Suppression of targeting of Dbf4 ‐dependent kinase to pre‐replicative complex in G0 nuclei

Intact G0 nuclei isolated from quiescent cells are not capable of DNA replication in interphase Xenopus egg extracts, which allow efficient replication of permeabilized G0 nuclei. Previous studies have shown multiple control mechanisms for maintaining the quiescent state, but DNA replication inhibition of intact G0 nuclei in the extracts remains poorly understood. Here, we showed that pre‐RC is assembled on chromatin, but its activation is inhibited after incubating G0 nuclei isolated from quiescent NIH3T3 cells in the extracts. Concomitant with the inhibition of replication, Mcm4 phosphorylation mediated by Dbf4‐dependent kinase (DDK) as well as chromatin binding of DDK is suppressed in G0 nuclei without affecting the nuclear transport of DDK. We further found that the nuclear extracts of G0 but not proliferating cells inhibit the binding of recombinant DDK to pre‐RC assembled plasmids. In addition, we observed rapid activation of checkpoint kinases after incubating G0 nuclei in the egg extracts. However, specific inhibitors of ATR/ATM are unable to promote DNA replication in G0 nuclei in the egg extracts. We suggest that a novel inhibitory mechanism is functional to prevent the targeting of DDK to pre‐RC in G0 nuclei, thereby suppressing DNA replication in Xenopus egg extracts. Intact G0 nuclei isolated from quiescent cells are not capable of DNA replication in interphase Xenopus egg extracts. We showed that pre‐RC is assembled on chromatin, but its activation is...
Source: Genes to Cells - Category: Genetics & Stem Cells Authors: Tags: ORIGINAL ARTICLE Source Type: research
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