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氨甲环酸联合凝血因子 VIII 浓缩剂在重度甲型血友病预防性治疗中的止血效果:一项临床前研究。

Hemostatic effect of tranexamic acid combined with factor VIII concentrate in prophylactic setting in severe hemophilia A: A preclinical study.

作者信息

Janbain Maissa, Enjolras Nathalie, Bordet Jean-Claude, Bolbos Radu, Brevet Marie, Leissinger Cindy, Dargaud Yesim

机构信息

Tulane School of Medicine, Hematology, New Orleans, LA, USA.

EA4609 Unite de Recherche Hemostase et Cancer, Universite Lyon 1, Lyon, France.

出版信息

J Thromb Haemost. 2020 Mar;18(3):584-592. doi: 10.1111/jth.14694. Epub 2019 Dec 22.

Abstract

BACKGROUND

Hemophilia is characterized by a compromised hemostatic response with delayed development of a clot and the formation of clots that are vulnerable to fibrinolysis. We proposed to study, in vitro and in factor VIII knockout mice (FVIII-KO), whether hemostasis is improved with the addition of tranexamic acid (TXA) to low FVIII plasma concentrations.

METHODS

In vitro, blood samples from adults with severe hemophilia-A, spiked to final concentrations of 0-3-10 and 30IU.dL of FVIII, were studied with and without TXA 0.1 mg/mL using thromboelastography in the presence of tPA (ROTEM-tPA), thrombin generation (TG) assay, and scanning electron microscopy. FVIII-KO mice received prophylaxis before trauma, to obtain circulating plasma FVIII at 3 IU.dL or FVIII 3IU.dL  + TXA 0.1 mg/mL. After trauma-induced knee joint bleeding, magnetic resonance imaging, histological analysis, and tail clip assay were used to compare hemostastic efficacy of the two prophylactic strategies.

RESULTS

A dose-dependent improvement of TG was observed with recombinant FVIII (rFVIII) alone (P = .024). As expected, no effect of TXA on TG capacity was observed. Fibrin fiber diameters were significantly decreased with TXA + rFVIII compared to rFVIII, suggesting a stronger fibrin network. Surprisingly, ROTEM-tPA was normalized with TXA alone. In FVIII-KO mice, blood loss after tail clip was lower after prophylaxis with rFVIII + TXA compared to rFVIII, with no statistical significance (P = .15). However, MRI results and histological analysis of knee joints showed that the addition of TXA significantly decreased joint bleeding (P = .022).

CONCLUSION

Our results suggest a potential benefit of TXA when used in combination with FVIII in prophylactic settings.

摘要

背景

血友病的特征是止血反应受损,凝血延迟发展且形成的凝块易发生纤维蛋白溶解。我们建议在体外以及在因子VIII基因敲除小鼠(FVIII-KO)中研究,在低FVIII血浆浓度下添加氨甲环酸(TXA)是否能改善止血功能。

方法

在体外,使用血栓弹力图(ROTEM-tPA)、凝血酶生成(TG)测定法和扫描电子显微镜,对重度血友病A成年患者的血样进行研究,将FVIII终浓度分别调至0 - 3 - 10和30IU/dL,并添加或不添加0.1mg/mL的TXA。FVIII-KO小鼠在创伤前接受预防治疗,以使循环血浆FVIII浓度达到3IU/dL或FVIII 3IU/dL + TXA 0.1mg/mL。在创伤诱导的膝关节出血后,使用磁共振成像、组织学分析和尾夹试验来比较两种预防策略的止血效果。

结果

单独使用重组FVIII(rFVIII)时观察到TG呈剂量依赖性改善(P = 0.024)。正如预期的那样,未观察到TXA对TG能力有影响。与rFVIII相比,TXA + rFVIII组的纤维蛋白纤维直径显著减小,表明纤维蛋白网络更强。令人惊讶的是,单独使用TXA可使ROTEM-tPA恢复正常。在FVIII-KO小鼠中,与rFVIII相比,rFVIII + TXA预防后尾夹后的失血量较低,但无统计学意义(P = 0.15)。然而,MRI结果和膝关节组织学分析表明,添加TXA可显著减少关节出血(P = 0.022)。

结论

我们的结果表明,在预防性治疗中,TXA与FVIII联合使用可能有益。

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