Expression profiling identifies epoxy anthraquinone derivative as a DNA topoisomerase inhibitor

拓扑异构酶 DNA 神经母细胞瘤 化学 蒽醌 DNA复制 DNA微阵列 分子生物学 生物 生物化学 基因 基因表达 细胞培养 遗传学 有机化学
作者
Jinesh S. Gheeya,Peter Johansson,Qingrong Chen,Thomas S. Dexheimer,Belhu Metaferia,Young Song,Jun S. Wei,Jianbin He,Yves Pommier,Javed Khan
出处
期刊:Cancer Letters [Elsevier]
卷期号:293 (1): 124-131 被引量:29
标识
DOI:10.1016/j.canlet.2010.01.004
摘要

To discover novel drugs for neuroblastoma treatment, we have previously screened a panel of drugs and identified 30 active agents against neuroblastoma cells. Here we performed microarray gene expression analysis to monitor the impact of these agents on a neuroblastoma cell line and used the connectivity map (cMAP) to explore putative mechanism of action of unknown drugs. We first compared the expression profiles of 10 compounds shared in both our dataset and cMAP database and observed the high connectivity scores for 7 of 10 matched drugs regardless of the differences of cell lines utilized. The screen of cMAP for uncharacterized drugs indicated the signature of Epoxy anthraquinone derivative (EAD) matched the profiles of multiple known DNA targeted agents (topoisomerase I/II inhibitors, DNA intercalators, and DNA alkylation agents) as predicted by its structure. Similar result was obtained by querying against our internal NB-cMAP (http://pob.abcc.ncifcrf.gov/cgi-bin/cMAP), a database containing the profiles of 30 active drugs. These results suggest that Epoxy anthraquinone derivative may inhibit neuroblastoma cells by targeting DNA replication inhibition. Experimental data also demonstrate that Epoxy anthraquinone derivative indeed induces DNA double-strand breaks through DNA alkylation and inhibition of topoisomerase activity. Our study indicates that Epoxy anthraquinone derivative may be a novel DNA topoisomerase inhibitor that can be potentially used for treatment of neuroblastoma or other cancer patients.
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