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1. Sae2 and Rif2 regulate MRX endonuclease activity at DNA double-strand breaks in opposite manners

2. Functions and regulation of the MRX complex at DNA double-strand breaks

3. Tel1 and Rif2 Regulate MRX Functions in End-Tethering and Repair of DNA Double-Strand Breaks.

4. Structure–function relationships of the Mre11 protein in the control of DNA end bridging and processing

5. Coupling end resection with the checkpoint response at DNA double-strand breaks

6. The ATP-bound conformation of the Mre11-Rad50 complex is essential for Tel1/ATM activation

7. The <scp>MRX</scp> complex regulates Exo1 resection activity by altering <scp>DNA</scp> end structure

8. Escape of Sgs1 from Rad9 inhibition reduces the requirement for Sae2 and functional <scp>MRX</scp> in <scp>DNA</scp> end resection

9. Structurally distinct Mre11 domains mediate MRX functions in resection, end-tethering and DNA damage resistance

10. Regulation of telomere metabolism by the RNA processing protein Xrn1

11. Vhs2 is a novel regulator of septin dynamics in budding yeast

12. Budding yeast Dma1 and Dma2 participate in regulation of Swe1 levels and localization

13. Functions and regulation of the MRX complex at DNA double-strand breaks

14. PP2A Controls Genome Integrity by Integrating Nutrient-Sensing and Metabolic Pathways with the DNA Damage Response

15. Saccharomyces cerevisiae Dma proteins participate in cytokinesis by controlling two different pathways

16. Protein Phosphorylation is an Important Tool to Change the Fate of Key Players in the Control of Cell Cycle Progression in Saccharomyces cerevisiae

17. Budding yeast Swe1 is involved in the control of mitotic spindle elongation and is regulated by Cdc14 phosphatase during mitosis

18. Telomere uncapping at the crossroad between cell cycle arrest and carcinogenesis

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