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输注于人血友病患者后,与单独的 FVIII 相比,源自血浆的 FVIII/VWF 复合物显示出对抑制剂更高的保护作用:一项转化研究。

Plasma-derived FVIII/VWF complex shows higher protection against inhibitors than isolated FVIII after infusion in haemophilic patients: A translational study.

机构信息

Bioscience Research Group, Grifols, Barcelona, Spain.

Thrombosis and Haemostasis Unit - IdiPAZ, University Hospital La Paz, Madrid, Spain.

出版信息

Haemophilia. 2022 Sep;28(5):737-744. doi: 10.1111/hae.14589. Epub 2022 Jun 2.

Abstract

INTRODUCTION

Presence of von Willebrand factor (VWF) in FVIII concentrates offers protection against neutralizing inhibitors in haemophilia A (HA). Whether this protection is more evident in plasma-derived (pd) FVIII/VWF or recombinant (r) FVIII concentrates remains controversial.

AIM

We investigated the protection exerted by VWF against FVIII inhibitors in an in vivo mouse model of HA exposed to pdFVIII/VWF or to various rFVIII concentrates.

METHODS

Haemophilia A mice received the different FVIII concentrates after administration of vehicle or an inhibitory IgG purified from a commercial pool of HA plasma with inhibitors and FVIII:C recoveries were measured. Furthermore, using a novel clinically oriented ex vivo approach, Bethesda inhibitory activities (BU) of a commercial pool of HA plasma with inhibitors were assessed using normal plasma, or plasma from severe HA patients, without inhibitors, after treatment with the same concentrates.

RESULTS

in vivo studies showed that pdFVIII/VWF offers markedly higher protection against inhibitors when compared with any of the FVIII products without VWF. More importantly, in the ex vivo studies, plasma from patients treated with pdFVIII/VWF showed higher protection against inhibitors (P values ranging .05-.001) in comparison with that observed in plasma from patients who received FVIII products without VWF, regardless of the type of product evaluated.

CONCLUSION

Data indicate that FVIII+VWF complexes assembled in the circulation after rFVIII infusion are not equivalent to the naturally formed complex in pdFVIII/VWF. Therefore, rFVIII infused into HA patients with inhibitors would be less protected by VWF than the FVIII in pdFVIII/VWF concentrates.

摘要

简介

VIII 因子浓缩物(FVIII)中存在血管性血友病因子(VWF)可防止血友病 A(HA)患者体内的中和抑制剂。在血浆源性(pd)FVIII/VWF 或重组(r)FVIII 浓缩物中,这种保护作用是否更为明显仍存在争议。

目的

我们通过在接受 pdFVIII/VWF 或各种 rFVIII 浓缩物的 HA 小鼠体内模型中研究 VWF 对 FVIII 抑制剂的保护作用,来解决这一问题。

方法

HA 小鼠在给予载体或从含有抑制剂的商业 HA 血浆池纯化的抑制性 IgG 后接受不同的 FVIII 浓缩物,并测量 FVIII:C 回收率。此外,使用一种新颖的临床导向的体外方法,使用正常血浆或无抑制剂的严重 HA 患者血浆,评估商业 HA 血浆池抑制剂的贝塞斯达抑制活性(BU),这些血浆在接受相同浓缩物治疗后使用。

结果

体内研究表明,与不含 VWF 的任何 FVIII 产品相比,pdFVIII/VWF 对抑制剂的保护作用明显更高。更重要的是,在体外研究中,与接受不含 VWF 的 FVIII 产品的患者血浆相比,接受 pdFVIII/VWF 治疗的患者血浆显示出对抑制剂更高的保护作用(P 值范围为.05-.001),无论评估的产品类型如何。

结论

数据表明,rFVIII 输注后在循环中组装的 FVIII+VWF 复合物与 pdFVIII/VWF 中天然形成的复合物不同。因此,与 pdFVIII/VWF 浓缩物中的 FVIII 相比,含有抑制剂的 HA 患者输注的 rFVIII 受到 VWF 的保护作用较小。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f28a/9545517/212e2d998b35/HAE-28-737-g003.jpg

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