| Literature DB >> 24874653 |
Jinlei Bian1, Bang Deng1, Lili Xu1, Xiaoli Xu1, Nan Wang1, Tianhan Hu2, Zeyu Yao2, Jianyao Du2, Li Yang1, Yonghua Lei1, Xiang Li3, Haopeng Sun1, Xiaojin Zhang4, Qidong You5.
Abstract
A series of L-shaped ortho-quinone analogs were designed by analyzing the binding mode with NQO1. Metabolic studies demonstrated that compounds 2m, 2n and 2q exhibited higher metabolic rates than β-lapachone. The docking studies, which supported the rationalization of the metabolic studies, constituted a prospective rational basis for the development of optimized ortho-quinone analogs. Besides, good substrates (2m, 2n and 2r) for NQO1 showed higher selective toxicity than β-lapachone toward A549 (NQO1-rich) cancer cells versus H596 (NQO1-deficient) cells. Determination of superoxide (O2(•-)) production and in vitro cytotoxicity evaluation in the presence of the NQO1 inhibitor dicoumarol confirmed that the ortho-quinones exerted their antitumor activity through NQO1-mediated ROS production by redox cycling. It was suggested that the L-shaped quinone substrates for NQO1 possessed better specificity and safety than β-lapachone.Entities:
Keywords: Antitumor; NQO1 substrates; Ortho-quinones; Tanshione IIA; β-Lapachone
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Year: 2014 PMID: 24874653 DOI: 10.1016/j.ejmech.2014.05.041
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514