| Literature DB >> 33704179 |
Lauren E Winquist1, Michael Sanatani1,2, Richard B Kim1,3, Eric Winquist1,2.
Abstract
5-fluorouracil (5-FU) and its pro-drug capecitabine are widely used anticancer agents. Most 5-FU catabolism is dependent on dihydropyrimidine dehydrogenase (DPD) encoded by the DPYD gene, and DPYD variants that reduce DPD function increase 5-FU toxicity. Most DPD deficient patients are heterozygous and can be treated with reduced 5-FU dosing. We describe a patient with a genotype associated with near complete absence of DPD function, and severe and likely fatal toxicity with 5-FU treatment. The patient was treated effectively with alternative systemic therapy. Routine pretreatment DPYD genotyping is recommended by the European Medicines Agency, and guidelines for use of 5-FU in DPD deficient patients are available. However, outside the province of Quebec, routine pretreatment screening for DPD deficiency remains unavailable in Canada. It is likely our patient would have died from 5-FU toxicity under the current standard of care, but instead provides an example of the potential benefit of DPYD screening on patient outcomes.Entities:
Keywords: adverse effects; cancer; dihydropyrimidine dehydrogenase; drug therapy; fluoropyrimidines; single nucleotide polymorphisms
Year: 2020 PMID: 33704179 PMCID: PMC7816174 DOI: 10.3390/curroncol28010012
Source DB: PubMed Journal: Curr Oncol ISSN: 1198-0052 Impact factor: 3.677