What question did this study set out to answer?

To determine the impact of 30% dose reductions of irinotecan on survival outcomes in UGT1A1 poor metaboliser patients compared to fully-dosed patients.

February 26, 2026Open Access

Survival of patients with colorectal or pancreatic cancer who received UGT1A1 genotype-guided dosing of irinotecan in the Netherlands (2017–2024): a retrospective, multicentre cohort study

Key Points

To determine the impact of 30% dose reductions of irinotecan on survival outcomes in UGT1A1 poor metaboliser patients compared to fully-dosed patients.
Retrospective cohort design across six Dutch hospitals
Included patients with colorectal or pancreatic cancer
Compared progression-free survival (PFS) and overall survival (OS) between dose-reduced and fully-dosed patients
Utilized Kaplan–Meier and Cox regression analyses for survival assessment
No significant differences in PFS and OS rates between 30% dose-reduced PMs and fully-dosed IM/NMs
Adjusted hazard ratios showed no significant survival differences for both PFS and OS
Comparable severe toxicity rates in both patient groups

Abstract

SummaryBackground UGT1A1 genotype-guided dosing reduces severe toxicity in UGT1A1 poor metaboliser (PM) patients treated with irinotecan. However, the impact of a dose reduction on survival remains unknown. This study evaluated whether upfront 30% dose reductions of irinotecan in UGT1A1 PMs affect survival by comparing progression-free survival (PFS) and overall survival (OS) between 30% dose-reduced PMs and fully-dosed UGT1A1 intermediate and normal metaboliser (IM/NM) patients. Methods We conducted a retrospective, multicentre cohort study in patients with pancreatic cancer or colorectal cancer treated with UGT1A1 genotype-guided irinotecan dosing at six Dutch hospitals between August 2017 and April 2024. Patients were included in the primary analysis if irinotecan was dosed according to UGT1A1 genotype (i.e. an initial 100% ± 10% dose intensity for IM/NMs and an initial 70% ± 10% dose intensity for PMs) in at least cycle 1. Survival analyses for PFS and OS were performed using Kaplan–Meier estimates and univariable and multivariable Cox regressions, stratified by tumour type. Safety was also assessed. Findings The primary analysis included 779 patients, 76 (9.8%) of whom were PMs. The median follow-up was 27.8 months (95% CI 15.2–31.6). No significant differences in PFS and OS rates were found between 30% dose-reduced PMs and fully-dosed IM/NMs (stratified log-rank test: PFS: P = 0.54; OS: P = 0.42). In stratified Cox regression analyses, the adjusted hazard ratio of PMs vs IM/NMs was 1.02 (95% CI 0.78–1.32; P = 0.90) for PFS and 1.10 (95% CI 0.82–1.48; P = 0.51) for OS, indicating no significant differences exist in PFS or OS between 30% dose-reduced PMs and fully-dosed IM/NMs. Severe toxicity rates were comparable between 30% dose-reduced PMs and fully-dosed IM/NMs (P = 0.59). Interpretation An upfront 30% dose reduction of irinotecan in UGT1A1 PMs does not lead to statistically significant differences in survival outcomes compared to fully-dosed IM/NMs. Therefore, UGT1A1 genotype-guided dosing of irinotecan can be confidently performed to improve patient safety. Funding No funding.

Survival of patients with colorectal or pancreatic cancer who received UGT1A1 genotype-guided dosing of irinotecan in the Netherlands (2017–2024): a retrospective, multicentre cohort study

Key Points

Abstract

Cite This Study