| Literature DB >> 33980827 |
Florian Roisné-Hamelin1, Sabrina Pobiega1, Kévin Jézéquel1, Simona Miron2, Jordane Dépagne3, Xavier Veaute3, Didier Busso3, Marie-Hélène Le Du2, Isabelle Callebaut4, Jean-Baptiste Charbonnier2, Philippe Cuniasse2, Sophie Zinn-Justin2, Stéphane Marcand5.
Abstract
Specific proteins present at telomeres ensure chromosome end stability, in large part through unknown mechanisms. In this work, we address how the Saccharomyces cerevisiae ORC-related Rif2 protein protects telomere. We show that the small N-terminal Rif2 BAT motif (Blocks Addition of Telomeres) previously known to limit telomere elongation and Tel1 activity is also sufficient to block NHEJ and 5' end resection. The BAT motif inhibits the ability of the Mre11-Rad50-Xrs2 complex (MRX) to capture DNA ends. It acts through a direct contact with Rad50 ATP-binding Head domains. Through genetic approaches guided by structural predictions, we identify residues at the surface of Rad50 that are essential for the interaction with Rif2 and its inhibition. Finally, a docking model predicts how BAT binding could specifically destabilise the DNA-bound state of the MRX complex. From these results, we propose that when an MRX complex approaches a telomere, the Rif2 BAT motif binds MRX Head in its ATP-bound resting state. This antagonises MRX transition to its DNA-bound state, and favours a rapid return to the ATP-bound state. Unable to stably capture the telomere end, the MRX complex cannot proceed with the subsequent steps of NHEJ, Tel1-activation and 5' resection.Entities:
Year: 2021 PMID: 33980827 PMCID: PMC8115599 DOI: 10.1038/s41467-021-23035-w
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919