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Innovative Approaches for Immune Tolerance to Factor VIII in the Treatment of Hemophilia A

机译:对A型血友病的免疫耐受性-VIII因子的创新方法

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摘要

Hemophilia A (coagulation factor VIII deficiency) is a debilitating genetic disorder that is primarily treated with intravenous replacement therapy. Despite a variety of factor VIII protein formulations available, the risk of developing anti-dug antibodies (“inhibitors”) remains. Overall, 20–30% of patients with severe disease develop inhibitors. Current clinical immune tolerance induction protocols to eliminate inhibitors are not effective in all patients, and there are no prophylactic protocols to prevent the immune response. New experimental therapies, such as gene and cell therapies, show promising results in pre-clinical studies in animal models of hemophilia. Examples include hepatic gene transfer with viral vectors, genetically engineered regulatory T cells (Treg), in vivo Treg induction using immune modulatory drugs, and maternal antigen transfer. Furthermore, an oral tolerance protocol is being developed based on transgenic lettuce plants, which suppressed inhibitor formation in hemophilic mice and dogs. Hopefully, some of these innovative approaches will reduce the risk of and/or more effectively eliminate inhibitor formation in future treatment of hemophilia A.
机译:A型血友病(凝血因子VIII缺乏症)是一种使人衰弱的遗传疾病,主要通过静脉内替代疗法治疗。尽管有多种可用的VIII因子蛋白质制剂,但仍存在开发抗Dug抗体(“抑制剂”)的风险。总体而言,重症患者中有20–30%会产生抑制剂。当前消除抑制剂的临床免疫耐受诱导方案并非对所有患者都有效,并且没有预防方案来预防免疫反应。基因和细胞疗法等新的实验疗法在血友病动物模型的临床前研究中显示出令人鼓舞的结果。实例包括通过病毒载体进行肝基因转移,基因工程调节性T细胞(Treg),使用免疫调节药物进行体内Treg诱导以及母体抗原转移。此外,正在基于转基因生菜植物开发口服耐受方案,其抑制了血友病小鼠和狗中抑制剂的形成。希望这些创新方法中的一些能够在将来治疗血友病A时降低和/或更有效地消除抑制剂形成的风险。

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