Study of polymorphisms of UGT1A1 and DPYD genes in chemotherapy for colorectal cancer

Автор: Timoshkina Natalya N., Bogomolova Olga A., Zhuzhelenko Irina A., Kabanov Sergei N., Kalabanova Elena A., Mitashok Irina S., Svetitskaya Yana V., Vodolazhskii Dmitrij I.

Журнал: Сибирский онкологический журнал @siboncoj

Рубрика: Клинические исследования

Статья в выпуске: 6 т.17, 2018 года.

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Background. The personalized approach implies an individual choice of medicines and their doses for the patient, providing the most effective and safe pharmacotherapy. objective: analysis of the frequencies of UGT1A1 and DPYD polymorphisms and comparison of genotyping data with irinotecan and 5-fluorouracilinduced toxicity, respectively. materials and methods. Venous blood of 94 Caucasian patients (46 men and 48 women, median age 61 years). The *6 and *28 UGT1A1 alleles were identified by pyrosequencing, and the *2А DPYD allele was identified by Real-Time PCR. results. The genotyping of 94 patients with colon cancer did not reveal the *2A SNP in the DPYD gene. The frequency rate of the *6 and *28 alleles of the UGT1A1 gene was 0.346 and 0.016, respectively. 24 % of patients receiving chemotherapy with 5-fluorouracil developed side effects associated with the circulatory system and the gastrointestinal tract. Hematological and nonhematological toxic reactions were noted in 48 % and 50 % of patients receiving irinotecan. Severe bilirubinemia was associated with the *28/*28 UGT1A1 genotype. The presence of a high-risk genotype (*28/*1, *28/*28 UGT1A1 ) correlated with the development of side effects (p=0.040). conclusion. The absence of carriers of the *2А DPYD allele in the sample with a significant proportion of pronounced adverse toxic reactions to 5-fluorouracil causes the need for the inclusion of new polymorphisms of the DPYD gene in pharmacogenetic testing. The inclusion of genotyping of UGT1A1 polymorphisms into a complex of preliminary examination is advisable when planning treatment with irinotecan.

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Colorectal cancer, irinotecan, 5-fluorouracil, toxicity, UGT1A1, DPYD, ethnicity, chemotherapy, genotype

Короткий адрес: https://sciup.org/140254226

IDR: 140254226   |   DOI: 10.21294/1814-4861-2018-17-6-49-56

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