化学
脂锚定蛋白
体内
药理学
血糖性
药品
赛马鲁肽
糖尿病
代谢稳定性
药物发现
体外
2型糖尿病
生物化学
医学
内分泌学
细胞凋亡
利拉鲁肽
生物技术
自噬
生物
作者
Chuanliang Zhang,Yang Xianmin,Xinjia Meng,Lijuan Wu,Xiaochun Liu,Jiangming Gao,Shan Liu,Juan Wu,Dingmin Huang,Zhenwei Wang,Xianbin Su
标识
DOI:10.1021/acs.jmedchem.2c02003
摘要
Poor medication adherence in patients with type 2 diabetes mellitus has become one of the main causes of suboptimal glycemic control. Once-weekly drugs can markedly improve the convenience, adherence, and quality of life of T2DM patients; thus, they are clinically needed and preferred. PTP1B plays a negative role in both insulin and leptin signaling pathways, which makes it an important target for diabetes. Herein, we design and synthesize 35 analogues of core BimBH3 peptide via lipidation/acylation strategy based on our previous work and evaluate their PTP1B inhibitory activity, obtaining the primary structure–activity relationship. Five compounds with good PPT1B inhibitory activity, target selectivity, and significantly improved stability were selected for molecular docking study and searching candidate molecules with long-acting antidiabetic potential. The in vivo anti-T2DM evaluation validated the once-weekly therapeutic potential of analogues 19, 26, 27, 31, and 33, which were comparable with semaglutide and therefore presented as promising drug candidates.
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