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一种用于人类NR5A核受体的通用且灵敏的直接配体结合分析方法的开发。

Development of a Versatile and Sensitive Direct Ligand Binding Assay for Human NR5A Nuclear Receptors.

作者信息

D'Agostino Emma H, Flynn Autumn R, Cornelison Jeffery L, Mays Suzanne G, Patel Anamika, Jui Nathan T, Ortlund Eric A

机构信息

Department of Biochemistry and Department of Chemistry, Emory University, Atlanta, Georgia 30322, United States.

出版信息

ACS Med Chem Lett. 2019 Nov 21;11(3):365-370. doi: 10.1021/acsmedchemlett.9b00442. eCollection 2020 Mar 12.

Abstract

As regulators of steroidogenesis, development, and metabolism, the nuclear receptor 5A (NR5A) subfamily members steroidogenic factor 1 (SF-1) and liver receptor homologue 1 (LRH-1) are important pharmacological targets for cancers and metabolic diseases. Evaluation of small molecule modulators and candidate endogenous ligands for these orphan receptors has been hindered by the lack of accessible, robust direct-binding assays. Here, we leverage the potency of our new NR5A agonist (6N) to create a high-affinity probe for fluorescence polarization competition assays by conjugating 6N to fluorescein (FAM). The 6N-FAM probe tightly binds the NR5A receptors and detects direct binding of synthetic and phospholipid ligands. For 25 LRH-1 agonists, affinity predicts potency in cellular activation assays, demonstrating the potential for this assay in drug discovery. Moreover, phospholipids dilauroylphosphatidylcholine and phosphatidylinositol(4,5)phosphate bind with high affinity, demonstrating this assay is robust for evaluation of candidate endogenous ligands for human NR5A receptors.

摘要

作为类固醇生成、发育和代谢的调节因子,核受体5A(NR5A)亚家族成员类固醇生成因子1(SF-1)和肝脏受体同源物1(LRH-1)是癌症和代谢疾病的重要药理学靶点。由于缺乏可及的、可靠的直接结合测定方法,对这些孤儿受体的小分子调节剂和候选内源性配体的评估受到了阻碍。在此,我们利用新型NR5A激动剂(6N)的效力,通过将6N与荧光素(FAM)偶联,创建了一种用于荧光偏振竞争测定的高亲和力探针。6N-FAM探针紧密结合NR5A受体,并检测合成配体和磷脂配体的直接结合。对于25种LRH-1激动剂,亲和力可预测细胞激活测定中的效力,证明了该测定在药物发现中的潜力。此外,磷脂二月桂酰磷脂酰胆碱和磷脂酰肌醇(4,5)二磷酸以高亲和力结合,表明该测定对于评估人NR5A受体的候选内源性配体是可靠的。

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