Dipartimento di Patologia Generale, Seconda Università degli Studi di Napoli, Vico L. De Crecchio 7, 80138 Napoli, Italy.
Mol Cancer Ther. 2011 Dec;10(12):2394-404. doi: 10.1158/1535-7163.MCT-11-0525. Epub 2011 Oct 6.
Deregulation of the epigenome is recognized as cause of cancer and epigenetic factors are receiving major attention as therapeutic targets; yet, the molecular mode of action of existing epi-drugs is largely elusive. Here, we report on the decryption of the mechanism of action of UVI5008, a novel epigenetic modifier, that inhibits histone deacetylases, sirtuins, and DNA methyltransferases. UVI5008 highly efficiently induces cancer cell-selective death in a variety of models and exerts its activities in several human tumor xenografts and genetic mouse models of human breast cancer in vivo. Its anticancer activity involves independent activation of death receptors and reactive oxygen species production. Importantly, UVI5008 action is not critically dependent on p53, Bcl-2 modifying factor, and/or TNF-related apoptosis-inducing ligand as cell death is efficiently induced in cells mutated or deficient for these factors limiting the risk of drug resistance development and maximizing its application spectrum. The simultaneous modulation of multiple (epigenetic) targets promises to open new avenues with unanticipated potential against cancer.
表观基因组的失调被认为是癌症的原因,表观遗传因素作为治疗靶点受到了极大的关注;然而,现有表观遗传药物的分子作用模式在很大程度上仍难以捉摸。在这里,我们报告了一种新型表观遗传修饰剂 UVI5008 的作用机制的破译,它可以抑制组蛋白去乙酰化酶、沉默调节蛋白和 DNA 甲基转移酶。UVI5008 在多种模型中高效诱导癌细胞选择性死亡,并在几种人类肿瘤异种移植和体内遗传的人类乳腺癌小鼠模型中发挥其活性。其抗癌活性涉及死亡受体的独立激活和活性氧物质的产生。重要的是,UVI5008 的作用并不严重依赖于 p53、Bcl-2 修饰因子和/或 TNF 相关凋亡诱导配体,因为在这些因子发生突变或缺失的细胞中,细胞死亡被有效地诱导,从而限制了耐药性发展的风险,并最大限度地扩大了其应用范围。对多种(表观遗传)靶点的同时调节有望开辟新的途径,为癌症治疗带来意想不到的潜力。
