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基于QT离散度早期检测亚临床蒽环类药物心脏毒性。

Early detection of subclinical anthracycline cardiotoxicity on the basis of QT dispersion.

作者信息

Uchikoba Yohko, Fukazawa Ryuji, Ohkubo Takashi, Maeda Miho, Ogawa Shunichi

机构信息

Department of Pediatrics, Graduate School of Medicine, Nippon Medical School, Japan.

出版信息

J Nippon Med Sch. 2010 Oct;77(5):234-43. doi: 10.1272/jnms.77.234.

Abstract

BACKGROUND

We examined whether dobutamine-stress QT dispersion (QTd) and heart-rate corrected QT dispersion (QTcd) are useful for detecting subclinical anthracycline cardiotoxicity.

METHODS

The subjects were 10 control subjects and 37 patients divided into 4 groups according to cumulative anthracycline dose: non-anthracycline group (group N), 7 patients; low anthracycline cumulative dose group (group L), 8 patients (< 200 mg/m²); medium anthracycline cumulative dose group (group M), 16 patients (200 to < 400 mg/m²); and high cumulative group (group H), 6 patients (≥ 400 mg/m²). Standard 12-lead electrocardiograms were recorded. QTd and QTcd were measured and calculated at rest and after administration of dobutamine at 5 or 30 µg/kg/min. We also estimated cardiac function and cardiac reserve function at rest and after administration of dobutamine at a dose of 5 or 30 µg/kg/min.

RESULTS

At rest, QTd and QTcd were significantly greater in groups M and H. After administration of dobutamine at 30 µg/kg/min, QTd and QTcd were significantly greater in groups L, M, and H. There was good correlation between QTd and the cumulative anthracycline dose; the correlation formula was y=0.051 x + 42.2 (r = 0.81, p < 0.001). The cumulative anthracycline dose of 152.9 mg/m², calculated from the correlation formula, was the cut-off for detection of electrophysiological cardiac abnormalities. Cardiac performance data at rest and dobutamine stress by echocardiography and pulsed Doppler echocardiography are less sensitive for detecting cardiac abnormalities than are QTd and QTcd.

CONCLUSIONS

Dobutamine-stress QTd and QTcd are useful for detecting anthracycline cardiotoxicity and subclinical cardiac abnormality at low cumulative anthracycline doses. We must be aware of the possibility of subclinical myocardial abnormalities in patients with a cumulative anthracycline dose of ≥ 150 mg/m².

摘要

背景

我们研究了多巴酚丁胺负荷试验QT离散度(QTd)和心率校正QT离散度(QTcd)是否有助于检测亚临床蒽环类药物心脏毒性。

方法

研究对象为10名对照者和37例患者,根据蒽环类药物累积剂量分为4组:非蒽环类药物组(N组),7例患者;低蒽环类药物累积剂量组(L组),8例患者(<200mg/m²);中等蒽环类药物累积剂量组(M组),16例患者(200至<400mg/m²);高累积剂量组(H组),6例患者(≥400mg/m²)。记录标准12导联心电图。在静息状态下以及以5或30μg/kg/min的剂量静脉注射多巴酚丁胺后,测量并计算QTd和QTcd。我们还评估了静息状态下以及以5或30μg/kg/min的剂量静脉注射多巴酚丁胺后的心脏功能和心脏储备功能。

结果

静息状态下,M组和H组的QTd和QTcd显著更高。以30μg/kg/min的剂量静脉注射多巴酚丁胺后,L组、M组和H组的QTd和QTcd显著更高。QTd与蒽环类药物累积剂量之间存在良好的相关性;相关公式为y = 0.051x + 42.2(r = 0.81,p < 0.001)。根据该相关公式计算得出的蒽环类药物累积剂量152.9mg/m²是检测心脏电生理异常的临界值。与QTd和QTcd相比,静息状态下以及多巴酚丁胺负荷试验时通过超声心动图和脉冲多普勒超声心动图测得的心脏功能数据对检测心脏异常的敏感性较低。

结论

多巴酚丁胺负荷试验QTd和QTcd有助于检测低蒽环类药物累积剂量时的蒽环类药物心脏毒性和亚临床心脏异常。我们必须意识到,蒽环类药物累积剂量≥150mg/m²的患者存在亚临床心肌异常的可能性。

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