Ex vivo evaluation of the effect of plasma-derived factor VIII/von Willebrand factor in patients with severe hemophilia A on emicizumab prophylaxis.

IF 3.2 4区医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL Clinical and Experimental Medicine Pub Date : 2024-12-21 DOI:10.1007/s10238-024-01528-4

Aida Raventós, Elena G Arias-Salgado, Alba Pérez, María Teresa Alvarez-Román, Nora V Butta, Elena Monzon Manzano, Paula Acuña, Víctor Jiménez-Yuste, Montserrat Costa, María Isabel Bravo

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Abstract

Hemophilia A (HA) patients under emicizumab prophylaxis may require the concomitant use of procoagulant factors for breakthrough bleedings or immune tolerance induction (ITI). The aim of this study is to evaluate the ex vivo procoagulant effect of plasma-derived FVIII concentrates containing von Willebrand factor (pdFVIII/VWF) in samples from patients with severe HA without inhibitors on emicizumab prophylaxis. Samples from healthy controls (HC) and HA patients were drawn in sodium citrate plus corn trypsin inhibitor tubes and spiked with increasing concentrations of pdFVIII/VWF concentrates (10-400 IU/dL) (Fanhdi^®/Alphanate^®, Grifols), activated prothrombin complex concentrate (aPCC, 0.5 U/mL) or recombinant activated factor VII (rFVIIa, 0.9 µg/mL). Global coagulation was measured by rotational thromboelastometry (ROTEM) (clotting time [CT] and time to maximum clot formation velocity [MAXV-t]) and thrombin generation (TG) assay (thrombin peak [TP] and endogenous thrombin potential [ETP]). Samples from HA patients under emicizumab prophylaxis showed CT and MAXV-t values above HC levels, while TP and ETP were below HC levels. Ex vivo pdFVIII/VWF supplementation increased TP and ETP and shortened CT and MAXV-t dose-dependently. At 50 IU/dL (≈25 IU/kg), pdFVIII/VWF normalized clot formation and restored TG within HC normal range. The highest pdFVIII/VWF concentration (400 IU/dL) and rFVIIa did not result in an excessive procoagulant profile. However, aPCC induced ex vivo an excessive TG and markedly decreased ROTEM parameters (CT and MAXV-t). Coagulation parameters of both methods significantly correlated at baseline and with increasing concentrations of pdFVIII/VWF. High doses of pdFVIII/VWF concentrates, similar to those used for ITI, did not trigger a multiplying procoagulant effect to samples from HA patients on emicizumab prophylaxis, evidencing their low thrombotic risk in these patients.

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血浆源性因子VIII/血管性血友病因子在重度A型血友病患者中对emicizumab预防作用的体外评价

在emicizumab预防下的血友病A （HA）患者可能需要同时使用促凝因子来治疗突破性出血或免疫耐受诱导（ITI）。本研究的目的是评估含有血管性血友病因子（pdFVIII/VWF）的血浆来源FVIII浓缩物在未使用emicizumab预防的严重HA患者样本中的体外促凝作用。健康对照（HC）和HA患者的样本在柠檬酸钠加玉米胰蛋白酶抑制剂管中抽取，并加入浓度逐渐增加的pdFVIII/VWF浓缩物（10-400 IU/dL）（Fanhdi®/ alpha - ate®，Grifols）、活化凝血酶原复合物浓缩物（aPCC, 0.5 U/mL）或重组活化因子VII （rFVIIa, 0.9µg/mL）。通过旋转血栓弹性测量（ROTEM）（凝血时间[CT]和最大凝块形成速度时间[MAXV-t]）和凝血酶生成（TG）测定（凝血酶峰值[TP]和内源性凝血酶电位[ETP]）测量整体凝血情况。接受emicizumab预防的HA患者样本显示CT和MAXV-t值高于HC水平，而TP和ETP低于HC水平。体外补充pdFVIII/VWF增加TP和ETP，缩短CT和MAXV-t剂量依赖性。在50 IU/dL（≈25 IU/kg）时，pdFVIII/VWF使凝块形成正常化，并使TG恢复在HC正常范围内。最高pdFVIII/VWF浓度（400 IU/dL）和rFVIIa不会导致过多的促凝剂。然而，aPCC诱导体外TG过高，并显著降低ROTEM参数（CT和MAXV-t）。两种方法的凝血参数在基线和pdFVIII/VWF浓度升高时显著相关。高剂量的pdFVIII/VWF浓缩物，类似于用于ITI的那些，对使用emicizumab预防的HA患者的样本没有触发倍增的促凝作用，证明它们在这些患者中的血栓形成风险较低。

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来源期刊

Clinical and Experimental Medicine 医学-医学：研究与实验

CiteScore

4.80

自引率

2.20%

发文量

159

审稿时长

2.5 months

期刊介绍： Clinical and Experimental Medicine (CEM) is a multidisciplinary journal that aims to be a forum of scientific excellence and information exchange in relation to the basic and clinical features of the following fields: hematology, onco-hematology, oncology, virology, immunology, and rheumatology. The journal publishes reviews and editorials, experimental and preclinical studies, translational research, prospectively designed clinical trials, and epidemiological studies. Papers containing new clinical or experimental data that are likely to contribute to changes in clinical practice or the way in which a disease is thought about will be given priority due to their immediate importance. Case reports will be accepted on an exceptional basis only, and their submission is discouraged. The major criteria for publication are clarity, scientific soundness, and advances in knowledge. In compliance with the overwhelmingly prevailing request by the international scientific community, and with respect for eco-compatibility issues, CEM is now published exclusively online.