Preincubation-dependent inhibition of organic anion transporting polypeptide 2B1

IF 4.3 3区 医学 Q1 PHARMACOLOGY & PHARMACY
Alli Sinokki, Annika Miinalainen, Wilma Kiander, Heidi Kidron
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引用次数: 0

Abstract

Preincubation with inhibitor in organic anion transporting polypeptide (OATP) in vitro assays may increase the inhibition potency of inhibitors compared to conventional inhibition assays with only short inhibitor coincubation with substrate. The decrease in IC50 may affect prediction of drug-drug interactions (DDI) involving these transporters and inhibitors. Only few drugs, however, have been assessed for the preincubation-dependent inhibition of the OATP2B1 transporter. Therefore, we studied the effect of preincubation on OATP2B1 inhibition with five known OATP2B1 inhibitors (atorvastatin, erlotinib, ezetimibe, ticagrelor and simeprevir) in HEK293 cells transiently overexpressing OATP2B1. IC50 values were determined with and without inhibitor preincubation for 20 min with three different OATP2B1 substrates (dibromofluorescein, DBF; 5-carboxyfluorescein, 5-CF; estrone sulfate). Atorvastatin, ezetimibe, and simeprevir displayed more than 2-fold lower IC50 values after preincubation with at least one of the tested substrates. Altogether, 4 out of 15 inhibitor/substrate combinations exhibited more than 2-fold potentiation of IC50 after inhibitor preincubation. In addition, preincubation by itself, without inhibitor present with the substrate, resulted in more than 50% inhibition of OATP2B1-mediated uptake of DBF and/or 5-CF by atorvastatin, ticagrelor and simeprevir. Thus, erlotinib was the only inhibitor with no indication of potentiation of inhibition by preincubation with any of the tested substrates. In conclusion, preincubation resulted in inhibitor- and substrate-dependent inhibition of OATP2B1. These results support the conclusion that to reduce the risk of false negative DDI prediction, preincubation should be considered also in OATP2B1 inhibition assays.

Abstract Image

对有机阴离子转运多肽 2b1 的预孵育抑制作用。
在有机阴离子转运多肽(OATP)体外试验中与抑制剂预孵育可提高抑制剂的抑制效力,而传统的抑制试验中抑制剂只与底物短时间孵育。IC50 的降低可能会影响涉及这些转运体和抑制剂的药物间相互作用 (DDI) 的预测。然而,只有少数药物对 OATP2B1 转运体的预孵育依赖性抑制作用进行了评估。因此,我们用五种已知的 OATP2B1 抑制剂(阿托伐他汀、厄洛替尼、依折麦布、替卡格雷和西美瑞韦)在瞬时过表达 OATP2B1 的 HEK293 细胞中研究了预孵育对 OATP2B1 抑制的影响。IC50 值是在抑制剂与三种不同的 OATP2B1 底物(二溴荧光素,DBF;5-羧基荧光素,5-CF;硫酸雌酮)预孵育 20 分钟后测定的。阿托伐他汀、依泽替米贝和西美普韦在与至少一种测试底物预孵育后,IC50 值降低了 2 倍以上。抑制剂预孵育后,15 种抑制剂/底物组合中有 4 种的 IC50 增效超过 2 倍。此外,在没有抑制剂与底物同时存在的情况下,预孵育本身会导致阿托伐他汀、替卡格雷和西美瑞韦对 OATP2B1 介导的 DBF 和/或 5-CF 吸收的抑制率超过 50%。因此,厄洛替尼是唯一一种没有迹象表明与任何测试底物预孵育会增强抑制作用的抑制剂。总之,预孵育会导致对 OATP2B1 的抑制作用依赖于抑制剂和底物。这些结果支持这样的结论,即为了降低 DDI 预测假阴性的风险,在 OATP2B1 抑制试验中也应考虑预孵育。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
9.60
自引率
2.20%
发文量
248
审稿时长
50 days
期刊介绍: The journal publishes research articles, review articles and scientific commentaries on all aspects of the pharmaceutical sciences with emphasis on conceptual novelty and scientific quality. The Editors welcome articles in this multidisciplinary field, with a focus on topics relevant for drug discovery and development. More specifically, the Journal publishes reports on medicinal chemistry, pharmacology, drug absorption and metabolism, pharmacokinetics and pharmacodynamics, pharmaceutical and biomedical analysis, drug delivery (including gene delivery), drug targeting, pharmaceutical technology, pharmaceutical biotechnology and clinical drug evaluation. The journal will typically not give priority to manuscripts focusing primarily on organic synthesis, natural products, adaptation of analytical approaches, or discussions pertaining to drug policy making. Scientific commentaries and review articles are generally by invitation only or by consent of the Editors. Proceedings of scientific meetings may be published as special issues or supplements to the Journal.
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