DNA甲基转移酶抑制剂联合治疗血液恶性肿瘤。

Steven D Gore
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引用次数: 86

摘要

多种表观遗传变化导致骨髓增生异常综合征(mds)和急性髓性白血病(AML)的转录失调。DNA甲基转移酶(DNMT)抑制剂——阿扎胞苷和地西他滨——在治疗MDS中具有显著的活性。尽管在髓系恶性肿瘤中有明显的活性,但DNMT抑制剂的单药治疗受到低完全和部分缓解率(7-20%)和中位缓解持续时间15个月的限制。与经典的细胞毒治疗一样,靶向生物途径和机制可能最好是通过提供互补机制和协同药效学相互作用的药物组合来实现。这种方法的目标是提高反应率、质量和持续时间,并尽量减少不良事件。目前正在开发许多治疗MDS和AML的新疗法。这篇综述文章触及了在不同研究阶段的一些更有前途的联合方案。MDS和AML的治疗正在经历快速发展。细胞遗传学完全缓解和延长生存期是重要的目标。疾病状态和生活质量问题的逐步改善对患者也很重要。鉴于细胞毒性化疗在治愈MDS和MDS相关AML方面的总体失败,应用毒性较小的生物定向药物可能是一种更有希望的治疗方法。DNMT抑制剂联合治疗采用最佳剂量方案,专注于较长时间内较低剂量的甲基化逆转,而不是直接的细胞毒性作用,在MDS和AML中开始显示出有希望的结果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Combination therapy with DNA methyltransferase inhibitors in hematologic malignancies.

A variety of epigenetic changes contribute to transcriptional dysregulation in myelodysplastic syndromes (MDSs) and acute myeloid leukemia (AML). DNA methyltransferase (DNMT) inhibitors--azacitidine and decitabine--have significant activity in the treatment of MDS. Despite marked activity in myeloid malignancy, monotherapy with DNMT inhibitors is limited by low complete and partial response rates (7-20%) and median response durations of 15 months. As with classical cytotoxic therapy, the targeting of biologic pathways and mechanisms may best be accomplished using a combination of agents offering complementary mechanisms and synergistic pharmacodynamic interactions. The goal of this approach is to improve response rates, quality, and duration, and to minimize adverse events. There are a number of new therapies under development for the management of MDS and AML. This review article touches on some of the more promising combination regimens in various phases of investigation. The treatment of MDS and AML is undergoing rapid evolution. Cytogenetic complete remission and prolonged survival represent important goals. Incremental improvements in disease state and quality-of-life issues are also important for patients. Given the overall failure of cytotoxic chemotherapy in the achievement of cures in MDS and MDS-related AML, the application of less toxic, biologically directed agents may represent a more promising approach to treatment. Combination therapies with DNMT inhibitors using optimal dosing regimens to focus on methylation reversal with lower doses over longer periods of time, rather than direct cytotoxic effects, are beginning to suggest promising results in MDS and AML.

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