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Endothelial-fibroblast interactions in diabetic foot ulcer: deciphering the intercellular communication


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-26-0291  

Direction

DRF

Thesis topic details

Category

Life Sciences

Thesis topics

Endothelial-fibroblast interactions in diabetic foot ulcer: deciphering the intercellular communication responsible for the chronic wound persistence

Contract

Thèse

Job description

Diabetic foot ulcer (DFU), a severe complication of diabetes affecting approximately 18.6 million people worldwide each year, is associated with high rates of amputation and mortality. Like other chronic wounds, DFUs exhibit impaired healing due to a dysregulated cascade of cellular signalling and behavioural events that normally ensure rapid closure of the skin barrier. Among the key cellular players, fibroblasts and endothelial cells are central to the proliferative and remodelling phases of wound repair – processes that are notably dysfunctional in chronic wounds. Although endothelial-fibroblast crosstalk is recognized as an essential driver of normal skin healing, the specific mechanisms governing their interaction in DFU is poorly understood.
The main objective of this PhD project is to decipher the intercellular communication between endothelial cells and fibroblasts that underlies the chronicity of DFU. Particular attention will be devoted to extracellular vesicle-associated microRNAs (miRNAs), which are pivotal regulators of intercellular communication through modulation of gene expression in recipient cells. By characterizing the repertoire of pro- and anti-healing miRNAs exchanged between endothelial cells and fibroblasts, this project seeks to uncover novel molecular targets and therapeutic strategies to promote wound repair in diabetic foot ulcers.

University / doctoral school

Chimie et Sciences du Vivant (EDCSV)
Université Grenoble Alpes

Thesis topic location

Site

Grenoble

Requester

Position start date

01/10/2026

Person to be contacted by the applicant

VIGUIER Marie marie.viguier@cea.fr
UGA
BGE IRIG
BGE-UA13 INSERM/CEA/UGA
IRIG/CEA Grenoble
17, Rue des Martyrs
38054 Grenoble Cedex 09
04 38 78 22 36

Tutor / Responsible thesis director

CHERRADI Nadia nadia.cherradi@cea.fr
INSERM
DRF/IRIG/BCI/UMR1292 Biosanté
BCI-Biosanté-UMR1292 INSERM/CEA/UGA
IRIG/CEA Grenoble
17, Rue des Martyrs
38054 Grenoble Cedex 09
04 38 78 35 01

En savoir plus

www.linkedin.com/in/marie-viguier
https://www.bge-lab.fr/
https://biosante-lab.fr/Pages/IMAC/Presentation.aspx