Díaz-Ricart M, Isola I M, Escolar G
Hematopatologia, Anatomia Patològica, Centre de Diagnòstic Biomèdic (CDB), Hospital Clínic, IDIBAPS, Universitat de Barcelona, Barcelona, Spain.
Drugs Today (Barc). 2018 Oct;54(10):591-600. doi: 10.1358/dot.2018.54.10.2869771.
Hemophilia A is an X-linked bleeding disorder caused by defects in the gene encoding factor VIII (FVIII). Routine prophylaxis with exogenous FVIII requires frequent intravenous injections. One of the most challenging issues in the treatment of hemophilia A is the development of alloantibodies against infused FVIII. Presence of inhibitors results in an ineffective factor replacement therapy and increases the risk of morbidity and mortality in these patients. Therefore, there is growing interest in the development of new strategies for the prophylaxis and prevention of bleeding in patients with hemophilia to circumvent these drawbacks. Emicizumab (ACE-910; Roche, Genentech and Chugai Pharmaceutical) is a recombinant humanized bispecific antibody that restores the function of missing FVIII by bridging activated FIX and FX, simulating the cofactor function of FVIII.
甲型血友病是一种X连锁出血性疾病,由编码凝血因子VIII(FVIII)的基因缺陷引起。使用外源性FVIII进行常规预防需要频繁静脉注射。甲型血友病治疗中最具挑战性的问题之一是产生针对输注FVIII的同种抗体。抑制剂的存在导致因子替代治疗无效,并增加了这些患者发病和死亡的风险。因此,人们越来越关注开发新的策略来预防和防止血友病患者出血,以规避这些缺点。艾美赛珠单抗(ACE-910;罗氏、基因泰克和中外制药)是一种重组人源化双特异性抗体,通过桥接活化的FIX和FX来恢复缺失的FVIII的功能,模拟FVIII的辅因子功能。
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