4.8 Article

Sgs1 function in the repair of DNA replication intermediates is separable from its role in homologous recombinational repair

Journal

EMBO JOURNAL
Volume 28, Issue 7, Pages 915-925

Publisher

WILEY
DOI: 10.1038/emboj.2009.28

Keywords

DNA repair; DNA replication; homologous recombination; Sgs1; yeast

Funding

  1. National Institute of Health grants [GM50237, GM67055, GM078840, GM73567]
  2. Associazione Italiana per la Ricerca sul Cancro
  3. Association for International Cancer Research to MF
  4. National Science Foundation graduate fellowship to ES

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Mutations in human homologues of the bacterial RecQ helicase cause diseases leading to cancer predisposition and/or shortened lifespan (Werner, Bloom, and Rothmund-Thomson syndromes). The budding yeast Saccharomyces cerevisiae has one RecQ helicase, Sgs1, which functions with Top3 and Rmi1 in DNA repair. Here, we report separation-of-function alleles of SGS1 that suppress the slow growth of top3 Delta and rmi1 Delta cells similar to an SGS1 deletion, but are resistant to DNA damage similar to wild-type SGS1. In one allele, the second acidic region is deleted, and in the other, only a single aspartic acid residue 664 is deleted. sgs1-D664 Delta, unlike sgs1 Delta, neither disrupts DNA recombination nor has synthetic growth defects when combined with DNA repair mutants. However, during S phase, it accumulates replication-associated X-shaped structures at damaged replication forks. Furthermore, fluorescent microscopy reveals that the sgs1-D664 Delta allele exhibits increased spontaneous RPA foci, suggesting that the persistent X-structures may contain single-stranded DNA. Taken together, these results suggest that the Sgs1 function in repair of DNA replication intermediates can be uncoupled from its role in homologous recombinational repair.

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