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. 2016 Aug;12(2):1223-1232.
doi: 10.3892/ol.2016.4780. Epub 2016 Jun 24.

Therapeutic drug monitoring and tyrosine kinase inhibitors

Pauline Herviou  1 Emilie Thivat  2 Damien Richard  3 Lucie Roche  3 Joyce Dohou  2 Mélanie Pouget  4 Alain Eschalier  5 Xavier Durando  6 Nicolas Authier  5
Affiliations

Therapeutic drug monitoring and tyrosine kinase inhibitors

Pauline Herviou et al. Oncol Lett. 2016 Aug.

Abstract

The therapeutic activity of drugs can be optimized by establishing an individualized dosage, based on the measurement of the drug concentration in the serum, particularly if the drugs are characterized by an inter-individual variation in pharmacokinetics that results in an under- or overexposure to treatment. In recent years, several tyrosine kinase inhibitors (TKIs) have been developed to block intracellular signaling pathways in tumor cells. These oral drugs are candidates for therapeutic drug monitoring (TDM) due to their high inter-individual variability for therapeutic and toxic effects. Following a literature search on PubMed, studies on TKIs and their pharmacokinetic characteristics, plasma quantification and inter-individual variability was studied. TDM is commonly used in various medical fields, including cardiology and psychiatry, but is not often applied in oncology. Plasma concentration monitoring has been thoroughly studied for imatinib, in order to evaluate the usefulness of TDM. The measurement of plasma concentration can be performed by various analytical techniques, with liquid chromatography-mass spectrometry being the reference method. This method is currently used to monitor the efficacy and tolerability of imatinib treatments. Although TDM is already being used for imatinib, additional studies are required in order to improve this practice with the inclusion of other TKIs.

Keywords: pharmacokinetics; plasma concentration; target value; therapeutic drug monitoring; tyrosine kinase inhibitor.

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