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首页> 外文期刊>Journal of Medicinal Chemistry >KDM4B as a Target for Prostate Cancer:Structural Analysis and Selective Inhibition by a Novel Inhibitor
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KDM4B as a Target for Prostate Cancer:Structural Analysis and Selective Inhibition by a Novel Inhibitor

机译:KDM4B作为前列腺癌的靶点:结构分析和新型抑制剂的选择性抑制。

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摘要

The KDM4/JMJD2 Jumonji C-containing histone lysine demethylases (KDM4A-KDM4D), which selectively remove the methyl group(s) from tri/dimethylated lysine 9/36 of H3, modulate transcriptional activation and genome stability. The overexpression of KDM4A/KDM4B in prostate cancer and their association with androgen receptor suggest that KDM4A/KDM4B are potential progression factors for prostate cancer. Here, we report the crystal structure of the KDM4B?pyridine 2,4-dicarboxylic acid?H3K9me3 ternary complex, revealing the core active-site region and a selective K9/K36 site. A selective KDM4A/KDM4B inhibitor, 4, that occupies three subsites in the binding pocket is identified by virtual screening. Pharmacological and genetic inhibition of KDM4A/KDM4B significantly blocks the viability of cultured prostate cancer cells, which is accompanied by increased H3K9me3 staining and transcriptional silencing of growth-related genes. Significantly, a substantial portion of differentially expressed genes are AR-responsive, consistent with the roles of KDM4s as critical AR activators. Our results point to KDM4 as a useful therapeutic target and identify a new inhibitor scaffold.
机译:含有KDM4 / JMJD2 Jumonji C的组蛋白赖氨酸脱甲基酶(KDM4A-KDM4D),可选择性地从H3的三/二甲基化赖氨酸9/36中除去甲基,从而调节转录激活和基因组稳定性。 KDM4A / KDM4B在前列腺癌中的过表达及其与雄激素受体的关系表明,KDM4A / KDM4B是前列腺癌的潜在进展因素。在这里,我们报告了KDM4B?吡啶2,4-二羧酸?H3K9me3三元配合物的晶体结构,揭示了核心活性位点区域和选择性的K9 / K36位点。通过虚拟筛选鉴定选择性KDM4A / KDM4B抑制剂4,其在结合袋中占据三个亚位点。 KDM4A / KDM4B的药理和遗传抑制作用显着阻断了培养的前列腺癌细胞的生存能力,并伴随着H3K9me3染色增加和生长相关基因的转录沉默。重要的是,差异表达基因的很大一部分是AR反应性的,与KDM4s作为关键AR激活剂的作用一致。我们的结果表明KDM4是有用的治疗靶标,并确定了新的抑制剂支架。

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