| Literature DB >> 24900594 |
Jianwei Wu1, Wenteng Chen1, Guangxin Xia2, Jing Zhang2, Jiaan Shao1, Biqin Tan3, Chunchun Zhang2, Wanwan Yu1, Qinjie Weng3, Haiyan Liu2, Miao Hu1, Hailin Deng2, Yu Hao2, Jingkang Shen4, Yongping Yu1.
Abstract
This letter describes the construction of conformationally constrained quinazoline analogues. Structure-activity relationship studies led to the identification of the lead compound 9n . Compound 9n exhibits effective in vitro activity against A431(WT,overexpression) and H1975([L858R/T790M]) cancer cell lines but is significantly less effective against EGFR negative cancer cell lines (SW620, A549, and K562). Compound 9n was also assessed for potency in enzymatic assays and in vivo antitumor studies. The results indicated that 9n is a potent kinase inhibitor against both wild-type and T790M mutant EGFR kinase. Meanwhile, an oral administration of 9n at a dose of 200 mg/kg produced a considerable antitumor effect in a A431 xenograft model, as compared to gefitinib. A preliminary pharmacokinetic study of 9n also indicates it has good pharmacokinetic properties, and therefore, it is a good starting point for further development.Entities:
Keywords: Anticancer; EGFR; conformationally constrained; kinase inhibitor
Year: 2013 PMID: 24900594 PMCID: PMC4027470 DOI: 10.1021/ml4002437
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.345