Page de résumé pour ULgetd-10052010-172725

Auteur :

Keutgens, Aurore

E-mail de l'auteur :

A.Keutgens@chu.ulg.ac.be

URN :

ULgetd-10052010-172725

Langue :

Anglais/English

Titre :

Insight into the mechanisms underlying the oncogenic potential of BCL-3 through interactomic studies / Etude des mécanismes requis pour le potentiel oncogénique de BCL-3 par l'intermédiaire d'études d'interactome.

Intitulé du diplôme :

Doctorat en sciences biomédicales et pharmaceutiques

Département :

Médecine - Département de pharmacie

Jury :

Nom :	Titre :
ANGENOT, Luc	Membre du jury/Committee Member
BEYAERT, Rudi	Membre du jury/Committee Member
BOURS, Vincent	Membre du jury/Committee Member
COURTOIS, Gilles	Membre du jury/Committee Member
NOEL, Agnès	Membre du jury/Committee Member
PEERS, Bernard	Membre du jury/Committee Member
STRUMAN, Ingrid	Membre du jury/Committee Member
PIETTE, Jacques	Président du jury/Committee Chair
CHARIOT, Alain	Promoteur/Director
MERVILLE, Marie-Paule	Promoteur/Director

Mots-clés :

BCL-3
TBLR1
CtBP
Interactomic studies
Ubiquitination
Degradation
Regulation of transcription

Date de soutenance :

2010-10-21

Type d'accès :

Restreint/Intranet

Résumé :

The oncogenic protein BCL-3, a member of the IκB family, was originally identified in a subset of human B-cell chronic lymphocytic leukemias that carry a translocation t(14,19), which results in BCL-3 overexpression. BCL-3 is also overexpressed in many solid tumors, such as in breast cancers and in cylindromas. This IκB protein activates or represses gene transcription through binding with the NF-κB proteins p50 and p52. Furthermore, BCL-3 is K63-linked polyubiquitinated, which leads to its translocation into the nucleus and to its target genes expression. BCL-3 is also K48-linked polyubiquitinated after GSK3 phosphorylation, which leads to its subsequent proteasomal degradation. However, the mechanisms underlying both its polyubiquitination and its ability to repress gene transcription remain poorly understood.

In order to gain more insight into these BCL-3 functions, parallel screenings involving both yeast-two-hybrid experiments and biochemical purifications led to the identification of BCL-3-interacting partners. Those screenings identified CtBP as a molecule required for the ability of BCL-3 to repress gene transcription. CtBP is also required for the stability, for the oncogenic potential and for the ability of BCL-3 to inhibit UV-mediated cell apoptosis in keratinocytes. We also defined the E3 ligase TBLR1 as a key element involved in BCL-3 polyubiquitination and degradation through a GSK3-independent pathway and the proteasome subunit PSMB1 as a protein required for the GSK3-dependent and -independent proteasomal degradation of polyubiquitinated BCL-3. Importantly, all interactions require unique motifs within the amino-terminal domain of BCL-3.

In conclusion, our data define multiple BCL-3-associated proteins that differentially and specifically regulate its function and stability and indicate that a better understanding of the mechanisms underlying the oncogenic properties of this IκB protein could be achieved through similar interactomic studies.

Autre version :

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