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华法林治疗中凝血酶原反应的贝叶斯药代动力学/药效学预测:初步评估

Bayesian pharmacokinetic/pharmacodynamic forecasting of prothrombin response to warfarin therapy: preliminary evaluation.

作者信息

Svec J M, Coleman R W, Mungall D R, Ludden T M

出版信息

Ther Drug Monit. 1985;7(2):174-80. doi: 10.1097/00007691-198506000-00006.

DOI:10.1097/00007691-198506000-00006
PMID:4024210
Abstract

The ability of a pharmacokinetic/pharmacodynamic Bayesian forecasting computer program to predict prothrombin response to warfarin therapy was investigated. The performance of the program was evaluated retrospectively in an inpatient study population of 45 subjects. Predictions of prothrombin response at discharge, based on zero to five serially measured prothrombin ratios, were compared. Precision of prediction was measured by root mean squared error (rmse), bias was measured by average prediction error, and significance (p less than 0.05) was determined by 95% confidence intervals and correlation coefficients. Eleven (3.8%) predictions exceeded established limitations of the pharmacokinetic/pharmacodynamic model and were excluded from data analysis. Correlations between measured and predicted prothrombin ratios for all methods were significant. The five prothrombin ratio feedbacks provided the most accurate predictions (rmse 0.219). These predictions were significantly better than the population parameter (rmse 0.418), one (rmse 0.401), and two (rmse 0.459) prothrombin ratio feedback predictions. The predictions based on population parameters and one prothrombin ratio feedback were significantly biased. When provided with sufficient feedback, the bias was not apparent and the predictive performance improved with each additional prothrombin ratio. The predictive performance of the four and five prothrombin ratio feedbacks is sufficient to provide clinically useful dosage guidelines early in the course of warfarin therapy. The population parameter estimates require further delineation in order to improve the performance of limited prothrombin ratio feedback predictions.

摘要

研究了药代动力学/药效学贝叶斯预测计算机程序预测华法林治疗中凝血酶原反应的能力。在一项包含45名受试者的住院患者研究群体中,对该程序的性能进行了回顾性评估。比较了基于零至五次连续测量的凝血酶原比值对出院时凝血酶原反应的预测。预测精度通过均方根误差(rmse)衡量,偏差通过平均预测误差衡量,显著性(p<0.05)通过95%置信区间和相关系数确定。11个(3.8%)预测超出了药代动力学/药效学模型的既定限制,被排除在数据分析之外。所有方法测量的和预测的凝血酶原比值之间的相关性均具有显著性。五次凝血酶原比值反馈提供了最准确的预测(rmse为0.219)。这些预测明显优于群体参数(rmse为0.418)、一次(rmse为0.401)和两次(rmse为0.459)凝血酶原比值反馈预测。基于群体参数和一次凝血酶原比值反馈的预测存在显著偏差。当提供足够的反馈时,偏差不明显,并且随着每次增加的凝血酶原比值,预测性能会提高。四次和五次凝血酶原比值反馈的预测性能足以在华法林治疗过程早期提供临床上有用的剂量指南。为了提高有限凝血酶原比值反馈预测的性能,需要进一步明确群体参数估计。

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