Optimization of the first small-molecule relaxin/insulin-like family peptide receptor (RXFP1) agonists: Activation results in an antifibrotic gene expression profile

第一个小分子松弛素/胰岛素样家族肽受体(RXFP1)激动剂的优化:激活导致抗纤维化基因表达谱

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作者:Kenneth J Wilson, Jingbo Xiao, Catherine Z Chen, Zaohua Huang, Irina U Agoulnik, Marc Ferrer, Noel Southall, Xin Hu, Wei Zheng, Xin Xu, Amy Wang, Courtney Myhr, Elena Barnaeva, Emmett R George, Alexander I Agoulnik, Juan J Marugan

Abstract

A dose responsive quantitative high throughput screen (qHTS) of >350,000 compounds against a human relaxin/insulin-like family peptide receptor (RXFP1) transfected HEK293 cell line identified 2-acetamido-N-phenylbenzamides 1 and 3 with modest agonist activity. An extensive structure-activity study has been undertaken to optimize the potency, efficacy, and physical properties of the series, resulting in the identification of compound 65 (ML-290), which has excellent in vivo PK properties with high levels of systemic exposure. This series, exemplified by 65, has produced first-in-class small-molecule agonists of RXFP1 and is a potent activator of anti-fibrotic genes.

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