Center for Biologics Evaluation and Research, U.S. Food and Drug Administration, Silver Spring, MD 20993, USA.
Int J Mol Sci. 2023 May 11;24(10):8584. doi: 10.3390/ijms24108584.
Factor VIII (FVIII) is an important component of blood coagulation as its congenital deficiency results in life-threatening bleeding. Current prophylactic therapy of the disease (hemophilia A) is based on 3-4 intravenous infusions of therapeutic FVIII per week. This poses a burden on patients, demanding reduction of infusion frequency by using FVIII with extended plasma half-life (EHL). Development of these products requires understanding FVIII plasma clearance mechanisms. This paper overviews (i) an up-to-date state of the research in this field and (ii) current EHL FVIII products, including recently approved efanesoctocog alfa, for which the plasma half-life exceeds a biochemical barrier posed by von Willebrand factor, complexed with FVIII in plasma, which results in ~1 per week infusion frequency. We focus on the EHL FVIII products' structure and function, in particular related to the known discrepancy in results of one-stage clotting (OC) and chromogenic substrate (CS) assays used to assign the products' potency, dosing, and for clinical monitoring in plasma. We suggest a possible root cause of these assays' discrepancy that is also pertinent to EHL factor IX variants used to treat hemophilia B. Finally, we discuss approaches in designing future EHL FVIII variants, including those to be used for hemophilia A gene therapy.
凝血因子 VIII(FVIII)是血液凝固的重要组成部分,因为其先天性缺乏会导致危及生命的出血。目前,该疾病(血友病 A)的预防性治疗基于每周进行 3-4 次静脉输注治疗性 FVIII。这给患者带来了负担,需要通过使用半衰期延长的 FVIII(EHL)来减少输注频率。这些产品的开发需要了解 FVIII 血浆清除机制。本文综述了(i)该领域的最新研究现状和(ii)当前的 EHL FVIII 产品,包括最近批准的 efanesoctocog alfa,其半衰期超过了 von Willebrand 因子与 FVIII 在血浆中形成的复合物所构成的生化屏障,从而使输注频率达到每周 1 次。我们重点介绍了 EHL FVIII 产品的结构和功能,特别是与用于确定产品效价、剂量和临床监测的一期凝血(OC)和显色底物(CS)测定结果的已知差异有关。我们提出了这些测定结果差异的可能根本原因,这也与用于治疗血友病 B 的 EHL 因子 IX 变体有关。最后,我们讨论了设计未来 EHL FVIII 变体的方法,包括用于血友病 A 基因治疗的变体。
