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Discovery of HPG1860, a Structurally Novel Nonbile Acid FXR Agonist Currently in Clinical Development for the Treatment of Nonalcoholic Steatohepatitis

Cheng Mo, Xiaoqing Xu, Xiaoqing Xu, Pan Zhang, Yihong Peng, Xinpeng Zhao, Shijia Chen, Fang Guo, Yating Xiong, Xin‐Jie Chu, Xiaodong Xu, Xiaodong Xu

2023Journal of Medicinal Chemistry17 citationsDOIOpen Access PDF

Abstract

The farnesoid X receptor (FXR) is a ligand-activated nuclear receptor. Activation of FXR significantly impacts the expressions of the pivotal genes involved in bile acid metabolism, inflammation, fibrosis, and homeostasis of lipid and glucose, leading to considerable interests in developing FXR agonists for the treatment of nonalcoholic steatohepatitis (NASH) or other FXR-relevant diseases. Herein, we describe the design, optimization, and characterization of a series of N -methylene-piperazinyl derivatives as the nonbile acid FXR agonists. Particularly, compound 23 ( HPG1860 ), a potent full FXR agonist, shows high selectivity, favorable ADME and pharmacokinetics profile, along with favorable in vivo activities demonstrated in both rodent PD model and HFD-CCl 4 model and is currently in clinical development in patients with NASH in phase II.

Topics & Concepts

Farnesoid X receptorChemistryNuclear receptorAgonistNonalcoholic steatohepatitisGlucose homeostasisPharmacologyBile acidADMEObeticholic acidInternal medicineReceptorEndocrinologyBiochemistryNonalcoholic fatty liver diseaseIn vitroMedicineTranscription factorDiabetes mellitusGeneFatty liverDiseaseInsulin resistanceDrug Transport and Resistance MechanismsLiver Disease Diagnosis and TreatmentHepatitis B Virus Studies
Discovery of HPG1860, a Structurally Novel Nonbile Acid FXR Agonist Currently in Clinical Development for the Treatment of Nonalcoholic Steatohepatitis | Litcius