Targeting factor XI as a compromise between thrombosis and bleeding
Research article published in Cardiology journal (2025)
Abstract
Thromboembolic diseases have long been a leading cause of morbidity and mortality, necessitating advances in anticoagulant drugs. Heparins, vitamin K inhibitors, and direct oral anticoagulants (DOACs) are well-established drug classes that help prevent thromboembolic complications. While effective, they pose significant risks during long-term therapy, including bleeding, osteoporosis, heparin-induced thrombocytopenia, and the need for frequent monitoring and dose adjustments. Factor XI (FXI) inhibitors represent an innovative approach in anticoagulation therapy, aiming to balance thromboembolic events with the risk of bleeding complications. They include: a) orally administered small molecule inhibitors such as milvexian and asundexian; b) monoclonal antibodies such as abelacimab, osocimab, and xisomab, which specifically bind and inactivate FXI; c) FXI-antisense oligonucleotide (FXI-ASO), which downregulate FXI synthesis at the mRNA level and reduce plasma FXI concentrations. Available data indicate that FXI inhibitors decrease the risk of thromboembolic events and are associated with a lower incidence of major bleeding than current gold standard methods. Hence, FXI inhibitors may become the preferred anticoagulant class, especially for patients with elevated bleeding risk. Their development is an important step in the history of anticoagulant therapy, striving to find a balance between preventing thromboembolism and reducing bleeding risk, ultimately improving patient outcomes. In this context, a discussion on the characteristics of FXI inhibitors, a summary on data regarding the efficacy and safety of FXI inhibitors based on preclinical and clinical studies, and an outline of future perspectives regarding therapeutic strategies of FXI inhibition in venous thrombosis are presented in this study.
Abstract sourced from PubMed (NCBI) for the cited record. See the original publication for the authoritative version.
Resumen
Peer-reviewed research on safety and infection-control considerations relevant to leech therapy and anticoagulation. Indexed in PubMed and verified against the NCBI record.
Por qué esto importa para la hirudoterapia
Esta revisión analiza los inhibidores del Factor XI (FXI) —moléculas pequeñas (milvexian, asundexian), anticuerpos monoclonales (abelacimab, osocimab, xisomab) y oligonucleótidos antisentido— como una clase de anticoagulantes diseñados para desvincular la prevención de la trombosis del riesgo de hemorragia, señalando que los datos disponibles sugieren una reducción de los eventos tromboembólicos con menos hemorragias mayores que los estándares actuales. Esto es relevante para la historia del secretoma de la sanguijuela porque refleja el objetivo farmacológico central que encarnan los anticoagulantes salivales de la sanguijuela medicinal a nivel local: interrumpir la coagulación limitando la hemorragia sistémica; el secretoma de la sanguijuela contiene inhibidores dirigidos al Factor Xa y a la trombina que históricamente fundamentaron el descubrimiento de fármacos anticoagulantes. La advertencia es que se trata de una revisión narrativa de fármacos en investigación y emergentes, no de datos originales ni sobre compuestos derivados de la sanguijuela, por lo que proporciona antecedentes y justificación en lugar de evidencia específica de la hirudoterapia.
Citación
Targeting factor XI as a compromise between thrombosis and bleeding.
Żuk-Łapan et al. · Cardiology journal, 2025
Contexto clínico relacionado
Explore cómo esta investigación se conecta con la práctica clínica
Añadido a la biblioteca ASH: May 28, 2026 · Última actualización del sitio: June 18, 2026