A well‐tolerated 5‐FU‐based treatment subsequent to severe capecitabine‐induced toxicity in a DPD‐deficient patient

5-Fluorouracil (5-FU) is widely administered as a continuous infusion to treat gastrointestinal tract or head and neck cancers, and as bolus injections in breast cancer chemotherapy regimens. Grade 3–4 toxicity occurs in about 30% of patients receiving 5-FU as a continuous infusion, and proves lethal in 0.5% of these patients [1]. 5-FU-related toxicity has mostly been reported with intravenous administration [1–3]. However, some cases of severe toxicity, including deaths, have been described after oral administration of 5-FU derivatives, such as capecitabine (Xeloda®) [4, 5]. A polymorphism of the dihydropyrimidine dehydrogenase (DPD) gene has been identified as a frequent cause of such toxicity [6, 7]. DPD catalyses the rate-limiting step of fluoropyrimidine catabolism. Partial or total DPD deficiency therefore leads to substantial overexposure in patients treated with the standard dose, exacerbating drug toxicity. This raises questions about possible screening for DPD deficiency before the administration of fluoropyrimidine drugs, including their oral forms. Patients found to have a deficiency on screening before treatment or following signs of toxicity during a previous course are usually given alternative treatments based on nonfluoropyrimidine compounds. However, 5-FU is highly active and its use may be essential in patients who fail to respond to other treatments. We report the case of a patient with DPD deficiency detected due to severe toxicity during capecitabine treatment, who has since received a continuous infusion of 5-FU at almost the standard dose with no significant signs of toxicity.