Journal of Personalized Medicine (Aug 2021)

<i>TPMT*3C</i> as a Predictor of 6-Mercaptopurine-Induced Myelotoxicity in Thai Children with Acute Lymphoblastic Leukemia

  • Thawinee Jantararoungtong,
  • Supaporn Wiwattanakul,
  • Rawiporn Tiyasirichokchai,
  • Santirhat Prommas,
  • Rattanaporn Sukprasong,
  • Napatrupron Koomdee,
  • Pimonpan Jinda,
  • Jiratha Rachanakul,
  • Nutthan Nuntharadthanaphong,
  • Samart Pakakasama,
  • Usanarat Anurathapan,
  • Suradej Hongeng,
  • Chonlaphat Sukasem

DOI
https://doi.org/10.3390/jpm11080783
Journal volume & issue
Vol. 11, no. 8
p. 783

Abstract

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The response to 6-mercaptopurine (6-MP) can be altered by genetic polymorphisms in genes encoding drug-metabolizing enzymes and drug transporters. The purpose of this study was to investigate the association between genetic polymorphisms of drug-metabolizing enzymes (TPMT 719A > G (*3C), ITPA 94C > A and ITPA 123G > A) and drug transporters (MRP4 912C > A and MRP4 2269G > A) with 6-MP-related myelotoxicity and hepatotoxicity in Thai children with acute lymphoblastic leukemia (ALL). The prescribed dosage of 6-MP and its adverse effects were assessed from medical records during the first 8 weeks and 9–24 weeks of maintenance therapy. Children with the TPMT*1/*3C genotype had a higher risk of leukopenia with an odds ratio (OR) of 4.10 (95% confidence interval (CI) of 1.06–15.94; p = 0.033) compared to wild type (TPMT*1/*1) patients. Heterozygous TPMT*3C was significantly associated with severe neutropenia with an increased risk (OR, 4.17; 95% CI, 1.25–13.90); p = 0.014) during the first 8 weeks. No association was found among ITPA94C > A, ITPA123G > A, MRP4 912C > A, and MRP4 2269G > A with myelotoxicity and hepatotoxicity. The evidence that TPMT heterozygotes confer risks of 6-MP-induced myelotoxicity also supports the convincing need to genotype this pharmacogenetic marker before the initiation of 6-MP therapy.

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