Abstract 1753P
Background
In up to 30% of gastrointestinal (GI) malignancies, fluoropyrimidines (FP) are associated with severe adverse drug reactions (ADRs). Dihydropyrimidine dehydrogenase (DPYD), is a polymorphic gene involved in FP catabolism. The identification of deleterious variants associated with increased toxicity is recommended before treatment initiation [c.1905+1G>A (*2A); c.1679T>G (*13); c.1129-5923C>G (*IVS10); c.2846A>T (*949) or during treatment in case of ADR [c.2194G>A (*6)]. The estimated prevalence of DPYD deficient genotypes in the European population is <8%. This study aimed to determine the prevalence and implication of systematic DPYD testing in an unselected population with GI tumours.
Methods
The germline DPYD test was conducted on a consecutive series of 1000 pts diagnosed with GI malignancies at our Department between June 2020 and December 2022, candidates for FP for colorectal (CRC 69%), gastroesophageal (GEC 15%), biliopancreatic (BPC 12%), other GI tumours (4%) or double GI malignancy (<1%).
Results
Overall, 819 pts (82%) were DPYD wild type (WT) and 181 (18%) had a deleterious DPYD variant. Among DPYD mutated pts, 134 had CRC (74%), 23 GEC (13%), 17 BPC (9%), 5 other GI tumours (2%) and 1 had CRC and GEC (1%). 184 deleterious variants were observed in 181 pts, the most prevalent was DPYD *6 (N=146 15%) (Table). In 4 pts *6 coexisted with other variants, requiring dose personalization. Of 133 pts enrolled in interventional trials including FP treatment, 24 (18%) reported a deleterious variant: 2A N=1, IVS10 N=2, *6 N=21.
Table: 1753P
| DPYD status | N= 1000 | % | FP dosea |
| DPYD WT | 819 | 82% | 100% |
| DPYD6_c2194G>A homozygosis heterozygosis | 146 * 5 141 | 15% | 70% 85% |
| IVS10_1129_5923c>G | 20 | 2% | 50-70% |
| DPYD2A_1905+1G>A | 12 | 1% | 50% |
| DPYD949_c2846A>T | 5 | <1% | 50% |
| DPYD13_c1679T>G | 2 | <1% | 50% |
a recommended dose based on SIF and CPIC guidelines *4 patients presented a double heterozygosis DPYD6 and *2A (N=1), FP dose <50% DPYD6 and c*949 (N=1), FP dose <50% DPYD6 and *IVS10 (N=2), FP dose 50%FP= fluoropyrimidines, WT=wild type
Conclusions
Our large cohort of GI pts revealed a higher prevalence of deleterious DPYD variants compared to previous reports. DPYD*6 was the most frequent genotype and, at a low rate, occurred with other variants requiring major dose adjustments. To prevent severe ADR and to adequately report toxicity and changes in pts' quality of life, our data suggest that DPYD assessment should be mandatory and included in all FP-based clinical trials.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
Istituto Nazionale Tumori-IRCCS-Fondazione G. Pascale.
Funding
Has not received any funding.
Disclosure
C. Cardone: Financial Interests, Personal and Institutional, Advisory Board: Bayer. All other authors have declared no conflicts of interest.
Resources from the same session
2375P - Neoadjuvant sintilimab combined with gemcitabine and cisplatin (GP) for muscle-invasive bladder cancer (MIBC) patients followed by selective bladder sparing surgery
Presenter: Zhou Tong
Session: Poster session 23
2376P - Pembrolizumab monotherapy following tri-modality treatment for selected patients with muscle-invasive bladder cancer
Presenter: Shang Bin Qin
Session: Poster session 23
2378P - Efficacy and safety outcomes with pembrolizumab (pembro) rechallenge for patients (pts) with advanced/metastatic urothelial cancer (UC) who responded to first-course treatment
Presenter: Vadim Koshkin
Session: Poster session 23
2379P - AVENANCE: Subgroup analysis of patients (pts) with advanced urothelial carcinoma (aUC) with histological variants from a real-world (RW) study of avelumab first-line maintenance (1LM)
Presenter: Philippe Barthélémy
Session: Poster session 23