A predictable conserved DNA base composition signature defines human core DNA replication origins

Author:

Akerman IldemORCID,Kasaai Bahar,Bazarova Alina,Sang Pau BiakORCID,Peiffer Isabelle,Artufel Marie,Derelle Romain,Smith Gabrielle,Rodriguez-Martinez Marta,Romano Manuela,Kinet SandrinaORCID,Tino Peter,Theillet CharlesORCID,Taylor NaomiORCID,Ballester BenoitORCID,Méchali Marcel

Abstract

AbstractDNA replication initiates from multiple genomic locations called replication origins. In metazoa, DNA sequence elements involved in origin specification remain elusive. Here, we examine pluripotent, primary, differentiating, and immortalized human cells, and demonstrate that a class of origins, termed core origins, is shared by different cell types and host ~80% of all DNA replication initiation events in any cell population. We detect a shared G-rich DNA sequence signature that coincides with most core origins in both human and mouse genomes. Transcription and G-rich elements can independently associate with replication origin activity. Computational algorithms show that core origins can be predicted, based solely on DNA sequence patterns but not on consensus motifs. Our results demonstrate that, despite an attributed stochasticity, core origins are chosen from a limited pool of genomic regions. Immortalization through oncogenic gene expression, but not normal cellular differentiation, results in increased stochastic firing from heterochromatin and decreased origin density at TAD borders.

Funder

Diabetes UK

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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