凝血酶
组织因子
出血时间
体内
血栓
凝结
抗凝血酶
内科学
化学
医学
因子IX
凝血活酶
凝血时间激活
内分泌学
血小板
抗凝剂
肝素
生物
血小板聚集
生物技术
作者
Sebastien Verhenne,Geneviève Mccluskey,Hortense Maynadié,Frédéric Adam,Caterina Casari,Laurence Panicot‐Dubois,Lydie Crescence,Christophe Dubois,Cécile V. Denis,Peter J. Lenting,Olivier D. Christophe
出处
期刊:Blood
[American Society of Hematology]
日期:2024-04-15
卷期号:144 (2): 227-236
被引量:3
标识
DOI:10.1182/blood.2023023404
摘要
Abstract Factor X (FX) deficiency is a rare bleeding disorder manifesting a bleeding tendency caused by low FX activity levels. We aim to explore the use of fitusiran (an investigational small interfering RNA that silences antithrombin expression) to increase thrombin generation and the in vivo hemostatic potential under conditions of FX deficiency. We therefore developed a novel model of inducible FX deficiency, generating mice expressing <1% FX activity and antigen (f10low mice). Compared with control f10WT mice, f10low mice had sixfold and fourfold prolonged clotting times in prothrombin time and activated partial prothrombin time assays, respectively (P < .001). Thrombin generation was severely reduced, irrespective of whether tissue factor or factor XIa was used as an initiator. In vivo analysis revealed near-absent thrombus formation in a laser-induced vessel injury model. Furthermore, in 2 distinct bleeding models, f10low mice displayed an increased bleeding tendency compared with f10WT mice. In the tail-clip assay, blood loss was increased from 12 ± 16 μL to 590 ± 335 μL (P < .0001). In the saphenous vein puncture (SVP) model, the number of clots generated was reduced from 19 ± 5 clots every 30 minutes for f10WT mice to 2 ± 2 clots every 30 minutes (P < .0001) for f10low mice. In both models, bleeding was corrected upon infusion of purified FX. Treatment of f10low mice with fitusiran (2 × 10 mg/kg at 1 week interval) resulted in 17 ± 6% residual antithrombin activity and increased thrombin generation (fourfold and twofold to threefold increase in endogenous thrombin potential and thrombin peak, respectively). In the SVP model, the number of clots was increased to 8 ± 6 clots every 30 minutes (P = .0029). Altogether, we demonstrate that reduction in antithrombin levels is associated with improved hemostatic activity under conditions of FX deficiency.
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