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A Review of A Priori Regression Models for Warfarin Maintenance Dose Prediction

机译:华法林维持剂量预测的先验回归模型综述

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摘要

A number of a priori warfarin dosing algorithms, derived using linear regression methods, have been proposed. Although these dosing algorithms may have been validated using patients derived from the same centre, rarely have they been validated using a patient cohort recruited from another centre. In order to undertake external validation, two cohorts were utilised. One cohort formed by patients from a prospective trial and the second formed by patients in the control arm of the EU-PACT trial. Of these, 641 patients were identified as having attained stable dosing and formed the dataset used for validation. Predicted maintenance doses from six criterion fulfilling regression models were then compared to individual patient stable warfarin dose. Predictive ability was assessed with reference to several statistics including the R-square and mean absolute error. The six regression models explained different amounts of variability in the stable maintenance warfarin dose requirements of the patients in the two validation cohorts; adjusted R-squared values ranged from 24.2% to 68.6%. An overview of the summary statistics demonstrated that no one dosing algorithm could be considered optimal. The larger validation cohort from the prospective trial produced more consistent statistics across the six dosing algorithms. The study found that all the regression models performed worse in the validation cohort when compared to the derivation cohort. Further, there was little difference between regression models that contained pharmacogenetic coefficients and algorithms containing just non-pharmacogenetic coefficients. The inconsistency of results between the validation cohorts suggests that unaccounted population specific factors cause variability in dosing algorithm performance. Better methods for dosing that take into account inter- and intra-individual variability, at the initiation and maintenance phases of warfarin treatment, are needed.
机译:已经提出了许多使用线性回归方法推导的先验华法林剂量算法。尽管这些剂量算法可能已使用来自同一中心的患者进行了验证,但很少使用从另一中心招募的患者队列来进行验证。为了进行外部验证,利用了两个队列。一个队列由前瞻性试验的患者组成,第二个队列由EU-PACT试验的对照组的患者组成。其中,有641名患者被确定具有稳定剂量,并形成了用于验证的数据集。然后将来自六个符合标准的回归模型的预测维持剂量与各个患者稳定的华法林剂量进行比较。预测能力是根据包括R平方和平均绝对误差在内的几种统计数据进行评估的。六个回归模型解释了在两个验证队列中患者稳定维持华法林剂量所需的不同程度的可变性。调整后的R平方值介于24.2%至68.6%之间。汇总统计数据的概述表明,没有一种给药算法可以被认为是最佳的。来自前瞻性试验的更大的验证队列在六个剂量算法中产生了更一致的统计数据。研究发现,与派生队列相比,所有回归模型在验证队列中的表现都较差。此外,包含药物遗传学系数的回归模型与仅包含非药物遗传学系数的算法之间几乎没有差异。验证队列之间的结果不一致表明,未说明的特定人群因素导致加药算法性能的差异。在华法林治疗的起始和维持阶段,需要考虑个体之间和个体内部差异的更好的给药方法。

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