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Incorporating novel approaches in the management of MDS beyond conventional hypomethylating agents

机译:在常规的低甲基化试剂的MDS管理中纳入新的方法

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In the last decade, the treatment of higher-risk myelodysplastic syndromes (MDS) has revolved around the azanucleosides, azacitidine and decitabine, which at lower doses are postulated to work predominantly via their effects on inhibition of DNA methyltransferases and consequent DNA hypomethylation. For patients who relapse after, or do not respond to, hypomethylating agent therapy, the outcome is dismal, and new agents and approaches that have the potential to alter the natural history of these diseases are desperately needed. Allogeneic stem cell transplant is the only known potentially curative approach in MDS, but its applicability has been limited by the advanced age of patients and attendant comorbidities. There is now an increasing array of new agents under clinical investigation in MDS that aim to exploit our expanding understanding of molecular pathways that are important in the pathogenesis of MDS. This review focuses on a critical appraisal of novel agents being evaluated in higher-risk MDS that go beyond the conventional hypomethylating agent therapies approved by the US Food and Drug Administration.
机译:在过去的十年中,偶核苷,氮杂氨磺酸亚沙氨啶和脱蛋白的含有更高风险的髓细胞增强综合征(MDS)的治疗,其在较低剂量下假设以主要通过它们对DNA甲基转移酶的抑制作用主要工作和随后的DNA低甲基化。对于后复发的患者,或者没有响应甲基化剂治疗,结果是令人沮丧的,并且迫切需要新的药剂和具有改变这些疾病自然历史的潜力。同种异体干细胞移植是唯一已知的MDS潜在的疗效方法,但其适用性受到患者和伴随着者的高龄人的限制。现在在MDS的临床调查下,旨在利用我们对MDS发病机制重要的分子途径的扩大理解,增加了一系列新的新试剂。本综述重点介绍了在高风险的MDS中评估的新型药剂的关键评估,超出了美国食品和药物管理局批准的常规的低甲基化剂疗法。

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    《Hematology》 |2017年第1期|共10页
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