Factor XIa inhibitors show indication-specific benefits for cancer-associated thrombosis and secondary stroke prevention, but provide weaker support for broad substitution for direct oral anticoagulants.
Do Factor XIa inhibitors provide effective thrombosis prevention with reduced bleeding risk compared to direct oral anticoagulants in specific patient populations?
Factor XIa inhibitors demonstrate indication-specific benefits for thrombosis prevention, particularly in high bleeding risk scenarios, but may not broadly replace direct oral anticoagulants.
Purpose of review Factor XI (FXI) and its activated form, factor XIa (FXIa), have emerged as a leading novel anticoagulant target of the past decade. This review summarizes mechanistic and clinical data from 2023 through 2026 and proposes an indication-specific framework for FXIa inhibitor positioning. Recent findings Three large randomized studies diverged by indication. Abelacimab reduced major and clinically relevant nonmajor bleeding by 62% versus rivaroxaban in atrial fibrillation (AZALEA-TIMI 71). Asundexian was inferior to apixaban for stroke prevention in atrial fibrillation (OCEANIC-AF) yet reduced recurrent stroke after noncardioembolic events (OCEANIC-STROKE). Milvexian entered a three-trial phase 3 program. FXIa has been found to drive platelet and endothelial activation in inflammation-associated thrombosis, whereas the FXI zymogen has noncoagulation roles that include activation of bone morphogenetic protein 7–SMAD1/5 cardioprotection. A fifth drug class of allosteric FXI activation inhibitors was further characterized. Summary FXIa contribution to thrombus formation varies by anatomic site, flow conditions, and inflammatory phenotype. The clinical data support indication-specific positioning for cancer-associated thrombosis, secondary stroke prevention, and patients at high bleeding risk, but provide weaker support for broad substitution for direct oral anticoagulants.
Kidder et al. (Thu,) conducted a review in Thrombosis. Factor XIa inhibitors vs. Direct oral anticoagulants was evaluated. Factor XIa inhibitors show indication-specific benefits for cancer-associated thrombosis and secondary stroke prevention, but provide weaker support for broad substitution for direct oral anticoagulants.