Abstract 2157P
Background
Fluoropyrimidines are used widely to treat cancer but their cardiotoxicity, which remains incompletely understood, has serious consequences for some patients. The fluoropyrimidine S-1 (Teysuno®) has recently been approved for the management of colorectal cancer in patients who develop cardiovascular toxicity with other fluoropyrimidines.
Methods
This was a single-centre phase II prospective randomised open-label blinded endpoint trial that investigated the cardiotoxicity of capecitabine and S-1 in patients treated between May 2014 and March 2020. Patients were randomized 1:1 to receive oral capecitabine or S-1, alone or with oxaliplatin, for days 1-14 of a 21-day cycle. Baseline computed tomography coronary angiogram (CTCA) was performed. Myocardial ischaemia was quantified by ST-segment analysis of continuous 12-lead electrocardiography before and during days 3-5 of oral chemotherapy, by a blinded analyst. Alpha-fluoro-beta-alanine (FBAL) was measured using a validated liquid chromatography tandem mass spectrometry method.
Results
Fifty-nine patients (29 capecitabine; 30 S-1; mean age 64 years (range 40-83)) were enrolled, 56 started treatment and 72% (capecitabine) and 70% (S-1) received oxaliplatin. CTCA was performed in 53 patients, coronary artery disease (CAD) was seen in 30 (capecitabine, n=14/26; S-1, n=16/27). Duration of ST change was not significantly different between groups (p = 0.2198) but change in mean daily ischaemic burden (p=0.0442) was significantly higher for capecitabine compared to S-1. Ischaemic burden was unrelated to the presence of underlying CAD. FBAL (precursor to cardiotoxic fluoroacetate) was significantly increased with capecitabine compared to S-1 during treatment (Table).
Table: 2157P
Mean FBAL (ng/mL) during fluoropyrimidine treatment
| Week | Capecitabine (n=23) | S-1 (n=23) | P value |
| 1 | 2507 | 95 | <0.0001 |
| 2 | 2632 | 103 | <0.0001 |
| 3 | 12 | 3 | 0.0083 |
Conclusions
In this prospective randomised trial, capecitabine was associated with significantly higher ischaemic burden and higher levels of FBAL than S-1 and this was unrelated to presence of CAD.
Clinical trial identification
NCT01845337.
Editorial acknowledgement
Wilco Coers, Meducom.
Legal entity responsible for the study
ACCORD, NHS Lothian R+D and the University of Edinburgh.
Funding
Nordic Pharma.
Disclosure
S. Clive: Non-Financial Interests, Personal and Institutional, Research Funding: Nordic. All other authors have declared no conflicts of interest.
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