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Post-replicative repair involves separase-dependent removal of the kleisin subunit of cohesin

  • Alexandra McAleenan
  • , Andres Clemente-Blanco
  • , Violeta Cordon-Preciado
  • , Nicholas Sen
  • , Miguel Esteras
  • , Adam Jarmuz
  • , Luis Aragón*
  • *Autor correspondiente de este trabajo
  • Imperial College London

Producción científica: Contribución a una revistaArtículorevisión exhaustiva

49 Citas (Scopus)

Resumen

DNA double-strand break repair is critical for cell viability and involves highly coordinated pathways to restore DNA integrity at the lesion. An early event during homology-dependent repair is resection of the break to generate progressively longer 3′ single-strand tails that are used to identify suitable templates for repair. Sister chromatids provide near-perfect sequence homology and are therefore the preferred templates during homologous recombination. To provide a bias for the use of sisters as donors, cohesin - the complex that tethers sister chromatids together - is recruited to the break to enforce physical proximity. Here we show that DNA breaks promote dissociation of cohesin loaded during the previous S phase in budding yeast, and that damage-induced dissociation of cohesin requires separase, the protease that dissolves cohesion in anaphase. Moreover, a separase-resistant allele of the gene coding for the α-kleisin subunit of cohesin, Mcd1 (also known as Scc1), reduces double-strand break resection and compromises the efficiency of repair even when loaded during DNA damage. We conclude that post-replicative DNA repair involves cohesin dissociation by separase to promote accessibility to repair factors during the coordinated cellular response to restore DNA integrity.

Idioma originalInglés
Páginas (desde-hasta)250-254
Número de páginas5
PublicaciónNature
Volumen493
N.º7431
DOI
EstadoPublicada - 10 ene 2013
Publicado de forma externa

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