化学
体内
生物利用度
最大值
铅化合物
药代动力学
药理学
EC50型
离体
效力
广告
体外
生物化学
医学
生物
生物技术
作者
Jun Liang,Birong Zhang,Sharada S. Labadie,Daniel F. Ortwine,Maia Vinogradova,James R. Kiefer,Victor Gehling,Jean-Christophe Harmange,Richard Cummings,Tommy Lai,Jiangpeng Liao,Xiaoping Zheng,Yichin Liu,Amy Gustafson,Erica Van der Porten,Weifeng Mao,Bianca M. Liederer,Gauri Deshmukh,Marie Classon,Patrick Trojer
标识
DOI:10.1016/j.bmcl.2016.06.078
摘要
Starting with a lead [1,5-a]pyrimidin-7(4H)-one-containing molecule (1), we generated potent, selective and orally bioavailable KDM5 inhibitors. Using structure- and property-based approaches, we designed 48 with improved cell potency (PC9 H3K4Me3 EC50=0.34μM). Furthermore, 48 maintained suitable physiochemical properties and displayed an excellent pharmacokinetic (PK) profile in mice. When dosed orally in mice at 50mg/kg twice a day (BID), 48 showed an unbound maximal plasma concentration (Cmax) >15-fold over its cell EC50, thereby providing a robust chemical probe for studying KDM5 biological functions in vivo.
科研通智能强力驱动
Strongly Powered by AbleSci AI
Grayball
MchemG
迟大猫
开心岩
VDC
归尘
迷人秋烟
iNk
小白
andrele
竹筏过海
笔记本
遇上就这样吧
英勇的鼠标
小杨同学
YSM
zho
Xiaoxiao
从容芮
morena
皖公网安备34019202002308
