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Rethinking Disease Definitions and Therapeutic Strategies in Essential Thrombocythemia and Polycythemia Vera

机译:对原发性血小板增多症和真性红细胞增多症的疾病定义和治疗策略的重新思考

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The seminal discovery of the JAK2V617F mutation, which is highly prevalent in Philadelphia-negative myeloproliferative disorders, now renamed neoplasms, triggered an almost unprecedented explosion of interest and data in the field. Descriptions of additional mutations in exon 12 of JAK2, at position 515 in MPL, and a number of other mutations at low frequency followed these discoveries. These advances in our understanding of molecular pathogenesis of these conditions coincided with the publication of results from two major clinical studies, ECLAP and PT-1, which contributed important clinical insights and facilitated significant correlative data collection. This article, focusing mainly upon essential thrombocythemia and polycythemia vera, reviews four major themes: the impact upon classification of these disorders considering a radical review of current terminology, and then three areas pertinent to clinical management: the indications for cytoreductive therapy in which the key targets are to reduce thrombohemorrhagic complications, relieve disease-related symptoms, and minimize the risk of transformation to secondary myeloid malignancy such as myelodysplasia, leukemia, and secondary myelofibrosis; and second reviewing current and, last, future therapeutic options, in particular interferon and JAK2 inhibitors.
机译:JAK2V617F突变的开创性发现在费城负性骨髓增生性疾病中高度流行,现已更名为肿瘤,引发了该领域几乎前所未有的兴趣和数据爆炸。在这些发现之后,描述了JAK2外显子12中MPL位置515处的其他突变,以及许多其他低频突变。我们对这些疾病的分子发病机理的了解方面的这些进展与ECLAP和PT-1这两项主要临床研究结果的发布相吻合,这两项研究对重要的临床见解做出了贡献,并促进了重要的相关数据收集。本文主要关注原发性血小板增多症和真性红细胞增多症,回顾了四个主要主题:考虑到当前术语的全面回顾对这些疾病分类的影响,然后是与临床管理相关的三个领域:细胞减少疗法的适应症,其中关键目标是减少血栓出血性并发症,减轻疾病相关症状,并最大程度地降低转化为继发性骨髓恶性肿瘤(如骨髓增生异常,白血病和继发性骨髓纤维化)的风险;第二次回顾当前和最后一个未来的治疗选择,特别是干扰素和JAK2抑制剂。

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