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本文引用的文献

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2
International Society on Thrombosis and Haemostasis clinical practice guideline for treatment of congenital hemophilia A and B based on the Grading of Recommendations Assessment, Development, and Evaluation methodology.国际血栓与止血学会先天性 A 型和 B 型血友病治疗临床实践指南基于推荐评估、制定和评估方法学的分级。
J Thromb Haemost. 2024 Sep;22(9):2629-2652. doi: 10.1016/j.jtha.2024.05.026. Epub 2024 Jun 20.
3
Multicenter evaluation of the hemostatic activity of emicizumab in patients with severe hemophilia A.多中心评估艾美赛珠单抗在严重 A 型血友病患者中的止血活性。
J Thromb Haemost. 2024 Jul;22(7):1857-1866. doi: 10.1016/j.jtha.2024.03.022. Epub 2024 Apr 6.
4
Differences in venous clot structures between hemophilic mice treated with emicizumab factor VIII or factor VIIIFc.接受依库珠单抗、FVIII 或 Fc 融合蛋白治疗的血友病小鼠静脉血栓结构的差异。
Haematologica. 2024 Jun 1;109(6):1836-1848. doi: 10.3324/haematol.2023.284142.
5
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Thromb Haemost. 2023 Oct;123(10):955-965. doi: 10.1055/s-0043-1769788. Epub 2023 Jun 19.
6
In vitro validation of chromogenic substrate assay for evaluation of surrogate FVIII-activity of emicizumab.用于评估emicizumab替代FVIII活性的显色底物测定法的体外验证
Thromb Res. 2023 Feb;222:131-139. doi: 10.1016/j.thromres.2023.01.007. Epub 2023 Jan 13.
7
Comparisons of global coagulation potential and bleeding episodes in emicizumab-treated hemophilia A patients and mild hemophilia A patients.比较依库珠单抗治疗的 A 型血友病患者和轻度 A 型血友病患者的整体凝血潜能和出血发作情况。
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8
Thrombin generation for monitoring hemostatic therapy in hemophilia A: A narrative review.用于监测血友病 A 止血治疗的凝血酶生成:叙述性综述。
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9
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使用全球止血检测方法估算依美珠单抗的VIII因子等效活性

Estimating the Factor VIII-Equivalent Activity of Emicizumab Using Global Assays of Haemostasis.

作者信息

Kraemmer Daniel, Ay Cihan, Rejtő Judit, Heinze Georg, Quehenberger Peter, Pabinger Ingrid, Königsbrügge Oliver

机构信息

Division of Hematology and Hemostaseology, Department of Medicine I, Medical University of Vienna, Vienna, Austria.

Institute of Clinical Biometrics, Center for Medical Data Science, Medical University of Vienna, Vienna, Austria.

出版信息

Haemophilia. 2025 Sep;31(5):1092-1102. doi: 10.1111/hae.70085. Epub 2025 Jul 17.

DOI:10.1111/hae.70085
PMID:40674258
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12462556/
Abstract

BACKGROUND

Emicizumab is a bispecific monoclonal antibody mimicking factor (F) VIII activity and an effective therapy for prophylaxis in people with haemophilia A (PWHA). The FVIII-equivalent activity (FVIIIeq) of emicizumab remains unknown.

OBJECTIVES

To estimate FVIIIeq of emicizumab using global assays of haemostasis.

PATIENTS/METHODS: We sampled plasma from (1) PWHA of all severities and therapeutic regimens and (2) persons with severe haemophilia A on emicizumab. Thrombin generation assay (TGA) and clot formation and lysis assay (CLA) were measured by commercially available (Technothrombin, Technoclone) and turbidimetric assays, respectively. FVIII was measured by a chromogenic (CSA) and emicizumab by a modified one-stage assay (OSA). Using principal components (PC) or individual parameters as dependent and independent variables in linear regression with (1) FVIII and (2) emicizumab levels, respectively, we estimated FVIIIeq (95% CI) of emicizumab.

RESULTS

We collected 253 samples from 110 PWHA and 41 samples from nine individuals on emicizumab prophylaxis. TGA parameters of emicizumab-treated subjects clustered distinctly, with no correlation amongst samples with only endo-/exogenous FVIII. Consequently, FVIIIeq varied substantially between parameters: Using individual TGA parameters, endogenous thrombin potential (ETP) and thrombin peak resulted in conversion factors of 0.85 (0.60-1.24) and 0.25 (0.15-0.37) IU/dL FVIIIeq per µg/mL emicizumab, respectively. CLA parameters showed broader overlap, with an FVIIIeq estimate of 0.82 (0.44-1.38).

CONCLUSION

Distinct clustering of emicizumab and FVIII samples in TGA leads to conflicting FVIIIeq estimates between parameters, highlighting systematic limitations and questioning their clinical usefulness. A, possibly conservative, FVIIIeq conversion factor estimate as determined by the thrombin peak could range from 0.15 to 0.37.

摘要

背景

艾美赛珠单抗是一种模拟因子(F)VIII活性的双特异性单克隆抗体,是治疗甲型血友病(PWHA)患者预防出血的有效疗法。艾美赛珠单抗的FVIII等效活性(FVIIIeq)尚不清楚。

目的

使用全球止血检测方法估算艾美赛珠单抗的FVIIIeq。

患者/方法:我们采集了以下人群的血浆样本:(1)所有严重程度和治疗方案的PWHA,以及(2)接受艾美赛珠单抗治疗的重度甲型血友病患者。凝血酶生成检测(TGA)和凝血形成与溶解检测(CLA)分别通过市售检测方法(Technothrombin、Technoclone)和比浊法进行测量。FVIII通过发色底物法(CSA)测量,艾美赛珠单抗通过改良的一步法(OSA)测量。在分别以(1)FVIII和(2)艾美赛珠单抗水平为因变量和自变量的线性回归中,使用主成分(PC)或个体参数,我们估算了艾美赛珠单抗的FVIIIeq(95%CI)。

结果

我们从110例PWHA中收集了253份样本,从9例接受艾美赛珠单抗预防治疗的个体中收集了41份样本。接受艾美赛珠单抗治疗的受试者的TGA参数明显聚类,仅含内源性/外源性FVIII的样本之间无相关性。因此,FVIIIeq在不同参数之间差异很大:使用个体TGA参数时,内源性凝血酶潜力(ETP)和凝血酶峰值导致每微克/毫升艾美赛珠单抗的转化因子分别为0.85(0.60 - 1.24)和0.25(0.15 - 0.37)IU/dL FVIIIeq。CLA参数显示出更广泛的重叠,FVIIIeq估计值为0.82(0.44 - 1.38)。

结论

TGA中艾美赛珠单抗和FVIII样本的明显聚类导致不同参数之间FVIIIeq估计值相互矛盾,突出了系统局限性并质疑其临床实用性。由凝血酶峰值确定的一个可能较为保守的FVIIIeq转化因子估计值范围为0.15至0.37。