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重组凝血因子VIII治疗甲型血友病的药代动力学药物评价

Pharmacokinetic drug evaluation of recombinant factor VIII for the treatment of hemophilia A.

作者信息

Castaman Giancarlo, Linari Silvia

机构信息

a Center for Bleeding Disorders, Department of Oncology , Careggi University Hospital , Florence , Italy.

出版信息

Expert Opin Drug Metab Toxicol. 2018 Feb;14(2):143-151. doi: 10.1080/17425255.2018.1420161. Epub 2017 Dec 27.

Abstract

The prevention of bleeding by prophylactic factor replacement is the recommended approach for the treatment of severe hemophilia. Prophylaxis should be individualized to provide the best clinical benefit to each patient. Therefore, a pharmacokinetic approach is crucial. Areas covered: This review aims to concisely describe the basic principles of pharmacokinetics of FVIII, the role of population pharmacokinetic, the available different recombinant FVIII concentrates and the new extended half-life FVIII molecules with possible improvement in hemophilia A treatment. Expert opinion: Pharmacokinetic is a useful tool to predict the outcome of replacement therapy, even though a large inter-individual variability exists, becauseof several factors: age, weight, von Willebrand factor level, blood group, active bleed, presence of inhibitors to FVIII, FVIII concentrate. Among the different recombinant FVIII concentrates pharmacokinetic differences are minor and clinically not significant. The extended half-life FVIII products brings only moderate advances, as half life extension is limited to 1.5-1.8-fold in comparison to that of native FVIII. Thus, infusions could be done every fourth, rarely fifth day to ensure a safe through level and a significant benefit can be offered only to patients treated every other day or three times weekly.

摘要

通过预防性因子替代预防出血是治疗重度血友病的推荐方法。预防应个体化,以便为每位患者提供最佳临床效益。因此,药代动力学方法至关重要。涵盖领域:本综述旨在简要描述FVIII药代动力学的基本原理、群体药代动力学的作用、现有的不同重组FVIII浓缩物以及可能改善A型血友病治疗的新型延长半衰期FVIII分子。专家观点:尽管由于年龄、体重、血管性血友病因子水平、血型、活动性出血、FVIII抑制剂的存在、FVIII浓缩物等多种因素存在较大个体间变异性,但药代动力学仍是预测替代治疗结果的有用工具。在不同的重组FVIII浓缩物中,药代动力学差异较小且临床意义不大。延长半衰期的FVIII产品仅带来适度进展,因为与天然FVIII相比,半衰期延长仅限于1.5至1.8倍。因此,可以每四天(很少每五天)进行一次输注,以确保安全的血药浓度,并且只有对每隔一天或每周三次治疗的患者才能提供显著益处。

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