Pretreatment With Rifampicin and Tyrosine Kinase Inhibitor Dasatinib Potentiates the Inhibitory Effects Toward OATP1B1- and OATP1B3-Mediated Transport

Pahwa, Sonia; Alam, Khondoker; Crowe, Alexandra; Farasyn, Taleah; Neuhoff, Sibylle; Hatley, Oliver; Ding, Kai; Yue, Wei

doi:10.1016/j.xphs.2017.03.022

Cited by 49 publications

(58 citation statements)

References 54 publications

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“…Assuming almost complete inhibition of transporter-mediated uptake of pitavastatin at 1 mM rifamycin SV (Thakare et al, 2017), this uninhibited uptake should represent the contribution of passive diffusion to total cellular uptake, which in this case was higher compared with estimates obtained by mechanistic modeling of kinetic data done over short incubation times. Such incomplete inhibition of uptake for pitavastatin has previously been reported in monkey hepatocytes using rifampicin and cyclosporine (Takahashi et al, 2013) and in human hepatocytes using rifampicin (Pahwa et al, 2017) and may reflect the combination of passive diffusion and involvement of transporter uptake not inhibited by these inhibitors.…”

Section: Resultssupporting

confidence: 58%

“…For example, rifampicin in vitro K i values were shown to be several fold higher than the in vivo K i estimated from the clinical DDI data using mechanistic modeling Barnett et al, 2017;Yoshikado et al, 2017). In addition, a number of studies demonstrated potentiation of OATP1B inhibition following preincubation with the inhibitor, trend particularly evident for cyclosporine (Amundsen et al, 2010;Gertz et al, 2013;Izumi et al, 2015;Takahashi et al, 2016;Pahwa et al, 2017) and incorporated in the recent Food and Drug Administration DDI guidance document (https://www.fda.gov/downloads/ Drugs/Guidances/UCM581965.pdf). Although the clinical DDIs with cyclosporine are well recovered with the IC 50 obtained following preincubation (Gertz et al, 2013), there is limited understanding of the significance of preincubation in predicting DDIs of other inhibitor drugs.…”

Section: Introductionmentioning

confidence: 98%

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In Vitro–In Vivo Extrapolation of OATP1B-Mediated Drug–Drug Interactions in Cynomolgus Monkey

Ufuk

Kosa

Gao

et al. 2018

J Pharmacol Exp Ther

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Hepatic organic anion-transporting polypeptides (OATP) 1B1 and 1B3 are clinically relevant transporters associated with significant drug-drug interactions (DDIs) and safety concerns. Given that OATP1Bs in cynomolgus monkey share >90% degree of gene and amino acid sequence homology with human orthologs, we evaluated the in vitro-in vivo translation of OATP1B-mediated DDI risk using this preclinical model. In vitro studies using plated cynomolgus monkey hepatocytes showed active uptake K values of 2.0 and 3.9 M for OATP1B probe substrates, pitavastatin and rosuvastatin, respectively. Rifampicin inhibited pitavastatin and rosuvastatin active uptake in monkey hepatocytes with IC values of 3.0 and 0.54 M, respectively, following preincubation with the inhibitor. Intravenous pharmacokinetics ofH-pitavastatin and H-rosuvastatin (0.2 mg/kg) and the oral pharmacokinetics of cold probes (2 mg/kg) were studied in cynomolgus monkeys ( = 4) without or with coadministration of single oral ascending doses of rifampicin (1, 3, 10, and 30 mg/kg). A rifampicin dose-dependent reduction in i.v. clearance of statins was observed. Additionally, oral pitavastatin and rosuvastatin plasma exposure increased up to 19- and 15-fold at the highest dose of rifampicin, respectively. Use of in vitro IC obtained following 1 hour preincubation with rifampicin (0.54 M) predicted correctly the change in mean i.v. clearance and oral exposure of statins as a function of mean unbound maximum plasma concentration of rifampicin. This study demonstrates quantitative translation of in vitro OATP1B IC to predict DDIs using cynomolgus monkey as a preclinical model and provides further confidence in application of in vitro hepatocyte data for the prediction of clinical OATP1B-mediated DDIs.

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Section: Resultssupporting

confidence: 58%

Section: Introductionmentioning

confidence: 98%

In Vitro–In Vivo Extrapolation of OATP1B-Mediated Drug–Drug Interactions in Cynomolgus Monkey

Ufuk

Kosa

Gao

et al. 2018

J Pharmacol Exp Ther

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“…RIF model‐based in vivo Ki values were 3–4‐fold lower compared with in vitro parameters obtained in human hepatocytes with the corresponding probes and following preincubation with inhibitor ( Figure b ). None of the previous literature RIF inhibition studies considered the preincubation effect, with the exception of the current analysis and recent study . Although the shift in RIF inhibition potency with preincubation was not as prominent as reported in the case of cyclosporine, it reduced the disconnect between in vitro and in vivo inhibition parameter estimates.…”

Section: Discussioncontrasting

confidence: 53%

“…The simulation was based on a two period one‐way crossover study design where in the first period plasma/urine samples of CPI are observed under baseline condition and following a period of washout the same subjects received a single dose of 600 mg RIF and plasma/urine samples of CPI were collected again for analysis. Power curves were calculated for each modified I/Ki ratio by performing a one‐sample paired t ‐test on the ratio of logarithmic transformed AUC following simulation at predefined sample sizes . At each sample size, the simulation and tests were repeated 5,000 times and the power of the test was calculated as the proportion of the simulations during which the null hypothesis was rejected at the significance level (0.05 and 0.01).…”

Section: Methodsmentioning

confidence: 99%

Gaining Mechanistic Insight Into Coproporphyrin I as Endogenous Biomarker for OATP1B‐Mediated Drug–Drug Interactions Using Population Pharmacokinetic Modeling and Simulation

Barnett

Ogungbenro

Ménochet³

et al. 2018

Clin Pharma and Therapeutics

138

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This study evaluated coproporphyrin I (CPI) as a selective endogenous biomarker of OATP1B‐mediated drug–drug interactions (DDIs) relative to clinical probe rosuvastatin using nonlinear mixed‐effect modeling. Plasma and urine CPI data in the presence/absence of rifampicin were modeled to describe CPI synthesis, elimination clearances, and obtain rifampicin in vivo OATP Ki. The biomarker showed stable interoccasion baseline concentrations and low interindividual variability (<25%) in subjects with wildtype SLCO1B1. Biliary excretion was the dominant CPI elimination route (maximal >85%). Estimated rifampicin in vivo unbound OATP Ki (0.13 μM) using CPI data was 2‐fold lower relative to rosuvastatin. Model‐based simulations and power calculations confirmed sensitivity of CPI to identify moderate and weak OATP1B inhibitors in an adequately powered clinical study. Current analysis provides the most detailed evaluation of CPI as an endogenous OATP1B biomarker to support optimal DDI study design; further pharmacogenomic and DDI data with a panel of inhibitors are required.

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“…In vitro, in vivo, and clinical data were extracted. The details of the articles were inserted into tables (shown in Supplementary Materials Tables S1–S9 ) [ 43 , 44 , 45 , 46 , 47 ] For alectinib, avapritinib, baracitinib, binimetinib, brigatinib, cobimetinib, dacomitinib, encorafenib, erdafitnib, fedratinib, gilteritinib, ibrutinib, laroctrectinib, lorlatinib, midostaurin, pexidartinib, ponatinib, trametinib, and zanbrutinib no published reports were found. In data collected for 17 TKIs, the results of the published data were largely inconsistent in that some of the published results for a given TKI identified the TKI as an inhibitor of OATP1B1 or OATP1B3, while other sources identified it expressly as a non-inhibitor.…”

Section: Effects Of Tkis On the Function Of Oatp1b1 And Oatp1b3mentioning

confidence: 99%

Role of OATP1B1 and OATP1B3 in Drug-Drug Interactions Mediated by Tyrosine Kinase Inhibitors

Garrison¹,

Talebi²,

Eisenmann³

et al. 2020

Pharmaceutics

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Failure to recognize important features of a drug’s pharmacokinetic characteristics is a key cause of inappropriate dose and schedule selection, and can lead to reduced efficacy and increased rate of adverse drug reactions requiring medical intervention. As oral chemotherapeutic agents, tyrosine kinase inhibitors (TKIs) are particularly prone to cause drug-drug interactions as many drugs in this class are known or suspected to potently inhibit the hepatic uptake transporters OATP1B1 and OATP1B3. In this article, we provide a comprehensive overview of the published literature and publicly-available regulatory documents in this rapidly emerging field. Our findings indicate that, while many TKIs can potentially inhibit the function of OATP1B1 and/or OATP1B3 and cause clinically-relevant drug-drug interactions, there are many inconsistencies between regulatory documents and the published literature. Potential explanations for these discrepant observations are provided in order to assist prescribing clinicians in designing safe and effective polypharmacy regimens, and to provide researchers with insights into refining experimental strategies to further predict and define the translational significance of TKI-mediated drug-drug interactions.

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Pretreatment With Rifampicin and Tyrosine Kinase Inhibitor Dasatinib Potentiates the Inhibitory Effects Toward OATP1B1- and OATP1B3-Mediated Transport

Cited by 49 publications

References 54 publications

In Vitro–In Vivo Extrapolation of OATP1B-Mediated Drug–Drug Interactions in Cynomolgus Monkey

In Vitro–In Vivo Extrapolation of OATP1B-Mediated Drug–Drug Interactions in Cynomolgus Monkey

Gaining Mechanistic Insight Into Coproporphyrin I as Endogenous Biomarker for OATP1B‐Mediated Drug–Drug Interactions Using Population Pharmacokinetic Modeling and Simulation

Role of OATP1B1 and OATP1B3 in Drug-Drug Interactions Mediated by Tyrosine Kinase Inhibitors

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