化学
IC50型
伊马替尼
三氟甲基
背景(考古学)
激酶
生长抑制
细胞生长
细胞培养
细胞凋亡
突变体
立体化学
药理学
分子生物学
体外
生物化学
癌症研究
生物
遗传学
基因
有机化学
古生物学
髓系白血病
烷基
作者
Binhua Li,Aoli Wang,Juan Liu,Ziping Qi,Xiaochuan Liu,Kailin Yu,Wu Hong,Chen Cheng,Chen Hu,Wenchao Wang,Jiaxin Wu,Zhenquan Hu,Ling Ye,Fengming Zou,Feiyang Liu,Beilei Wang,Li Wang,Tao Ren,Shaojuan Zhang,Mingfeng Bai
标识
DOI:10.1021/acs.jmedchem.6b00902
摘要
cKIT kinase inhibitors, e.g., imatinib, could induce drug-acquired mutations such as cKIT T670I that rendered drug resistance after chronic treatment. Through a type II kinase inhibitor design approach we discovered a highly potent type II cKIT kinase inhibitor compound 35 (CHMFL-KIT-8140), which potently inhibited both cKIT wt (IC50 = 33 nM) and cKIT gatekeeper T670I mutant (IC50 = 99 nM). Compound 35 displayed strong antiproliferative effect against GISTs cancer cell lines GIST-T1 (cKIT wt, GI50 = 4 nM) and GIST-5R (cKIT T670I, GI50 = 26 nM). In the cellular context it strongly inhibited c-KIT mediated signaling pathways and induced apoptosis. In the BaF3-TEL-cKIT-T670I isogenic cell inoculated xenograft mouse model, 35 exhibited dose dependent tumor growth suppression efficacy and 100 mg/kg dosage provided 47.7% tumor growth inhibition (TGI) without obvious toxicity. We believe compound 35 would be a good pharmacological tool for exploration of the cKIT-T670I mutant mediated pathology in GISTs.
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(2025-6-4)
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