmed/hcm072. Epub 2007 Sep 19.

Abstract

BACKGROUND

Although QT prolongation is associated with increased risk of torsade de pointes (TdP), the precise relationship is not well defined.

AIM

To evaluate the performance of a QT nomogram in assessing the risk of TdP from QT-RR combinations.

DESIGN

Systematic review.

METHODS

We systematically searched MEDLINE/EMBASE for cases of drug-induced TdP. Controls were patients taking non-cardiotoxic drugs in overdose. Inclusion criteria were definite TdP, normal ECG before or after the event, association with a drug/toxin and QT-RR measurements available. The upper bound of a QT-RR cloud diagram developed from human preclinical studies was converted into a QT nomogram [QT vs. heart rate (HR)]. QT-HR combinations for TdP cases and controls were plotted with the QT nomogram, and curves corresponding to a QTc = 440 ms and QTc = 500 ms for comparison (Bazett's correction).

RESULTS

We identified 129 cases of TdP. TdP cases occurred at lower HR values with longer QT intervals, with most cases occurring at HR 30-90 bpm. Controls were more evenly distributed, with HR 40-160 bpm. The sensitivity and specificity of the QT nomogram were 96.9% (95%CI 93.9-99.9) and 98.7% (95%CI 96.8-100), respectively. For Bazett QTc = 440 ms, sensitivity and specificity were 98.5% (95%CI 96.3-100) and 66.7% (95%CI 58.6-74.7), respectively, whereas for Bazett QTc =500 ms they were 93.8% (95%CI 89.6-98.0) and 97.2% (95%CI 94.3-100), respectively.

DISCUSSION

The QT nomogram is a clinically relevant risk assessment tool that accurately predicts arrhythmogenic risk for drug-induced QT prolongation. Further prospective evaluation of the nomogram is needed.

摘要

背景

虽然QT间期延长与尖端扭转型室速(TdP)风险增加相关,但确切关系尚不明确。

目的

评估QT列线图在根据QT-RR组合评估TdP风险方面的性能。

设计

系统评价。

方法

我们系统检索MEDLINE/EMBASE以查找药物诱导的TdP病例。对照为过量服用非心脏毒性药物的患者。纳入标准为明确的TdP、事件前后心电图正常、与药物/毒素相关且有QT-RR测量值。将从人体临床前研究得出的QT-RR云图的上限转换为QT列线图[QT与心率(HR)]。将TdP病例和对照的QT-HR组合绘制在QT列线图上,并绘制对应于校正QTc = 440 ms和QTc = 500 ms的曲线进行比较(Bazett校正)。

结果

我们确定了129例TdP病例。TdP病例发生在心率较低且QT间期较长时,大多数病例发生在心率30 - 90次/分钟。对照分布更均匀,心率为40 - 160次/分钟。QT列线图的敏感性和特异性分别为96.9%(95%CI 93.9 - 99.9)和98.7%(95%CI 96.8 - 100)。对于Bazett QTc = 440 ms,敏感性和特异性分别为98.5%(95%CI 96.3 - 100)和66.7%(95%CI 58.6 - 74.7),而对于Bazett QTc = 500 ms,它们分别为93.8%(95%CI 89.6 - 98.0)和97.2%(95%CI 94.3 - 100)。

讨论

QT列线图是一种临床相关的风险评估工具,可准确预测药物诱导的QT间期延长的致心律失常风险。需要对该列线图进行进一步的前瞻性评估。

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