Preferential binding of a G-quadruplex ligand to human chromosome ends

Christine Granotier; Gaëlle Pennarun; Lydia Riou; Françoise Hoffschir; Laurent R. Gauthier; Anne De Cian; Dennis Gomez; Eliane Mandine; Jean François Riou; Jean Louis Mergny; Patrick Mailliet; Bernard Dutrillaux; François D. Boussin

doi:10.1093/nar/gki722

Preferential binding of a G-quadruplex ligand to human chromosome ends

Christine Granotier
, Gaëlle Pennarun
, Lydia Riou
, Françoise Hoffschir
, Laurent R. Gauthier
, Anne De Cian
, Dennis Gomez
, Eliane Mandine
, Jean François Riou
, Jean Louis Mergny
, Patrick Mailliet
, Bernard Dutrillaux
, François D. Boussin

Research output: Contribution to journal › Article › peer-review

Abstract

The G-overhangs of telomeres are thought to adopt particular conformations, such as T-loops or G-quadruplexes. It has been suggested that G-quadruplex structures could be stabilized by specific ligands in a new approach to cancer treatment consisting in inhibition of telomerase, an enzyme involved in telomere maintenance and cell immortality. Although the formation of G-quadruplexes was demonstrated in vitro many years ago, it has not been definitively demonstrated in living human cells. We therefore investigated the chromosomal binding of a tritiated G-quadruplex ligand, ³H-360A (2,6-N, N′-methyl-quinolinio-3-yl)-pyridine dicarboxamide [methyl-³H]. We verified the in vitro selectivity of ³H-360A for G-quadruplex structures by equilibrium dialysis. We then showed by binding experiments with human genomic DNA that ³H-360A has a very potent selectivity toward G-quadruplex structures of the telomeric 3′-overhang. Finally, we performed autoradiography of metaphase spreads from cells cultured with ³H-360A. We found that ³H-360A was preferentially bound to chromosome terminal regions of both human normal (peripheral blood lymphocytes) and tumor cells (T98G and CEM1301). In conclusion, our results provide evidence that a specific G-quadruplex ligand interacts with the terminal ends of human chromosomes. They support the hypothesis that G-quadruplex ligands induce and/or stabilize G-quadruplex structures at telomeres of human cells.

Original language	English
Pages (from-to)	4182-4190
Number of pages	9
Journal	Nucleic Acids Research
Volume	33
Issue number	13
DOIs	https://doi.org/10.1093/nar/gki722
Publication status	Published - 31 Oct 2005
Externally published	Yes

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10.1093/nar/gki722

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@article{4d44a908e3074e37acfa98713805f79a,

title = "Preferential binding of a G-quadruplex ligand to human chromosome ends",

abstract = "The G-overhangs of telomeres are thought to adopt particular conformations, such as T-loops or G-quadruplexes. It has been suggested that G-quadruplex structures could be stabilized by specific ligands in a new approach to cancer treatment consisting in inhibition of telomerase, an enzyme involved in telomere maintenance and cell immortality. Although the formation of G-quadruplexes was demonstrated in vitro many years ago, it has not been definitively demonstrated in living human cells. We therefore investigated the chromosomal binding of a tritiated G-quadruplex ligand, 3H-360A (2,6-N, N′-methyl-quinolinio-3-yl)-pyridine dicarboxamide [methyl-3H]. We verified the in vitro selectivity of 3H-360A for G-quadruplex structures by equilibrium dialysis. We then showed by binding experiments with human genomic DNA that 3H-360A has a very potent selectivity toward G-quadruplex structures of the telomeric 3′-overhang. Finally, we performed autoradiography of metaphase spreads from cells cultured with 3H-360A. We found that 3H-360A was preferentially bound to chromosome terminal regions of both human normal (peripheral blood lymphocytes) and tumor cells (T98G and CEM1301). In conclusion, our results provide evidence that a specific G-quadruplex ligand interacts with the terminal ends of human chromosomes. They support the hypothesis that G-quadruplex ligands induce and/or stabilize G-quadruplex structures at telomeres of human cells.",

author = "Christine Granotier and Ga{\"e}lle Pennarun and Lydia Riou and Fran{\c c}oise Hoffschir and Gauthier, \{Laurent R.\} and \{De Cian\}, Anne and Dennis Gomez and Eliane Mandine and Riou, \{Jean Fran{\c c}ois\} and Mergny, \{Jean Louis\} and Patrick Mailliet and Bernard Dutrillaux and Boussin, \{Fran{\c c}ois D.\}",

note = "Funding Information: The authors would like to thank T. Hercend (Sanofi-Aventis), D. Grierson (Institut Curie), L. Guittat (Mus{\'e}um National d{\textquoteright}Histoire Naturelle, Paris) and P. Fouchet (CEA) for scientific advices and O. Etienne (CEA) for technical assistance. This work was founded by SANOFI-AVENTIS and by an Action Concert{\'e}e Incitative {\textquoteleft}M{\'e}dicament et Cibles th{\'e}rapeu-tiques{\textquoteright} from the Minist{\`e}re de la Recherche et de la Technologie to J.-L.M., P.M., J.-F.R. and F.D.B., and by the ARC (\#\#3365) to J.-L.M. and ARC (\#3364) to J.-F.R. Funding to pay the Open Access publication charges for this article was provided by CEA/DSV/DRR/LRP.",

year = "2005",

month = oct,

day = "31",

doi = "10.1093/nar/gki722",

language = "English",

volume = "33",

pages = "4182--4190",

journal = "Nucleic Acids Research",

issn = "0305-1048",

number = "13",

}

TY - JOUR

T1 - Preferential binding of a G-quadruplex ligand to human chromosome ends

AU - Granotier, Christine

AU - Pennarun, Gaëlle

AU - Riou, Lydia

AU - Hoffschir, Françoise

AU - Gauthier, Laurent R.

AU - De Cian, Anne

AU - Gomez, Dennis

AU - Mandine, Eliane

AU - Riou, Jean François

AU - Mergny, Jean Louis

AU - Mailliet, Patrick

AU - Dutrillaux, Bernard

AU - Boussin, François D.

N1 - Funding Information: The authors would like to thank T. Hercend (Sanofi-Aventis), D. Grierson (Institut Curie), L. Guittat (Muséum National d’Histoire Naturelle, Paris) and P. Fouchet (CEA) for scientific advices and O. Etienne (CEA) for technical assistance. This work was founded by SANOFI-AVENTIS and by an Action Concertée Incitative ‘Médicament et Cibles thérapeu-tiques’ from the Ministère de la Recherche et de la Technologie to J.-L.M., P.M., J.-F.R. and F.D.B., and by the ARC (##3365) to J.-L.M. and ARC (#3364) to J.-F.R. Funding to pay the Open Access publication charges for this article was provided by CEA/DSV/DRR/LRP.

PY - 2005/10/31

Y1 - 2005/10/31

N2 - The G-overhangs of telomeres are thought to adopt particular conformations, such as T-loops or G-quadruplexes. It has been suggested that G-quadruplex structures could be stabilized by specific ligands in a new approach to cancer treatment consisting in inhibition of telomerase, an enzyme involved in telomere maintenance and cell immortality. Although the formation of G-quadruplexes was demonstrated in vitro many years ago, it has not been definitively demonstrated in living human cells. We therefore investigated the chromosomal binding of a tritiated G-quadruplex ligand, 3H-360A (2,6-N, N′-methyl-quinolinio-3-yl)-pyridine dicarboxamide [methyl-3H]. We verified the in vitro selectivity of 3H-360A for G-quadruplex structures by equilibrium dialysis. We then showed by binding experiments with human genomic DNA that 3H-360A has a very potent selectivity toward G-quadruplex structures of the telomeric 3′-overhang. Finally, we performed autoradiography of metaphase spreads from cells cultured with 3H-360A. We found that 3H-360A was preferentially bound to chromosome terminal regions of both human normal (peripheral blood lymphocytes) and tumor cells (T98G and CEM1301). In conclusion, our results provide evidence that a specific G-quadruplex ligand interacts with the terminal ends of human chromosomes. They support the hypothesis that G-quadruplex ligands induce and/or stabilize G-quadruplex structures at telomeres of human cells.

AB - The G-overhangs of telomeres are thought to adopt particular conformations, such as T-loops or G-quadruplexes. It has been suggested that G-quadruplex structures could be stabilized by specific ligands in a new approach to cancer treatment consisting in inhibition of telomerase, an enzyme involved in telomere maintenance and cell immortality. Although the formation of G-quadruplexes was demonstrated in vitro many years ago, it has not been definitively demonstrated in living human cells. We therefore investigated the chromosomal binding of a tritiated G-quadruplex ligand, 3H-360A (2,6-N, N′-methyl-quinolinio-3-yl)-pyridine dicarboxamide [methyl-3H]. We verified the in vitro selectivity of 3H-360A for G-quadruplex structures by equilibrium dialysis. We then showed by binding experiments with human genomic DNA that 3H-360A has a very potent selectivity toward G-quadruplex structures of the telomeric 3′-overhang. Finally, we performed autoradiography of metaphase spreads from cells cultured with 3H-360A. We found that 3H-360A was preferentially bound to chromosome terminal regions of both human normal (peripheral blood lymphocytes) and tumor cells (T98G and CEM1301). In conclusion, our results provide evidence that a specific G-quadruplex ligand interacts with the terminal ends of human chromosomes. They support the hypothesis that G-quadruplex ligands induce and/or stabilize G-quadruplex structures at telomeres of human cells.

UR - https://www.scopus.com/pages/publications/23044460408

U2 - 10.1093/nar/gki722

DO - 10.1093/nar/gki722

M3 - Article

C2 - 16052031

AN - SCOPUS:23044460408

SN - 0305-1048

VL - 33

SP - 4182

EP - 4190

JO - Nucleic Acids Research

JF - Nucleic Acids Research

IS - 13

ER -

Preferential binding of a G-quadruplex ligand to human chromosome ends

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