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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Life in the shadow of a dominant partner: the FVIII-VWF association and its clinical implications for hemophilia A
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Life in the shadow of a dominant partner: the FVIII-VWF association and its clinical implications for hemophilia A

机译:在主要伴侣的阴影下生活:FVIII-VWF协会及其对A型血友病的临床意义

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摘要

A normal hemostatic response to vascular injury requires both factor VIII (FVIII) and von Willebrand factor (VWF). In plasma, VWF and FVIII normally circulate as a non-covalent complex, and each has a critical function in the maintenance of hemostasis. Furthermore, the interaction between VWF and FVIII plays a crucial role in FVIII function, immunogenicity, and clearance, with VWF essentially serving as a chaperone for FVIII. Several novel recombinant FVIII (rFVIII) therapies for hemophilia A have been in clinical development, which aim to increase the half-life of FVIII (similar to 12 hours) and reduce dosing frequency by utilizing bioengineering techniques including PEGylation, Fc fusion, and single-chain design. However, these approaches have achieved only moderate increases in half-life of 1.5- to 2-fold compared with marketed FVIII products. Clearance of PEGylated rFVIII, rFVIIIFc, and rVIII-SingleChain is still regulated to a large extent by interaction with VWF. Therefore, the half-life of VWF (similar to 15 hours) appears to be the limiting factor that has confounded attempts to extend the half-life of rFVIII. A greater understanding of the interaction between FVIII and VWF is required to drive novel bioengineering strategies for products that either prolong the survival of VWF or limit VWF-mediated clearance of FVIII.
机译:正常的血管损伤止血反应需要VIII因子(FVIII)和von Willebrand因子(VWF)。在血浆中,VWF和FVIII通常以非共价复合物的形式循环,并且各自在维持止血方面起关键作用。此外,VWF和FVIII之间的相互作用在FVIII功能,免疫原性和清除中起着至关重要的作用,而VWF基本上充当FVIII的伴侣。几种针对A型血友病的重组FVIII(rFVIII)治疗方法已经在临床开发中,旨在通过利用生物工程技术(包括PEG化,Fc融合和单链设计。但是,与市售的FVIII产品相比,这些方法的半衰期仅实现了1.5到2倍的适度增加。聚乙二醇化的rFVIII,rFVIIIFc和rVIII-SingleChain的清除仍在很大程度上通过与VWF的相互作用来调节。因此,VWF的半衰期(类似于15小时)似乎是限制尝试延长rFVIII半衰期的限制因素。需要更深入地了解FVIII与VWF之间的相互作用,以驱动产品的新颖生物工程策略,从而延长VWF的存活时间或限制VWF介导的FVIII清除。

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