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Sgs1’s roles in DNA end resection, HJ dissolution, and crossover suppression require a two-step SUMO regulation dependent on Smc5/6

  • Marcelino Bermúdez-López
  • , María Teresa Villoria
  • , Miguel Esteras
  • , Adam Jarmuz
  • , Jordi Torres-Rosell
  • , Andres Clemente-Blanco
  • , Luis Aragon*
  • *Autor correspondiente de este trabajo
  • Imperial College London
  • Instituto de Biologia Funcional y Genomica (IBFG)

Producción científica: Contribución a una revistaArtículorevisión exhaustiva

55 Citas (Scopus)

Resumen

The RecQ helicase Sgs1 plays critical roles during DNA repair by homologous recombination, fromend resection to Holliday junction (HJ) dissolution. Sgs1 has both pro- and anti-recombinogenic roles, and therefore its activity must be tightly regulated. However, the controls involved in recruitment and activation of Sgs1 at damaged sites are unknown. Here we show a two-step role for Smc5/6 in recruiting and activating Sgs1 through SUMOylation. First, auto-SUMOylation of Smc5/6 subunits leads to recruitment of Sgs1 as part of the STR (Sgs1–Top3–Rmi1) complex, mediated by two SUMO-interacting motifs (SIMs) on Sgs1 that specifically recognize SUMOylated Smc5/6. Second, Smc5/6-dependent SUMOylation of Sgs1 and Top3 is required for the efficient function of STR. Sgs1 mutants impaired in recognition of SUMOylated Smc5/6 (sgs1-SIMΔ) or SUMO-dead alleles (sgs1-KR) exhibit unprocessed HJs at damaged replication forks, increased crossover frequencies during double-strand break repair, and severe impairment in DNA end resection. Smc5/6 is a key regulator of Sgs1’s recombination functions.

Idioma originalInglés
Páginas (desde-hasta)1339-1356
Número de páginas18
PublicaciónGenes and Development
Volumen30
N.º11
DOI
EstadoPublicada - 1 jun 2016
Publicado de forma externa

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