兴奋剂
痛苦
药理学
化学
脂肪变性
非酒精性脂肪性肝炎
受体
生物信息学
医学
药物发现
脂肪性肝炎
激素
肥胖
功能选择性
非酒精性脂肪肝
治疗方法
内分泌学
减肥
内科学
体内
药品
核受体
功能(生物学)
作者
Nan Zheng,Ly Tu,Pu Xu,Rongfang Chen,Jiang Lu,Wan Dai,Yanxia Lin,Jianmei Ouyang,Jinying Qiu,You Wang,Leiming Wang,Weijun Shen
标识
DOI:10.1021/acs.jmedchem.5c03845
摘要
Harnessing the simultaneous activation of GLP-1R, GIPR, and GCGR has emerged as a highly promising therapeutic paradigm for obesity and related metabolic diseases, including nonalcoholic steatohepatitis (NASH). Here, we report the discovery of TPM003, a novel unimolecular GLP-1R/GIPR/GCGR triple agonist engineered by using a long-acting PEG-fatty acid (PEG-FA) stapling technology. TPM003 exhibits balanced triple receptor agonism and demonstrates an extended systemic half-life across multiple species. In obese mice, TPM003 induced robust and durable weight loss, accompanied by broad improvements in metabolic parameters, outperforming current GLP-1RA standards. Importantly, TPM003 also effectively reversed hepatic steatosis and improved markers of liver function in multiple NASH models. Furthermore, TPM003 is compatible with SNAC-based absorption enhancement, enabling oral delivery in a tablet formulation. Collectively, these findings highlight the therapeutic advantages of balanced GLP-1R/GIPR/GCGR agonism for obesity and NASH and support TPM003 as a promising preclinical candidate with translational potential.
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