CMG helicase disassembly is essential and driven by two pathways in budding yeast

Cristian Polo Rivera, Tom D. Deegan (Lead / Corresponding author), Karim P M Labib (Lead / Corresponding author)

Research output: Contribution to journalArticlepeer-review

2 Citations (Scopus)
54 Downloads (Pure)

Abstract

The CMG helicase is the stable core of the eukaryotic replisome and is ubiquitylated and disassembled during DNA replication termination. Fungi and animals use different enzymes to ubiquitylate the Mcm7 subunit of CMG, suggesting that CMG ubiquitylation arose repeatedly during eukaryotic evolution. Until now, it was unclear whether cells also have ubiquitin-independent pathways for helicase disassembly and whether CMG disassembly is essential for cell viability. Using reconstituted assays with budding yeast CMG, we generated the mcm7-10R allele that compromises ubiquitylation by SCFDia2. mcm7-10R delays helicase disassembly in vivo, driving genome instability in the next cell cycle. These data indicate that defective CMG ubiquitylation explains the major phenotypes of cells lacking Dia2. Notably, the viability of mcm7-10R and dia2Δ is dependent upon the related Rrm3 and Pif1 DNA helicases that have orthologues in all eukaryotes. We show that Rrm3 acts during S-phase to disassemble old CMG complexes from the previous cell cycle. These findings indicate that CMG disassembly is essential in yeast cells and suggest that Pif1 family helicases might have mediated CMG disassembly in ancestral eukaryotes.
Original languageEnglish
Pages (from-to)3818-3845
Number of pages28
JournalThe EMBO Journal
Volume43
Issue number18
Early online date22 Jul 2024
DOIs
Publication statusPublished - 16 Sept 2024

Keywords

  • CMG helicase
  • SCFDia2
  • DNA replication
  • Ubiquitylation
  • Pif1-Rrm3
  • CMG Helicase
  • SCF
  • DNA Replication

ASJC Scopus subject areas

  • General Neuroscience
  • Molecular Biology
  • General Biochemistry,Genetics and Molecular Biology
  • General Immunology and Microbiology

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