Regulation of replication origin licensing by ORC phosphorylation reveals a two-step mechanism for Mcm2-7 ring closing

Regulation of replication origin licensing by ORC phosphorylation reveals a two-step mechanism for Mcm2-7 ring closing

Eukaryotic DNA replication must occur exactly once per cell cycle to maintain cell ploidy. This outcome is ensured by temporally separating replicative helicase loading (G1 phase) and activation (S phase). In budding yeast, helicase loading is prevented outside of G1 by cyclin-dependent kinase (CDK)...

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Published in:Proceedings of the National Academy of Sciences - PNAS Vol. 120; no. 29; p. e2221484120
Main Authors: Amasino, Audra L, Gupta, Shalini, Friedman, Larry J, Gelles, Jeff, Bell, Stephen P
Format: Journal Article
Language:English
Published: United States National Academy of Sciences 18-07-2023
Subjects:
Biological Sciences
Cell cycle
Cell Cycle Proteins - metabolism
Complex formation
Cyclin-dependent kinase
Cyclin-dependent kinases
Cyclin-Dependent Kinases - metabolism
DNA biosynthesis
DNA helicase
DNA Replication
G1 phase
Kinases
Licensing
Minichromosome Maintenance Proteins - metabolism
Origin recognition complex
Origin Recognition Complex - genetics
Origin Recognition Complex - metabolism
Phosphorylation
Ploidy
Proteins
Replication
Replication Origin
Replication origins
S phase
Saccharomyces cerevisiae - metabolism
Saccharomyces cerevisiae Proteins - genetics
Saccharomyces cerevisiae Proteins - metabolism
Yeasts
DNA replication
initiation
helicase
origin recognition complex (ORC)
Mcm2-7
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Summary:Eukaryotic DNA replication must occur exactly once per cell cycle to maintain cell ploidy. This outcome is ensured by temporally separating replicative helicase loading (G1 phase) and activation (S phase). In budding yeast, helicase loading is prevented outside of G1 by cyclin-dependent kinase (CDK) phosphorylation of three helicase-loading proteins: Cdc6, the Mcm2-7 helicase, and the origin recognition complex (ORC). CDK inhibition of Cdc6 and Mcm2-7 is well understood. Here we use single-molecule assays for multiple events during origin licensing to determine how CDK phosphorylation of ORC suppresses helicase loading. We find that phosphorylated ORC recruits a first Mcm2-7 to origins but prevents second Mcm2-7 recruitment. The phosphorylation of the Orc6, but not of the Orc2 subunit, increases the fraction of first Mcm2-7 recruitment events that are unsuccessful due to the rapid and simultaneous release of the helicase and its associated Cdt1 helicase-loading protein. Real-time monitoring of first Mcm2-7 ring closing reveals that either Orc2 or Orc6 phosphorylation prevents Mcm2-7 from stably encircling origin DNA. Consequently, we assessed formation of the MO complex, an intermediate that requires the closed-ring form of Mcm2-7. We found that ORC phosphorylation fully inhibits MO complex formation and we provide evidence that this event is required for stable closing of the first Mcm2-7. Our studies show that multiple steps of helicase loading are impacted by ORC phosphorylation and reveal that closing of the first Mcm2-7 ring is a two-step process started by Cdt1 release and completed by MO complex formation.
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Edited by Bruce Stillman, Cold Spring Harbor Laboratory, Cold Spring Harbor, NY; received December 19, 2022; accepted June 3, 2023
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.2221484120