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The multiple roles of cohesin in genome stability


Thesis topic details

General information

Organisation

The French Alternative Energies and Atomic Energy Commission (CEA) is a key player in research, development and innovation in four main areas :
• defence and security,
• nuclear energy (fission and fusion),
• technological research for industry,
• fundamental research in the physical sciences and life sciences.

Drawing on its widely acknowledged expertise, and thanks to its 16000 technicians, engineers, researchers and staff, the CEA actively participates in collaborative projects with a large number of academic and industrial partners.

The CEA is established in ten centers spread throughout France
  

Reference

SL-DRF-26-0622  

Direction

DRF

Thesis topic details

Category

Miscellaneous

Thesis topics

The multiple roles of cohesin in genome stability

Contract

Thèse

Job description

Cohesin, a ring-shaped protein complex, is crucial for genome stability, gene expression, sister chromatid cohesion, and DNA repair. It forms intrachromosomal loops during interphase, aiding in chromatin organization by bringing enhancers and promoters together. Cohesin also ensures sister chromatid cohesion during DNA replication and repairs double-strand breaks (DSBs). In response to DNA damage, cohesin binds to DSBs and enhances cohesion via damage-induced cohesion (DI-cohesion). Our recent findings show that cohesin tethers DSB ends through oligomer formation (Phipps et al., 2025).
This research project aims, in the frame of an ANR funded project, to explore how DNA damage influences cohesin’s functions in genome stability. The main hypothesis is that DNA damage activates distinct cohesin populations with specific roles critical for maintaining genome integrity. Using Saccharomyces cerevisiae as a model, the project focuses on three goals: analyzing the impact of DNA damage on cohesin composition and modifications, studying oligomerization in DSB tethering, and identifying the cohesin populations involved in DI-cohesion.
The methodology combines biochemical, genetic, and genomic approaches. Key tasks include identifying new cohesin interactors, analyzing cohesin in specific mutants, and investigating post-translational modifications.
This project aims to provide comprehensive insights into cohesin’s diverse roles in genome stability beyond traditional sister chromatid cohesion.

University / doctoral school

Structure et Dynamique des Systèmes Vivants (SDSV)

Thesis topic location

Site

Saclay

Requester

Position start date

01/10/2026

Person to be contacted by the applicant

DUBRANA Karine karine.dubrana@cea.fr
CEA
DRF/JACOB//SIGRR
18 route du panorama
92265 Fontenay aux roses
0146549343

Tutor / Responsible thesis director

DUBRANA Karine karine.dubrana@cea.fr
CEA
DRF/JACOB//SIGRR
18 route du panorama
92265 Fontenay aux roses
0146549343

En savoir plus


https://jacob.cea.fr/drf/ifrancoisjacob/Pages/Departements/IRCM/Equipes/LION.aspx