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Development and implementation of a cell-based assay to discover agonists of the nuclear receptor REV-ERBα

机译:基于细胞的检测方法的开发和实施以发现核受体REV-ERBα的激动剂

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摘要

The nuclear receptors are transcription factors involved in the regulation of a variety of physiological processes whose activity can be modulated by binding to relevant small molecule ligands. Their dysfunction has been shown to play a role in disease states such as diabetes, cancer, inflammatory diseases, and hormonal resistance ailments, which makes them interesting targets for drug discovery. The nuclear receptor REV-ERBα is involved in regulating the circadian rhythm and metabolism. Its natural ligand is heme and there is significant interest in identifying novel synthetic modulators to serve as tools to characterize its function and to serve as drugs in treating metabolic disorders. To do so, we established a mammalian cell-based two-hybrid assay system capable of measuring the interaction between REV-ERBα and its co-repressor, nuclear co-repressor 1. This assay was validated to industry standard criteria and was used to screen a subset of the LOPAC®1280 library and 29568 compounds from a diverse compound library. Profiling of the primary hits in a panel of counter and selectivity assays confirmed that REV-ERBα activity can be modulated pharmacologically and chemical scaffolds have been identified for optimization.
机译:核受体是参与多种生理过程调节的转录因子,其活性可通过与相关的小分子配体结合而调节。它们的功能障碍已被证明在糖尿病,癌症,炎性疾病和荷尔蒙抵抗疾病等疾病状态中起作用,这使其成为有趣的药物发现靶标。核受体REV-ERBα参与调节昼夜节律和新陈代谢。它的天然配体是血红素,在鉴定新型合成调节剂以表征其功能和治疗代谢性疾病的药物方面引起了极大的兴趣。为此,我们建立了一个基于哺乳动物细胞的双杂交检测系统,该系统能够测量REV-ERBα及其共抑制子,核共抑制子1之间的相互作用。该实验经过行业标准验证,并用于筛选LOPAC ®1280库的子集和来自不同化合物库的29568种化合物。在一系列计数器和选择性分析中对主要命中进行分析,证实REV-ERBα活性可通过药理调节,并且已确定化学支架可进行优化。

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