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Genetic Polymorphism of Inosine Triphosphate Pyrophosphatase Is a Determinant of Mercaptopurine Metabolism and Toxicity During Treatment for Acute Lymphoblastic Leukemia

机译:肌苷三磷酸焦磷酸酶的遗传多态性是急性淋巴细胞白血病治疗期间巯基嘌呤代谢和毒性的决定因素。

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摘要

The influence of genetic polymorphism in inosine triphosphate pyrophosphatase (ITPA) on thiopurine-induced adverse events has not been investigated in the context of combination chemotherapy for acute lymphoblastic leukemia (ALL). This study investigated the effects of a common ITPA variant allele (rs41320251) on mercaptopurine metabolism and toxicity during treatment of children with ALL. Significantly higher concentrations of methyl mercaptopurine nucleotides were found in patients with the nonfunctional ITPA allele. Moreover, there was a significantly higher probability of severe febrile neutropenia in patients with a variant ITPA allele among patients whose dose of mercaptopurine had been adjusted for TPMT genotype. In a cohort of patients whose mercaptopurine dose was not adjusted for TPMT phenotype, the TPMT genotype had a greater effect than the ITPA genotype. In conclusion, genetic polymorphism of ITPA is a significant determinant of mercaptopurine metabolism and of severe febrile neutropenia, after combination chemotherapy for ALL in which mercaptopurine doses are individualized on the basis of TPMT genotype.
机译:肌苷三磷酸焦磷酸酶(ITPA)的遗传多态性对硫嘌呤诱导的不良事件的影响尚未在急性淋巴细胞白血病(ALL)联合化疗的背景下进行研究。这项研究调查了常见的ITPA变异等位基因(rs41320251)对ALL儿童的治疗期间巯基嘌呤代谢和毒性的影响。在无功能ITPA等位基因的患者中发现甲基巯基嘌呤核苷酸的浓度明显更高。此外,在巯基嘌呤剂量已针对TPMT基因型进行了调整的患者中,ITPA等位基因变异的患者发生严重发热性中性粒细胞减少的可能性更高。在未针对TPMT表型调整巯基嘌呤剂量的一组患者中,TPMT基因型的影响大于ITPA基因型。总之,在ALL联合化疗后,ITPA的基因多态性是巯基嘌呤代谢和严重发热性中性粒细胞减少的重要决定因素,其中根据TPMT基因型对巯基嘌呤的剂量进行个体化。

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