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MCM2-7 loading-dependent ORC release ensures genome-wide origin licensing.

L Maximilian ReuterSanjay P KhadayateAudrey MosslerKorbinian LieblSarah V FaullMohammad M KarimiChristian Speck
Published in: Nature communications (2024)
Origin recognition complex (ORC)-dependent loading of the replicative helicase MCM2-7 onto replication origins in G1-phase forms the basis of replication fork establishment in S-phase. However, how ORC and MCM2-7 facilitate genome-wide DNA licensing is not fully understood. Mapping the molecular footprints of budding yeast ORC and MCM2-7 genome-wide, we discovered that MCM2-7 loading is associated with ORC release from origins and redistribution to non-origin sites. Our bioinformatic analysis revealed that origins are compact units, where a single MCM2-7 double hexamer blocks repetitive loading through steric ORC binding site occlusion. Analyses of A-elements and an improved B2-element consensus motif uncovered that DNA shape, DNA flexibility, and the correct, face-to-face spacing of the two DNA elements are hallmarks of ORC-binding and efficient helicase loading sites. Thus, our work identified fundamental principles for MCM2-7 helicase loading that explain how origin licensing is realised across the genome.
Keyphrases
  • genome wide
  • circulating tumor
  • dna methylation
  • single molecule
  • cell free
  • copy number
  • high resolution
  • binding protein
  • high density