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基于个体化 PK 的重度血友病预防治疗。

Individualized PK-based prophylaxis in severe haemophilia.

机构信息

Unité d'Hémostase Clinique, Hôpital Cardiologique Louis Pradel, CRTH de Lyon, CHU de Lyon, France.

INSERM, UMR 1059, Pôle Biologie-Pathologie, Hôpital Nord, CHU de Saint-Etienne, France.

出版信息

Haemophilia. 2018 Mar;24 Suppl 2:3-17. doi: 10.1111/hae.13397.

Abstract

Over the past decades, haemophilia management has continually evolved, with prophylaxis now considered the treatment of choice. Prophylaxis primarily seeks to prevent bleeding and haemarthrosis episodes from occurring and avert the otherwise inevitable haemophilic arthropathy. Yet, numerous unanswered issues remain. These concern dose levels, dosing intervals, ways of integrating variability in bleeding phenotype, patient age, joint status, lifestyle, physical activity, treatment adherence and individual responses to FVIII or FIX concentrates. Individualized prophylaxis may thus be paramount. One crucial tool that may allow more accurate prophylaxis regimens to be implemented is the individual pharmacokinetic (PK) study. Therefore, physicians in charge of managing those living with haemophilia must be comfortable with PK profiling in order to be in a position to tailor patients' treatment, taking into account PK data, while minimizing patients' inconvenience, discomfort, as well as, possibly, treatment costs. For optimization of prophylaxis, recent development of recombinant molecules with more attractive PK properties, such as prolonged elimination half-life, increases the choice of dosing regimens, enabling decreased frequency of dosing for some, if deemed appropriate. For each patient, PK parameters can be determined, including trough levels, AUC, and time spent under a predefined threshold, with additional pharmacodynamic (PD) parameters possibly established by means of a global coagulation test like the thrombin generation test. Most importantly, target PK/PD parameters will need to consider clinical variables like patient age, body weight, joint status, treatment adherence, number of bleeding episodes, activity index or lifestyle.

摘要

在过去的几十年中,血友病的管理不断发展,目前预防治疗被认为是首选治疗方法。预防治疗主要旨在预防出血和关节积血发作,并避免不可避免的血友病性关节病。然而,仍有许多未解决的问题。这些问题涉及剂量水平、给药间隔、如何整合出血表型的可变性、患者年龄、关节状况、生活方式、体力活动、治疗依从性以及对 FVIII 或 FIX 浓缩物的个体反应。因此,个体化预防治疗可能是至关重要的。一个可以实现更准确预防治疗方案的重要工具是个体药代动力学(PK)研究。因此,负责管理血友病患者的医生必须熟悉 PK 分析,以便能够根据 PK 数据为患者量身定制治疗方案,同时最大限度地减少患者的不便、不适以及可能的治疗费用。为了优化预防治疗,最近开发了具有更理想 PK 特性的重组分子,如延长的消除半衰期,增加了给药方案的选择,对于一些合适的患者,可以减少给药频率。对于每个患者,可以确定 PK 参数,包括谷浓度、AUC 和在预定义阈值下花费的时间,并通过像血栓生成试验这样的全局凝血试验确定其他药效动力学(PD)参数。最重要的是,目标 PK/PD 参数将需要考虑临床变量,如患者年龄、体重、关节状况、治疗依从性、出血发作次数、活动指数或生活方式。

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