因子 XIII 与止血剂共同治疗血友病 A 可增加纤维蛋白 α 链交联。
Factor XIII cotreatment with hemostatic agents in hemophilia A increases fibrin α-chain crosslinking.
机构信息
Department of Medicine, Division of Hematology and Oncology, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
Department of Pathology and Laboratory Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.
出版信息
J Thromb Haemost. 2018 Jan;16(1):131-141. doi: 10.1111/jth.13887. Epub 2017 Nov 20.
UNLABELLED
Essentials Factor XIII (FXIII)-mediated fibrin crosslinking is delayed in hemophilia. We determined effects of FXIII cotreatment with hemostatic agents on clot parameters. FXIII cotreatment accelerated FXIII activation and crosslinking of fibrin and α -antiplasmin. These data provide biochemical rationale for FXIII cotreatment in hemophilia.
SUMMARY
Background Hemophilia A results from the absence, deficiency or inhibition of factor VIII. Bleeding is treated with hemostatic agents (FVIII, recombinant activated FVII [rFVIIa], anti-inhibitor coagulation complex [FEIBA], or recombinant porcine FVIII [rpFVIII]). Despite treatment, some patients have prolonged bleeding. FXIII-A B (FXIII) is a protransglutaminase. During clot contraction, thrombin-activated FXIII (FXIIIa) crosslinks fibrin and α -antiplasmin, which promotes red blood cell retention and increases clot stability and weight. We hypothesized that FXIII cotreatment in hemophilia would accelerate FXIII activation, leading to increased fibrin crosslinking. Methods FVIII-deficient plasma and whole blood were clotted with or without hemostatic agents (FVIII, rFVIIa, FEIBA, or recombinant B-domain-deleted porcine FVIII [rpFVIII]) and/or FXIII. The effects on FXIII activation, thrombin generation, fibrin and α -antiplasmin crosslinking, clot formation and clot weight were measured by western blotting, calibrated automated thrombography, thromboelastography, and clot contraction assays. Results As compared with FVIII-treated hemophilic plasma, FVIII + FXIII cotreatment accelerated FXIIIa formation without increasing thrombin generation. As compared with buffer-treated or FXIII-treated hemophilic plasma, FVIII treatment and FVIII + FXIII cotreatment increased the generation and amount of crosslinked fibrin, including α-chain-rich high molecular weight species and crosslinked α -antiplasmin. In the presence of FVIII inhibitors, as compared with hemostatic treatments (rFVIIa, FEIBA, or rpFVIII) alone, FXIII cotreatment increased whole blood clot weight. Conclusion In hemophilia A plasma and whole blood, FXIII cotreatment with hemostatic agents accelerated FXIIIa formation, increased the generation and amount of fibrin α-chain crosslinked species, accelerated α -antiplasmin crosslinking, and increased clot weight. FXIII cotreatment with hemostatic therapy may augment hemostasis through increased crosslinking of fibrin and α -antiplasmin.
目的
因子 XIII (FXIII)介导的纤维蛋白交联在血友病中延迟。我们确定了 FXIII 与止血剂共同治疗对血栓参数的影响。FXIII 共同治疗加速了 FXIII 的激活和纤维蛋白和 α -抗纤溶酶的交联。这些数据为血友病中 FXIII 的共同治疗提供了生化依据。
背景
血友病 A 是由于因子 VIII 的缺失、缺乏或抑制引起的。出血用止血剂(FVIII、重组激活的 FVII [rFVIIa]、抗抑制剂凝血复合物 [FEIBA] 或重组猪 FVIII [rpFVIII])治疗。尽管进行了治疗,但一些患者仍有出血时间延长。FXIII-A B (FXIII) 是一种前转谷氨酰胺酶。在血栓收缩过程中,凝血酶激活的 FXIII (FXIIIa) 交联纤维蛋白和 α -抗纤溶酶,促进红细胞保留,增加血栓稳定性和重量。我们假设在血友病中 FXIII 共同治疗会加速 FXIII 的激活,导致纤维蛋白交联增加。
方法
用或不用止血剂(FVIII、rFVIIa、FEIBA 或重组 B 结构域缺失的猪 FVIII [rpFVIII])和/或 FXIII 对 FVIII 缺乏的血浆和全血进行凝血。通过 Western 印迹、校准自动血栓形成、血栓弹性描记术和血栓收缩测定来测量 FXIII 激活、凝血酶生成、纤维蛋白和 α -抗纤溶酶交联、血栓形成和血栓重量的影响。
结果
与 FVIII 治疗的血友病血浆相比,FVIII+FXIII 共同治疗加速了 FXIIIa 的形成,而不增加凝血酶的产生。与缓冲液处理或 FXIII 处理的血友病血浆相比,FVIII 治疗和 FVIII+FXIII 共同治疗增加了交联纤维蛋白的生成和量,包括 α 链丰富的高分子量物种和交联的 α -抗纤溶酶。在存在 FVIII 抑制剂的情况下,与单独使用止血剂(rFVIIa、FEIBA 或 rpFVIII)相比,FXIII 共同治疗增加了全血血栓的重量。
结论
在血友病 A 血浆和全血中,FXIII 与止血剂共同治疗加速了 FXIIIa 的形成,增加了纤维蛋白 α 链交联物的生成和量,加速了 α -抗纤溶酶的交联,并增加了血栓的重量。FXIII 与止血治疗的共同治疗可能通过增加纤维蛋白和 α -抗纤溶酶的交联来增强止血。
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