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A New Steroid Derivative Stabilizes G-Quadruplexes and Induces Telomere Uncapping in Human Tumor Cells

端粒 端粒酶 DNA 化学 G-四倍体 生物 DNA损伤 分子生物学 生物化学 细胞生物学 基因
作者
Bertrand Brassart,Dennis Gómez,Anne De Cian,Rajaa Boujemaa‐Paterski,Alain Montagnac,KHUONG‐HUU QUI KHUONG‐HUU QUI,Nassima Temime‐Smaali,Chantal Trentesaux,Jean‐Louis Mergny,Françoise Guéritte,Jean‐François Riou
出处
期刊:Molecular Pharmacology [American Society for Pharmacology & Experimental Therapeutics]
卷期号:72 (3): 631-640 被引量:82
标识
DOI:10.1124/mol.107.036574
摘要

Human telomeric DNA consists of tandem repeats of the sequence d(TTAGGG) with a 3′ single-stranded extension (the G-overhang). The stabilization of G-quadruplexes in the human telomeric sequence by small-molecule ligands inhibits the activity of telomerase and results in telomere uncapping, leading to senescence or apoptosis of tumor cells. Therefore, the search for new and selective G-quadruplex ligands is of considerable interest because a selective ligand might provide a telomere-targeted therapeutic approach to treatment of cancer. We have screened a bank of derivatives from natural and synthetic origin using a temperature fluorescence assay and have identified two related compounds that induce G-quadruplex stabilization: malouetine and steroid FG. These steroid derivatives have nonplanar and nonaromatic structures, different from currently known G-quadruplex ligands. Malouetine is a natural product isolated from the leaves of Malouetia bequaaertiana E. Woodson and is known for its curarizing and DNA-binding properties. Steroid FG, a funtumine derivative substituted with a guanylhydrazone moiety, interacted selectively with the telomeric G-quadruplex in vitro. This derivative induced senescence and telomere shortening of HT1080 tumor cells at submicromolar concentrations, corresponding to the phenotypic inactivation of telomerase activity. In addition, steroid FG induced a rapid degradation of the telomeric G-overhang and the formation of anaphase bridges, characteristics of telomere uncapping. Finally, the expression of protection of telomere 1 (POT1) induced resistance to the growth effect of steroid FG. These results indicate that these steroid ligands represent a new class of telomere-targeted agents with potential as antitumor drugs.
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