Up2Europe est un accélérateur d’idées pour des projets de coopération.
La plateforme Ma Région Sud fait partie de l'écosystème de Up2Europe qui permet de booster la coopération à un niveau supérieur!
Besoin d'aide ? La Région Sud vous accompagne
Laissez-vous guider par notre équipe d'experts ! Saisissez votre mail et nous reviendrons vers vous rapidement
The role of activation-induced cytidine deaminase .. (InflAIDCan)
The role of activation-induced cytidine deaminase in inflammation-induced carcinogenesis
(InflAIDCan)
Date du début: 1 mars 2010,
Date de fin: 31 août 2011
PROJET
TERMINÉ
Activation-induced cytidine deaminase (AID) is a DNA-modifying enzyme essential for somatic hypermutation and class switch recombination in B cells. However, deregulation of AID can induce mutations and chromosomal translocations in B cells thus promoting neoplastic transformation and cancer development. AID expression is controlled by several transcription factors like those of the Rel/NF-kappa B family. The NF-kappa B pathway can be activated by a variety of different stimuli and constitutive activation of NF-kappa B is implicated in various malignancies. Indeed, the well established link between chronic inflammation and cancer has been correlated to constitutive NF-kappa B activation by inflammatory cytokines. Although the expression of AID was originally thought to be restricted to B cells, it has been shown recently that stimulation with inflammatory cytokines also induces AID expression in different epithelial cells. Furthermore, expression of AID has been found in hepatocarcinomas, gastric cancer and bile duct carcinomas suggesting a link between inflammation, NF-kappaB activation, AID expression and cancer development. However, it remains unclear if in the observed cases AID expression is just a by-product of NF-kappa B activity or if AID actively contributes to cancer development and/or progression in vivo. In the proposed research project, I am aiming to address the role of AID in the development and progression of carcinomas in vivo. For this purpose, I am going to compare the tumour incidence and aggressiveness between wt and AID-/- mice in a model for colitis-induced carcinogenesis. In addition, I am planning to generate a reporter system in which the expression of the oncogenic KRasV12 mutant depends on the reversion of a STOP codon by AID. This will decrease the amount of mutations required for tumour development and will allow for the efficient tracking and quantification of AID activity in different tissues in vitro and in vivo.
Accédez au prémier réseau pour la cooperation européenne
Se connecter
Bonjour, vous êtes sur la plateforme Région Sud Provence-Alpes-Côte d’Azur dédiée aux programmes thématiques et de coopération territoriale. Une équipe d’experts vous accompagne dans vos recherches de financements.
Contactez-nous !
Contactez la Région Sud Provence-Alpes-Côte d'Azur
Vous pouvez nous écrire en Anglais, Français et Italien