BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. rs4950928, CYP51, Angiogenesis, Allergy to pollen, Breast, Metabolism of nitric oxide)
Bookmark Forward

Interaction of nilotinib, dasatinib and bosutinib with ABCB1 and ABCG2: implications for altered anti-cancer effects and pharmacological properties.

C Hegedus, C Ozvegy-Laczka, A Apáti, M Magócsi, K Német, L Orfi, G Kéri, M Katona, Z Takáts, A Váradi, G Szakács, B Sarkadi

British journal of pharmacology 2009 Oct


filter terms:
  • abc transporters (1)
  • ABCB1 (4)
  • abcb1 protein, human (1)
  • ABCG2 (4)
  • abcg2 protein, human (1)
  • ATP (8)
  • bcr abl (6)
  • bosutinib (4)
  • cancer (6)
  • chronic myeloid leukaemia (1)
  • cyclosporins (2)
  • dasatinib (7)
  • fusion proteins, bcr- abl (2)
  • help (1)
  • humans (1)
  • imatinib (1)
  • indoles (2)
  • kinases (2)
  • neoplasm proteins (2)
  • nilotinib (5)
  • nitriles (2)
  • protein human (2)
  • pyrimidines (2)
  • quinolines (2)
  • thiazoles (2)
  • tyrosine kinase inhibitors (6)
  • valspodar (1)
    • Sizes of these terms reflect their relevance to your search.

    ABC multidrug transporters (MDR-ABC proteins) cause multiple drug resistance in cancer and may be involved in the decreased anti-cancer efficiency and modified pharmacological properties of novel specifically targeted agents. It has been documented that ABCB1 and ABCG2 interact with several first-generation, small-molecule, tyrosine kinase inhibitors (TKIs), including the Bcr-Abl fusion kinase inhibitor imatinib, used for the treatment of chronic myeloid leukaemia. Here, we have investigated the specific interaction of these transporters with nilotinib, dasatinib and bosutinib, three clinically used, second-generation inhibitors of the Bcr-Abl tyrosine kinase activity. MDR-ABC transporter function was screened in both membrane- and cell-based (K562 cells) systems. Cytotoxicity measurements in Bcr-Abl-positive model cells were coupled with direct determination of intracellular TKI concentrations by high-pressure liquid chromatography-mass spectrometry and analysis of the pattern of Bcr-Abl phosphorylation. Transporter function in membranes was assessed by ATPase activity. Nilotinib and dasatinib were high-affinity substrates of ABCG2, and this protein mediated an effective resistance in cancer cells against these compounds. Nilotinib and dasatinib also interacted with ABCB1, but this transporter provided resistance only against dasatinib. Neither ABCB1 nor ABCG2 induced resistance to bosutinib. At relatively higher concentrations, however, each TKI inhibited both transporters. A combination of in vitro assays may provide valuable preclinical information for the applicability of novel targeted anti-cancer TKIs, even in multidrug-resistant cancer. The pattern of MDR-ABC transporter-TKI interactions may also help to understand the general pharmacokinetics and toxicities of new TKIs.

    Citation

    C Hegedus, C Ozvegy-Laczka, A Apáti, M Magócsi, K Német, L Orfi, G Kéri, M Katona, Z Takáts, A Váradi, G Szakács, B Sarkadi. Interaction of nilotinib, dasatinib and bosutinib with ABCB1 and ABCG2: implications for altered anti-cancer effects and pharmacological properties. British journal of pharmacology. 2009 Oct;158(4):1153-64

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 19785662

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.