Global ETD Search

1	Brain lipid binding protein expression in lamina-propria olfactory ensheathing cells is regulated by delta/notch-like epidermal growth factor-related receptor Westendorf, Kathryn A 05 1900 (has links) The olfactory system exhibits remarkable regenerative ability in it’s neuronal population. The success of continuous neurogenesis is thought to be due, at least in part, to its unique glia – olfactory ensheathing cells (OECs). OECs bear characteristics of both peripheral and central glia, and serve to ensheath, guide and promote growth of olfactory receptor neurons (ORNs) throughout both development and adult life. Brain lipid binding protein (BLBP) is most highly expressed by radial glia during embryonic development. It is largely down-regulated in the adult CNS, but BLBP expression is retained in the adult by special subpopulations of glia, including OECs. BLBP expression is induced in radial glia via Notch signaling, but it is not known if these same mechanisms regulate BLBP expression in the adult CNS. Axonal-glial signaling is a dynamic process whereby closely apposed neuronal and glial cells regulate the growth, maintenance and plasticity of one another through direct cell-cell signaling. Delta/Notch-like EGF-related receptor (DNER) is a transmembrane protein expressed by Purkinje cells which has been implicated in the regulation of BLBP in Bergmann glia during cerebellum development through Notch1 deltex-dependent non-canonical signaling. We have found that DNER is expressed in more mature ORNs, and other exclusive subpopulations of cells within the CNS. OECs in close apposition with DNER-expressing ORNs in vivo appear to maintain the highest BLBP expression found in the nervous system through development and adulthood. Immunofluorescence shows that this close relationship between BLBP expressing cells and DNER expressing cells also appears to be retained in specialized areas such as the hippocampus, retina and spinal cord, throughout mouse CNS development as well as in the mature system. Removing DNER or axonal input in vivo decreases the robustness of OEC BLBP expression, and the number of cells in OEC culture expressing BLBP decreases rapidly with time. OEC co-culture with a DNER expressing monolayer increases the number of OECs in vitro which express BLBP, providing evidence for the regulation of BLBP expression in OECs by DNER expression in apposing ORNs. Notch Olfactory Ensheathing Glia BLBP DNER
2	Brain lipid binding protein expression in lamina-propria olfactory ensheathing cells is regulated by delta/notch-like epidermal growth factor-related receptor Westendorf, Kathryn A 05 1900 (has links) The olfactory system exhibits remarkable regenerative ability in it’s neuronal population. The success of continuous neurogenesis is thought to be due, at least in part, to its unique glia – olfactory ensheathing cells (OECs). OECs bear characteristics of both peripheral and central glia, and serve to ensheath, guide and promote growth of olfactory receptor neurons (ORNs) throughout both development and adult life. Brain lipid binding protein (BLBP) is most highly expressed by radial glia during embryonic development. It is largely down-regulated in the adult CNS, but BLBP expression is retained in the adult by special subpopulations of glia, including OECs. BLBP expression is induced in radial glia via Notch signaling, but it is not known if these same mechanisms regulate BLBP expression in the adult CNS. Axonal-glial signaling is a dynamic process whereby closely apposed neuronal and glial cells regulate the growth, maintenance and plasticity of one another through direct cell-cell signaling. Delta/Notch-like EGF-related receptor (DNER) is a transmembrane protein expressed by Purkinje cells which has been implicated in the regulation of BLBP in Bergmann glia during cerebellum development through Notch1 deltex-dependent non-canonical signaling. We have found that DNER is expressed in more mature ORNs, and other exclusive subpopulations of cells within the CNS. OECs in close apposition with DNER-expressing ORNs in vivo appear to maintain the highest BLBP expression found in the nervous system through development and adulthood. Immunofluorescence shows that this close relationship between BLBP expressing cells and DNER expressing cells also appears to be retained in specialized areas such as the hippocampus, retina and spinal cord, throughout mouse CNS development as well as in the mature system. Removing DNER or axonal input in vivo decreases the robustness of OEC BLBP expression, and the number of cells in OEC culture expressing BLBP decreases rapidly with time. OEC co-culture with a DNER expressing monolayer increases the number of OECs in vitro which express BLBP, providing evidence for the regulation of BLBP expression in OECs by DNER expression in apposing ORNs. Notch Olfactory Ensheathing Glia BLBP DNER
3	Brain lipid binding protein expression in lamina-propria olfactory ensheathing cells is regulated by delta/notch-like epidermal growth factor-related receptor Westendorf, Kathryn A 05 1900 (has links) The olfactory system exhibits remarkable regenerative ability in it’s neuronal population. The success of continuous neurogenesis is thought to be due, at least in part, to its unique glia – olfactory ensheathing cells (OECs). OECs bear characteristics of both peripheral and central glia, and serve to ensheath, guide and promote growth of olfactory receptor neurons (ORNs) throughout both development and adult life. Brain lipid binding protein (BLBP) is most highly expressed by radial glia during embryonic development. It is largely down-regulated in the adult CNS, but BLBP expression is retained in the adult by special subpopulations of glia, including OECs. BLBP expression is induced in radial glia via Notch signaling, but it is not known if these same mechanisms regulate BLBP expression in the adult CNS. Axonal-glial signaling is a dynamic process whereby closely apposed neuronal and glial cells regulate the growth, maintenance and plasticity of one another through direct cell-cell signaling. Delta/Notch-like EGF-related receptor (DNER) is a transmembrane protein expressed by Purkinje cells which has been implicated in the regulation of BLBP in Bergmann glia during cerebellum development through Notch1 deltex-dependent non-canonical signaling. We have found that DNER is expressed in more mature ORNs, and other exclusive subpopulations of cells within the CNS. OECs in close apposition with DNER-expressing ORNs in vivo appear to maintain the highest BLBP expression found in the nervous system through development and adulthood. Immunofluorescence shows that this close relationship between BLBP expressing cells and DNER expressing cells also appears to be retained in specialized areas such as the hippocampus, retina and spinal cord, throughout mouse CNS development as well as in the mature system. Removing DNER or axonal input in vivo decreases the robustness of OEC BLBP expression, and the number of cells in OEC culture expressing BLBP decreases rapidly with time. OEC co-culture with a DNER expressing monolayer increases the number of OECs in vitro which express BLBP, providing evidence for the regulation of BLBP expression in OECs by DNER expression in apposing ORNs. / Medicine, Faculty of / Graduate Notch Olfactory Ensheathing Glia BLBP DNER
4	Caractérisation moléculaire du rôle de Lhx2 dans le développement de l'oeil et du cerveau Tétreault, Nicolas 12 1900 (has links) Le développement du système nerveux central (SNC) chez les vertébrés est un processus d'une extrême complexité qui nécessite une orchestration moléculaire très précise. Certains gènes exprimés très tôt lors du développement embryonnaire sont d'une importance capitale pour la formation du SNC. Parmi ces gènes, on retrouve le facteur de transcription à Lim homéodomaine Lhx2. Les embryons de souris mutants pour Lhx2 (Lhx2-/-) souffre d'une hypoplasie du cortex cérébral, sont anophtalmiques et ont un foie de volume réduit. Ces embryons mutants meurent in utero au jour embryonnaire 16 (e16) dû à une déficience en érythrocytes matures. L'objectif principal de cette thèse est de caractériser le rôle moléculaire de Lhx2 dans le développement des yeux et du cortex cérébral. Lhx2 fait partie des facteurs de transcription à homéodomaine exprimé dans la portion antérieure de la plaque neurale avec Rx, Pax6, Six3. Le développement de l'oeil débute par une évagination bilatérale de cette région. Nous démontrons que l'expression de Lhx2 est cruciale pour les premières étapes de la formation de l'oeil. En effet, en absence de Lhx2, l'expression de Rx, Six3 et Pax6 est retardée dans la plaque neurale antérieure. Au stade de la formation de la vésicule optique, l'absence de Lhx2 empêche l'activation de Six6 (un facteur de transcription également essentiel au développement de l'œil). Nous démontrons que Lhx2 et Pax6 coopèrent en s'associant au promoteur de Six6 afin de promouvoir sa trans-activation. Donc, Lhx2 est un gène essentiel pour la détermination de l'identité rétinienne au niveau de la plaque neurale. Plus tard, il collabore avec Pax6 pour établir l'identité rétinienne définitive et promouvoir la prolifération cellulaire. De plus, Lhx2 est fortement exprimé dans le télencéphale, région qui donnera naissance au cortex cérébral. L'absence de Lhx2 entraîne une diminution de la prolifération des cellules progénitrices neurales dans cette région à e12.5. Nous démontrons qu'en absence de Lhx2, les cellules progénitrices neurales (cellules de glie radiale) se différencient prématurément en cellules progénitrices intermédiaires et en neurones post-mitotiques. Ces phénotypes sont corrélés à une baisse d'activité de la voie Notch. En absence de Lhx2, DNER (un ligand atypique de la voie Notch) est fortement surexprimé dans le télencéphale. De plus, Lhx2 et des co-répresseurs s'associent à la chromatine de la région promotrice de DNER. Nous concluons que Lhx2 permet l'activation de la voie Notch dans le cortex cérébral en développement en inhibant la transcription de DNER, qui est un inhibiteur de la voie Notch dans ce contexte particulier. Lhx2 permet ainsi la maintenance et la prolifération des cellules progénitrices neurales. / Central nervous system (CNS) development in vertebrates is an extremely complex process that requires tight molecular control. Some very early expressed genes during embryonic development are of tremendous importance for CNS development. Among those, we find the LIM homeodomain protein Lhx2. Embryos that lack Lhx2 (Lhx2-/-) suffer from cerebral cortex hypoplasia, are anophtalmic and have smaller liver. The mutant embryos die in utero at embryonic day 16 (e16) due to a deficit in mature erythrocytes. The principal objective of this thesis was to characterize the molecular function of Lhx2 in eye and cerebral cortex development. Lhx2 is a part of the homeodomain transcription factors expressed in the anterior neural plate along with Rx, Pax6 and Six3. Eye development starts by a bilateral evagination of this region. We show here that Lhx2 expression is crucial for the first steps of eye formation. Indeed, in absence of Lhx2, Rx, Six3 and Pax6 expression is delayed in the anterior neural plate. At the optic vesicle stage, Lhx2 mutation precludes the initiation of Six6 expression (an homeodomain transcription factor essential for eye development). We demonstrate that Lhx2 and Pax6 bind to Six6 promoter and cooperate for its trans‐activation. So, Lhx2 is essential for retinal identity determination in the neural plate. Later on, it cooperates with Pax6 to establish definitive retinal identity and promote cell proliferation. Lhx2 is strongly express in the telencephalon, the embryonic region that will give rise to cerebral cortex. Lhx2 ablation causes a decrease in neural progenitor cells proliferation in this region. We show that the lack of Lhx2 causes a premature differentiation of the radial glia cells into intermediate progenitors and post‐mitotic neurons. These phenotypes correlate with a decrease activity of the Notch pathway. In Lhx2-/- telencephalon, the atypical Notch‐ligand DNER is strongly overexpressed. Furthermore, Lhx2 and co‐repressors associate at the DNER promoter region. We conclude that Lhx2 allows Notch pathway activation in the developing cerebral cortex. It does so by inhibiting DNER transcription, which is a Notch pathway repressor in this particular context. Thus, Lhx2 allows the maintenance and the proliferation of neural progenitor cells. Rétinogénèse Vésicule optique Télencephale Neurogénèse Voie Notch Retinogenesis Cellules souches/progenitrices neurales Neurogenesis Voie Notch Optic Vesicle DNER Neural stem cells/progenitors Pax6 Telencephalon Lhx2 Notch Pathway
5	Caractérisation moléculaire du rôle de Lhx2 dans le développement de l'oeil et du cerveau Tétreault, Nicolas 12 1900 (has links) Le développement du système nerveux central (SNC) chez les vertébrés est un processus d'une extrême complexité qui nécessite une orchestration moléculaire très précise. Certains gènes exprimés très tôt lors du développement embryonnaire sont d'une importance capitale pour la formation du SNC. Parmi ces gènes, on retrouve le facteur de transcription à Lim homéodomaine Lhx2. Les embryons de souris mutants pour Lhx2 (Lhx2-/-) souffre d'une hypoplasie du cortex cérébral, sont anophtalmiques et ont un foie de volume réduit. Ces embryons mutants meurent in utero au jour embryonnaire 16 (e16) dû à une déficience en érythrocytes matures. L'objectif principal de cette thèse est de caractériser le rôle moléculaire de Lhx2 dans le développement des yeux et du cortex cérébral. Lhx2 fait partie des facteurs de transcription à homéodomaine exprimé dans la portion antérieure de la plaque neurale avec Rx, Pax6, Six3. Le développement de l'oeil débute par une évagination bilatérale de cette région. Nous démontrons que l'expression de Lhx2 est cruciale pour les premières étapes de la formation de l'oeil. En effet, en absence de Lhx2, l'expression de Rx, Six3 et Pax6 est retardée dans la plaque neurale antérieure. Au stade de la formation de la vésicule optique, l'absence de Lhx2 empêche l'activation de Six6 (un facteur de transcription également essentiel au développement de l'œil). Nous démontrons que Lhx2 et Pax6 coopèrent en s'associant au promoteur de Six6 afin de promouvoir sa trans-activation. Donc, Lhx2 est un gène essentiel pour la détermination de l'identité rétinienne au niveau de la plaque neurale. Plus tard, il collabore avec Pax6 pour établir l'identité rétinienne définitive et promouvoir la prolifération cellulaire. De plus, Lhx2 est fortement exprimé dans le télencéphale, région qui donnera naissance au cortex cérébral. L'absence de Lhx2 entraîne une diminution de la prolifération des cellules progénitrices neurales dans cette région à e12.5. Nous démontrons qu'en absence de Lhx2, les cellules progénitrices neurales (cellules de glie radiale) se différencient prématurément en cellules progénitrices intermédiaires et en neurones post-mitotiques. Ces phénotypes sont corrélés à une baisse d'activité de la voie Notch. En absence de Lhx2, DNER (un ligand atypique de la voie Notch) est fortement surexprimé dans le télencéphale. De plus, Lhx2 et des co-répresseurs s'associent à la chromatine de la région promotrice de DNER. Nous concluons que Lhx2 permet l'activation de la voie Notch dans le cortex cérébral en développement en inhibant la transcription de DNER, qui est un inhibiteur de la voie Notch dans ce contexte particulier. Lhx2 permet ainsi la maintenance et la prolifération des cellules progénitrices neurales. / Central nervous system (CNS) development in vertebrates is an extremely complex process that requires tight molecular control. Some very early expressed genes during embryonic development are of tremendous importance for CNS development. Among those, we find the LIM homeodomain protein Lhx2. Embryos that lack Lhx2 (Lhx2-/-) suffer from cerebral cortex hypoplasia, are anophtalmic and have smaller liver. The mutant embryos die in utero at embryonic day 16 (e16) due to a deficit in mature erythrocytes. The principal objective of this thesis was to characterize the molecular function of Lhx2 in eye and cerebral cortex development. Lhx2 is a part of the homeodomain transcription factors expressed in the anterior neural plate along with Rx, Pax6 and Six3. Eye development starts by a bilateral evagination of this region. We show here that Lhx2 expression is crucial for the first steps of eye formation. Indeed, in absence of Lhx2, Rx, Six3 and Pax6 expression is delayed in the anterior neural plate. At the optic vesicle stage, Lhx2 mutation precludes the initiation of Six6 expression (an homeodomain transcription factor essential for eye development). We demonstrate that Lhx2 and Pax6 bind to Six6 promoter and cooperate for its trans‐activation. So, Lhx2 is essential for retinal identity determination in the neural plate. Later on, it cooperates with Pax6 to establish definitive retinal identity and promote cell proliferation. Lhx2 is strongly express in the telencephalon, the embryonic region that will give rise to cerebral cortex. Lhx2 ablation causes a decrease in neural progenitor cells proliferation in this region. We show that the lack of Lhx2 causes a premature differentiation of the radial glia cells into intermediate progenitors and post‐mitotic neurons. These phenotypes correlate with a decrease activity of the Notch pathway. In Lhx2-/- telencephalon, the atypical Notch‐ligand DNER is strongly overexpressed. Furthermore, Lhx2 and co‐repressors associate at the DNER promoter region. We conclude that Lhx2 allows Notch pathway activation in the developing cerebral cortex. It does so by inhibiting DNER transcription, which is a Notch pathway repressor in this particular context. Thus, Lhx2 allows the maintenance and the proliferation of neural progenitor cells. Rétinogénèse Vésicule optique Télencephale Neurogénèse Voie Notch Retinogenesis Cellules souches/progenitrices neurales Neurogenesis Voie Notch Optic Vesicle DNER Neural stem cells/progenitors Pax6 Telencephalon Lhx2 Notch Pathway
6	Análise comparativa de pavimentos dimensionados através dos métodos empírico do DNER e mecanístico e proposta de um catálogo simplificado de pavimentos para a região de Campo Grande (MS) / Comparative analysis of pavements designed by the empirical (DNER) and mechanistic methods and proposal of a simplified catalog of pavements for the area of Campo Grande (MS) Bezerra Neto, Rogerio Silveira 19 February 2004 (has links) Este estudo tem como objetivo principal comparar estruturas de pavimentos flexíveis projetadas através dos métodos empírico do DNER e mecanístico, considerando-se alguns materiais de pavimentação utilizados na região de Campo Grande, estado do Mato Grosso do Sul. Como objetivos decorrentes, pode-se destacar a obtenção das características resilientes e de fadiga destes materiais e a proposta de um catálogo simplificado de estruturas de pavimentos para a referida região. Para a efetivação da pesquisa, foram coletados materiais típicos do subleito da região e daqueles mais utilizados na composição de bases e capas dos pavimentos locais. Após as suas caracterizações, realizaram-se ensaios de compactação, CBR, triaxiais cíclicos e compressão diametral estática e dinâmica. As análises mecanísticas foram realizadas utilizando-se o programa computacional FEPAVE, que leva em conta o comportamento elástico não-linear dos materiais, considerando-se o critério de confiabilidade. A partir da análise comparativa dos métodos de dimensionamento, observou-se que, ora as estruturas estabelecidas pelo método mecanístico são idênticas às determinadas pelo método do DNER, ora são mais esbeltas, ora são menos esbeltas, dependendo do tipo de material que constitui as camadas e do nível de confiabilidade adotado. Verificou-se ainda que a caracterização dos materiais através dos ensaios de módulo de resiliência, vida de fadiga e deformação permanente é imprescindível quando se deseja projetar um pavimento empregando-se o método mecanístico. Por fim, elaborou-se um catálogo simplificado de pavimentos flexíveis para a região de Campo Grande MS, com as intenções de contemplar o uso de materiais locais e auxiliar os engenheiros na concepção de seus projetos / This study has as main objective to compare structures of flexible pavements designed by two different methods, the DNER empirical method and the mechanistic method, being considered some paving materials used in the area of Campo Grande, state of Mato Grosso do Sul. As secondary objectives, it can stand out the obtaining of the mechanical properties of these materials and the proposal of a simplified catalog of flexible pavements for the referred area. For the accomplishment of the research, typical materials of subgrade, base course and surface layer were collected. After their characterizations, tests of compaction, CBR and repeated load were executed. The mechanistic analyses were accomplished being used the software FEPAVE, that takes into account the non-linear resilient modulus of the materials, being considered the reliability criterion. Starting from the comparative analysis of the design methods, it was observed that the structures established by the mechanistic method can be identical, more slender or less slender to the ones obtained by the empirical method, depending on the type of the material that constitutes the layers and the reliability level adopted. It was also verified that the characterization of the materials by repeated load tests (resilient modulus, fatigues life and permanent deformation) is indispensable when one want to project a pavement being used the mechanistic method. Finally, a simplified catalog of flexible pavements was elaborated for the area of Campo Grande MS, with the intentions of to contemplate the use of local materials and to aid the engineers in the conception of their projects análise mecanística curva de fadiga design of pavements diametrical compression test dimensionamento de pavimentos empirical method ensaios de compressão diametral ensaios triaxiais cíclicos fatigue curve flexible pavements mechanistic method método do DNER método empírico método mecanístico módulo de resiliência pavimentação pavimentos flexíveis paving projeto de pavimentos repeated load triaxial test resilient modulus
7	Análise comparativa de pavimentos dimensionados através dos métodos empírico do DNER e mecanístico e proposta de um catálogo simplificado de pavimentos para a região de Campo Grande (MS) / Comparative analysis of pavements designed by the empirical (DNER) and mechanistic methods and proposal of a simplified catalog of pavements for the area of Campo Grande (MS) Rogerio Silveira Bezerra Neto 19 February 2004 (has links) Este estudo tem como objetivo principal comparar estruturas de pavimentos flexíveis projetadas através dos métodos empírico do DNER e mecanístico, considerando-se alguns materiais de pavimentação utilizados na região de Campo Grande, estado do Mato Grosso do Sul. Como objetivos decorrentes, pode-se destacar a obtenção das características resilientes e de fadiga destes materiais e a proposta de um catálogo simplificado de estruturas de pavimentos para a referida região. Para a efetivação da pesquisa, foram coletados materiais típicos do subleito da região e daqueles mais utilizados na composição de bases e capas dos pavimentos locais. Após as suas caracterizações, realizaram-se ensaios de compactação, CBR, triaxiais cíclicos e compressão diametral estática e dinâmica. As análises mecanísticas foram realizadas utilizando-se o programa computacional FEPAVE, que leva em conta o comportamento elástico não-linear dos materiais, considerando-se o critério de confiabilidade. A partir da análise comparativa dos métodos de dimensionamento, observou-se que, ora as estruturas estabelecidas pelo método mecanístico são idênticas às determinadas pelo método do DNER, ora são mais esbeltas, ora são menos esbeltas, dependendo do tipo de material que constitui as camadas e do nível de confiabilidade adotado. Verificou-se ainda que a caracterização dos materiais através dos ensaios de módulo de resiliência, vida de fadiga e deformação permanente é imprescindível quando se deseja projetar um pavimento empregando-se o método mecanístico. Por fim, elaborou-se um catálogo simplificado de pavimentos flexíveis para a região de Campo Grande MS, com as intenções de contemplar o uso de materiais locais e auxiliar os engenheiros na concepção de seus projetos / This study has as main objective to compare structures of flexible pavements designed by two different methods, the DNER empirical method and the mechanistic method, being considered some paving materials used in the area of Campo Grande, state of Mato Grosso do Sul. As secondary objectives, it can stand out the obtaining of the mechanical properties of these materials and the proposal of a simplified catalog of flexible pavements for the referred area. For the accomplishment of the research, typical materials of subgrade, base course and surface layer were collected. After their characterizations, tests of compaction, CBR and repeated load were executed. The mechanistic analyses were accomplished being used the software FEPAVE, that takes into account the non-linear resilient modulus of the materials, being considered the reliability criterion. Starting from the comparative analysis of the design methods, it was observed that the structures established by the mechanistic method can be identical, more slender or less slender to the ones obtained by the empirical method, depending on the type of the material that constitutes the layers and the reliability level adopted. It was also verified that the characterization of the materials by repeated load tests (resilient modulus, fatigues life and permanent deformation) is indispensable when one want to project a pavement being used the mechanistic method. Finally, a simplified catalog of flexible pavements was elaborated for the area of Campo Grande MS, with the intentions of to contemplate the use of local materials and to aid the engineers in the conception of their projects análise mecanística curva de fadiga dimensionamento de pavimentos ensaios de compressão diametral ensaios triaxiais cíclicos método do DNER método empírico método mecanístico módulo de resiliência pavimentação pavimentos flexíveis projeto de pavimentos design of pavements diametrical compression test empirical method fatigue curve flexible pavements mechanistic method paving repeated load triaxial test resilient modulus

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