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新生儿和婴儿在西沙必利治疗前及治疗期间的24小时心电图。

24-hour electrocardiogram before and during cisapride treatment in neonates and infants.

作者信息

Zamora Samuel A, Belli Dominique C, Friedli Beat, Jaeggi Edgar

机构信息

Gastroenterology Unit, Department of Pediatrics, University Hospital, Geneva, Switzerland.

出版信息

Biol Neonate. 2004;85(4):229-36. doi: 10.1159/000076237. Epub 2004 Jan 16.

Abstract

We studied prospectively the effects of cisapride on heart rate and rhythm using standard ECG and 24-hour ECG recordings in term and preterm neonates and infants. We studied subjects with gastroesophageal reflux disease (apparent life-threatening events, apneas, bradycardias) before and 3 days after starting cisapride (0.8 mg/kg/day in 4 doses). We performed standard ECGs for determination of corrected Q-T interval (QTc) and Q-T dispersion (QTd) and 24-hour ECG recordings for analysis of heart rate, heart rate variability, and heart rhythm. Fourteen term and 17 preterm subjects (gestational age range 28-36 weeks) were studied at a median chronological age of 29 (range 3-132) days. Cisapride significantly increased the QTc in preterm infants (before vs. after: 408 +/- 7 vs. 433 +/- 7 ms, p = 0.001). Two preterm and 1 term infant had a QTc >450 ms before cisapride. Four preterm (4/15 = 27%) and 2 term (2/13 = 15%) subjects had a QTc >450 ms on cisapride. After cisapride the QTd remained normal, and no relevant arrhythmias were documented on Holter recordings. Cisapride significantly decreased peak and mean heart rates of all study subjects without affecting the heart rate variability, while it increased the minimal heart rate of preterm infants only (before vs. after: 66 +/- 5 vs. 78 +/- 5 bpm, p = 0.02). The maximally measured R-R intervals (pauses) decreased after cisapride in preterm infants (before vs. after: 1.33 +/- 0.2 s vs. 1.05 +/- 0.2 s, p = 0.04). Although cisapride did cause a significant prolongation of the ventricular action potential duration in preterm infants, the QTd remained unaffected, and no clinically relevant arrhythmias were documented in this small sample. On the other hand, cisapride had a direct lowering effect on the maximal and mean heart rates of both term and preterm infants, while the drug increased the minimal heart rate and reduced the severity of bradycardia episodes in preterm infants.

摘要

我们采用标准心电图和24小时心电图记录,对足月儿、早产儿和婴儿进行前瞻性研究,以观察西沙必利对心率和心律的影响。我们研究了患有胃食管反流病(明显危及生命的事件、呼吸暂停、心动过缓)的受试者,在开始使用西沙必利(0.8毫克/千克/天,分4次给药)之前及之后3天进行观察。我们进行标准心电图检查以测定校正QT间期(QTc)和QT离散度(QTd),并进行24小时心电图记录以分析心率、心率变异性和心律。共研究了14名足月儿和17名早产儿(胎龄范围28 - 36周),中位实际年龄为29(范围3 - 132)天。西沙必利使早产儿的QTc显著延长(用药前与用药后:408±7毫秒对433±7毫秒,p = 0.001)。两名早产儿和一名足月儿在使用西沙必利前QTc>450毫秒。使用西沙必利后,15名早产儿中有4名(4/15 = 27%)、13名足月儿中有2名(2/13 = 15%)的QTc>450毫秒。使用西沙必利后QTd保持正常,动态心电图记录未发现相关心律失常。西沙必利显著降低了所有研究对象的峰值心率和平均心率,但不影响心率变异性,而仅增加了早产儿的最低心率(用药前与用药后:66±5次/分钟对78±5次/分钟,p = 0.02)。使用西沙必利后,早产儿的最大测量R - R间期(停搏)缩短(用药前与用药后:1.33±0.2秒对1.05±0.2秒,p = 0.04)。尽管西沙必利确实使早产儿的心室动作电位持续时间显著延长,但QTd未受影响,且在这个小样本中未记录到临床相关的心律失常。另一方面,西沙必利对足月儿和早产儿的最大心率和平均心率有直接降低作用,同时该药物增加了早产儿的最低心率并减轻了心动过缓发作的严重程度。

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