Impact of cancer on outcomes following breakthrough ischaemic stroke on oral anticoagulants for atrial fibrillation: insights from the ASPERA-R study

Foschi, M.; De Santis, F.; Gabriele, F.; D'Anna, L.; Zini, A.; Paolucci, M.; Forlivesi, S.; Migliaccio, L.; Viola, M. M.; Rizzo, A. C.; Sessa, M.; Schwarz, G.; Tortorella, R.; Banerjee, S.; Desai, G.; Jaffar, M.; Prandin, G.; Pantoni, L.; Mele, F.; Scopelliti, G.; Cova, I.; Valente, M.; Maisano, D.; Antonelli, L.; Bagnato, M. R.; Di Mauro, G.; Bernocchi, F.; Di Donna, M. G.; Casolla, B.; Mazloum, M. P.; Kacani, K.; Djeghlal, N. -A.; Gonzalez-Martin, L.; Rigual, R.; Fuentes, B.; Hervas, C.; Candelaresi, P.; Andreone, V.; De Mase, A.; Spina, E.; De Sousa, D. A.; Souza, M. A.; Fior, A.; Serodio, M.; Caliandro, P.; Zauli, A.; Reale, G.; Abdelalim, A.; Ahmed, S.; Soliman, N. M.; Zhang, L.; Latimer, T.; Elboghday, M.; Elbassiouny, A. A.; Roushdy, T.; Shokri, H.; Ferrari, F.; Loizzo, N. D.; Mazzacane, F.; Guarino, M.; Barone, V.; Forti, P.; Rinaldi, G.; Rossi, M. V.; Laterza, V.; Frisullo, G.; Rizzo, P. A.; Broccolini, A.; Mannino, M.; Terruso, V.; Caggiula, M.; Rizzo, A.; Fonseca, A. C.; Antunes, B.; Barbosa, A. M.; Budincevic, H.; Crnac, P.; Viticchi, G.; Silvestrini, M.; Barba, L.; Otto, M.; Lochner, P.; Landau, B.; Buddha, S.; Khalil, R.; Piscaglia, M. G.; Minguzzi, E.; Zedde, M.; Nasreldein, A.; Vinciguerra, L.; Costa, L.; Elsayed, A. E.; Albanna, M.; Tudisco, L.; Mosconi, M. G.; Merlino, G.; Polymeris, A.; Ornello, R.; Sacco, S.

doi:10.1093/esj/aakag015

BACKGROUND: Breakthrough ischaemic stroke during oral anticoagulation (OAC) for atrial fibrillation (AF) represents a major therapeutic challenge, especially in patients with cancer, who face competing risks of thrombosis and bleeding. This study investigated the impact of cancer on 90-day outcomes after ischaemic stroke on OAC. PATIENTS AND METHODS: We analysed patients with AF who experienced ischaemic stroke while on continuous OAC enrolled in the international retrospective ASPERA-R study, comprising 35 stroke centres across 9 countries. Inverse probability weighting was applied to adjust for baseline imbalances, and weighted Cox, ordinal logistic and generalised linear models were used to estimate adjusted 90-day risks for the primary (ischaemic stroke or TIA), secondary (mRS shift, vascular/all-cause death) and safety (moderate-to-severe bleeding, ICH, 24-h haemorrhagic transformation) outcomes. RESULTS: Among 1649 included patients (mean age 78.0 ± 10.7 years; 45.8% male), 247 (15.0%) had cancer, of whom 87 (35.2%) had active cancer and 160 (64.8%) were in remission. After weighting, patients with cancer had a significantly higher 90-day risk of new ischaemic stroke or TIA (8.2% vs 2.8%; adjusted hazard ratio [aHR] 2.56; 95% CI, 1.59-4.13; P < .001) and worse 90-day mRS score distribution (adjusted odds ratio 1.29; 95% CI, 1.08-1.54; P = .005) than those without cancer. Active cancer conferred a > 4-fold higher risk of new ischaemic stroke or TIA (HR 4.48, 95% CI, 2.46-8.13; P < .001) and nearly 3-fold higher risk of moderate-to-severe bleeding (HR 2.77; 95% CI, 1.30-5.88; P = .008). Patients with cancer in remission showed increased ischaemic risk (HR 2.60; 95% CI, 1.59-5.25; P = .001) but not bleeding risk. Haematological malignancies carried a higher risk for both new ischaemic stroke or TIA (HR 3.06; 95% CI, 1.69-5.54; P = .001) and moderate-to-severe bleeding (HR 3.47, 95% CI, 1.57-7.70; P = .006) compared to solid malignancies. CONCLUSION: Cancer, particularly active and haematological malignancies, substantially worsens 90-day prognosis after breakthrough stroke on OAC, underscoring the need for refined risk stratification and tailored secondary prevention. TRIAL REGISTRATION: URL: www.clinicaltrials.gov; Unique identifier: NCT06823466.