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首个同类首创的肝细胞核因子4激动剂。

A First-in-Class Hepatocyte Nuclear Factor 4 Agonist.

作者信息

Schallmayer Espen, Morozov Vasily, Duensing-Kropp Silke, Schallmayer Lasse, Schüffner Leann, Schubert-Zsilavecz Manfred, Pabel Jörg, Höfner Georg, Heering Jan, Marschner Julian A, Merk Daniel

机构信息

Goethe University Frankfurt, Institute of Pharmaceutical Chemistry, 60438 Frankfurt, Germany.

Ludwig-Maximilians-Universität (LMU) München, Department of Pharmacy, 81377 Munich, Germany.

出版信息

J Med Chem. 2025 May 22;68(10):10410-10424. doi: 10.1021/acs.jmedchem.5c00595. Epub 2025 May 8.

Abstract

Hepatocyte nuclear factor 4 (HNF4) is an orphan nuclear receptor implicated, for example, in pancreatic islet gene expression and hepatic regulation of glucose and lipid metabolism. Mutations in the HNF4α gene are responsible for the inheritable maturity-onset diabetes of the young 1 (MODY-1), supporting the therapeutic potential of HNF4 activation in metabolic diseases. However, exploration and validation of HNF4 as a therapeutic target is hindered by the lack of suitable ligands. Here, we report the development of the first high-affinity HNF4 agonists by extension of a fragment screening hit and systematic SAR elucidation. Structural modification allowed tuning of the chemotype for both HNF4 agonism and inverse agonism. X-ray structure analysis demonstrated orthosteric site occupation by the new ligand scaffold mimicking the natural fatty acid ligand binding. The most active descendant displayed low nanomolar HNF4 agonist potency and binding affinity and favorable selectivity, enabling unprecedented studies on HNF4 biology as a chemical tool.

摘要

肝细胞核因子4(HNF4)是一种孤儿核受体,例如,它参与胰岛基因表达以及肝脏对葡萄糖和脂质代谢的调节。HNF4α基因的突变是导致青年发病的成年型糖尿病1型(MODY - 1)的原因,这支持了激活HNF4在代谢疾病中的治疗潜力。然而,由于缺乏合适的配体,对HNF4作为治疗靶点的探索和验证受到了阻碍。在此,我们报告了通过扩展片段筛选命中物并进行系统的构效关系阐明,开发出了首个高亲和力的HNF4激动剂。结构修饰使得能够调整化学类型以实现HNF4激动作用和反向激动作用。X射线结构分析表明,新的配体支架占据了正构位点,模拟了天然脂肪酸配体的结合。活性最高的衍生物表现出低纳摩尔级的HNF4激动剂效力和结合亲和力以及良好的选择性,从而能够以前所未有的方式将其作为化学工具对HNF4生物学进行研究。

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