Andexanet alfa versus PCC products for factor Xa inhibitor bleeding: A systematic review with meta-analysis
Research article published in Pharmacotherapy (2024)
Abstract
Previous meta-analyses assessed andexanet alfa (AA) or prothrombin complex concentrate (PCC) products for the treatment of Factor Xa inhibitor (FXaI)-associated major bleeding. However, they did not include recent studies or assess the impact of the risk of bias. We conducted a systematic review with meta-analysis on the effectiveness of AA versus PCC products for FXaI-associated major bleeding, inclusive of the studies' risk of bias. PubMed and Embase were searched for comparative studies assessing major bleeding in patients using FXaI who received AA or PCC. We used the Methodological Index for NOn-Randomized Studies (MINORS) checklist and one question from the Joanna Briggs Institute (JBI) Critical Appraisal of Case Series tool to assess the risk of bias. Random-effects meta-analyses were performed to provide a pooled estimate for the effect of AA versus PCC products on hemostatic efficacy, in-hospital mortality, 30-day mortality, and thrombotic events. Low-moderate risk of bias studies were meta-analyzed separately, as well as combined with high risk of bias studies. Eighteen comparative evaluations of AA versus PCC were identified. Twenty-eight percent of the studies (n = 5) had low-moderate risk and 72% (n = 13) had a high risk of bias. Studies with low-moderate risk of bias suggested improvements in hemostatic efficacy [Odds Ratio (OR) 2.72 (95% Confidence Interval (CI): 1.15-6.44); one study], lower in-hospital mortality [OR 0.48 (95% CI: 0.38-0.61); three studies], and reduced 30-day mortality [OR 0.49 (95% CI: 0.30-0.80); two studies] when AA was used versus PCC products. When studies were included regardless of the risk of bias, pooled effects showed improvements in hemostatic efficacy [OR 1.36 (95% CI: 1.01-1.84); 12 studies] and reductions in 30-day mortality [OR 0.53 (95% CI: 0.37-0.76); six studies] for AA versus PCC. The difference in thrombotic events with AA versus PCC was not statistically significant in the low-moderate, high, or combined risk of bias groups. The evidence from low-moderate quality real-world studies suggests that AA is superior to PCC in enhancing hemostatic efficacy and reducing in-hospital and 30-day mortality. When studies are assessed regardless of the risk of bias, the pooled hemostatic efficacy and 30-day mortality risk remain significantly better with AA versus PCC.
Abstract sourced from PubMed (NCBI) for the cited record. See the original publication for the authoritative version.
Summary
Peer-reviewed research on anticoagulant and antithrombotic drug development relevant to thrombin and factor inhibition. Indexed in PubMed and verified against the NCBI record.
Why This Matters for Hirudotherapy
This systematic review with meta-analysis compared andexanet alfa (AA) against prothrombin complex concentrate (PCC) products for factor Xa inhibitor–associated major bleeding across 18 comparative evaluations, and after formally appraising risk of bias reported that low-to-moderate-bias studies suggested better hemostatic efficacy and lower in-hospital and 30-day mortality with AA, with no statistically significant difference in thrombotic events. For the ASH evidence picture this is part of the broader antithrombotic-reversal landscape rather than leech-specific content: factor Xa inhibitors and their reversal agents are not leech-secretome molecules, but they map the wider anticoagulation field within which leech-derived thrombin inhibitors are positioned. Honest caveat: this is a meta-analysis of mostly observational, real-world studies, and the authors note that 72% of included studies carried a high risk of bias; the favorable signals come largely from a small number of lower-bias studies, so conclusions are suggestive rather than definitive and carry no hirudotherapy implication of their own.
Citation
Andexanet alfa versus PCC products for factor Xa inhibitor bleeding: A systematic review with meta-analysis.
White et al. · Pharmacotherapy, 2024
Added to ASH library: May 28, 2026 · Site last updated: June 18, 2026