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首页> 外文期刊>Journal of Medicinal Chemistry >Discovery and Optimization of Novel, Selective Histone Methyltransferase SET7 Inhibitors by Pharmacophore- and Docking-Based Virtual Screening
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Discovery and Optimization of Novel, Selective Histone Methyltransferase SET7 Inhibitors by Pharmacophore- and Docking-Based Virtual Screening

机译:通过药理学和对接的虚拟筛选发现和优化新型,选择性组蛋白甲基转移酶SET7抑制剂。

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Histone methyltransferases are involved in various biological functions, and these methylation regulating enzymes' abnormal expression or activity has been noted in several human cancers. Within this context, SET domain-containing (lysine methyltransferase) 7 (SET7, also called KMT7, SETD7, SET9) is of increasing significance due to its diverse roles in biological functions and diseases, such as diabetes, cancers, alopecia areata, atherosclerotic vascular disease, HIV, and HCV. In this study, DC-S100, which was discovered by pharmacophore- and docking-based virtual screening, was identified as the hit compound of SET7 inhibitor. Structure-activity relationship (SAR) analysis was performed on analogs of DC-S100 and according to the putative binding mode of DC-S100, structure modifications were made to improve its activity. Of note, compounds DC-S238 and DC-S239, with IC50 values of 4.88 and 4.59 mu M, respectively, displayed selectivity for DNMT1, DOT1L, EZH2, NSD1, SETD8, and G9a. Taken together, DC-S238 and DC-S239 can serve as leads for further investigation as SET7 inhibitors and the chemical toolkits for functional biology studies of SET7.
机译:组蛋白甲基转移酶涉及多种生物学功能,并且在几种人类癌症中已注意到这些甲基化调节酶的异常表达或活性。在此背景下,含SET结构域的(赖氨酸甲基转移酶)7(SET7,也称为KMT7,SETD7,SET9)由于其在生物学功能和疾病(例如糖尿病,癌症,斑秃,动脉粥样硬化血管)中的多种作用而具有越来越重要的意义。疾病,HIV和HCV。在这项研究中,通过基于药效团和对接的虚拟筛选发现的DC-S100被确定为SET7抑制剂的命中化合物。对DC-S100的类似物进行了结构-活性关系(SAR)分析,并根据DC-S100的假定结合方式进行了结构修饰以提高其活性。值得注意的是,化合物DC-S238和DC-S239的IC50值分别为4.88和4.59μM,显示出对DNMT1,DOT1L,EZH2,NSD1,SETD8和G9a的选择性。两者合计,DC-S238和DC-S239可以作为SET7抑制剂和SET7功能生物学研究的化学工具包的进一步研究线索。

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