| Literature DB >> 26789553 |
Xiaofei Liang1,2, Xiaochuan Liu1,3, Beilei Wang1,2, Fengming Zou1,2, Aoli Wang1,4, Shuang Qi1,2, Cheng Chen1,2, Zheng Zhao1,2, Wenchao Wang1,2, Ziping Qi1,2, Fengchao Lv1,4, Zhenquan Hu1,2, Li Wang1,2, Shanchun Zhang2,5, Qingsong Liu1,2,4,6, Jing Liu1,2.
Abstract
Starting from a dihydropyrimidopyrimidine core scaffold based compound 27 (GNF-7), we discovered a highly potent (ABL1: IC50 of 70 nM) and selective (S score (1) = 0.02) BCR-ABL inhibitor 18a (CHMFL-ABL-053). Compound 18a did not exhibit apparent inhibitory activity against c-KIT kinase, which is the common target of currently clinically used BCR-ABL inhibitors. Through significant suppression of the BCR-ABL autophosphorylation (EC50 about 100 nM) and downstream mediators such as STAT5, Crkl, and ERK's phosphorylation, 18a inhibited the proliferation of CML cell lines K562 (GI50 = 14 nM), KU812 (GI50 = 25 nM), and MEG-01 (GI50 = 16 nM). A pharmacokinetic study revealed that 18a had over 4 h of half-life and 24% bioavailability in rats. A 50 mg/kg/day dosage treatment could almost completely suppress tumor progression in the K562 cells inoculated xenograft mouse model. As a potential useful drug candidate for CML, 18a is under extensive preclinical safety evaluation now.Entities:
Mesh:
Substances:
Year: 2016 PMID: 26789553 DOI: 10.1021/acs.jmedchem.5b01618
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446