Literature DB >> 24755470

Influence of drug formulation on OATP1B-mediated transport of paclitaxel.

Annemieke J M Nieuweboer1, Shuiying Hu1, Chunshan Gui1, Bruno Hagenbuch1, Inge M Ghobadi Moghaddam-Helmantel1, Alice A Gibson1, Peter de Bruijn1, Ron H J Mathijssen2, Alex Sparreboom3.   

Abstract

Taxane antineoplastic agents are extensively taken up into hepatocytes by OATP1B-type transporters before metabolism and excretion. Because the biodistributional properties imposed upon these agents by different solubilizers drive clinically important pharmacodynamic endpoints, we tested the hypothesis that the in vitro and in vivo interaction of taxanes with OATP1B transporters is affected by the choice of drug delivery system. Transport of paclitaxel, docetaxel, and cabazitaxel was studied in vitro using various cell lines transfected with OATP1B1, OATP1B3, or the rodent equivalent OATP1B2. Pharmacokinetic studies were done in wild-type and OATP1B2-knockout mice in the presence or absence of polysorbate 80 (PS80) or Kolliphor EL (formerly Cremophor EL; CrEL). Paclitaxel and docetaxel, but not cabazitaxel, were transported substrates of OATP1B1, OATP1B3, and OATP1B2, and these in vitro transport processes were strongly reduced in the presence of clinically relevant concentrations of PS80 and CrEL. When paclitaxel was administered without any solubilizers, deficiency of OATP1B2 in mice was associated with a significantly decreased systemic clearance because of a liver distribution defect (P=0.000484). However, this genotype dependence of paclitaxel clearance was masked in the presence of PS80 or CrEL because of significant inhibition of OATP1B2-mediated hepatocellular uptake of the drug (P<0.05). Our findings confirm the importance of OATP1B-type transporters in the hepatic elimination of taxanes and indicate that this process can be inhibited by PS80 and CrEL. These results suggest that the likelihood of drug-drug interactions mediated by these transporters is strongly dependent on the selected taxane solubilizer. ©2014 American Association for Cancer Research.

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Year:  2014        PMID: 24755470      PMCID: PMC4161133          DOI: 10.1158/0008-5472.CAN-13-3634

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  47 in total

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6.  Identification of drugs and drug metabolites as substrates of multidrug resistance protein 2 (MRP2) using triple-transfected MDCK-OATP1B1-UGT1A1-MRP2 cells.

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9.  Influence of polymorphic OATP1B-type carriers on the disposition of docetaxel.

Authors:  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
Journal:  Clin Cancer Res       Date:  2012-06-18       Impact factor: 12.531

Review 10.  Transporter-mediated drug-drug interactions.

Authors:  Fabian Müller; Martin F Fromm
Journal:  Pharmacogenomics       Date:  2011-07       Impact factor: 2.533

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Review 4.  Organic Anion Transporting Polypeptides: Emerging Roles in Cancer Pharmacology.

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Journal:  Mol Pharmacol       Date:  2019-02-19       Impact factor: 4.436

5.  CCR 20th anniversary commentary: BMS-247550—microtubule stabilization as successful targeted therapy.

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Review 6.  Pharmacogenomics in Cytotoxic Chemotherapy of Cancer.

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7.  Sustained Accumulation of Microtubule-Binding Chemotherapy Drugs in the Peripheral Nervous System: Correlations with Time Course and Neurotoxic Severity.

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8.  Hepatic uptake transporters and docetaxel disposition in mice-letter.

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Review 9.  Exploring pharmacogenetics of paclitaxel- and docetaxel-induced peripheral neuropathy by evaluating the direct pharmacogenetic-pharmacokinetic and pharmacokinetic-neuropathy relationships.

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10.  OATP1B2 deficiency protects against paclitaxel-induced neurotoxicity.

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Journal:  J Clin Invest       Date:  2018-01-16       Impact factor: 14.808

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