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西沙必利对早产儿校正QT间期和QT离散度的影响。

The effect of cisapride on the corrected QT interval and QT dispersion in premature infants.

作者信息

Cools F, Benatar A, Bougatef A, Vandenplas Y

机构信息

Academic Hospital, Free University of Brussels, Brussels, Belgium.

出版信息

J Pediatr Gastroenterol Nutr. 2001 Aug;33(2):178-81. doi: 10.1097/00005176-200108000-00015.

Abstract

BACKGROUND

Cisapride is used frequently in premature neonates as a gastrointestinal prokinetic drug. Concerns exist, however, about its safety because of its effect on the QT interval. Premature infants could be at higher risk for side effects because of their immaturity. This prospective study investigated the pharmacokinetics of cisapride and its effects on corrected QT interval (QTc) and QT dispersion in premature infants.

METHODS

Electrocardiogram examination was performed just before and after 72 hours of treatment with cisapride (0.2 mg/kg per dose, four times daily) in 10 premature infants. Trough and anticipated peak plasma level of cisapride and norcisapride were quantified after 72 hours of treatment. Results were compared with a cohort of 41 term infants aged 0 to 3 months receiving cisapride treatment.

RESULTS

The QTc interval increased significantly from 423 ms to 461 ms after 72 hours of treatment (P = 0.0007). No effect was seen on QT dispersion (44.3 ms vs. 45.9 ms). The change in QTc interval was inversely related to postnatal age (R2 = 0.52; P = 0.02), whereas there was no correlation with gestational age or plasma levels of cisapride or norcisapride. Trough and anticipated peak plasma levels of cisapride and norcisapride were significantly higher in the premature infants compared with the term infants aged 0 to 3 months (P < 0.001).

CONCLUSIONS

Premature infants less than 1 month of age could be at higher risk for cardiac side effects of cisapride when used in the same dosage as in older infants. The daily dose should be reduced (0.1 mg/kg per dose, maximum four times daily), and the QTc interval should be monitored closely. The benefits and safety of cisapride in premature infants less than 1 month of age should be reconsidered.

摘要

背景

西沙必利作为一种胃肠动力药物,常用于早产儿。然而,由于其对QT间期的影响,人们对其安全性存在担忧。早产儿因其不成熟可能面临更高的副作用风险。这项前瞻性研究调查了西沙必利在早产儿中的药代动力学及其对校正QT间期(QTc)和QT离散度的影响。

方法

对10名早产儿在西沙必利治疗72小时前后(0.2mg/kg每剂,每日4次)进行心电图检查。治疗72小时后对西沙必利和去甲西沙必利的谷浓度和预期峰浓度进行定量分析。将结果与41名0至3个月接受西沙必利治疗的足月儿队列进行比较。

结果

治疗72小时后,QTc间期从423毫秒显著增加到461毫秒(P = 0.0007)。未观察到对QT离散度的影响(44.3毫秒对45.9毫秒)。QTc间期的变化与出生后年龄呈负相关(R2 = 0.52;P = 0.02),而与胎龄、西沙必利或去甲西沙必利的血浆水平无关。与0至3个月的足月儿相比,早产儿中西沙必利和去甲西沙必利的谷浓度和预期峰浓度显著更高(P < 0.001)。

结论

1月龄以下的早产儿在使用与较大婴儿相同剂量的西沙必利时,可能面临更高的心脏副作用风险。每日剂量应减少(0.1mg/kg每剂,每日最大4次),并应密切监测QTc间期。应重新考虑西沙必利在1月龄以下早产儿中的益处和安全性。

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