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  • DOSE-INDIVIDUALISATION OF FLUOROPYRIMIDINES BASED ON PRE-TREATMENT SERUM URACIL LEVELS: THE ALPE2U STUDY.

Dose-individualisation of fluoropyrimidines based on pre-treatment serum uracil levels: the Alpe2U study.

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  • Jonathan E Knikman
  • Mirjam de With
  • Niels Heersche
  • Marta Lopez-Yurda
  • Arnold Baars
  • Geert-Jan Creemers
  • Helga J Droogendijk
  • Edward Fiets
  • Alexander L T Imholz
  • Liselot Valkenburg-van Iersel
  • Caroline M P W Mandigers
  • Alina J van de Vendel
  • Frank J F Jeurissen
  • Peter Nieboer
  • Maarten J Deenen
  • Marlène H W van de Poel
  • Machteld N M Wymenga
  • Ron H N van Schaik
  • Bianca J C van den Bosch
  • Esther Oomen-de Hoop
  • Hilde Rosing
  • Jesse J Swen
  • Hans Gelderblom
  • Jan H M Schellens
  • Jos H Beijnen
  • Ron H J Mathijssen
  • Henk-Jan Guchelaar
  • Annemieke Cats

Abstract

BACKGROUND

DPYD-guided dosing enhances safety of fluoropyrimidine-based chemotherapy. However, approximately 23 % of patients still experience severe toxicity unexplained by the four commonly tested DPYD-variant alleles. Elevated pre-treatment uracil levels have been proposed as a surrogate marker for reduced DPD activity and an independent predictor of toxicity. This prospective study evaluated whether uracil-guided dose individualisation can reduce severe fluoropyrimidine-induced toxicity in DPYD wild-type patients.

METHODS

Pre-treatment plasma uracil levels were quantified in patients scheduled to receive fluoropyrimidine-based therapy. DPYD wild-type individuals with uracil concentrations > 16 ng/mL (DPYDwt/Uhigh) received a 50 % dose reduction, in accordance with French RNPGx guidelines. The incidence of grade ≥ 3 fluoropyrimidine-related toxicity was compared between dose-reduced DPYDwt/Uhigh patients, DPYDwt patients with uracil ≤ 16 ng/mL (DPYDwt/Unormal), and a historical cohort of DPYDwt/Uhigh patients treated at full dose. Pharmacokinetic data were compared to a second historical cohort.

CONCLUSION

Uracil-guided dosing of fluoropyrimidines may reduce toxicity risk but leads to subtherapeutic 5-fluorouracil exposure in DPYD wild-type patients. This indicates that these patients are treated sub-optimally and that uracil is not a reliable predictor of DPD deficiency in DPYD wild-type patients.

RESULTS

Among 612 evaluable patients, 22 were DPYDwt/Uhigh. The incidence of severe toxicity in the dose-reduced group was significantly lower than in historical full-dose DPYDwt/Uhigh patients (20 % vs 43 %, P = 0.03) and comparable during the first 2 treatment cycles to DPYDwt/Unormal patients (10 % vs 11 %). However, 5-fluorouracil exposure was markedly reduced in nineteen dose-reduced DPYDwt/Uhigh patients (177 vs 381 ng*h/mL), while five subsequently treated fully dosed DPYDwt/Uhigh patients exhibited comparable exposure to historical wild-type controls (456 vs 381 ng*h/mL). No correlation was found between uracil levels and DPD enzyme activity (R=-0.006, P = 0.98).

More about this publication

European journal of cancer (Oxford, England : 1990)
  • Volume 224
  • Pages 115483
  • Publication date 25-06-2025
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