| Literature DB >> 25677663 |
Jinlei Bian1, Lili Xu1, Bang Deng1, Xue Qian1, Jun Fan2, Xiuwen Yang2, Fang Liu1, Xiaoli Xu1, Xiaoke Guo1, Xiang Li1, Haopeng Sun1, Qidong You3, Xiaojin Zhang4.
Abstract
Natural product (±)-dunnione (2) and its ortho-quinone analogues (3-8) were synthesized and found to be substrates for NQO1. The structure-activity relationship study revealed that the biological activity was favored by the presence of methyl group at the C ring and methoxy group at the A ring. The docking studies supported the rationalization of the metabolic studies. Deeper location in the active site of NQO1, interactions with hydrophobic pocket and C-H…π interactions with the adjacent Phe178 residue contributed to the better catalytic efficiency and specificity to NQO1. Cytotoxicity studies and determination of superoxide (O2(-)) production in the presence and absence of the NOQ1 inhibitor dicoumarol confirmed that the ortho-quinones exerted their antitumor activity through NQO1-mediated ROS production by redox cycling.Entities:
Keywords: Antitumor; Dunnione; NQO1; Natural product; Reactive oxygen species (ROS)
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Year: 2015 PMID: 25677663 DOI: 10.1016/j.bmcl.2015.01.057
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823