Repair of DNA broken ends is similar in embryonic fibroblasts with and without telomerase

Laura Latre, Anna Genescà, Marta Mart́in, Montserrat Ribas, Josep Egozcue, María A. Blasco, Laura Tusell

Producción científica: Contribución a una revistaArtículoInvestigaciónrevisión exhaustiva

10 Citas (Scopus)

Resumen

Telomeres cap the ends of chromosomes, preventing end-to-end fusions and subsequent chromosome instability. Here we used a telomerase knockout model to investigate whether telomerase participates in the processes of DNA break repair by de novo synthesis of telomere repeats at broken chromosome ends (chromosome healing). Chromosome healing giving rise to new detectable telomeric signals has not been observed in embryonic fibroblasts of telomerase-proficient mice exposed to ionizing radiation. Since the synthesis of telomeric sequences to broken DNA ends would make them refractory to rejoining events, the efficiency of rejoining of broken chromosomes in cell environments with and without telomerase has also been investigated. We conclude that the efficiency of rejoining broken chromosomes is not significantly different in the two cell environments. All together, our results indicate that there is no significant involvement of telomerase in the healing of broken DNA ends by synthesizing new telomeres in mouse embryo fibroblasts after exposure to ionizing radiation. © 2004 by Radiation Research Society.
Idioma originalInglés
Páginas (desde-hasta)136-142
PublicaciónRadiation Research
Volumen162
DOI
EstadoPublicada - 1 ago 2004

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