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Research ArticleArticle

Prediction of In Vivo Rat Biliary Drug Clearance from an In Vitro Hepatocyte Efflux Model

Patrik Lundquist, Johan Loof, Urban Fagerholm, Ingemo Sjogren, Jenny Johansson, Sveinn Briemm, Janet Hoogstraate, Lovisa Afzelius and Tommy B. Andersson
Drug Metabolism and Disposition January 6, 2014, dmd.113.054155; DOI: https://doi.org/10.1124/dmd.113.054155
Patrik Lundquist
1 AstraZeneca/Uppsala University;
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Johan Loof
2 AstraZeneca;
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Urban Fagerholm
2 AstraZeneca;
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Ingemo Sjogren
2 AstraZeneca;
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Jenny Johansson
2 AstraZeneca;
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Sveinn Briemm
2 AstraZeneca;
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Janet Hoogstraate
2 AstraZeneca;
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Lovisa Afzelius
2 AstraZeneca;
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Tommy B. Andersson
3 Astra Zeneca Research and Development MoIndal
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  • For correspondence: tommy.b.andersson@astrazeneca.com
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Abstract

Well established techniques are available to predict in vivo hepatic uptake and metabolism from in vitro data, but predictive models for biliary clearance remain elusive. Several studies have verified the expression and activity of ATP-binding cassette (ABC) efflux transporters central to biliary clearance in freshly isolated rat hepatocytes, raising the possibility to predict biliary clearance from in vitro efflux measurements. In the present study short term plated rat hepatocytes were evaluated as a model to predict biliary clearance from in vitro efflux measurements, prior to major changes in transporter expression known to take place in long term hepatocyte cultures. The short term cultures were carefully characterized for their uptake and metabolic properties using a set of model compounds. In vitro efflux was studied using digoxin, fexofenadine, napsagatran, and rosuvastatin, representing compounds with over 100-fold differences in efflux rates in vitro and 60-fold difference in measured in vivo biliary clearance. The predicted biliary clearances from short term plated rat hepatocytes were within two-fold of measured in vivo values. As in vitro efflux includes both basolateral and canalicular effluxes, pronounced basolateral efflux may introduce errors in predictions for some compounds. In addition, in vitro rat hepatocyte uptake rates corrected for simultaneous efflux, predicted rat in vivo hepatic clearance of the biliary cleared compounds with less than two-fold error. Short term plated hepatocytes could thus be used to quantify hepatocyte uptake, metabolism, and efflux of compounds and considerably improve the prediction of hepatic clearance, especially for compounds with a large biliary clearance component.

  • ABC transporters
  • biliary excretion
  • drug distribution
  • drug efflux
  • drug transport
  • hepatic transport
  • hepatic uptake
  • hepatobiliary transport
  • hepatocytes
  • in vitro-in vivo prediction
  • The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition: 51 (6)
Drug Metabolism and Disposition
Vol. 51, Issue 6
1 Jun 2023
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Research ArticleArticle

Prediction of In Vivo Rat Biliary Drug Clearance from an In Vitro Hepatocyte Efflux Model

Patrik Lundquist, Johan Loof, Urban Fagerholm, Ingemo Sjogren, Jenny Johansson, Sveinn Briemm, Janet Hoogstraate, Lovisa Afzelius and Tommy B. Andersson
Drug Metabolism and Disposition January 6, 2014, dmd.113.054155; DOI: https://doi.org/10.1124/dmd.113.054155

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Research ArticleArticle

Prediction of In Vivo Rat Biliary Drug Clearance from an In Vitro Hepatocyte Efflux Model

Patrik Lundquist, Johan Loof, Urban Fagerholm, Ingemo Sjogren, Jenny Johansson, Sveinn Briemm, Janet Hoogstraate, Lovisa Afzelius and Tommy B. Andersson
Drug Metabolism and Disposition January 6, 2014, dmd.113.054155; DOI: https://doi.org/10.1124/dmd.113.054155
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