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Novel role for SOX2 in the development of the zebrafish epithalamusPavlou, Sofia January 2013 (has links)
The sex determining region Y-box 2 (sox2) gene is one of the most important transcription factors during development, particularly the development of the central nervous system (CNS). It is expressed in embryonic stem cells and later in neural stem cells, where it modulates their maintenance and differentiation. In humans, heterozygous mutations are associated with eye malformations, including anophthalmia and severe microphthalmia. Also, a subset of patients has extra-ocular phenotypes, such as hearing loss, seizures and pituitary hypoplasia. Although the roles of sox2 in embryonic stem cells and eye development are well studied, the function of sox2 in brain development and disease is still elusive. The aim of this project was to characterize a novel role for sox2 in the development of zebrafish epithalamus, which was identified from an in silico screen previously performed in our laboratory. The zebrafish epithalamus, located in the dorsal diencephalon, consists of three main structures: the pineal gland, the parapineal organ and the habenular nuclei. The pineal gland, also known as epiphysis, is a photoreceptive (in zebrafish) and neuroendocrine organ that detects light and rhythmically produces melatonin in order to regulate the circadian rhythms. The parapineal organ is located to the left side of the pineal gland and is important for the elaboration of the asymmetries observed between the left and right habenular nuclei. Finally, the bilateral habenulae are part of the dorsal diencephalic conduction system that links the forebrain with the mid- and hindbrain. The left and right habenulae show both molecular and neuroanatomical asymmetries, including differences in neuropil organization, in levels of gene expression and in the morphology and connectivity of their neurons’ projections. The relatively simple architecture of the pineal gland and the asymmetric character of the habenulae provide a useful tool for studying cell-fate determination, cell migration and establishment of brain asymmetries. In this study, we used zebrafish as a model to dissect the novel functions of sox2 in the development of the epithalamus. We showed that sox2 works synergistically with Notch pathway to negatively regulate neurogenesis within the pineal gland. The pineal gland consists of only two cell types: the photoreceptors and the projection neurons. Previous studies showed that the Notch and BMP pathways are important for the proper specification of these cells. Here, we show that sox2 normally inhibits the photoreceptor cell fate, whereas it has no effect on the number of projection neurons. Therefore, sox2 complements Notch and BMP pathways in cell-fate determination within the pineal gland. In addition, downregulation of sox2 results in abnormal parapineal organ development and disruption of the asymmetric architecture of the habenulae. A subset of sox2 morphant embryos develops right-sided parapineal organs, which is consistent with abnormal bilateral expression of the Nodal gene, pitx2 (paired-like homeodomain transcription factor 2). Also, timelapse experiments showed that migration of the parapineal cells is defective, resulting in scattered cells. The aberrant parapineal development leads to disorganization of the habenular nuclei, as shown by the abnormal neuropil arrangement and the expression of the asymmetric marker kctd12.1 (potassium channel tetramerisation domain containing 12.1).
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Zebrafish Epithalamus as a Model System for Studying Circadian Rhythms and Left-Right AsymmetryLu, Po-Nien 19 June 2012 (has links)
No description available.
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Interaction entre les voies de signalisation FGF et Notch lors de la migration de la parapineale dans le cerveau asymétrique du poisson zèbre / Crosstalk between FGF and Notch signaling pathways during the collective migration of parapineal cells in the left right asymmetric zebrafish brainWei, Lu 26 November 2018 (has links)
Lors du développement de l'asymétrie gauche droite dans le cerveau du poisson zèbre, un petit groupe de cellules, le parapinéale, migre collectivement depuis la ligne médiane vers la partie gauche de l'épithalamus. Cette migration est défectueuse dans des mutants pour le gène fgf8, indiquant que le facteur Fgf8 (Fibroblast Growth Factor 8), sécrété de part et d'autre de la ligne médiane, est requis pour la migration. Cependant, l'orientation gauche de la migration dépend de l'activation, plus précocement dans l'épithalamus gauche, de la voie de signalisation Nodal/TGFb (Transforming Growth Factor). Par conséquent, la parapinéale est un modèle de choix pour comprendre comment les cellules migrent collectivement en réponse aux Fgf et pour étudier comment d'autres voies de signalisation modulent ce processus. L'imagerie en temps réel d'un transgène rapporteur de la signalisation FGF a révélé que la voie FGF est activée préférentiellement dans quelques cellules de tête, c'est à dire localisées au front de migration. L'expression globale d'un récepteur aux Fgf activé de façon constitutive (CA-FgfR1) interfère avec la migration de la parapinéale en contexte sauvage mais est capable de restaurer à la fois la migration de la parapinéale et l'activation focale de la voie FGF au front de migration dans les mutants fgf8-/-. De plus, l'activation focale de la voie FGF dans seulement quelques cellules de parapinéale est suffisante pour restaurer la migration de tout le collectif dans les mutants fgf8-/-. Finalement, nos données montrent que la signalisation Nodal contribue à restreindre et à biaiser l'activation de la voie FGF afin d'orienter la migration de la parapinéale vers le côté gauche (Manuscript n°1). Par la suite, mes travaux de thèse ont visé à comprendre comment l'activation de la voie FGF est restreinte à quelques cellules, bien que toutes les cellules de parapinéale semblent compétentes pour activer la voie. Nos résultats montrent que la signalisation Notch est capable de restreindre l'activation de la voie FGF. La perte ou le gain de fonction de la voie Notch entrainent respectivement une augmentation ou une diminution de l'activité FGF, associés à des défauts de migration de la parapinéale dans les deux contextes. De plus, la diminution ou l'augmentation artificielle du niveau d'activation de la voie FGF peut respectivement restaurer la migration de la parapinéale ou aggraver les défauts de migration en absence d'activité Notch. Nos données indiquent que la signalisation Notch restreint l'activation de la voie FGF au sein des cellules de parapinéale pour permettre la migration du collectif (Manuscript n°2). La voie Notch est également requise pour la spécification d'un nombre correct de cellules de parapinéale, indépendamment de la voie FGF. En parallèle, nous avons analysé la fonction de MMP2 (Matrix Metalloprotease 2), une protéine exprimée mosaïquement dans la parapinéale et candidate pour moduler la signalisation FGF. Cependant, nous n'avons observé aucun défaut de spécification ou de migration de la parapinéale dans les embryons mutants pour le gène mmp2 -/- (Manuscript n°3). Mon travail de thèse révèle un rôle de la voie Notch pour restreindre l'activation de la signalisation FGF dans quelques cellules de parapinéale, un processus qui est biaisé par la voie Nodal afin d'orienter la migration du collectif vers la gauche. Ces données pourraient permettre de mieux comprendre les interactions entre les voies de signalisation FGF, Notch et Nodal dans d'autres modèles de migration cellulaire collective comme, par exemple, la migration des cellules cancéreuses. / During the establishment of left-right asymmetry in the zebrafish brain, a small group of cells, the parapineal, collectively migrates from the dorsal midline of the epithalamus to the left in most wild-type embryos. Parapineal migration requires Fibroblastic Growth Factor 8 (Fgf8), a secreted signal expressed bilaterally in epithalamic tissues surrounding the parapineal. The left bias in the orientation of parapineal migration depends on the activity of Cyclops, a secreted factor of the Nodal/TGFß family that is transiently expressed in the left epithalamus prior to parapineal migration. Therefore, the parapineal provides a powerful new model to understand FGF dependent collective cell migration and to study how other signaling pathways modulate this process. Live imaging of an FGF reporter transgene revealed that the FGF pathway is activated in only few parapineal cells that are usually located at the leading edge of migration. Global expression of a constitutively activated Fgf receptor (CA-FGFR) delays migration in wild-type, while it partially restores both parapineal migration and focal activation of the FGF reporter transgene in fgf8-/- mutant embryos. Importantly, focal activation of FGF signaling in few parapineal cells is sufficient to restore collective migration in fgf8-/- mutants. Finally, Nodal asymmetry contributes to restrict and left-bias the activation of the FGF pathway (Manuscript n°1). Following this work, my thesis project aimed at understanding how the activation of the FGF pathway is restricted to few cells, despite all parapineal cells apparently being competent to activate the pathway. We showed that Notch signaling is able to restrict FGF activity. Loss or gain of function of the Notch pathway respectively triggers an increase or decrease in FGF activity, which correlate with PP migration defects. Moreover, decreasing or increasing FGF activity levels respectively rescues or aggravates parapineal migration defects in Notch loss-of-function context. Our data indicate that Notch signaling restricts the activation of the FGF pathway within parapineal cells to promote their collective migration (Manuscript n°2). We also found that Notch pathway is required for the specification of a correct number of parapineal cells, independently of FGF pathway. In parallel, we analysed the function of MMP2 (Matrix Metalloprotease 2), a protein mosaïcally expressed in the parapineal and a candidate to modulate FGF signaling. However, we found no significant defects in the specification or migration of parapineal cells in mmp2-/- mutant embryos (Manuscript n°3). My PhD work reveals a role for Notch signaling in restricting the activation of FGF signaling within few parapineal cells, a process that is biased by Nodal pathway to the left and required for the migration of the entire parapineal. These data provide insights into the interaction of FGF, Notch and Nodal/TGFb signaling pathways that may be applicable to other models of collective cell migration, such as cancer cells migration for instance.
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