4.7 Article

Dbf4 recruitment by forkhead transcription factors defines an upstream rate-limiting step in determining origin firing timing

Journal

GENES & DEVELOPMENT
Volume 31, Issue 23-24, Pages 2405-2415

Publisher

COLD SPRING HARBOR LAB PRESS, PUBLICATIONS DEPT
DOI: 10.1101/gad.306571.117

Keywords

DNA replication timing; limiting factors; Dbf4; forkhead transcription factor

Funding

  1. National Natural Science Foundation of China [31630005, 31770084, 31628011, 31771382]
  2. State Key Laboratory of Microbial Resources
  3. State Key Laboratory of Agrobiotechnology [2016SKLAB6-10]
  4. Chinese Universities Scientific Fund [2015TC039]
  5. Agence Nationale pour la Recherche (ANR)
  6. Institut National du Cancer (INCa)
  7. Ligue contre le Cancer (equipe labellisee)
  8. MSDAvenir fund
  9. Foundation for Polish Science (TEAM)

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Initiation of eukaryotic chromosome replication follows a spatiotemporal program. The current model suggests that replication origins compete for a limited pool of initiation factors. However, it remains to be answered how these limiting factors are preferentially recruited to early origins. Here, we report that Dbf4 is enriched at early origins through its interaction with forkhead transcription factors Fkh1 and Fkh2. This interaction is mediated by the Dbf4 C terminus and was successfully reconstituted in vitro. An interaction-defective mutant, dbf4 Delta C, phenocopies fkh alleles in terms of origin firing. Remarkably, genome-wide replication profiles reveal that the direct fusion of the DNA-binding domain (DBD) of Fkh1 to Dbf4 restores the Fkh-dependent origin firing but interferes specifically with the pericentromeric origin activation. Furthermore, Dbf4 interacts directly with Sld3 and promotes the recruitment of downstream limiting factors. These data suggest that Fkh1 targets Dbf4 to a subset of non-centromeric origins to promote early replication in a manner that is reminiscent of the recruitment of Dbf4 to pericentromeric origins by Ctf19.

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