解释健康亚洲和高加索人群中 OATP1B1 和 BCRP 等位基因频率的转运体底物药代动力学的种族变异性：一种机制建模分析。

Explaining Ethnic Variability of Transporter Substrate Pharmacokinetics in Healthy Asian and Caucasian Subjects with Allele Frequencies of OATP1B1 and BCRP: A Mechanistic Modeling Analysis.

机构信息

Systems Modeling and Simulation, Medicine Design, World Wide Research and Development, Pfizer Inc., Cambridge, MA, USA.

Translational Modeling and Simulation, Biomedicine Design, World Wide Research and Development, Pfizer Inc., Groton, CT, USA.

出版信息

Clin Pharmacokinet. 2018 Apr;57(4):491-503. doi: 10.1007/s40262-017-0568-7.

BACKGROUND

Ethnic variability in the pharmacokinetics of organic anion transporting polypeptide (OATP) 1B1 substrates has been observed, but its basis is unclear. A previous study hypothesizes that, without applying an intrinsic ethnic variability in transporter activity, allele frequencies of transporters cannot explain observed ethnic variability in pharmacokinetics. However, this hypothesis contradicts the data collected from compounds that are OATP1B1 substrates but not breast cancer resistance protein (BCRP) substrates.

OBJECTIVE

The objective of this study is to evaluate a hypothesis that is physiologically reasonable and more consistent with clinical observations.

METHODS

We evaluated if allele frequencies of two transporters (OATP1B1 and BCRP) are key contributors to ethnic variability. In this hypothesis, the same genotype leads to the same activity independent of ethnicity, in contrast to the previous hypothesis of intrinsic ethnic variability in OATP1B1 activity. As a validation, we perform mechanistic pharmacokinetic modeling for SLCO1B1 (encoding OATP1B1) and ABCG2 (encoding BCRP) genotyped pharmacokinetic data from 18 clinical studies with healthy Caucasian and/or Asian subjects.

RESULTS

Simulations based on the current hypothesis reasonably describe SLCO1B1 and ABCG2 genotyped pharmacokinetic time course data for five transporter substrates (atorvastatin, pitavastatin, pravastatin, repaglinide, and rosuvastatin) in Caucasian and Asian populations.

CONCLUSION

This hypothesis covers the observations that can (e.g., ethnic differences in rosuvastatin pharmacokinetics) or cannot (e.g., lack of differences for pitavastatin pharmacokinetics) be explained by the previous hypothesis. It helps to characterize sources of ethnic variability and provides a foundation for predicting ethnic variability in transporter substrate pharmacokinetics.

背景

有机阴离子转运多肽（OATP）1B1 底物的药代动力学存在种族变异性，但其基础尚不清楚。先前的研究假设，在没有应用转运体固有种族变异性的情况下，转运体的等位基因频率不能解释观察到的药代动力学种族变异性。然而，这一假设与从不是乳腺癌耐药蛋白（BCRP）底物但却是 OATP1B1 底物的化合物收集到的数据相矛盾。

目的

本研究旨在评估一个假设，该假设在生理学上是合理的，并且更符合临床观察。

方法

我们评估了两种转运体（OATP1B1 和 BCRP）的等位基因频率是否是种族变异性的主要贡献因素。在这个假设中，相同的基因型导致相同的活性，而与之前 OATP1B1 活性固有种族变异性的假设相反，这种活性与种族无关。作为验证，我们对 SLCO1B1（编码 OATP1B1）和 ABCG2（编码 BCRP）进行了机制药代动力学建模，这些基因分型的药代动力学数据来自 18 项健康白种人和/或亚洲人参与的临床研究。