Literature DB >> 17050546

Telomestatin-induced telomere uncapping is modulated by POT1 through G-overhang extension in HT1080 human tumor cells.

Dennis Gomez1, Thomas Wenner, Bertrand Brassart, Céline Douarre, Marie-Françoise O'Donohue, Victoria El Khoury, Kazuo Shin-Ya, Hamid Morjani, Chantal Trentesaux, Jean-François Riou.   

Abstract

Telomestatin is a potent G-quadruplex ligand that interacts with the 3' telomeric overhang, leading to its degradation, and induces a delayed senescence and apoptosis of cancer cells. POT1 and TRF2 were recently identified as specific telomere-binding proteins involved in telomere capping and t-loop maintenance and whose interaction with telomeres is modulated by telomestatin. We show here that the treatment of HT1080 human tumor cells by telomestatin induces a rapid decrease of the telomeric G-overhang and of the double-stranded telomeric repeats. Telomestatin treatment also provokes a strong decrease of POT1 and TRF2 from their telomere sites, suggesting that the ligand triggers the uncapping of the telomere ends. The effect of the ligand is associated with an increase of the gamma-H2AX foci, one part of them colocalizing at telomeres, thus indicating the occurrence of a DNA damage response at the telomere, but also the presence of additional DNA targets for telomestatin. Interestingly, the expression of GFP-POT1 in HT1080 cells increases both telomere and G-overhang length. As compared with HT1080 cells, HT1080GFP-POT1 cells presented a resistance to telomestatin treatment characterized by a protection to the telomestatin-induced growth inhibition and the G-overhang shortening. This protection is related to the initial G-overhang length rather than to its degradation rate and is overcome by increased telomestatin concentration. Altogether these results suggest that telomestatin induced a telomere dysfunction in which G-overhang length and POT1 level are important factors but also suggest the presence of additional DNA sites of action for the ligand.

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Year:  2006        PMID: 17050546     DOI: 10.1074/jbc.M605828200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  60 in total

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Review 3.  In vivo veritas: using yeast to probe the biological functions of G-quadruplexes.

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8.  FANCJ helicase defective in Fanconia anemia and breast cancer unwinds G-quadruplex DNA to defend genomic stability.

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9.  Quantitative visualization of DNA G-quadruplex structures in human cells.

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Journal:  Nat Chem       Date:  2013-01-20       Impact factor: 24.427

10.  G-quadruplex nucleic acids as therapeutic targets.

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Journal:  Curr Opin Chem Biol       Date:  2009-06-08       Impact factor: 8.822

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