Momparler Richard L, Côté Sylvie, Momparler Louise F, Idaghdour Youssef
Département de Pharmacologie, Université de Montréal, Montreal, QC, Canada; Centre de recherche, Service d'hématologie/oncologie, CHU-Saint-Justine, Montréal, QC, Canada.
Centre de recherche, Service d'hématologie/oncologie, CHU-Saint-Justine , Montréal, QC , Canada.
Front Oncol. 2017 Feb 15;7:19. doi: 10.3389/fonc.2017.00019. eCollection 2017.
Epigenetic alterations play an important role in the development of acute myeloid leukemia (AML) by silencing of genes that suppress leukemogenesis and differentiation. One of the key epigenetic changes in AML is gene silencing by DNA methylation. The importance of this alteration is illustrated by the induction of remissions in AML by 5-aza-2'-deoxycytidine (5-AZA-CdR, decitabine), a potent inhibitor of DNA methylation. However, most patients induced into remission by 5-AZA-CdR will relapse, suggesting that a second agent should be sought to increase the efficacy of this epigenetic therapy. An interesting candidate for this purpose is 3-deazaneplanocin A (DZNep). This analog inhibits EZH2, a histone methyltransferase that trimethylates lysine 27 histone H3 (H3K27me3), a marker for gene silencing. This second epigenetic silencing mechanism also plays an important role in leukemogenesis as shown in preclinical studies where DZNep exhibits potent inhibition of colony formation by AML cells. We reported previously that 5-AZA-CdR in combination with DZNep exhibits a synergistic antineoplastic action against human HL-60 AML cells and the synergistic activation of several tumor suppressor genes. In this report, we showed that this combination also induced a synergistic activation of apoptosis in HL-60 cells. The synergistic antineoplastic action of 5-AZA-CdR plus DZNep was also observed on a second human myeloid leukemia cell line, AML-3. In addition, 5-AZA-CdR in combination with the specific inhibitors of EZH2, GSK-126, or GSK-343, also exhibited a synergistic antineoplastic action on both HL-60 and AML-3. The combined action of 5-AZA-CdR and DZNep on global gene expression in HL-60 cells was investigated in greater depth using RNA sequencing analysis. We observed that this combination of epigenetic agents exhibited a synergistic activation of hundreds of genes. The synergistic activation of so many genes that suppress malignancy by 5-AZA-CdR plus DZNep suggests that epigenetic gene silencing by DNA and histone methylation plays a major role in leukemogenesis. Targeting DNA and histone methylation is a promising approach that merits clinical investigation for the treatment of AML.
表观遗传改变在急性髓系白血病(AML)的发生发展中起着重要作用,它通过使抑制白血病发生和分化的基因沉默来实现。AML中关键的表观遗传变化之一是DNA甲基化导致的基因沉默。5-氮杂-2'-脱氧胞苷(5-AZA-CdR,地西他滨)是一种有效的DNA甲基化抑制剂,它能诱导AML缓解,这说明了这种改变的重要性。然而,大多数通过5-AZA-CdR诱导缓解的患者会复发,这表明应该寻找第二种药物来提高这种表观遗传疗法的疗效。3-去氮杂环丙烷A(DZNep)是一个有趣的候选药物。这种类似物抑制EZH2,EZH2是一种组蛋白甲基转移酶,可使组蛋白H3赖氨酸27位点三甲基化(H3K27me3),这是基因沉默的一个标志。如临床前研究所示,这种第二种表观遗传沉默机制在白血病发生中也起着重要作用,在这些研究中DZNep对AML细胞的集落形成表现出强大的抑制作用。我们之前报道过,5-AZA-CdR与DZNep联合对人HL-60 AML细胞具有协同抗肿瘤作用,并能协同激活多个肿瘤抑制基因。在本报告中,我们表明这种联合还能诱导HL-60细胞凋亡的协同激活。在第二种人髓系白血病细胞系AML-3上也观察到了5-AZA-CdR加DZNep的协同抗肿瘤作用。此外,5-AZA-CdR与EZH2的特异性抑制剂GSK-126或GSK-343联合,对HL-60和AML-3也表现出协同抗肿瘤作用。使用RNA测序分析更深入地研究了5-AZA-CdR和DZNep对HL-60细胞全局基因表达的联合作用。我们观察到这种表观遗传药物组合能协同激活数百个基因。5-AZA-CdR加DZNep对如此多抑制恶性肿瘤的基因的协同激活表明,DNA和组蛋白甲基化导致的表观遗传基因沉默在白血病发生中起主要作用。针对DNA和组蛋白甲基化是一种有前景的方法,值得进行治疗AML的临床研究。
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