Author
Listed:
- Boris Bartholdy
(Albert Einstein College of Medicine)
- Rituparna Mukhopadhyay
(Albert Einstein College of Medicine)
- Julien Lajugie
(Albert Einstein College of Medicine)
- Mirit I. Aladjem
(Laboratory of Molecular Pharmacology, Center for Cancer Research, National Cancer Institute)
- Eric E. Bouhassira
(Albert Einstein College of Medicine)
Abstract
The mechanisms that control the location and timing of firing of replication origins are poorly understood. Using a novel functional genomic approach based on the analysis of SNPs and indels in phased human genomes, we observe that replication asynchrony is associated with small cumulative variations in the initiation efficiency of multiple origins between the chromosome homologues, rather than with the activation of dormant origins. Allele-specific measurements demonstrate that the presence of G-quadruplex-forming sequences does not correlate with the efficiency of initiation. Sequence analysis reveals that the origins are highly enriched in sequences with profoundly asymmetric G/C and A/T nucleotide distributions and are almost completely depleted of antiparallel triplex-forming sequences. We therefore propose that although G4-forming sequences are abundant in replication origins, an asymmetry in nucleotide distribution, which increases the propensity of origins to unwind and adopt non-B DNA structure, rather than the ability to form G4, is directly associated with origin activity.
Suggested Citation
Boris Bartholdy & Rituparna Mukhopadhyay & Julien Lajugie & Mirit I. Aladjem & Eric E. Bouhassira, 2015.
"Allele-specific analysis of DNA replication origins in mammalian cells,"
Nature Communications, Nature, vol. 6(1), pages 1-12, November.
Handle:
RePEc:nat:natcom:v:6:y:2015:i:1:d:10.1038_ncomms8051
DOI: 10.1038/ncomms8051
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