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Faculté de Médecine
Faculté de Médecine
MASTER THESIS
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Thesis, COLLÉGIALITÉ

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Ndong Penda, Rosa Melvine ULiège
Promotor(s) : Nguyen, Laurent ULiège
Date of defense : 4-Jul-2023 • Permalink : http://hdl.handle.net/2268.2/17904
Details
Title : Thesis, COLLÉGIALITÉ
Translated title : [fr] Décrypter la contribution de COUP-TF1 dans le défauts de migration des neurones de projection survenant lors d’une exposition prénatale à l’alcool
Author : Ndong Penda, Rosa Melvine ULiège
Date of defense  : 4-Jul-2023
Advisor(s) : Nguyen, Laurent ULiège
Committee's member(s) : Voz, Marianne ULiège
Franzen, Rachelle ULiège
Seutin, Vincent ULiège
Language : English
Number of pages : 50
Keywords : [en] FASD
[en] COUP-TF1
[en] Migrating projection neurons
Discipline(s) : Human health sciences > Multidisciplinary, general & others
Funders : FNRS
Research unit : GIGA STEM CELLS: Laboratory of molecular regulation of neurogenesis
Name of the research project : Deciphering the contribution of COUP-TF1 in the migration defects of projection neurons occurring upon prenatal alcohol exposure
Target public : Researchers
Professionals of domain
Institution(s) : Université de Liège, Liège, Belgique
Degree: Master en sciences biomédicales, à finalité approfondie
Faculty: Master thesis of the Faculté de Médecine

Abstract

[en] Fetal alcohol spectrum disorder (FASD) is a major public health issue worldwide and the most
preventable cause of intellectual disability. The most severe form of FASD is fetal alcohol
syndrome (FAS), which is characterized by growth deficiencies (mild microcephaly), specific facial
malformations and severe central nervous system (CNS) impairments. The lack of awareness on
the devastating effects of alcohol in utero and the insufficient expertise in diagnosing FASD have
led to an increase in the prevalence of this pathology over the past years.
FASD has been reported to impact diverse neural cell types and activity across the developing
cerebral cortex, but the precise pathophysiological effects on developing projection neurons
(PNs) are unclear. Studies in rodents reported that in utero alcohol exposure alters PN
development at several stages like proliferation, migration, differentiation and maturation.
Previous experiments in the host laboratory focusing on PNs revealed impairments in migration
dynamics upon PAE coupled with COUP-TF1 upregulation.
In the present research study, we used the drinking in the dark paradigm (DID) model of alcohol
administration to assess the role of COUP-TF1 in the migratory defects observed upon PAE. This
mode of ethanol administration was chosen compared to other models such as gavage and
injection because it was shown to mimic the human pattern of binge-drinking, induce a slow
increase in blood alcohol (BAC) and less maternal stress.
We showed that alcohol-induced migratory defects in PNs were rescued by the downregulation
of COUP-TF1 in migrating PNs by in utero electroporation of a plasmid expressing miRNA against
COUP-TF1 under the promoter DCX in PAE dams. Altogether, these findings suggest that COUP TF1 is the main target gene responsible for migratory defects upon PAE. This reinforces the
interest to further investigate the molecular mechanisms by which COUP-TF1 affects migration
of PNs upon PAE which might contribute to better understanding the pathophysiology of FASD.


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Author

  • Ndong Penda, Rosa Melvine ULiège Université de Liège > Master sc. bioméd., à fin.

Promotor(s)

Committee's member(s)

  • Voz, Marianne ULiège Université de Liège - ULiège > Département des sciences de la vie > Département des sciences de la vie
    ORBi View his publications on ORBi
  • Franzen, Rachelle ULiège Université de Liège - ULiège > Département des sciences biomédicales et précliniques > Neuro-anatomie
    ORBi View his publications on ORBi
  • Seutin, Vincent ULiège Université de Liège - ULiège > Département des sciences biomédicales et précliniques > Pharmacologie
    ORBi View his publications on ORBi
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