Impact of extracorporeal membrane oxygenation treatments on acquired von Willebrand syndrome in patients with out-of-hospital cardiac arrest: a retrospective observational study.

IF 2.6 4区 医学 Q2 HEMATOLOGY Thrombosis Journal Pub Date : 2024-05-31 DOI:10.1186/s12959-024-00617-4
Yuki Chiba, Kota Goto, Misako Suzuki, Hisanori Horiuchi, Mineji Hayakawa
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Abstract

Background: Von Willebrand factor (vWF) plays a crucial role in hemostasis, acting as a key factor for platelet adhesion/aggregation and as a transport protein for coagulation factor VIII. vWF is secreted as a giant multimer, and it undergoes shear stress-dependent cleavage by a specific metalloproteinase in plasma. Among vWF multimers, high-molecular-weight (large) multimers are essential for hemostasis. Acquired von Willebrand syndrome, linked to various conditions, is a hemostatic disorder due to reduced vWF activity. Extracorporeal membrane oxygenation (ECMO), utilized recently for out-of-hospital cardiac arrest patients, generates high shear stress inside the pump. This stress may induce a conformational change in vWF, enhancing cleavage by a specific metalloproteinase and thereby reducing vWF activity. However, no study has investigated the effects of ECMO on vWF-related factors in patients receiving or not receiving ECMO. This study aimed to elucidate the relationship between ECMO treatment and acquired von Willebrand syndrome-related factors in patients with out-of-hospital cardiac arrest.

Methods: This study included patients with cardiogenic out-of-hospital cardiac arrest admitted to our hospital. The patients were categorized into two groups (ECMO and non-ECMO) based on the presence or absence of ECMO treatment. Plasma samples were collected from patients admitted to the emergency department (days 0-4). The vWF antigen (vWF: Ag), vWF ristocetin cofactor activity (vWF: RCo), and factor VIII activity were measured. Additionally, a large multimer of vWF was evaluated through vWF multimer analysis, utilizing western blotting to probe vWF under non-reducing conditions.

Results: The ECMO and non-ECMO groups included 10 and 22 patients, respectively. The median ECMO treatment in the ECMO group was 64.6 h. No differences in vWF: Ag or factor VIII activity were observed between the two groups during the observation period. However, the ECMO group exhibited a decrease in large vWF multimers and vWF: RCo during ECMO. Strong correlations were observed between vWF: RCo and vWF: Ag in both groups, although the relationships were significantly different between the two groups.

Conclusions: ECMO treatment in patients with out-of-hospital cardiac arrest resulted in the loss of large vWF multimers and decreased vWF activity. Hence, decreased vWF activity should be considered as a cause of bleeding during ECMO management.

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体外膜氧合治疗对院外心脏骤停患者获得性冯-威廉综合征的影响:一项回顾性观察研究。
背景:Von Willebrand因子(vWF)在止血过程中起着至关重要的作用,它是血小板粘附/聚集的关键因子,也是凝血因子VIII的转运蛋白。在 vWF 多聚体中,高分子量(大)多聚体对止血至关重要。获得性冯-威廉综合征(Acquired von Willebrand syndrome)与多种疾病有关,是一种因 vWF 活性降低而导致的止血障碍。最近用于院外心脏骤停患者的体外膜肺氧合(ECMO)会在泵内产生高剪切应力。这种应力可能会诱导 vWF 发生构象变化,增强特定金属蛋白酶的裂解作用,从而降低 vWF 的活性。然而,还没有研究调查过接受或未接受 ECMO 的患者中,ECMO 对 vWF 相关因素的影响。本研究旨在阐明院外心脏骤停患者接受 ECMO 治疗与获得性 von Willebrand 综合征相关因素之间的关系:本研究纳入了本院收治的院外心源性心脏骤停患者。根据是否接受过 ECMO 治疗,将患者分为两组(ECMO 和非 ECMO)。从急诊科入院患者(第 0-4 天)处采集血浆样本。测定了 vWF 抗原(vWF:Ag)、vWF ristocetin 辅因子活性(vWF:RCo)和因子 VIII 活性。此外,还通过 vWF 多聚体分析评估了 vWF 的大型多聚体,利用 Western 印迹技术在非还原条件下探查 vWF:ECMO组和非ECMO组分别有10名和22名患者。在观察期间,两组患者的 vWF:Ag 或因子 VIII 活性未见差异。然而,ECMO 组在 ECMO 期间显示出大的 vWF 多聚体和 vWF: RCo 的减少。两组患者的 vWF:RCo 和 vWF:Ag 之间均存在很强的相关性,但两组之间的关系存在显著差异:结论:院外心脏骤停患者的 ECMO 治疗导致大的 vWF 多聚体丧失,vWF 活性降低。因此,在 ECMO 治疗期间,vWF 活性降低应被视为出血的原因之一。
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来源期刊
Thrombosis Journal
Thrombosis Journal Medicine-Hematology
CiteScore
3.80
自引率
3.20%
发文量
69
审稿时长
16 weeks
期刊介绍: Thrombosis Journal is an open-access journal that publishes original articles on aspects of clinical and basic research, new methodology, case reports and reviews in the areas of thrombosis. Topics of particular interest include the diagnosis of arterial and venous thrombosis, new antithrombotic treatments, new developments in the understanding, diagnosis and treatments of atherosclerotic vessel disease, relations between haemostasis and vascular disease, hypertension, diabetes, immunology and obesity.
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