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血友病人群的预防。

Prophylaxis in the haemophilia population.

机构信息

Division of Hematology/Oncology, Hospital for Sick Children, Toronto, ON, Canada.

出版信息

Haemophilia. 2010 Jul;16 Suppl 5:181-8. doi: 10.1111/j.1365-2516.2010.02318.x.

DOI:10.1111/j.1365-2516.2010.02318.x
PMID:20590879
Abstract

Prophylaxis is recommended as preventive therapy for young boys with severe haemophilia in countries where safe factor concentrates are available. This recommendation is supported by results from a randomized, controlled study that compared on-demand therapy with full-dose prophylaxis (Manco-Johnson MJ, Abshire TC, Shapiro AD et al. N Engl J Med 2007;357:535). It is important to distinguish primary vs. secondary prophylaxis. Primary prophylaxis refers to preventive treatment started before the onset of joint damage, whereas secondary prophylaxis refers to treatment started after joint damage has occurred. Whereas the benefits of primary prophylaxis are well documented, data relating to secondary prophylaxis are limited, especially in the adolescent/adult haemophilia population. Failure of prophylaxis may relate to several variables, including: (i) underlying status of the joints; (ii) poor compliance; (iii) participation in high-risk activities and (iv) unfavourable pharmacokinetics (PK), i.e., too rapid elimination of infused coagulation factors. There is evidence that the risk of joint bleeding in individuals with severe haemophilia A relates to time spent with factor levels < 1% (Collins PW, Blanchette VS, Fischer K et al. J Thromb Haemost 2009;7:413); this variable is strongly influenced by frequency of factor infusions and the individual's PK profile. Key ongoing questions relating to prophylaxis include: (1) what is the optimal regimen for initiating primary prophylaxis; (2) role of prophylaxis in the adolescent/young adult haemophilia population and (3) role of prophylaxis in individuals with severe von Willebrand's disease and other rare inherited coagulation disorders. The role of novel long-acting factor concentrates for prophylaxis will also need to be evaluated.

摘要

预防治疗推荐用于有安全因子浓缩物的国家中患有严重血友病的小男孩。该推荐基于一项比较按需治疗与全剂量预防治疗的随机对照研究结果(Manco-Johnson MJ、Abshire TC、Shapiro AD 等,N Engl J Med 2007;357:535)。区分初级预防与次级预防非常重要。初级预防是指在关节损伤发生之前开始的预防性治疗,而次级预防是指在关节损伤发生后开始的治疗。虽然初级预防的益处已有充分的记录,但与次级预防相关的数据有限,尤其是在青少年/成年血友病患者中。预防治疗失败可能与几个变量有关,包括:(i)关节的基本状况;(ii)依从性差;(iii)参与高风险活动和(iv)不利的药代动力学(PK),即输注的凝血因子过快消除。有证据表明,严重血友病 A 患者关节出血的风险与因子水平<1%的时间有关(Collins PW、Blanchette VS、Fischer K 等,J Thromb Haemost 2009;7:413);该变量受因子输注频率和个体 PK 特征的强烈影响。与预防治疗相关的关键问题包括:(1)启动初级预防的最佳方案是什么;(2)预防治疗在青少年/年轻成年血友病患者中的作用;(3)预防治疗在严重血管性血友病患者和其他罕见遗传性凝血障碍患者中的作用。新型长效因子浓缩物在预防治疗中的作用也需要进行评估。

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