化学
吡嗪
ED50公司
敌手
药理学
立体化学
冲程(发动机)
依达拉奉
心肌梗塞
缺血性中风
神经保护
受体拮抗剂
心脏病学
医学
缺血
受体
生物化学
工程类
机械工程
作者
Bing Zhang,Jinxin Li,Ruyu Wang,Qi Li,Qing Mao,Xuefeng Fu,Qingbo Song,Dan Liu,Xiwen Dai,Zhaocheng Du,Chang Liu,Ziyuan Liu,Chen Xing,Chengjun Wu,Yanhua Mou,Shaojie Wang
标识
DOI:10.1021/acs.jmedchem.5c01780
摘要
The P2Y 1 receptor is a promising target for treating an ischemic stroke. Herein, a conformational restriction strategy was applied to improve the brain exposure of our previously reported P2Y 1 antagonist HNW001. Compound 12g, containing an imidazo[1,5- a ]pyrazine scaffold, turned out to be a remarkable P2Y 1 antagonist (IC 50 = 1.95 μM) with improved brain drug exposure (AUC (compound 12g ) = 37.57 μg/g·h vs AUC ( HNW001 ) = 6.65 μg/g · h) and less bleeding risk, and it also displayed great potential for neuroprotection. Subsequently, the anti-ischemic stroke efficacy of compound 12g was validated using a rat MCAO model (ED 50 = 4.49 mg/kg), outperforming HNW001, BPTU, and edaravone. Additionally, compound 12g dose-dependently inhibited infarct sizes in a mouse myocardial infarction model. Collectively, these findings suggested that the imidazo[1,5- a ]pyrazine scaffold has potential for developing effective P2Y 1 antagonists, and compound 12g could be a promising anti-ischemic agent for treating ischemic stroke and myocardial infarction.
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