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Managing myelofibrosis (MF) that “blasts” through: advancements in the treatment of relapsed/refractory and blast-phase MF

机译:通过以下方式管理“爆炸”的骨髓纤维化(MF):复发/难治性和原始阶段MF的治疗进展

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Myelofibrosis (MF) is the most aggressive form of Philadelphia chromosome–negative myeloproliferative neoplasm, and it is complicated by severe symptom burden, thrombotic events, infections, cytopenias, and transformation to acute myeloid leukemia (AML). Ruxolitinib, the first-line therapy for symptomatic or intermediate- and high–prognostic risk MF, has improved overall survival for this population. However, approximately one-half of MF patients will discontinue ruxolitinib by the first few years of therapy due to a spectrum of resistance, intolerance, relapse, or progression to blast phase disease. Danazol, erythropoietin-stimulating agents, and spleen-directed therapies can be useful in the ruxolitinib-resistant setting. In the ruxolitinib-refractory or -intolerant setting, commercial and novel therapies, either alone or in combination with ruxolitinib, haveshownclinicalutility.Forblast-phaseMF,therecentadvancementsinavailableAMLtherapieshaveincreasedtheoptions with targeted and more tolerable therapies. In this article, we will discuss our paradigm for the management of relapsed/ refractory and blast-phase MF in the context of therapeutic advancements in both AML and MF.
机译:骨髓纤维化(MF)是费城染色体阴性的骨髓增生性肿瘤中最具有侵略性的形式,并伴有严重的症状负担,血栓形成事件,感染,血细胞减少和转化为急性髓细胞性白血病(AML)。 Ruxolitinib是有症状或中,高预后风险MF的一线治疗药物,改善了该人群的总体生存率。然而,由于耐药性,不耐受性,复发或发展为胚泡期疾病,大约一半的MF患者将在治疗的最初几年中停用ruxolitinib。达那唑,促红细胞生成素刺激剂和脾脏定向疗法可在鲁索替尼耐药的环境中使用。在鲁索替尼难治或难治性环境中,单独或与鲁索替尼联合使用的商业和新型疗法具有临床实用性。对于成骨期MF,可利用的AMLtherapiesh的近期进展增加了针对性和更可耐受的疗法的选择。在本文中,我们将讨论在AML和MF的治疗进展情况下管理复发/难治性和初生期MF的范例。

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