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The SNP rs460089 in the gene promoter of the drug transporter OCTN1 has prognostic value for treatment-free remission in chronic myeloid leukemia patients treated with imatinib

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POLAKOVA Katerina Machova ALBEER Ali POLIVKOVA Vaclava KRUTSKA Monika VLCANOVA Katerina CURIK Nikola FABARIUS Alice KLAMOVA Hana SPIESS Birgit WALLER Cornelius F BRUEMMENDORF Tim H DENGLER Jolanta KUNZMANN Volker BURCHERT Andreas BELOHLAVKOVA Petra MUSTJOKI Satu FABER Edgar MAYER Jiří ŽÁČKOVÁ Daniela PANAYIOTIDIS Panayiotis RICHTER Johan HJORTH-HANSEN Henrik KAMINSKA Magdalena PLONKA Magdalena SZCZEPANEK Elzbieta SZAREJKO Monika BOBER Grazyna HUS Iwona GRZYBOWSKA-IZYDORCZYK Olga WASILEWSKA Ewa PACZKOWSKA Edyta NIESIOBEDZKA-KREZEL Joanna GIANNOPOULOS Krzysztof MAHON Francois X SACHA Tomasz SAUSSELE Susanne PFIRRMANN Markus

Rok publikování 2024
Druh Článek v odborném periodiku
Časopis / Zdroj Leukemia
Fakulta / Pracoviště MU

Lékařská fakulta

Citace
www https://www.nature.com/articles/s41375-023-02109-2
Doi http://dx.doi.org/10.1038/s41375-023-02109-2
Klíčová slova chronic myeloid leukemia; imatinib
Popis Membrane transporters are important determinants of drug bioavailability. Their expression and activity affect the intracellular drug concentration in leukemic cells impacting response to therapy. Pharmacogenomics represents genetic markers that reflect allele arrangement of genes encoding drug transporters associated with treatment response. In previous work, we identified SNP rs460089 located in the promotor of SLC22A4 gene encoding imatinib transporter OCTN1 as influential on response of patients with chronic myeloid leukemia treated with imatinib. Patients with rs460089-GC pharmacogenotype had significantly superior response to first-line imatinib treatment compared to patients with rs460089-GG. This study investigated whether pharmacogenotypes of rs460089 are associated with sustainability of treatment-free remission (TFR) in patients from the EUROpean Stop Kinase Inhibitor (EURO-SKI) trial. In the learning sample, 176 patients showed a significantly higher 6-month probability of molecular relapse free survival (MRFS) in patients with GC genotype (73%, 95% CI: 60-82%) compared to patients with GG (51%, 95% CI: 41-61%). Also over time, patients with GC genotype had significantly higher MRFS probabilities compared with patients with GG (HR: 0.474, 95% CI: 0.280-0.802, p = 0.0054). Both results were validated with data on 93 patients from the Polish STOP imatinib study. In multiple regression models, in addition to the investigated genotype, duration of TKI therapy (EURO-SKI trial) and duration of deep molecular response (Polish study) were identified as independent prognostic factors. The SNP rs460089 was found as an independent predictor of TFR.

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