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1. A stable leading strand polymerase/clamp loader complex is required for normal and perturbed eukaryotic DNA replication

3. Can eukaryotic cells monitor the presence of unreplicated DNA?

4. Sen1 Is Recruited to Replication Forks via Ctf4 and Mrc1 and Promotes Genome Stability.

5. The S phase checkpoint promotes the Smc5/6 complex dependent SUMOylation of Pol2, the catalytic subunit of DNA polymerase ε.

6. A conserved Polϵ binding module in Ctf18-RFC is required for S-phase checkpoint activation downstream of Mec1.

7. Cdc48 and a ubiquitin ligase drive disassembly of the CMG helicase at the end of DNA replication.

8. Dpb2 integrates the leading-strand DNA polymerase into the eukaryotic replisome.

9. Eukaryotic replisome components cooperate to process histones during chromosome replication.

10. A conserved motif in the C-terminal tail of DNA polymerase α tethers primase to the eukaryotic replisome.

11. Mcm10 associates with the loaded DNA helicase at replication origins and defines a novel step in its activation.

12. Replisome stability at defective DNA replication forks is independent of S phase checkpoint kinases.

13. Surviving chromosome replication: the many roles of the S-phase checkpoint pathway.

14. The unnamed complex: what do we know about Smc5-Smc6?

15. The Smc5-Smc6 complex and SUMO modification of Rad52 regulates recombinational repair at the ribosomal gene locus.

16. Can eukaryotic cells monitor the presence of unreplicated DNA?

17. SMC proteins, new players in the maintenance of genomic stability.

18. Anaphase onset before complete DNA replication with intact checkpoint responses.

19. Smc5-Smc6 mediate DNA double-strand-break repair by promoting sister-chromatid recombination.

20. Transcription of ribosomal genes can cause nondisjunction.

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