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使用旋转血栓弹力图对艾美赛珠单抗和华法林的整体凝血潜力进行体外评估。

In vitro evaluation of global coagulation potential of emicizumab and warfarin using rotational thromboelastometry.

作者信息

Kajimoto Takahiro, Nakajima Yuto, Tsujii Nobuyuki, Nogami Keiji

机构信息

Department of Pediatrics, Nara Medical University, 840 Shijo-cho, Kashihara, Nara, 634-8522, Japan.

出版信息

Int J Hematol. 2025 Apr 28. doi: 10.1007/s12185-025-03986-2.

Abstract

Warfarin inhibits the generation of vitamin K-dependent proteins and emicizumab can prevent bleeding episodes in people with hemophilia A (PwHA), but their combined hemostatic potential remains unclear. We analyzed the coagulation potential of emicizumab combined with warfarin in a simulated model of PwHA. Nineteen samples were collected from ten patients taking warfarin, and the prothrombin time-international normalized ratio (PT-INR) was used to define near-normal (INR 1.2-1.48; n = 4), subtherapeutic (INR 1.56-1.9; n = 7) and therapeutic (INR > 2.0; n = 8) groups. Factor (F)VIII activity (FVIII:C) was neutralized using an anti-FVIII inhibitor antibody (termed FVIII-depleted) before the addition of emicizumab (50 µg/mL). Coagulation potential was measured using Ca2 + -triggered rotational thromboelastometry, and was compared with that in emicizumab-treated PwHA. The average PT-INR in the near-normal, subtherapeutic, and therapeutic groups was 1.3 ± 0.1, 1.7 ± 0.1, and 2.4 ± 0.3, respectively. The hemostatic potential in FVIII-depleted samples mixed with emicizumab in the near-normal group was comparable to that in emicizumab-treated PwHA. The coagulation potential in FVIII-depleted samples after addition of emicizumab in the subtherapeutic and therapeutic groups were lower than that in emicizumab-treated PwHA. PT-INR monitoring could be informative in emicizumab-treated PwHA due to the influence of vitamin K-dependent proteins.

摘要

华法林会抑制维生素K依赖蛋白的生成,而艾美赛珠单抗可以预防A型血友病患者(PwHA)的出血事件,但其联合止血潜力仍不清楚。我们在PwHA的模拟模型中分析了艾美赛珠单抗与华法林联合使用时的凝血潜力。从10名服用华法林的患者中采集了19份样本,采用凝血酶原时间-国际标准化比值(PT-INR)来定义接近正常(INR 1.2 - 1.48;n = 4)、治疗不足(INR 1.56 - 1.9;n = 7)和治疗有效(INR > 2.0;n = 8)组。在加入艾美赛珠单抗(50 μg/mL)之前,使用抗FVIII抑制剂抗体中和因子(F)VIII活性(FVIII:C)(称为FVIII缺失)。使用Ca2 +触发的旋转血栓弹力图测量凝血潜力,并与接受艾美赛珠单抗治疗的PwHA进行比较。接近正常组、治疗不足组和治疗有效组的平均PT-INR分别为1.3±0.1、1.7±0.1和2.4±0.3。接近正常组中与艾美赛珠单抗混合的FVIII缺失样本的止血潜力与接受艾美赛珠单抗治疗的PwHA相当。治疗不足组和治疗有效组中加入艾美赛珠单抗后FVIII缺失样本的凝血潜力低于接受艾美赛珠单抗治疗的PwHA。由于维生素K依赖蛋白的影响,PT-INR监测对于接受艾美赛珠单抗治疗的PwHA可能具有指导意义。

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