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A systematic evaluation of the safety and toxicity of fingolimod for its potential use in the treatment of acute myeloid leukaemia

机译:芬戈莫德在急性髓系白血病治疗中的潜在应用的安全性和毒性的系统评价

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Treatment of acute myeloid leukaemia (AML) is challenging and emerging treatment options include protein phosphatase 2A (PP2A) activators. Fingolimod is a known PP2A activator that inhibits multiple signalling pathways and has been used extensively in patients with multiple sclerosis and other indications. The initial positive results of PP2A activators in vitro and mouse models of AML are promising; however, its safety for use in AML has not been assessed. From human studies of fingolimod in other indications, it is possible to evaluate whether the safety and toxicity profile of the PP2A activators will allow their use in treating AML. A literature review was carried out to assess safety before the commencement of Phase I trials of the PP2A activator Fingolimod in AML. From human studies of fingolimod in other indications, it is possible to evaluate whether the safety and toxicity profile of the PP2A activators will allow their use in treating AML. A systematic review of published literature in Medline, EMBASE and the Cochrane Library of critical reviews was carried out. International standards for the design and reporting of search strategies were followed. Search terms and medical subject headings used in trials involving PP2A activators as well as a specific search were performed for 'adverse events','serious adverse events', 'delays in treatment', 'side effects' and 'toxicity' for primary objectives. Database searches were limited to papers published in the last 12 years and available in English. The search yielded 677 articles. A total of 69 journal articles were identified as relevant and included 30 clinical trials, 24 review articles and 15 case reports. The most frequently reported adverse events were nausea, diarrhoea, fatigue, back pain, influenza viral infections, nasopharyngitis and bronchitis. Specific safety concerns include monitoring of the heart rate and conduction at commencement of treatment as cardiotoxicity has been reported. There is little evidence to suggest specific bone marrow toxicity. Lymophopenia is a desired effect in the management of multiple sclerosis, but may have implications in patients with acute leukaemia as it may potentially increase susceptibility to viral infections such as influenza. Fingolimod is a potential treatment option for AML with an acceptable risk to benefit ratio, given its lack of bone marrow toxicity and the relatively low rate of serious side effects. As most patients with AML are elderly, specific monitoring for cardiac toxicity as well as infection would be required. Copyright (C) 2016 Wolters Kluwer Health, Inc. All rights reserved.
机译:急性髓细胞性白血病(AML)的治疗具有挑战性,新兴的治疗选择包括蛋白磷酸酶2A(PP2A)激活剂。芬戈莫德是一种已知的PP2A激活剂,可抑制多种信号传导途径,已广泛用于患有多发性硬化症和其他适应症的患者。 PP2A激活剂在体外和AML小鼠模型中的初步阳性结果令人鼓舞;但是,尚未评估其在AML中使用的安全性。从人类对芬戈莫德的其他适应症研究中,有可能评估PP2A激活剂的安全性和毒性概况是否将其用于治疗AML。在AML中PP2A激活剂芬戈莫德的I期试验开始之前,进行了文献综述以评估安全性。从人类对芬戈莫德的其他适应症研究中,有可能评估PP2A激活剂的安全性和毒性概况是否将其用于治疗AML。对Medline,EMBASE和Cochrane库中的重要评论文献进行了系统的综述。遵循了设计和报告搜索策略的国际标准。在涉及PP2A激活剂的试验中使用的搜索词和医学主题词以及针对主要目标的“不良事件”,“严重不良事件”,“治疗延迟”,“副作用”和“毒性”进行了专门搜索。数据库搜索仅限于最近12年来发表的论文,并且提供英文版本。搜索结果为677条。总共确定了69篇相关的期刊文章,包括30项临床试验,24篇评论文章和15例病例报告。最常见的不良反应是恶心,腹泻,疲劳,背痛,流感病毒感染,鼻咽炎和支气管炎。由于已经报道了心脏毒性,因此特别的安全问题包括在治疗开始时监测心率和传导。没有证据表明特定的骨髓毒性。淋巴细胞减少症是治疗多发性硬化症的理想疗效,但可能对急性白血病患者产生影响,因为它可能会增加对病毒感染(例如流感)的敏感性。由于芬戈莫德缺乏骨髓毒性且严重副作用发生率相对较低,因此芬戈莫德是一种潜在的AML治疗方法,风险获益率可以接受。由于大多数AML患者都是年老的,因此需要对心脏毒性和感染进行专门监测。版权所有(C)2016 Wolters Kluwer Health,Inc.保留所有权利。

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