Human Genetic Evidence Does Not Support a Causal Role for Reduced FXI Levels in Heart Failure Pathogenesis-Brief Report
- PMID: 40567226
- DOI: 10.1161/ATVBAHA.125.322971
Human Genetic Evidence Does Not Support a Causal Role for Reduced FXI Levels in Heart Failure Pathogenesis-Brief Report
Abstract
Background: Coagulation factor XI (FXI) is a promising therapeutic target for preventing thromboembolic disease while preserving hemostasis. However, recent translational and epidemiological findings have raised concerns that lowering FXI levels may increase heart failure risk. To clarify these potential risks, we investigated whether lifelong genetically reduced FXI levels were associated with risk of heart failure and imaging correlates of cardiovascular function.
Methods: We used a genome-wide association study of circulating FXI levels in the deCODE cohort (N=35 559) to identify a genetic proxy in the F11 gene for circulating FXI levels. To validate this genetic proxy, we examined its associations with positive control thromboembolic diseases and its mechanistic specificity using cardiovascular risk factors unrelated to coagulation. We then obtained genetic associations for the primary outcome of all-cause heart failure (139 533 cases and 1 568 809 controls) and secondary outcomes of heart failure subtypes (up to 42 081 cases), atrial fibrillation (181 446 cases), and magnetic resonance imaging correlates of cardiovascular function (up to 38 251 participants). We performed Mendelian randomization analyses using the Wald ratio method to estimate the association of a lifelong 1-SD reduction in genetically proxied FXI levels on each outcome.
Results: We identified an F11 variant that reduced circulating FXI levels by 0.33 SD units (P<1×10-200), conferred protection against venous thromboembolism (odds ratio per 1-SD reduction in FXI levels, 0.61 [95% CI, 0.60-0.63]; P=1.85×10-198), and showed no association with cardiovascular risk factors (P>0.05). Genetically proxied lower FXI levels were not associated with all-cause heart failure (odds ratio, 0.99 [95% CI, 0.96-1.01]; P=0.34), nor with any secondary clinical or radiographic outcomes (all P>0.05).
Conclusions: Current human genetic evidence does not support an adverse effect of lower FXI levels on heart failure risk or cardiovascular function. Further studies examining the effect of FXI levels on cardiac events and function are warranted.
Keywords: atrial fibrillation; factor XI; genome-wide association study; heart failure; magnetic resonance imaging.
Conflict of interest statement
D. Gill is the Chief Executive Officer of Sequoia Genetics, a private limited company that works with investors, pharma, biotech, and academia by performing research that leverages genetic data to help inform drug discovery and development. D. Gill has financial interests in several biotechnology companies. These biotechnology company interests are unrelated to anticoagulants or coagulation factor modulators. No funds or other support were provided to this study by a third party with a commercial interest in developing drugs that target factor XI. The other author reports no conflicts.
Comment in
-
Factor XI and Heart Failure.Arterioscler Thromb Vasc Biol. 2025 Sep;45(9):1670-1671. doi: 10.1161/ATVBAHA.125.323395. Epub 2025 Aug 7. Arterioscler Thromb Vasc Biol. 2025. PMID: 40772293 No abstract available.
MeSH terms
Substances
LinkOut - more resources
Full Text Sources
Medical
Miscellaneous
