Replication timing maintains the global epigenetic state in human cells.
Kyle N KleinPeiyao A ZhaoXiaowen LyuTakayo SasakiDaniel A BartlettAmar M SinghIpek TasanMeng ZhangLotte P WattsShin-Ichiro HiragaToyoaki NatsumeXuemeng ZhouTimour BaslanDanny Chi Yeu LeungMasato T KanemakiAnne D DonaldsonHuimin ZhaoStephen DaltonVictor G CorcesDavid M GilbertPublished in: Science (New York, N.Y.) (2021)
The temporal order of DNA replication [replication timing (RT)] is correlated with chromatin modifications and three-dimensional genome architecture; however, causal links have not been established, largely because of an inability to manipulate the global RT program. We show that loss of RIF1 causes near-complete elimination of the RT program by increasing heterogeneity between individual cells. RT changes are coupled with widespread alterations in chromatin modifications and genome compartmentalization. Conditional depletion of RIF1 causes replication-dependent disruption of histone modifications and alterations in genome architecture. These effects were magnified with successive cycles of altered RT. These results support models in which the timing of chromatin replication and thus assembly plays a key role in maintaining the global epigenetic state.