During DNA replication, epigenetic information carried by histone modifications is faithfully propagated and re-established on sister chromatids, ensuring cell identity. Chromatin reassembly is tightly coupled to DNA replication, however, whether and how perturbations to DNA replication affects the fidelity of epigenetic inheritance remain unclear. In this study, we reveal a critical role for replication fork reversal in maintaining the transmission of epigenetic information under replication stress. Cells defective in fork reversal exhibit reduced nucleosome density at replication forks, accompanied by the loss of parental histones during their transfer onto nascent DNA. Mechanistically, we demonstrate that PrimPol activation leads to single-stranded DNA gaps in fork reversal deficient cells, and that subsequent PARylation (poly ADP-ribosylation) and DNA-protein crosslinking on these gaps cause nucleosomes loss. Our findings demonstrate that replication fork reversal, a widespread physiological process, is not only essential for preserving genome integrity but also for safeguarding epigenetic stability.
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Liu et al. (Wed,) studied this question.
www.synapsesocial.com/papers/69a75bdcc6e9836116a23f59 — DOI: https://doi.org/10.21203/rs.3.rs-8544414/v1
Wenpeng Liu
Qiong Wu
Caixian Zhou
Pennsylvania State University
University of Virginia
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