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对健康男性志愿者心电图数据的荟萃分析:昼夜及个体内变异性,以及对临床药理学研究中心电图评估规划和统计分析的影响。

A meta-analysis of ECG data from healthy male volunteers: diurnal and intra-subject variability, and implications for planning ECG assessments and statistical analysis in clinical pharmacology studies.

作者信息

Harris R I, Steare S E

机构信息

Johnson and Johnson Pharmaceutical Research and Development, 50-100 Holmers Farm Way, High Wycombe, Buckinghamshire, HP12 4DP, UK.

出版信息

Eur J Clin Pharmacol. 2006 Nov;62(11):893-903. doi: 10.1007/s00228-006-0194-z. Epub 2006 Oct 6.

Abstract

OBJECTIVE

To evaluate the innate variability in key electrocardiography (ECG) parameters from clinical pharmacology studies.

METHODS

Meta-analysis of ECG data from seven clinical pharmacology studies in healthy male volunteers using model building and stepwise multiple regression analyses.

RESULTS

Data from 115 male subjects provided over 2,000 observations for all key ECG parameters from baseline (Day-1) and placebo treatment periods (Day 1). Only heart rate and uncorrected QT showed clear and marked changes over the day. QTcB had greater variability compared to QTcF. 1.4% of QTcB and 0.7% QTcF observations were >430 ms and 0.1% of QTcB and 0% of QTcF observations were >450 ms. We estimated that 8.9% of subjects would have at least one out of eight post-observation QTc value in the range 430-450 ms [assuming QTc mean 385 ms, standard deviation (SD) 20 ms] due to intrinsic variability alone. Time-matched within-subjects observations demonstrated that the SD between measurements taken 1 h apart was less than seen with a longer interval, but there was little increase in variability beyond 1 h. The probability of observing an increase in QTc of 30-60 ms in a subject was estimated as 3.0% and 21.8% for one and eight post-dose observations, respectively. The greater the number of observations used to define baseline the narrower the spread; for QTcF the SD of the baseline value was 17.1 ms for a single assessment, 13.3 ms for the mean of three assessments, and 13.2 ms for the mean of all Day-1 assessments.

CONCLUSIONS

The spontaneous variability in QTc measurements must be taken into account when designing studies and interpreting analyses of ECG data. The categorical analysis of QTc change of 30-60 ms is unlikely to be of any additional value to analyses of central tendency. For standard early clinical pharmacology studies, QTcF should be chosen as the primary correction method, while the mean of three measures taken in the afternoon and evening of Day-1 and pre-dose Day 1 should provide a reliable and representative baseline assessment.

摘要

目的

评估临床药理学研究中关键心电图(ECG)参数的固有变异性。

方法

对健康男性志愿者的七项临床药理学研究中的ECG数据进行荟萃分析,采用模型构建和逐步多元回归分析。

结果

115名男性受试者的数据提供了超过2000次关于基线(第-1天)和安慰剂治疗期(第1天)所有关键ECG参数的观察结果。仅心率和未校正QT在一天内呈现明显且显著的变化。与QTcF相比,QTcB的变异性更大。1.4%的QTcB观察值和0.7%的QTcF观察值>430毫秒,0.1%的QTcB观察值和0%的QTcF观察值>450毫秒。我们估计,仅由于固有变异性,8.9%的受试者在八次观察后的QTc值中至少有一次会处于430 - 450毫秒范围内[假设QTc均值385毫秒,标准差(SD)20毫秒]。受试者内时间匹配观察表明,相隔1小时测量的标准差小于间隔更长时间时的标准差,但超过1小时后变异性几乎没有增加。在一名受试者中观察到QTc增加30 - 60毫秒的概率,单次给药后观察为3.0%,八次给药后观察为21.8%。用于定义基线的观察次数越多,分布范围越窄;对于QTcF,单次评估的基线值标准差为17.1毫秒,三次评估均值的标准差为13.3毫秒,第1天所有评估均值的标准差为13.2毫秒。

结论

在设计研究和解释ECG数据分析时,必须考虑QTc测量的自发变异性。对QTc变化30 - 60毫秒进行分类分析对中心趋势分析不太可能有任何额外价值。对于标准的早期临床药理学研究,应选择QTcF作为主要校正方法,而在第1天下午和晚上以及给药前第1天进行的三次测量的均值应提供可靠且具有代表性的基线评估。

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