Literature DB >> 28388522

Hydrogen peroxide activated quinone methide precursors with enhanced DNA cross-linking capability and cytotoxicity towards cancer cells.

Yibin Wang1, Heli Fan1, Kumudha Balakrishnan2, Zechao Lin1, Sheng Cao1, Wenbing Chen1, Yukai Fan1, Quibria A Guthrie1, Huabing Sun1, Kelly A Teske1, Varsha Gandhi2, Leggy A Arnold1, Xiaohua Peng3.   

Abstract

Quinone methide (QM) formation induced by endogenously generated H2O2 is attractive for biological and biomedical applications. To overcome current limitations due to low biological activity of H2O2-activated QM precursors, we are introducing herein several new arylboronates with electron donating substituents at different positions of benzene ring and/or different neutral leaving groups. The reaction rate of the arylboronate esters with H2O2 and subsequent bisquinone methides formation and DNA cross-linking was accelerated with the application of Br as a leaving group instead of acetoxy groups. Additionally, a donating group placed meta to the nascent exo-methylene group of the quinone methide greatly improves H2O2-induced DNA interstrand cross-link formation as well as enhances the cellular activity. Multiple donating groups decrease the stability and DNA cross-linking capability, which lead to low cellular activity. A cell-based screen demonstrated that compounds 2a and 5a with a OMe or OH group dramatically inhibited the growth of various tissue-derived cancer cells while normal cells were less affected. Induction of H2AX phosphorylation by these compounds in CLL lymphocytes provide evidence for a correlation between cell death and DNA damage. The compounds presented herein showed potent anticancer activities and selectivity, which represent a novel scaffold for anticancer drug development.
Copyright © 2017 Elsevier Masson SAS. All rights reserved.

Entities:  

Keywords:  Anticancer activity; Arylboronates; DNA interstrand cross-linking agents; Hydrogen peroxide activation; Quinone methide

Mesh:

Substances:

Year:  2017        PMID: 28388522      PMCID: PMC5652303          DOI: 10.1016/j.ejmech.2017.03.041

Source DB:  PubMed          Journal:  Eur J Med Chem        ISSN: 0223-5234            Impact factor:   6.514


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