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A Cell-Permeable Ester Derivative of the JmjC Histone Demethylase Inhibitor IOX1

机译:JmjC组蛋白去甲基化酶抑制剂IOX1的细胞渗透性酯衍生物。

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摘要

The 2-oxoglutarate (2OG)-dependent Jumonji C domain (JmjC) family is the largest family of histone lysine demethylases. There is interest in developing small-molecule probes that modulate JmjC activity to investigate their biological roles. 5-Carboxy-8-hydroxyquinoline (IOX1) is the most potent broad-spectrum inhibitor of 2OG oxygenases, including the JmjC demethylases, reported to date; however, it suffers from low cell permeability. Here, we describe structure–activity relationship studies leading to the discovery of an n-octyl ester form of IOX1 with improved cellular potency (EC50 value of 100 to 4 μm). These findings are supported by in vitro inhibition and selectivity studies, docking studies, activity versus toxicity analysis in cell cultures, and intracellular uptake measurements. The n-octyl ester was found to have improved cell permeability; it was found to inhibit some JmjC demethylases in its intact ester form and to be more selective than IOX1. The n-octyl ester of IOX1 should find utility as a starting point for the development of JmjC inhibitors and as a use as a cell-permeable tool compound for studies investigating the roles of 2OG oxygenases in epigenetic regulation.
机译:2-氧戊二酸(2OG)依赖性Jumonji C域(JmjC)家族是组蛋白赖氨酸脱甲基酶的最大家族。有兴趣开发可调节JmjC活性以研究其生物学作用的小分子探针。 5-Carboxy-8-hydroxyquinoline(IOX1)是迄今为止报道的2OG加氧酶(包括JmjC脱甲基酶)最有效的广谱抑制剂;但是,其细胞渗透性低。在这里,我们描述了结构-活性关系研究,从而发现了具有增强的细胞效力(EC50值为100至4μm)的IOX1的正辛酯形式。这些发现得到了体外抑制和选择性研究,对接研究,细胞培养物中的活性与毒性分析以及细胞内摄取测量的支持。发现正辛基酯具有改善的细胞渗透性。它被发现以其完整的酯形式抑制某些JmjC脱甲基酶,并且比IOX1更具选择性。 IOX1的正辛酯应作为开发JmjC抑制剂的起点,并用作研究2OG加氧酶在表观遗传调控中的作用的细胞可渗透性工具化合物。

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