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血友病的新疗法。

New therapies for hemophilia.

机构信息

Department of Pediatrics and Communicable Diseases and.

Department of Pathology, University of Michigan, Ann Arbor, MI.

出版信息

Blood. 2019 Jan 31;133(5):389-398. doi: 10.1182/blood-2018-08-872291. Epub 2018 Dec 17.

Abstract

Hemophilia A (HA) and hemophilia B (HB) are the most common severe bleeding disorders. Replacement therapy, providing the missing coagulation factor, has been the mainstay of treatment both prophylactically and to treat bleeding. Despite widespread availability of safe and effective replacement therapy, patients with HA and HB continue to experience a tremendous burden of treatment, breakthrough bleeding, and progressive joint disease, as well as high rates of inhibitor development. These remaining challenges are now being addressed by incredible advances in bioengineering. Recombinant bioengineering has led to replacement therapies with easier modes of administration, decreased immunogenicity, increased efficacy, and extended half-lives. Emicizumab, a bispecific antibody that acts as a substitutive therapy for HA, has been approved for patients with and without inhibitors. Novel compounds are in development to exploit the natural balance of hemostasis by targeting the natural anticoagulants protein C, protein S, tissue factor pathway inhibitor, and antithrombin. The substitution and rebalancing therapies provide an opportunity for steady-state hemostatic control without exposure to immunogenic clotting factor proteins. As such, they may have broader applications outside those being investigated in the clinical trial programs.

摘要

血友病 A (HA) 和血友病 B (HB) 是最常见的严重出血性疾病。替代疗法,即提供缺失的凝血因子,一直是预防和治疗出血的主要治疗方法。尽管有广泛的安全有效的替代治疗方法,但 HA 和 HB 患者仍然面临着巨大的治疗负担、突破性出血和进行性关节疾病,以及高抑制剂发生率的挑战。这些遗留的挑战现在正在通过生物工程的惊人进步得到解决。重组生物工程导致替代疗法具有更简单的给药方式、降低免疫原性、提高疗效和延长半衰期。Emicizumab 是一种双特异性抗体,作为 HA 的替代治疗药物已被批准用于有和无抑制剂的患者。新型化合物正在开发中,通过靶向天然抗凝剂蛋白 C、蛋白 S、组织因子途径抑制剂和抗凝血酶,利用止血的自然平衡。替代和再平衡疗法为稳定的止血控制提供了机会,而不会接触免疫原性凝血因子蛋白。因此,它们可能有更广泛的应用,超出了临床试验项目中正在研究的应用。

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