Institute of Pharmaceutical Sciences , Albert-Ludwigs-Universität Freiburg , Albertstraße 25 , 79104 Freiburg i.Br. , Germany.
Chemistry Research Laboratory , University of Oxford , 12 Mansfield Road , Oxford OX1 3TA , United Kingdom.
ACS Chem Biol. 2019 Aug 16;14(8):1737-1750. doi: 10.1021/acschembio.9b00289. Epub 2019 Jul 19.
Fe(II)- and 2-oxoglutarate (2OG)-dependent JumonjiC domain-containing histone demethylases (JmjC KDMs) are "epigenetic eraser" enzymes involved in the regulation of gene expression and are emerging drug targets in oncology. We screened a set of clinically used iron chelators and report that they potently inhibit JMJD2A (KDM4A) . Mode of action investigations revealed that one compound, deferasirox, is a active site-binding inhibitor as shown by kinetic and spectroscopic studies. Synthesis of derivatives with improved cell permeability resulted in significant upregulation of histone trimethylation and potent cancer cell growth inhibition. Deferasirox was also found to inhibit human 2OG-dependent hypoxia inducible factor prolyl hydroxylase activity. Therapeutic effects of clinically used deferasirox may thus involve transcriptional regulation through 2OG oxygenase inhibition. Deferasirox might provide a useful starting point for the development of novel anticancer drugs targeting 2OG oxygenases and a valuable tool compound for investigations of KDM function.
依赖于 Fe(II)和 2-氧戊二酸(2OG)的 JumonjiC 结构域含有组蛋白去甲基酶(JmjC KDMs)是参与基因表达调控的“表观遗传擦除”酶,也是肿瘤学中新兴的药物靶点。我们筛选了一组临床使用的铁螯合剂,并报告它们能够强烈抑制 JMJD2A(KDM4A)。作用机制研究表明,一种化合物地拉罗司是一种活性位点结合抑制剂,这一点通过动力学和光谱研究得到了证实。合成具有改善细胞通透性的衍生物导致组蛋白三甲基化的显著上调和有效的癌细胞生长抑制。还发现地拉罗司抑制人 2OG 依赖性缺氧诱导因子脯氨酰羟化酶活性。因此,临床使用的地拉罗司的治疗效果可能涉及通过 2OG 加氧酶抑制的转录调节。地拉罗司可能为开发针对 2OG 加氧酶的新型抗癌药物提供有用的起点,并为 KDM 功能的研究提供有价值的工具化合物。
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