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预测个体药代动力学。

Forecasting individual pharmacokinetics.

作者信息

Sheiner L B, Beal S, Rosenberg B, Marathe V V

出版信息

Clin Pharmacol Ther. 1979 Sep;26(3):294-305. doi: 10.1002/cpt1979263294.

Abstract

Often drug dosage may be chosen rationally by use of plasma concentration (CP) as the "therapeutic" end point. The ability to accurately forecast the CP resulting from a dosage regimen is central to choosing that regimen. Tradionally forecasting has been attempted only by accounting for known influences on pharmacokinetics, such as sex, age, and renal disease. One must also adjust for previously observed CPs. Herein, we discuss and explain an approach to both of these tasks, mainly focusing on the latter. The approach balances observed outcomes against prior expectations taking account of observation CP error. For digoxin, use of 1 measured CP, as opposed to none, improves forecast precision for future CPs by 40% (decrement in variance of forecast error), and 2 CPs improve it by 67%. There is also an increase in forecast accuracy (decrement in mean of forecast error) as the number of CPs used increases. After only 2, forecast accuracy and precision are as good as theoretically possible. Moreover, information from CPs is far more valuable for forecasting than that from observable patient features-sex, age, and the like; use of all the latter information does not improve accuracy and precision as much as only 1 CP.

摘要

通常,可以通过将血浆浓度(CP)作为“治疗”终点来合理选择药物剂量。准确预测给药方案所产生的血浆浓度的能力对于选择该给药方案至关重要。传统上,仅通过考虑已知的对药代动力学的影响因素(如性别、年龄和肾脏疾病)来尝试进行预测。还必须根据先前观察到的血浆浓度进行调整。在此,我们讨论并解释针对这两项任务的一种方法,主要关注后者。该方法在考虑观察到的血浆浓度误差的情况下,将观察到的结果与先前的预期进行平衡。对于地高辛,使用1次测量的血浆浓度(与不使用相比)可将未来血浆浓度的预测精度提高40%(预测误差方差减小),使用2次血浆浓度可将其提高67%。随着所使用的血浆浓度数量增加,预测准确性(预测误差均值减小)也会提高。仅在使用2次血浆浓度后,预测准确性和精度就达到了理论上的最佳水平。此外,与可观察到的患者特征(如性别、年龄等)相比,血浆浓度信息对于预测更有价值;使用所有后者的信息在提高准确性和精度方面不如仅使用1次血浆浓度。

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