DEMLOVÁ, Regina, Martina MRKVICOVA, Jaroslav ŠTĚRBA, Hana BERNATÍKOVÁ, Jan STARY, Martina SUKOVA, Alena MIKUŠKOVÁ, Alica CHOCHOLOVA, Beata MLADOSIEVICOVA, Andrea SOLTYSOVA, Darina BEHULOVA, Kateřina PILÁTOVÁ, Lenka ZDRAŽILOVÁ DUBSKÁ a Dalibor VALÍK. Augmenting Clinical Interpretability of Thiopurine Methyltransferase Laboratory Evaluation. Oncology. Basel: Karger, 2014, roč. 86, č. 3, s. 152-158. ISSN 0030-2414. Dostupné z: https://dx.doi.org/10.1159/000357407. |
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@article{1202692, author = {Demlová, Regina and Mrkvicova, Martina and Štěrba, Jaroslav and Bernatíková, Hana and Stary, Jan and Sukova, Martina and Mikušková, Alena and Chocholova, Alica and Mladosievicova, Beata and Soltysova, Andrea and Behulova, Darina and Pilátová, Kateřina and Zdražilová Dubská, Lenka and Valík, Dalibor}, article_location = {Basel}, article_number = {3}, doi = {http://dx.doi.org/10.1159/000357407}, keywords = {Acute lymphoblastic leukemia; Compound heterozygote; Genotype-phenotype correlation; Rate-blanked pharmacophenotyping; Thiopurine methyltransferase}, language = {eng}, issn = {0030-2414}, journal = {Oncology}, title = {Augmenting Clinical Interpretability of Thiopurine Methyltransferase Laboratory Evaluation}, volume = {86}, year = {2014} }
TY - JOUR ID - 1202692 AU - Demlová, Regina - Mrkvicova, Martina - Štěrba, Jaroslav - Bernatíková, Hana - Stary, Jan - Sukova, Martina - Mikušková, Alena - Chocholova, Alica - Mladosievicova, Beata - Soltysova, Andrea - Behulova, Darina - Pilátová, Kateřina - Zdražilová Dubská, Lenka - Valík, Dalibor PY - 2014 TI - Augmenting Clinical Interpretability of Thiopurine Methyltransferase Laboratory Evaluation JF - Oncology VL - 86 IS - 3 SP - 152-158 EP - 152-158 PB - Karger SN - 00302414 KW - Acute lymphoblastic leukemia KW - Compound heterozygote KW - Genotype-phenotype correlation KW - Rate-blanked pharmacophenotyping KW - Thiopurine methyltransferase N2 - Objective: Individuals with decreased thiopurine methyltransferase (TPMT) activity are at risk of adverse effects of thiopurine administration whereas its increased activity may inactivate drugs faster. We evaluated genotype-phenotype correlations in patients with suspected hematological malignancies and inflammatory bowel disease from our region based on findings of nonlinear TPMT enzyme kinetics previously unreported. Patients and Methods: The study group comprised 267 individuals. They were screened for the most common variants of low TPMT activity. TPMT activity was measured in erythrocytes using the HPLC rate-blanked method. Results: Thirty-three patients (12.4%) were heterozygous (26 were TPMT*1/*3A, 5 TPMT*1/*2, 2 TPMT*1/*3C) and 1 was a compound heterozygote (*2/*3A). Normal and low normal TPMT activities substantially overlapped in wildtype and heterozygous individuals, whereas high activities were found in 29 wild-type genotyped patients. Extreme and life-threatening toxicity was observed in the compound heterozygote patient. Conclusion: Activity measurement performed at diagnosis provides clinicians with information on immediate pharmacokinetic-related adverse events and/or hypermetabolism, and genotyping may indicate the rate of pharmacodynamic thioguanine nucleotide accumulation due to slower overall thiopurine metabolism. (C) 2014 S. Karger AG, Basel ER -
DEMLOVÁ, Regina, Martina MRKVICOVA, Jaroslav ŠTĚRBA, Hana BERNATÍKOVÁ, Jan STARY, Martina SUKOVA, Alena MIKUŠKOVÁ, Alica CHOCHOLOVA, Beata MLADOSIEVICOVA, Andrea SOLTYSOVA, Darina BEHULOVA, Kateřina PILÁTOVÁ, Lenka ZDRAŽILOVÁ DUBSKÁ a Dalibor VALÍK. Augmenting Clinical Interpretability of Thiopurine Methyltransferase Laboratory Evaluation. \textit{Oncology}. Basel: Karger, 2014, roč.~86, č.~3, s.~152-158. ISSN~0030-2414. Dostupné z: https://dx.doi.org/10.1159/000357407.
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