特雷姆2
吞噬作用
虚拟筛选
药效团
变构调节
小分子
化学
神经保护
兴奋剂
细胞生物学
受体
小胶质细胞
变构调节剂
计算生物学
合理设计
神经科学
受体蛋白酪氨酸激酶
髓系细胞
生物化学
生物
血浆蛋白结合
癌症研究
细胞毒性
特瑞氟米特
信号转导
生物信息学
HEK 293细胞
结合位点
部分激动剂
作者
Sungwoo Cho,Baljit Kaur,Kevin Lam,Farida El Gaamouch,Katarzyna Kuncewicz,Niklas Piet Doering,Gerhard Wolber,Moustafa T. Gabr
出处
期刊:ChemMedChem
[Wiley]
日期:2026-01-01
卷期号:21 (2): e202500718-e202500718
被引量:2
标识
DOI:10.1002/cmdc.202500718
摘要
Triggering receptor expressed on myeloid cells 2 (TREM2) is a microglia‐specific receptor whose activation promotes phagocytosis and neuroprotection in Alzheimer's disease (AD) and related neurodegenerative disorders. While therapeutic efforts have largely focused on antibodies, small‐molecule TREM2 modulators remain limited. Here, we applied a structure‐based virtual screening workflow targeting a putative allosteric site on TREM2, guided by PyRod‐derived pharmacophores from molecular dynamics simulations. Screening of the Enamine Collection (ESC) yielded 20 candidate compounds, three of which demonstrated binding in TRIC assays. The top hit, EN020 , exhibited a K D of 14.2 µM (MST) and 35.9 µM (SPR), and significantly enhanced microglial phagocytosis in BV2 cells, outperforming the known TREM2 agonist VG‐3927 . A preliminary structure–activity relationship (SAR) study, including synthetic and catalog‐derived analogs, highlighted a narrow tolerance for scaffold modifications, with only T2V002 retaining partial TREM2 binding affinity. This work identifies EN020 as a novel small‐molecule TREM2 modulator with functional activity, providing a framework for rational optimization toward potential AD therapeutics.
科研通智能强力驱动
Strongly Powered by AbleSci AI