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局限性:使用血浆浓度和浓度-时间曲线下部分面积估算健康成年人转运体活性的非索非那定有限采样策略。

Limitations of fexofenadine limited sampling strategy using plasma concentrations and partial area under the concentration-time curve to estimate transporter activity in healthy adults.

出版信息

Int J Clin Pharmacol Ther. 2023 Jun;61(6):262-269. doi: 10.5414/CP204380.

DOI:10.5414/CP204380
PMID:37042268
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10339714/
Abstract

OBJECTIVE

Fexofenadine is a probe drug used to phenotype P-glycoprotein (P-gp) and organic anion transporting polypeptide (OATP) 1B1/3 activities. This study evaluated a limited sampling strategy using plasma concentrations and/or partial area under the concentration versus time curves (AUCs) to estimate systemic exposure and, potentially, P-gp and OATP1B1/3 activities.

MATERIALS AND METHODS

Plasma concentration versus time data were obtained from 53 healthy adult participants (22 females) from four published studies. Participants were administered a single oral dose (120 mg) of fexofenadine during constitutive P-gp and OATP1B1/3 conditions. Concentration-time data were divided into a training (n = 18) and validation (n = 35) set. Backwards stepwise linear regression generated single-, 2-timepoint, and partial AUC limited sampling models (LSMs). Noncompartmental analysis methods were used to determine total AUC (AUC) from intensive sampling. Coefficient of determination (r) and bias and precision were assessed via relative percent mean prediction error (%MPE), relative percent mean absolute error (%MAE), and relative percent root mean square error (%RMSE).

RESULTS

The geometric mean observed AUC was 1,680 ng×h/mL. The 2-, 5-, and 2- plus 5-hour LSMs met backwards stepwise linear regression significance (p < 0.15) to remain in the model but had unacceptable %RMSE (17 - 29%). The majority of partial AUC LSMs had unacceptable r (0.21 - 0.83), with all models having unacceptable %MAE (12 - 35%).

CONCLUSION

Fexofenadine limited sampling strategy using single-timepoint, 2-timepoint, and partial AUCs were unable to accurately estimate AUC and thus constitutive P-gp and OATB1B1/3 activities in healthy adults. Timepoints that were not measured or selected may have improved LSM performance.

摘要

目的

非索非那定是一种用于表型 P 糖蛋白(P-gp)和有机阴离子转运多肽(OATP)1B1/3 活性的探针药物。本研究评估了一种使用血浆浓度和/或部分浓度-时间曲线下面积(AUC)的有限采样策略,以估计全身暴露量,并可能评估 P-gp 和 OATP1B1/3 活性。

材料和方法

从四项已发表的研究中获得了 53 名健康成年参与者(22 名女性)的血浆浓度-时间数据。参与者在组成型 P-gp 和 OATP1B1/3 条件下单次口服给予非索非那定 120mg。将浓度-时间数据分为训练(n=18)和验证(n=35)集。向后逐步线性回归生成单一时点、双时间点和部分 AUC 有限采样模型(LSM)。非房室分析方法用于从密集采样中确定总 AUC(AUC)。通过相对平均预测误差(%MPE)、相对平均绝对误差(%MAE)和相对均方根误差(%RMSE)评估决定系数(r)和偏差与精度。

结果

观察到的几何平均 AUC 为 1680ng×h/mL。2、5 和 2 加 5 小时 LSM 通过向后逐步线性回归显著性(p<0.15)进入模型,但具有不可接受的%RMSE(17-29%)。大多数部分 AUC LSM 的 r 不可接受(0.21-0.83),所有模型的%MAE 均不可接受(12-35%)。

结论

使用单一时点、双时间点和部分 AUC 的非索非那定有限采样策略无法准确估计 AUC,因此无法在健康成年人中准确估计组成型 P-gp 和 OATB1B1/3 活性。未测量或选择的时间点可能会提高 LSM 性能。