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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
351

The role of microglia phenotypes in modulating CD4 + T cell responses

Ebner, Friederike 23 January 2014 (has links)
Die Invasion von Leukozyten in das zentrale Nervensystem (ZNS) ist ein wesentlicher Bestandteil bei der Pathogenese von Hirnverletzungen sowie akuten und chronischen Entzündungsvorgängen im Gehirn. Mikrogliazellen, die überwiegende Population immunkompetenter Zellen des ZNS, stellen die erste Verteidigungslinie im Hinblick auf Verletzungen und Erkrankungen des Gehirns dar. Im Rahmen vieler neurodegenerativer Erkrankungen wird die Zerstörung von Neuronen, aber auch die kollaterale Gewebsschädigung auf die Aktivierung der Mikrogliazellen zurückgeführt. Die vorliegende Arbeit beschreibt erstmalig einen regulatorischen Aktivierungszustand der Mikroglia (CD40dimCD86dimIL-10high), der zur Induktion regulatorischer Foxp3+ T-Zellen (Treg) führt. Die Stabilität und funktionelle Aktivität Mikroglia-induzierter Treg konnte sowohl in vitro als auch in vivo gezeigt werden. In vitro inhibierten sie die Proliferation antigen-spezifischer Effektorzellen, in vivo führte ein adoptiver Transfer der regulatorischen T-Zellen zur Abmilderung des Krankheitsverlaufes experimentell induzierter, autoimmuner Enzephalomyelitis (EAE). Mikrogliazellen unterstützten sowohl die Proliferation bereits ausgebildeter regulatorischer T-Zellen als auch deren Differenzierung aus naiven T-Zellen. Die Induktion regulatorischer T-Zellen durch Mikroglia war Major Histocompatibility Complex (MHC)-II-abhängig und antigenspezifisch. Für Untersuchungen zur in vivo Relevanz wurden MHC-II-chimäre Mäuse generiert und eine Läsion im entorhinalen Kortex gesetzt. Fehlte MHC-II in ZNS-residenten Zellen, wurden weniger regulatorische T-Zellen pro Leukozyt in die lädierten Hemispheren rekrutiert. Zusammenfassend demonstrieren diese Ergebnisse das Modulationspotential von Mikrogliazellen auf die CD4+ T-Zellantwort. Die Mikroglia-induzierte Differenzierung und Proliferation von Foxp3+ regulatorischen T-Zellen ist ein möglicher Mechanismus der Regulation von Entzündungsvorgängen im ZNS durch Mikrogliazellen. / The invasion of leukocytes into the central nervous system (CNS) is a key event in the pathogenesis of CNS injury and acute or chronic inflammatory neurological diseases. However, regulatory mechanisms of local innate immune responses that limit CNS inflammation are only poorly understood. Microglia are the predominant innate immune cells of the brain and present the first line of defence in CNS injury or disease. In the context of neurodegenerative disease, microglia activation accounts for collateral tissue damage and neurodestruction. This thesis for the first time describes a regulatory microglia phenotype (MHCII+CD40dimCD86dimIL-10high) that induced a strong Foxp3+ regulatory T cell (Treg) response. Microglia-induced Treg cells were stable and functionally active in vitro by inhibiting antigen-specific proliferation of effector T cells and in vivo, by attenuating experimental autoimmune encephalomyelitis (EAE) disease course after adoptive transfer. The data also suggested that regulatory microglia can mediate both, proliferation of Foxp3+ Treg cells and de novo differentiation from naive CD4+ T cells. Microglia-mediated Treg induction was proven to be MHCII and antigen-dependent. Using entorhinal cortex lesion (ECL) as a brain injury mouse model, diminished Foxp3+ Treg cell recruitment per infiltrated leukocyte in chimeric mice lacking MHCII specifically in the CNS was demonstrated, indicating in vivo relevance of antigen presentation by brain resident cells. Taken together, these findings demonstrate that microglial cells can directly modulate CD4+ T cell responses by regulating molecule levels for efficient antigen presentation and levels of secreted cytokines and chemokines. Microglia-mediated differentiation and proliferation of Foxp3+ Treg cells can be one of the mechanisms how microglia contribute to local immune homeostasis and limit CNS inflammation.
352

Tratamento com minociclina e transplante intraestriatal de células mononucleares da medula óssea após acidente vascular experimental encefálico

SILVA, Michelle Castro da 27 April 2011 (has links)
Submitted by Irvana Coutinho (irvana@ufpa.br) on 2012-10-25T14:35:53Z No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Dissertacao_TratamentoMinociclinaTransplante.pdf: 3658779 bytes, checksum: 28f17dbb304cfd0250e561d21b289b3c (MD5) / Approved for entry into archive by Ana Rosa Silva(arosa@ufpa.br) on 2012-10-25T15:06:37Z (GMT) No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Dissertacao_TratamentoMinociclinaTransplante.pdf: 3658779 bytes, checksum: 28f17dbb304cfd0250e561d21b289b3c (MD5) / Made available in DSpace on 2012-10-25T15:06:37Z (GMT). No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Dissertacao_TratamentoMinociclinaTransplante.pdf: 3658779 bytes, checksum: 28f17dbb304cfd0250e561d21b289b3c (MD5) Previous issue date: 2011 / CAPES - Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / CNPq - Conselho Nacional de Desenvolvimento Científico e Tecnológico / Diversos estudos sugerem que a tetraciciclina semi-sintética minociciclina e o transplante de células mononucleares da medula óssea (CMMOs) induzem neuroproteção em modelos experimentais de acidente vascular encefálico (AVENC). No entanto, poucos investigaram, comparativamente, os efeitos destas duas abordagens terapêuticas após AVENC induzido por microinjeções de endotelina – 1 (ET -1). Nesta dissertação, objetivou-se comparar os efeitos do bloqueio microglial com minociclina com os obtidos pelo transplante intraestriatal de CMMOs na fase aguda após acidente vascular encefálico experimental, sobre a área de lesão, neuroproteção, apoptose de recuperação funcional. Ratos machos adultos, da raça Wistar, pesando entre 250 e 350g, foram distribuídos em quatro grupos experimentais: controle (chamado de Salina) - isquêmico tratado com salina (N=4), isquêmico tratado com minociclina (N=4), isquêmico tratado com CMMOs (N=3) e doador de CMMOs (N=2). Testes comportamentais foram realizados em 1, 3 e 7 dias pós-isquemia para avaliar a recuperação funcional entre os grupos. Animais tratados com minociclina receberam 2 doses diárias de 50mg/kg nos 2 primeiros dias, e 5 aplicações únicas de 25mg/kg (i.p) nos dias subsequentes até o sexto dia após a indução isquêmica. 1x106 de CMMOs foram obtidas de ratos da mesma linhagem e transplantadas diretamente no estriato, 24h após a lesão isquêmica. Todos os animais foram perfundidos 7 dias após a indução isquêmica. Secções coronais foram coradas por violeta de cresila para análise histopatológica geral, e por imunohistoquímica para a identificação de corpos neuronais (neuN), microglia/macrófagos ativados (ED1) e células apoptóticas (Caspase-3). A análise histopatológica geral mostrou grande palor, perda tecidual e intensa ativação microglial/ macrofágica no estriato de animais tratados com solução salina estéril. O tratamento com CMMO foi mais eficaz do que a minociclina (P<0,05, ANOVA-Tukey) na redução do número de microglia/macrófagos ativados (salina 276,3 ± 9,3); CMMOs 133,8 ± 6,8) e minociclina 244,6 ± 7,1). CMMOs e minociclina reduziram a área de lesão, em 67,75% e 69,1%, respectivamente. Os dois tratamentos promoveram o mesmo nível de preservação neuronal (p< 0,05) em relação ao controle, 61,3 ± 1,5); 86,8 ± 3,4) e 81 ± 3,4). As CMMOs reduziram de forma mais eficaz (p<0,01) o número de células apoptóticas em relação à minociclina e grupo controle (26,5 ± 1,6); 13,1 ± 0,7) e 19,7 ± 1,1). Ambas as abordagens terapêuticas promoveram recuperação funcional dos animais isquêmicos. Os resultados sugerem que o tratamento com CMMOs é mais eficaz na modulação da resposta microglial e na diminuição da apoptose do que o tratamento com minociclina, apesar de ambos serem igualmente eficazes para indução da neuroproteção. Estudos futuros devem investigar se o tratamento com minociclina associado ao transplante de CMMOs produzem efeitos sinérgicos, o que poderia amplificar os níveis de neuroproteção observados. / Several studies suggest that both the semi-synthetic tetracycline minocycline and mononuclear bone marrow cell (BMMCs) transplantation induce neuroprotection in experimental models of stroke. However, a few studies comparatively investigated the effects of these therapeutic approaches following endothelin-1 (ET-1)-induced stroke. In this dissertation, we aimed at investigating the comparative effects of microglial inhibition with minocycline and BMMC transplantation in the acute phase of experimental stroke. Male adult Wistar rats were divided in four experimental groups: saline-treated (N=4), minocyclinetreated (N=4), BMMC-treated (N=4). Behavioral tests were performed at 1, 3 and 7 days post-ischemia to evaluate functional recovery between groups. Animals treated with minocycline received two 50mg/kg (i.p.) doses in the first two days plus five single 25mg/kg (i.p.) daily doses up to sixth days post-ischemia. 1x106 BMMCs were obtained from Wistar rats and directly transplanted into the striatum at 24h post-ischemia. Animals were perfused at 7 days after ischemia onset. Coronal sections were stained with cresyl violet for gross histopathological analysis and immunolabeled for identification of neuronal bodies (NeuN), activated microglia/macrophages (ED1) and apoptotic cells (active caspase-3). Gross histopathological analysis revealed pallor, tissue loss and intense microglial/macrophage activation in ischemic animals treated with sterile saline. BMMC transplantation induced a higher reduction (p<0.05, ANOVA-Tukey) in the number of ED1+ cells than (saline, 276, 3± 9,3;BMMCs, 133,8± 6,8; minocycline, 244,6 ± 7,1). BMMC transplantation and minocycline reduced the infarct area, compared to control, in about 67,75% and 69,1%, respectively, with no statistical differences between treatments (p>0.05). Both treatments afforded comparable levels (p>0.05) of neuronal preservation compared to control (61,3± 1,5; 86,8± 3,4; 81±3,4). BMMC treatment induce a higher decrease in the number of apoptotic cells compared to control and minocycline treatment (26,5± 1,6; 13,1± 0,7; 19,7± 1,1). Both therapeutic approaches improved functional recovery in the ischemic animals. The results suggest that BMMC transplantation is more effective in modulating microglial activation and reducing apoptic cell death than minocycline, although both treatments are equally efficacious on improving neuronal preservation. Future studies should investigate whether minocycline treatment concomitant with BMMC transplantation produces synergistic effects, which might improve neuroprotection.
353

Influência do tamanho da ninhada sobre o declínio cognitivo e a morfologia microglial da camada molecular do giro denteado em rattus novergicus

OLIVEIRA, Marcus Augusto de 11 October 2012 (has links)
Submitted by Edisangela Bastos (edisangela@ufpa.br) on 2013-02-14T20:42:43Z No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Dissertacao_InfluenciaTamanhoNinhada.pdf: 1712678 bytes, checksum: 20ff9d3d23dbf3106b406a77b22971f3 (MD5) / Approved for entry into archive by Ana Rosa Silva(arosa@ufpa.br) on 2013-02-15T13:14:23Z (GMT) No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Dissertacao_InfluenciaTamanhoNinhada.pdf: 1712678 bytes, checksum: 20ff9d3d23dbf3106b406a77b22971f3 (MD5) / Made available in DSpace on 2013-02-15T13:14:23Z (GMT). No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Dissertacao_InfluenciaTamanhoNinhada.pdf: 1712678 bytes, checksum: 20ff9d3d23dbf3106b406a77b22971f3 (MD5) Previous issue date: 2012 / Tem sido proposto que o envelhecimento está associado à alteração inflamatória no sistema nervoso central de roedores, mas não se sabe se as mudanças microgliais induzidas pelo envelhecimento são afetadas pelo ambiente pós-natal associado ao tamanho da ninhada. Por outro lado a camada molecular do giro denteado tem sido reconhecida como o alvo principal do input da via perfurante cuja integridade sináptica é essencial para formação de memória da identidade e da localização espacial de objetos. No presente trabalho investigamos se as mudanças morfológicas microgliais induzidas pelo envelhecimento são influenciadas por mudanças no tamanho da ninhada no início da vida. Para avaliar essas questões, ratos da variedade Wistar amamentados em ninhadas de 6 ou 12 filhotes por nutriz foram mantidos sedentários em grupos de 2-3 do 21o dia pós-natal em diante. Aos 4 (adulto) ou aos 23 (velho) meses de idade, os animais foram submetidos a testes de memória espacial e de reconhecimento da forma de objetos, sacrificados, perfundidos com fixador aldeídico e tiveram seus cérebros processados para imunomarcação seletiva para microglias/macrófagos com anticorpo anti Iba-1. A seguir uma fração representativa das células imunomarcadas da camada molecular do giro denteado foi reconstruída em três dimensões usando o programa Neurolucida e as características morfológicas de cada célula foram quantificadas com o software Neuroexplorer. Foi encontrado que os animais mantidos em gaiolas padrão de laboratório durante toda a vida apresentaram déficits de memória espacial independente da idade e não importando o tamanho da ninhada. Por outro lado todos os indivíduos idosos não importando o tamanho da ninhada tiveram sua memória de reconhecimento de objeto prejudicada. A análise da morfologia microglial revelou que a área e o perímetro do corpo celular e o volume dos ramos parecem ser afetados mais intensamente pelo envelhecimento e que essa alteração é mais acentuada nos animais de ninhada grande. Além disso, observou-se retração e espessamento dos ramos nos animais velhos em maior proporção nos animais de ninhadas grandes. Tomados em conjunto os resultados sugerem que a memória espacial parece ser mais suscetível ao processo de envelhecimento do que a memória de reconhecimento de objeto e que essas mudanças estão associadas a efeitos distintos sobre o soma e o padrão de ramificação das microglias da camada molecular dos animais maduros e idosos. / It has been proposed that aging is associated with neuroinflammation in the central nervous system but it is not known whether microglial changes induced by aging are affected by early in life effects of litter size. On the other hand the molecular layer of dentate gyrus has been recognized as the main target of the perforant pathway, whose synaptic integrity is essential for the recognition memories of identity and spatial location. In the present report we investigated if aging cognitive decline and microglial morphological changes in the molecular layer are influenced by litter size changes early in life and aging. To assess these questions Wistar rats suckled in litters of six or 12 pups/mother were raised sedentarily in groups of 2-3 from the 21st post-natal day onwards. At four (mature adult) or 23 (aged) months of age were submitted to spatial memory and object identity recognition tests, sacrificed, perfused with aldehyde fixatives and had their brains processed for selective microglia/macrophages immunolabeling with anti-IBA-1 antibodies. A representative sample of the immunolabeled cells in the molecular layer of dentate gyrus was analyzed after three-dimensional reconstruction with Neurolucida software (Microbright Field Inc.) and morphological features of each cell were quantified by Neuroexplorer (Microbright Field Inc.). It was found that Wistar rats maintained all life in standard laboratory cages showed spatial memory deficits in both mature and aged subjects no matter the litter size. On the other hand all aged subjects independent of the litter size had their object recognition identity memory impaired. Microglial morphological analysis revealed that cell soma area and perimeter and branches volume seem to be more intensely affected by aging and that these changes are mainly associated with animals from large litters. In addition it was observed important shrinkage and thickening of the microglial branches in aged individuals in higher proportion in the group from large litters. Taken together the results suggest that spatial memory seems to be more susceptible to the aging process than object recognition and that these changes are associated with distinct effects on the soma and branching patterns of microglia of molecular layer from young and aged subjects.
354

Influências do tamanho da ninhada e da atividade física sobre a plasticidade glial na formação hipocampal em modelo murino

VIANA, Lane Coelho 07 February 2014 (has links)
Submitted by Cleide Dantas (cleidedantas@ufpa.br) on 2014-06-26T12:59:21Z No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Tese_InfluenciasTamanhoNinhada.pdf: 7061769 bytes, checksum: c700c3851bd6127e32c00a9484622ce9 (MD5) / Approved for entry into archive by Ana Rosa Silva (arosa@ufpa.br) on 2014-07-30T13:47:39Z (GMT) No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Tese_InfluenciasTamanhoNinhada.pdf: 7061769 bytes, checksum: c700c3851bd6127e32c00a9484622ce9 (MD5) / Made available in DSpace on 2014-07-30T13:47:39Z (GMT). No. of bitstreams: 2 license_rdf: 23898 bytes, checksum: e363e809996cf46ada20da1accfcd9c7 (MD5) Tese_InfluenciasTamanhoNinhada.pdf: 7061769 bytes, checksum: c700c3851bd6127e32c00a9484622ce9 (MD5) Previous issue date: 2014 / CNPq - Conselho Nacional de Desenvolvimento Científico e Tecnológico / Estudos anteriores demonstraram efeitos importantes do estresse perinatal no desempenho cognitivo na vida adulta e durante o envelhecimento. Entretanto permanece por ser estudado em detalhe como o exercício físico em diferentes fases da vida contribui para reduzir esses déficits. Isso é particularmente verdadeiro quando se trata de documentar as alterações da matriz extracelular e das células da glia, largamente ignoradas nesses estudos. Assim o objetivo geral do presente trabalho é o de investigar as possíveis influências do tamanho da ninhada e da atividade física sobre a memória de reconhecimento de objetos na vida adulta e possíveis alterações associadas à plasticidade glial e da matriz extracelular da formação hipocampal em modelo murino. Para alcançar esses objetivos alteramos o tamanho da ninhada de ratos Wistar de modo a acentuar o grau de competição entre os filhotes por tetas funcionais e diminuir a quantidade de cuidado materno por indivíduo. Durante o período de aleitamento quantificamos o cuidado materno em ninhadas de diferentes tamanhos. Em várias janelas temporais submetemos grupos selecionados de sujeitos ao exercício em esteira durante 5 semanas adotando o mesmo protocolo de treinamento. Após o exercício alguns grupos de animais adultos e senis foram submetidos ao teste de memória de reconhecimento de objetos que é dependente do hipocampo, sendo sacrificados e processados para imunohistoquímica seletiva para micróglia. Outros grupos de animais adultos não submetidos aos testes comportamentais foram igualmente sacrificados sendo um dos hemisférios empregado para registro de parâmetros difusionais no hipocampo enquanto que o outro foi empregado para imunohistoquímicas seletivas para astrócitos, células NG2 e reelina. Encontramos que o aumento do tamanho da ninhada está relacionado à redução do cuidado materno, ao declínio cognitivo, à proliferação e alteração da morfologia microglial, astrocitária e de células NG2 positivas, assim como às alterações nos padrões de difusão encontradas no tecido hipocampal. Além disso que tais alterações podem ser revertidas pelo menos de forma parcial pela atividade física e que esse efeito é tanto maior quanto mais jovem é o sujeito. O envelhecimento agrava as alterações morfológicas microgliais induzidas pelo aumento do tamanho da ninhada e reduz o desempenho nos testes de memória de reconhecimento de objeto. Os mecanismos moleculares associados a esses efeitos permanecem por ser investigados. / Previous studies have shown significant effects of perinatal stress on cognitive performance in adulthood and during aging. However remains to be studied in detail as exercise at different stages of life helps to reduce these deficits. This is particularly true if we consider previous descriptions of extracellular matrix and glial cell changes, largely ignored in these studies. Thus, the aim of the present report is to investigate possible influences of litter size and physical activity on object recognition memory at adulthood and whether or not these influences affect glial plasticity and extracellular matrix of the hippocampal formation. To that end, we changed the litter size of Wistar rats to accentuate the degree of competition among siblings by functional teats and decrease the amount of maternal care per individual. During the suckling period, we have quantified the maternal care in litters of different sizes. At various time windows we submitted selected subjects to physical exercise on a treadmill, for 5 weeks, adopting the same training protocol. After exercise, some groups of adults and senile animals were submitted to the hippocampal-dependent object recognition memory test, sacrificed, and processed for selective microglia immunolabeling. Other groups of adult animals not subjected to behavioral tests were also euthanized and had one hemisphere used to record diffusional parameters in the hippocampal parenchyma while the other was used for selective immunolabeling to detect astrocytes, NG2 cells and reelin.We found that an increase in litter size was related to the reduction of maternal care, cognitive decline, altered morphology and proliferation of microglia, astrocytes and NG2 cells, as well as to a change in diffusion patterns in the hippocampal stroma. We also demonstrated that these changes may be reversed, at least partially, by physical activity and the extent of these beneficial effects are more pronounced in younger subjects. Finally, we demonstrated that ageing exacerbates microglial morphological changes induced by increased litter size and reduces memory performance.The molecular mechanisms associated to these effects remain to be investigated.
355

Cinética da infecção pelo arbovírus piry em modelo murino: a resposta do hospedeiro adulto

SANTOS, Zaire Alves dos 30 September 2011 (has links)
Submitted by Hellen Luz (hellencrisluz@gmail.com) on 2017-09-22T16:45:37Z No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Dissertacao_CineticaInfeccaoArbovirus.pdf: 1663059 bytes, checksum: 7d2fa792bd8036013ffb7d0bf979223a (MD5) / Rejected by Edisangela Bastos (edisangela@ufpa.br), reason: on 2017-10-10T17:01:00Z (GMT) / Submitted by Hellen Luz (hellencrisluz@gmail.com) on 2017-10-17T18:43:06Z No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Dissertacao_CineticaInfeccaoArbovirus.pdf: 1663059 bytes, checksum: 7d2fa792bd8036013ffb7d0bf979223a (MD5) / Approved for entry into archive by Edisangela Bastos (edisangela@ufpa.br) on 2017-11-24T15:23:33Z (GMT) No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Dissertacao_CineticaInfeccaoArbovirus.pdf: 1663059 bytes, checksum: 7d2fa792bd8036013ffb7d0bf979223a (MD5) / Made available in DSpace on 2017-11-24T15:23:33Z (GMT). No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Dissertacao_CineticaInfeccaoArbovirus.pdf: 1663059 bytes, checksum: 7d2fa792bd8036013ffb7d0bf979223a (MD5) Previous issue date: 2011-09-30 / CAPES - Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / No presente estudo, um membro do grupo das RNA viroses Sul Americanas encontrado no Brasil, que causa doença febril em humanos e encefalite em camundongos adultos e neonatos, foi selecionado como um modelo para estudar as consequências das encefalites por arbovírus. Em camundongos mantidos em condições padronizadas com acesso livre a água e comida, induziu-se encefalite por via intranasal empregando homogenado cerebral infectado pelo vírus Piry, correlacionando a resposta inflamatória celular quantitativa do hospedeiro na região septal, com os sinais clínicos e a neuroinvasão, utilizando como controle animais que receberam homogenado cerebral não infectado. Animais com três meses de idade receberam volume igual de homogenado cerebral infectante ou de homogenado cerebral normal nas narinas. Em cada um dos oito dias após a infecção, cinco sujeitos da colônia infectada foram sacrificados, perfundidos e processados para detecção dos antígenos virais e microglia. Sujeitos controle foram sacrificados no 5º dia após a inoculação do homogenado cerebral normal para os mesmos marcadores. A encefalite viral induziu ativação microglial e neuroinvasão das células gliais e neurônios, principalmente nas vias olfatórias nas fases iniciais (2 - 4 dpi), mas também incluiu o hipocampo, o cerebelo e núcleos do tronco cerebral mais tarde (5 - 8 dpi). A correlação das estimativas do número de microglias na área septal com os sinais clínicos e a neuroinvasão revelaram que o número e a morfologia daquelas mudou antes da neuroinvasão ter alcançado a região septal e os sinais clínicos aparecerem. Grande variabilidade na intensidade dos sintomas clínicos e na taxa de sobrevivência foi encontrada na variedade de camundongos albinos suíços quando comparados com o previamente descrito na variedade C57Bl6 sugerindo um background genético mais heterogêneo para aquela variedade. Tomados em conjunto nossos resultados prévios e atuais dedicados a investigar a progressão da encefalite induzida pelo vírus Piry no camundongo albino suiço pode abrir um novo campo de investigação das bases genéticas, anatômicas e imunes acerca das encefalites sub-letais tropicais. / In the present report, a member of a group of RNA South American viruses found in Brazil, that causes febrile disease in humans and encephalitis in neonate and adult murine models, was selected as a model to study encephalitis outcomes in adult albino Swiss mice. In mice housed under standard conditions with free access to water and food, we induced viral encephalitis by intranasal inoculation of Piry virus–infected brain homogenate and correlated neuropathological features. We quantified the cellular inflammatory response in the septal region using a stereologically based unbiased method with clinical signs and neuroinvasion, comparing the outcomes with those of animals inoculated with uninfected brain homogenate. Three-month-old female mice maintained in standard environment received an equal volume of Piry virus infected or normal brain homogenates into the nostrils. From the 1st to 8th days post-instillation (dpi), five subjects from the infected colony were fixed and processed to detect viral antigens and microglia. Control subjects were sacrificed in the 5th dpi and processed for the same markers. After Piry virus encephalitis induced microglial activation and neuroinvasion of glial cells and neurons mainly in the olfactory pathways early in the disease (2 – 4 dpi), but also included hippocampus, cerebellum and brain stem nuclei later on (5 - 8 dpi). The correlation of the host cellular inflammatory quantitative response in the septal area with clinical signs and neuroinvasion, revealed that the number and the morphology of microglias changed early in the disease before neuroinvasion had reached the septal region and clinical signs had appeared. Great variability in clinical symptoms intensity and survival rate were found in the outbred albino Swiss mice strain as compared with previous report in the inbred C57Bl6 strain suggesting less isogenic background. Taken together, our previous and present report dedicated to investigate Piry virus encephalitis progression in the outbred albino Swiss mice strain may open a new field of investigation of the genetics, anatomical and immune substrates of tropical sublethal arbovirus encepahlitis.
356

Imagerie moléculaire de la neuroinflammation dans la maladie de Parkinson : étude préclinique dans un modèle animal de rat

Maia, Serge 16 November 2012 (has links)
Bien que les mécanismes moléculaires précis à l’origine de la neurodégénérescence dopaminergique ne soient pas encore totalement connus, un ensemble de preuves épidémiologiques, cliniques et expérimentales indiquent que la neuroinflammation peut avoir un rôle important dans la pathogenèse de la MP. L’étude des liens spatio-temporels entre la neuroinflammation et la neurodégénérescence au cours de la MP pourrait améliorer la compréhension du mécanisme physiopathologique et aussi l'accessibilité à un diagnostic précoce et/ou à de nouvelles approches thérapeutiques anti-inflammatoires. Le développement actuel des méthodes non invasives d'imagerie moléculaire permettant la surveillance directe du processus de neuroinflammation devrait être utile à cet effet. La cible moléculaire de choix dans ce domaine est la protéine de 18 kDa translocateur (TSPO), biomarqueur sensible associée à la neuroinflammation, qui est surexprimé dans les microglies activées. Dans le travail présenté ici nous avons réalisé l'évaluation longitudinale des deux mécanismes physiopathologiques en parallèle avec les modifications de la fonction dopaminergique à plusieurs points au cours du temps après lésion à la 6-OHDA chez le rat, modèle qui imite un stade précoce de la MP. Après l'administration unilatérale, intra-striatale de la 6-OHDA, nous avons quantifié l'évolution temporelle de la TSPO, de l’immunoréactivité TH et du DAT dans le striatum et la SNC de 3 à 56 jours post-lésion (jpl). L’augmentation de la liaison des ligands de la TSPO utilisés, c-à-d [3H]-PK11195 et [125I]-CLINDE, a été observée dans le striatum lésé à 3, 7 et 14 jpl, suivie d'un retour progressif à un niveau basal à 56 jpl. Le profil de liaison dans la SNC a montré une augmentation progressive de la fixation qui débute à 3 jpl, avec un pic à 14 jpl, et diminue progressivement jusqu'à ce que 56 jpl. Dans ce modèle de rongeur de la MP, les processus neuroinflammatoire et neurodégénératif surviennent de façon concomitante. La présence transitoire de l'activation microgliale pourrait être impliquée dans l’apparition et l'installation durable de la perte neuronale dopaminergique. Cette étude confirme donc le lien entre la neuroinflammation et de la neurodégénérescence et met aussi l'accent sur l'intérêt du CLINDE comme traceur potentiel de la neuroinflammation in-vivo en fournissant des informations précieuses pour le diagnostic précoce et le suivi longitudinal de la progression de la maladie, avec des applications potentielles chez l'homme. En effet, la détection précoce de la neuroinflammation, de façon antérieure à une perte neuronale cliniquement significative, pourrait devenir un enjeu majeur dans la prise en charge pré-symptomatique de la MP. Dans ce sens, nous mettons en évidence l’existence d'une fenêtre thérapeutique, survenant juste après la lésion, qui peut être proposé pour l'introduction de traitements anti-inflammatoires qui viseraient à ralentir le processus neurodégénératif. La poursuite de l’exploration des relations entre la neuroinflammation et la neurodégénéréscence in-vivo dans le même modèle animal avec la méthode d’imagerie micro-TEP, transposable à l’homme, en utilisant en parallèle le [18F]-DPA714 pour la TSPO et le [18F]-LBT999 pour le DAT est en cours. / Although the precise molecular mechanisms causing the dopaminergic neurodegeneration are still not totally understood, a body of epidemiological, clinical and experimental evidence indicates that neuroinflammation may have an important role in the pathogenesis of PD. Study of spatio-temporal links between neuroinflammation and neurodegeneration during the course of PD would improve understanding of the physiopathological mechanism and also accessibility to early diagnosis and/or new antiinflammatory therapeutic approaches. The current development of non-invasive molecular imaging methods allowing direct monitoring of the neuroinflammation process should be valuable for this purpose. The molecular target of choice in this field is the 18 kDa translocator protein (TSPO), a sensitive biomarker associated with neuroinflammation, which is over-expressed in activated microglia. In the study presented here we achieved the longitudinal evaluation of both physiopayhological mechanisms in parallel with the modifications of dopaminergic function at several time-points after 6-OHDA lesion in the rat that mimics an early stage of PD. After unilateral intra-striatal 6-OHDA administration, we quantified the temporal evolution of the TSPO, TH immunoreactivity and DAT in the striatum and the SNc from 3 to 56 days post-lesion (dpl). Increased binding of TSPO ligands used, i.e. [3H]PK11195 and [125I]CLINDE, was observed in the lesioned striatum at 3, 7 and 14 dpl, followed by a progressive return to the basal level at 56 dpl. The binding profile in the SNc showed progressive binding beginning at 3 dpl, peaking at 14 dpl, and progressively decreasing until 56 dpl. In this rodent model of PD, the neuroinflammatory and neurodegenerative processes occurred concomitantly. The transitory occurrence of microglial activation could be involved in the advent and the lasting installation of dopaminergic neuron loss. This study supports the link between neuroinflammation and neurodegeneration and emphasizes the interest of CLINDE as potent in vivo tracer of neuroinflammation by providing valuable information for early diagnosis and longitudinal follow-up of disease progression, with potential applications to human patients. Indeed, early detection of neuroinflammation, prior to a clinically significant loss of neurons, could become a major issue in the management of pre-symptomatic PD. To support this idea, we demonstrate the existence of a therapeutic window, occurring just after the lesion, which may be proposed for the introduction of anti-inflammatory treatments that aimed to slow the neurodegenerative process. Further exploration of the relationship between neuroinflammation and neurodegeneration in vivo in the same animal model with the method of micro-PET imaging, transposable to humans, using in parallel the [18F]-DPA714 for TSPO and [18F]-LBT999 for DAT is pending.
357

Mecanismes moleculars implicats en la secreció de pèptids en cèl•lules glials del sistema nerviós central

Paco Mercader, Sonia 23 November 2011 (has links)
En els últims anys, diversos treballs han demostrat que els astròcits participen activament en el desenvolupament i la plasticitat del sistema nerviós central, així com en la modulació de la neurotransmissió. Característicament, la majoria de les accions descrites dels astròcits sobre la fisiologia i la patologia neuronal són mitjançades per secreció vesicular. En el aquest treball s’han identificat les molècules implicades en l’exocitosi de cèl•lules astroglials. Malgrat que alguns components són comuns amb les neurones, altres com sintaxina 4, VAMP3 i SNAP23 s’expressen de forma específica en les cèl•lules astroglials. Tractaments activadors o de maduració diferencialment regulen l’expressió de diferents isoformes de proteïnes exocítiques en cèl•lules glials in vitro. Així, l’activació amb citocines proinflamatòries augmenta l’expressió d’algunes SNAREs i els seus reguladors en glia, com sintaxina4 i munc18b. La correlació entre els nivells d’expressió d’aquestes proteïnes exocítiques i l’augment de la secreció de mediadors d’activació i inflamació suggereix un important paper d’aquestes molècules en la secreció de cèl•lules activades. Amb l’objectiu d’estudiar la secreció regulada per calci en astròcits madurs s’ha obtingut un fenotip madur glial in vitro mitjançant l’activació de la via del AMPc. L’anàlisi global amb "gene set enrichment analysis" del transcriptoma astrocitari ha demostrat que l’increment en els nivells intracel•lulars d’AMPc reprimeix la immaduresa i activació dels astròcits i promou la seva maduració. Aquesta maduració dependent de la via del AMPc augmenta l’expressió de proteïnes exocítiques, com per exemple VAMP2, així com la via de secreció regulada per calci dels pèptids ANP i SgII. Finalment, mitjançant assajos de pèrdua de funció, es demostra un paper d’aquestes proteïnes en la secreció de pèptids glials. Aquests resultats suggereixen que diferents molècules d’exocitosi mitjancen diferents processos de secreció glials. Per altra banda, en aquesta tesi s’ha identificat un nou component de la via de secreció astroglial, tant in vitro com in vivo, la SgIII. En cèl•lules neuroendocrines SgIII actua com un receptor de direccionament a grànuls secretors. En cèl•lules astroglials SgIII presenta una forma molecular i una dinàmica de secreció diferencial a cèl•lules neuroendocrines. A més, hem demostrat una notable sobreexpressió d’aquesta proteïna en astròcits reactius en lesions traumàtiques, la qual cosa suggereix una participació de SgIII en els mecanismes de protecció o dany cerebral en lesions del sistema nerviós central. / In recent years, several studies have demonstrated that astrocytes influences neuronal development, function and plasticity through vesicular transmitter release. However, secretory pathways and the involved molecular mechanisms in astroglial cells are poorly known. In this study, we showed that a variety of SNARE and Munc18 isoforms were expressed by cultured astrocytes, with syntaxin-4, Munc18c, SNAP-23 and VAMP-3 being the most abundant variants. Exocytotic protein expression was differentially regulated by activating and differentiating agents. Specifically, proteins controlling Ca2+-dependent secretion in neuroendocrine cells were up-regulated after long-term 8Br-cAMP administration in astrocytes, but not by proinflammatory cytokines. We also analyzed the global transcriptome of cultured astroglial cells incubated with activators of cAMP pathways. cAMP analogs strongly upregulated genes involved in typical functions of mature astrocytes, whereas they downregulated a considerable number of proliferating and immaturity-related transcripts. Gene Set Enrichment Analysis and evaluation in situ of gene expression in astrocytes in different states showed that cAMP signaling conferred a mature and in vivo–like transcriptional profile to cultured astrocytes. Moreover, 8Br-cAMP treatment greatly increased the cellular content of exocytotic proteins such as VAMP-2 and stimulated Ca2+-dependent secretion of secretogranin-2 and ANP. Regulation of both exocytotic protein expression and Ca2+-dependent peptide secretion in astrocytes by differentiating and activating agents suggested that glial secretory pathways were adjusted in different physiological states. In this thesis, we showed the expression, transcriptional regulation, trafficking and release of the secretory pathway component SgIII in astroglial cells. In endocrine cells, SgIII is a key sorting receptor for peptide hormones while astrocytes produced and released a non-processed form. Moreover, SgIII expression was specifically upregulated in reactive astrocytes after perforating brain injury. These results showed that SgIII is a reliable component of the astrocyte secretory pathway and suggest important roles for glial SgIII in the glia–neuron communication.
358

Evaluation of the cuprizone model / Einschätzung des Cuprizone-Modells

Awn, Najmy 25 March 2010 (has links)
No description available.
359

Plaque deposition and microglia response under the influence of hypoxia in a murine model of Alzheimer\'s disease

Viehweger, Adrian 03 January 2014 (has links) (PDF)
Clinical findings have linked multiple risk factors and associated pathologies to Alzheimer\'s disease (AD). Amongst them are vascular risk factors such as hypertension and pathologies such as stroke. Coexistence of AD and these associated pathologies worsenes dementia, the clinical hallmark of the disease, as compared to pure AD. One general common denominator of these associated pathologies is the presence of hypoxic tissue conditions. It was asked the question, whether there exists a mutual, causal interaction between hypoxia and AD pathology, that could explain the clinical observations. Alternatively, the worsened clinical state of multiple brain pathologies could \"simply\" be the consequence of multimorbidity, i.e. accumulated disease load, without any causal interaction between the constituents. To approach this question whether hypoxia influences AD progression, use was made of a murine animal model of AD (transgenic mice: APPswe, PSEN1dE). Animals of two ages (8 and 14 months, \"young\" and \"old\" respectively) and two genotypes (transgenic and wild- type) were either treated under hypoxia or normoxia, corresponding to 8% and 21% oxygen, for 20 consecutive days. The resulting changes in the brain were assessed with a variety of techniques, namely by histology, ELISA, dot and Western blotting. Additional experiments in primary cell cultures were performed. Animals exposed to hypoxia showed an increased hematocrit (HCT), weight loss, reactive angiogenesis, but no infarctions. This illustrates that our hypoxic treatment put significant stress on the animals, without causing major pathologies. A large number of variables exists that could potentially be measured to assess the effect of hypoxia on AD. The focus was put on three of them: First, there is the Abeta1-42- protein, known to be the Abeta- isoform associated with the most detrimental disease progression. In AD, the self-combinatory Amyloid- beta peptide (Abeta) accumulates in the brain in so- called plaques, which is a main histologic finding of the disease. Its quantity was determined through histology and ELISA. Secondly, it was attempted to estimate the structural quality of the Abeta- protein by assessing the amount of A!- oligomers present. Abeta- protein does self- accumulate in various grades of complexity, i.e. as monomer, oligomer or fibril. Since oligomers are known to be the most neurotoxic \"species\" of the Abeta- protein, it was hypothesized that under hypoxic treatment their quantity could increase. And third, the organism\'s response to the Abeta- protein stimulus was investigated. Microglial cells have been described as the first cells to encounter the Abeta- protein \"threat\" in the shape of plaques, i.e. Abeta- protein aggregates. They then try to encapsulate and subsequently degrade them. Therefore, the attention was put on this cellular population. It was asked whether hypoxia could change the Abeta- protein quantity in the brain. This was assessed in two ways: First histologically, by staining for Abeta- protein depositions and quantifying them. Second, an ELISA was performed. Our findings state that hypoxic treatment does not alter the Abeta1-42 protein load in the brain, neither in young nor old animals, as assessed by histology and by total ELISA quantification of Abeta1-42 protein. Since hypoxia did not alter the quantity of the Abeta- protein, it was asked whether it influenced it qualitatively? If hypoxia increased oligomer formation, this change in the spectrum of the Abeta- species could, without any change in total Abeta- protein load, lead to increased neurotoxicity in animals under hypoxia. Initial experiments showed that oligomer formation in the brain seems to increase. However, this was not statistically significant and future experiments are necessary to evaluate this hypothesis further. It was then asked, whether hypoxia alters the cellular response to the protein. The total number of microglia in the hippocampal dentate gyrus, our structure of interest for practical purposes, and, it can be argued, by extension the brain, changes dynamically with various factors. First, transgenic animals present an increase in microglia. Second, microglia increase with age. Third, microglia decrease under hypoxia, but only do so significantly in old animals. Next, a parameter called \"plaque occupancy\" was coined to assess the microglia function to confront Abeta- plaques. Plaque occupancy is defined as the number of microglia in spatial proximity to one square millimeter of Abeta- plaque. This means, that microglia restricting one plaque are counted, and then normalized to this plaque\'s area. It was hypothesized that hypoxia would decrease plaque occupancy. Indeed, plaque occupancy roughly halved under hypoxia. Summarizing, our results demonstrate that long- term exposure to hypoxia significantly reduces the number of microglia. The reduced number results in significantly reduced plaque occupancy and compromizes the function of microglia to confront Abeta- plaques. The Abeta1-42 load, however, is not affected. On the other hand, Abeta shows an increased trend towards oligomer formation. A variety of possible explanations to these phenomena have been presented, that in our opinion deserve further investigation.
360

Activation of murine microglial cells by muramyl dipeptide alone and in combination with Toll-like receptor agonists

Adam, Nina 01 October 2014 (has links)
No description available.

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