Coumarins as factor XIIa inhibitors: Potency and selectivity improvements using a fragment-based strategy
Research article published in European journal of medicinal chemistry (2023)
Abstract
Previously, we described weak coumarin inhibitors of factor XIIa, a promising target for artificial surface-induced thrombosis and various inflammatory diseases. In this work, we used fragment-based drug discovery approach to improve our coumarin series. First, we screened about 200 fragments for the S1 pocket. The S1 pocket of trypsin-like serine proteases, such as factor XIIa, is highly conserved and is known to drive a major part of the association energy. From the screening, we selected fragments displaying a micromolar activity and studied their selectivity on other serine proteases. Then, these fragments were merged to our coumarin templates, leading to the generation of nanomolar inhibitors. The mechanism of inhibition was further studied by mass spectrometry demonstrating the covalent binding through the formation of an acyl enzyme complex. The most potent compound was tested in plasma to evaluate its stability and efficacy on coagulation assays. It exhibited a plasmatic half-life of 1.9 h and a good selectivity for the intrinsic coagulation pathway over the extrinsic one.
Abstract sourced from PubMed (NCBI) for the cited record. See the original publication for the authoritative version.
Resumen
Peer-reviewed pharmacology and drug-development research relevant to antithrombotic agents and leech-derived compounds. Indexed in PubMed and verified against the NCBI record.
Por qué esto importa para la hirudoterapia
Utilizando una estrategia de descubrimiento de fármacos basada en fragmentos, este estudio mejoró los débiles inhibidores coumarínicos del factor XIIa en inhibidores de unión covalente de nanomolar con buena selectividad para la vía de coagulación intrínseca y una vida media plasmática de ~1.9 h, posicionando al FXIIa como un objetivo para la trombosis inducida por superficie artificial y la enfermedad inflamatoria. Para la ASH, refuerza que la vía de contacto/intrínseca, donde también operan los péptidos anticoagulantes derivados de lombrices de tierra (Hirudo medicinalis/verbana), es un objetivo de anticoagulación activamente perseguido, ayudando a delimitar la justificación detrás del estudio de moléculas del secretoma natural. Nota aclaratoria: esto es trabajo de química medicinal preclínica e in vitro/plasma sobre compuestos coumarínicos sintéticos sin datos de resultados animales o clínicos, y no implica lombrices ni hirudoterapia.
Citación
Coumarins as factor XIIa inhibitors: Potency and selectivity improvements using a fragment-based strategy.
Davoine et al. · European journal of medicinal chemistry, 2023
Contexto clínico relacionado
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Añadido a la biblioteca ASH: May 28, 2026 · Última actualización del sitio: June 18, 2026