AI Article Synopsis
- Thiopurines are commonly used in cancer treatment but have a narrow therapeutic range, often causing toxic side effects linked to genetic differences in TPMT.
- Recent research highlights NUDT15 genetic variations as significant contributors to thiopurine intolerance, yet the exact mechanisms and effects on treatment remain unclear.
- In a study with 270 children undergoing leukemia treatment across three countries, specific NUDT15 variants were found to severely impair enzyme activity, leading to higher toxicity and suggesting that personalized treatment plans considering NUDT15 genotypes could improve patient outcomes.
Article Abstract
Widely used as anticancer and immunosuppressive agents, thiopurines have narrow therapeutic indices owing to frequent toxicities, partly explained by TPMT genetic polymorphisms. Recent studies identified germline NUDT15 variation as another critical determinant of thiopurine intolerance, but the underlying molecular mechanisms and the clinical implications of this pharmacogenetic association remain unknown. In 270 children enrolled in clinical trials for acute lymphoblastic leukemia in Guatemala, Singapore and Japan, we identified four NUDT15 coding variants (p.Arg139Cys, p.Arg139His, p.Val18Ile and p.Val18_Val19insGlyVal) that resulted in 74.4-100% loss of nucleotide diphosphatase activity. Loss-of-function NUDT15 diplotypes were consistently associated with thiopurine intolerance across the three cohorts (P = 0.021, 2.1 × 10(-5) and 0.0054, respectively; meta-analysis P = 4.45 × 10(-8), allelic effect size = -11.5). Mechanistically, NUDT15 inactivated thiopurine metabolites and decreased thiopurine cytotoxicity in vitro, and patients with defective NUDT15 alleles showed excessive levels of thiopurine active metabolites and toxicity. Taken together, these results indicate that a comprehensive pharmacogenetic model integrating NUDT15 variants may inform personalized thiopurine therapy.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5029084 | PMC |
| http://dx.doi.org/10.1038/ng.3508 | DOI Listing |
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