Influence of Polymorphic OATP1B-Type Carriers on the Disposition of Docetaxel

Anne-Joy M. de Graan,Cynthia S. Lancaster,Amanda Obaidat,Bruno Hagenbuch,Laure Elens,Lena E. Friberg,Peter de Bruijn,Shuiying Hu,Alice A. Gibson,Gitte H. Bruun,Thomas J. Corydon,Torben S. Mikkelsen,Aisha L. Walker,Guoqing Du,Walter J. Loos,Ron H.N. van Schaik,Sharyn D. Baker,Ron H.J. Mathijssen,Alex Sparreboom

Influence of Polymorphic OATP1B-Type Carriers on the Disposition of Docetaxel

2012

Anne-Joy M. de Graan
Cynthia S. Lancaster
Amanda Obaidat
Bruno Hagenbuch
Laure Elens
Lena E. Friberg
Peter de Bruijn
Shuiying Hu
Alice A. Gibson
Gitte H. Bruun
Thomas J. Corydon
Torben S. Mikkelsen
Aisha L. Walker
Guoqing Du
Walter J. Loos
Ron H.N. van Schaik
Sharyn D. Baker
Ron H.J. Mathijssen
Alex Sparreboom

The existence of at least two potentially redundant uptake transporters in the human liver with similar affinity for docetaxel supports the possibility that functional defects in both of these proteins may be required to confer substantially altered disposition phenotypes. In view of the established exposure-toxicity relationships for docetaxel, we suggest that caution is warranted if docetaxel has to be administered together with agents that potently inhibit both OATP1B1 and OATP1B3.

Keywords:

Cancer research
Human liver
Organic anion transporter 1
Genotype
Pharmacology
Biology
Disposition
Docetaxel
Cell culture
Phenotype
uptake transporters

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