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Estudo dos efeitos da MT3 na plasticidade sináptica de longa duração e interações com a sinalização gabaérgica em hipocampo dorsal pela eletrofisiologia in vivo em animal anestesiadoZanona, Querusche Klippel January 2015 (has links)
A sinalização muscarínica exerce função modulatória sobre diferentes aspectos da cognição e emoções. Todos os cinco subtipos de receptores muscarínicos (mAChR), M1 a M5, são expressos no hipocampo de mamíferos e são ativados de forma sobreposta pela maioria dos fármacos, dificultando avanços significativos na compreensão da contribuição de cada componente desse sistema. A toxina muscarínica 3 (MT3) é um antagonista seletivo para o subtipo M4, permitindo a investigação das ações modulatórias deste receptor no aprendizado, memória e plasticidade sináptica. Os M4 são receptores acoplados à proteína G (GPCRs) que atuam via Gi/o desencadeando efeitos inibitórios sobre as células em que estão presentes. Estudos comportamentais anteriores indicam que a administração de MT3 imediatamente após o treino em uma tarefa aversiva produz efeito amnéstico, enquanto que a administração antes da evocação, causa facilitação. Uma explicação para estes resultados é que os circuitos locais envolvidos na consolidação e na evocação da memória diferem em sua natureza. Nesse contexto, sugere-se que o efeito amnéstico da MT3 sobre a consolidação seja consequência da supressão da inibição de interneurônios GABAérgicos; enquanto que na evocação, esse efeito se daria sobre as sinapses glutamatérgicas. Assim, no presente trabalho, com o objetivo de investigar como o receptor M4 modula a plasticidade sináptica de longa duração e interage com uma dessas sinalizações, no caso a GABAérgica, utilizou-se a técnica de eletrofisiologia in vivo de hipocampo de ratos anestesiados. Para tanto, foram realizados registros extracelulares do potencial excitatório pós-sináptico de campo (fEPSP) de CA1 evocados por estimulação contralateral da via Colateral de Schaffer com infusão dos fármacos 15 min antes ou depois da estimulação elétrica de alta ou baixa frequência (HFS: 10 trens 0,5 Hz, 20 pulsos 100 Hz; ou LFS: 600 pulsos 1 Hz, respectivamente). MT3 (4,0 μg/μl), bicuculina (0,06 μg/μl), baclofen (0,2 μg/μl) e veículo, isoladamente ou combinados, não alteraram a amplitude da resposta evocada basal ou a facilitação por pulso pareado (FPP) 15 min após a infusão. MT3 aparentemente atenuou, mas não de forma significativa, a potenciação de longa duração (LTP) em relação ao controle (potenciação 60 min após a HFS de 31,8% e 66,0%, respectivamente). Além disso, não houve diferença significativa entre a amplitude do fEPSP no período basal e 60 min após a HFS sob ação da MT3. Bicuculina, embora não tenha abolido a LTP e nem causado alteração na FPP, produziu uma potenciação de apenas 36,4%. Baclofen promoveu uma potenciação semelhante à dos controles. A administração de baclofen também reduziu significativamente a FPP em relação ao basal. A administração conjunta de MT3 com bicuculina ou baclofen promoveu uma potenciação semelhante ao controle. MT3 não apresentou efeito sobre a manutenção da LTP quando aplicada 15 min após a HFS. Por fim, não foi possível induzir a depressão de longa duração (LTD) com o protocolo de LFS utilizado. Embora não tenha ocorrido diferença estatisticamente significativa entre os grupos devido ao baixo número de animais utilizados, os dados sugerem a possibilidade de uma amplitude reduzida da LTP quando da injeção de bicuculina. Baclofen alterou a FPP em relação ao fEPSP basal, o mesmo não tendo sido observado no grupo controle. Com a administração concomitante de MT3, tais alterações deixam de ser identificadas. Ainda que os achados experimentais sejam inconclusivos e preliminares, este trabalho permitiu a padronização da técnica de eletrofisiologia in vivo em animal anestesiado o que abre portas para futuras investigações. / The cholinergic muscarinic system exerts modulatory function over different aspects of cognition and emotion. All five muscarinic receptors subtypes (mAChR), M1 to M5, are expressed at mammals hippocampus and at least two of them are simultaneously activated by most of the drugs, hindering significant advances on the role of each component of this system. The muscarinic toxin 3 (MT3) is a selective antagonist for the M4 subtype, allowing the investigation of the modulatory actions of this receptor over learning, memory and synaptic plasticity. The M4 are G protein coupled receptors (GPCRs) that act through Gi/o triggering inhibitory effects on which cells they are occur. Previous behavioral studies have shown that administration of MT3 soon after aversive task training exerts amnestic effects over memory, while administration prior to recall, leads to facilitation. A possible explanation to these results could be that the local circuits involved on memory consolidation and recall are different in nature. On this perspective, the amnestic effect of MT3 over memory consolidation should be consequence of GABAergic interneurons inhibition suppression; while the effect on recall, should be over glutamatergic synapses modulation. Thereby, the present work, with the objective to investigate how the M4 receptor modulates long-term synaptic plasticity and interacts with the GABAergic system, in vivo electrophysiological approach of anesthetized rats’ hippocampus was applied. Hence, field excitatory postsynaptic potentials (fEPSP) from CA1 were recorded after stimulation of contralateral Schaffer Collateral pathway with drugs infusion 15 min before or after high or low frequency electric stimulation (HFS: 10 trains 0.5 Hz, 20 pulses 100 Hz; LFS: 600 pulses 1 Hz, respectively). Neither MT3 (4.00 μg/μl), bicuculline (0.06 μg/μl), baclofen (0.20 μg/μl) nor vehicle, isolated or combined, changed the baseline evoked response amplitude 15 min after infusion nor the paired-pulse facilitation ratio (PPF). MT3 apparently attenuated, but not significantly, the long-term potentiation (LTP) compared to control (31.8% and 66.0% potentiation 60 min after HFS, respectively). In addition, there was no significant difference between baseline and 60 min after HFS fEPSP amplitude at MT3 group. Bicuculline, although did not abolish LTP neither changed PPF, it did produce a potentiation of only 36.4%. Baclofen induced a potentiation similar to control group. Baclofen administration also significantly reduced PPF compared to baseline. The simultaneous administration of MT3 and bicuculline or baclofen led to a potentiation similar to the control group. MT3 did not show any effect over LTP maintenance when applied 15 min after HFS. Lastly, it was not possible to induce long-term depression (LTD) with the used LFS protocol. Although there was no statistical significance between groups due to the low animal numbers used, data suggest that bicuculline had reduced LTP amplitude. Baclofen did alter PPF and the same was not observed on control group. When bicuculline or baclofen were injected with MT3, those alterations were not observed. These are inconclusive and preliminary results, notwithstanding this work allowed to set up the in vivo electrophysiology technique in anesthetized animals what will provide new tools for future research.
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Nutrição, natação e desenvolvimento cerebral em ratos: efeitos eletrofisiológicos sobre a potenciação do eletrocorticograma associada à depressão alastranteGONDIM, Mariana Barros e Silva 26 February 2016 (has links)
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Previous issue date: 2016-02-26 / CAPES / A nutrição no início da vida e o exercício físico podem alterar a excitabilidade cerebral, interferindo em processos de desenvolvimento e em parâmetros eletrofisiológicos. A depressão alastrante cortical (DAC) é um fenômeno relacionado com a excitabilidade cerebral. Em estudos anteriores, demonstramos potenciação da atividade elétrica cortical espontânea (ECoG) após a DAC. Nesta tese investigou-se a influência das condições de lactação e do exercício de natação, no início da vida e na idade adulta, sobre essa potenciação. Ratos Wistar machos foram amamentados em ninhadas com 6 ou 12 filhotes (grupos L6 e L12). A natação, precoce e tardia, foi realizada entre 8-23 e 60-75 dias de vida, respectivamente. O ECoG foi registrado aos 90-120 dias. Com um algoritmo específico (software Matlab™), determinou-se a amplitude do ECoG. Diferenças intergrupos de peso corporal e encefálico (L12<L6) confirmaram a deficiência nutricional do grupo L12. Diferenças, no mesmo animal, entre as amplitudes do ECoG antes e depois da DAC confirmaram a potenciação pós-DAC. Um grupo que não sofreu DAC não apresentou potenciação do ECoG. A natação precoce reduziu, e a tardia aumentou, essa potenciação do ECoG. A deficiência nutricional (condição L12) atenuou esse efeito. Estes dados sugerem que “condição de lactação”, “exercício de natação” e “idade ao exercício” modulam a potenciação do ECoG. A relevância desses resultados na fisiopatologia de doenças neurológicas dependentes da excitabilidade cerebral, como enxaqueca com aura e epilepsia, merecem futura investigação. / Nutrition in early life and physical exercise can alter brain excitability, interfering with development processes and electrophysiological parameters. Cortical spreading depression (CSD) is a phenomenon related to brain excitability. In previous studies, we demonstrated spontaneous brain electrical activity (ECoG) potentiation after CSD. In this thesis investigated the influence of the lactation conditions and swimming exercise in early life and adulthood, on this potentiation. Male Wistar rats were suckled in litters with 6 or 12 pups (L6 and L12 groups). The swimming, early and late, was carried out between 8-23 and 60-75 days of age, respectively. The ECoG was recorded at 90-120 days. With a specific algorithm (software Matlab ™), we determined the amplitude of the ECoG. Intergroup differences in body- and brain- weight (L12 <L6) confirmed the nutritional deficiency of the L12 group. Differences, in the same animal, between ECoG amplitudes before and after the CSD confirmed the post-CSD potentiation. A group that did not suffer CSD displayed no ECoG potentiation. Early swimming reduced, and later increased, this ECoG potentiation. The nutritional deficiency (L12 condition) attenuated this effect. These data suggest that "lactation condition", "swimming exercise" and "age to exercise" modulate ECoG potentiation. The relevance of these findings in the pathophysiology of brain excitability-dependent neurological diseases, such as migraine with aura and epilepsy, deserve further investigation.
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Altered NMDA Receptor Composition and Function Contribute to Deficits in Forebrain-Dependent Learning and Memory in Adult Rats Exposed to Ethanol as NeonatesGoodfellow, Molly Jo 06 June 2014 (has links)
No description available.
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Modulation cholinergique à long terme des potentiels évoqués visuels dans le cortex visuel chez le ratKang, Jun-Il January 2007 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal.
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Implication de la protéine kinase C dans les troubles bipolaires : vers de nouvelles cibles thérapeutiques / Role of protein kinase C in bipolar disorders : towards novel therapeutic targetsAbrial, Erika 05 February 2013 (has links)
Le trouble bipolaire est une maladie invalidante caractérisée par une alternance d’épisodes maniaques et dépressifs. Malgré des efforts de recherche notables, la physiopathologie et les mécanismes d’action des traitements du trouble bipolaire demeurent peu connus. La protéine kinase C (PKC) est récemment apparue comme une cible moléculaire potentielle pour le traitement du trouble bipolaire. Dans ce travail de thèse, nous avons cherché à étudier le rôle de la PKC dans les phases maniaque et dépressive du trouble bipolaire. Nous avons montré que l’inhibition de la PKC a un effet antimaniaque non seulement chez le rat naïf, mais aussi dans un modèle de manie basé sur une privation de sommeil, que nous avons validé au cours de notre étude. De plus, les inhibiteurs de la PKC sont capables de rétablir les déficits de prolifération cellulaire hippocampique que présentent les rats privés de sommeil. Ces effets prolifératifs et antimaniaques seraient indépendants, puisque le blocage de la prolifération cellulaire n’abolit pas l’efficacité antimaniaque des inhibiteurs de la PKC dans le modèle de privation de sommeil. En parallèle, nous avons montré que l’activation de la PKC a un effet antidépresseur chez le rat naïf, alors que son inhibition provoque un phénotype pseudodépressif qui s’accompagne d’une diminution de la prolifération cellulaire hippocampique. L’ensemble de ces données révèle une implication de la PKC dans les deux phases du trouble bipolaire, et soutient l’hypothèse qu’une suractivation du système PKC serait à l’origine des perturbations de neuroplasticité associées à la manie. / Bipolar disorder is a devastating long-term disease characterized by alternate episodes of mania and depression. Despite extensive research, the molecular and cellular underpinnings of bipolar disorder remain to be fully elucidated. Protein kinase C (PKC) has emerged as a potential molecular target for the treatment of bipolar disorder. The present study investigated the role of PKC in manic- and depressive-like behaviors. Our results showed that PKC inhibition produced an antimanic-like effect not only in naive rats, but also in an animal model of mania based on sleep deprivation, that we have validated in our study. Interestingly, PKC inhibitors rescued the hippocampal cell proliferation deficits displayed by sleep-deprived animals. These proliferative and antimanic effects were independent, since blockade of cell proliferation did not abolish the antimanic efficacy of PKC inhibitors in the sleep deprivation model. At the same time, we showed that PKC activation had an antidepressant-like effect in naive rats, whereas its inhibition caused a depressive-like phenotype accompanied by a decrease in hippocampal cell proliferation. Taken together, our results demonstrate the involvement of the PKC system in regulating opposite facets of bipolar disorder, and support the hypothesis that an overactivation of the PKC signaling system may be crucial for the deficits of neuroplasticity associated with mania.
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Elektrophysiologische Untersuchungen zur physiologischen und pathologischen neuronalen Plastizität im SubikulumWozny, Christian 18 January 2005 (has links)
Im Subikulum der Ratte finden sich zwei unterschiedliche Typen von Pyramidalzellen, die sich auf Grund ihres intrinsischen Entladungsverhaltens unterscheiden. Die Funktion dieser beiden Zelltypen hinsichtlich der synaptischer Neurotransmission ist unklar. Bursterzellen und regulär feuernde Zellen zeigten nach tetanischer Reizung ein unterschiedliches Ausmaß der LTP. Neben der zellspezifischen Ausprägung der LTP fanden sich mehrere Hinweise auf eine zielspezifische Projektion der Efferenzen der vorgeschalteten Area CA1. Die durchgeführten Experimente legen den Schluss nahe, dass Axone von Pyramidalzellen der Area CA1 selektiv auf subikuläre Pyramidenzellen projizieren und so den hippokampalen Informationsfluss steuern und regulieren können. NMDA-Rezeptoren auf beiden Seiten des synaptischen Spaltes spielen hier eine besondere Rolle. Präsynaptische NMDAR der Untereinheit NR2B scheinen an der LTP in Bursterzellen beteiligt zu sein und über einen vermehrten Kalziumeinstrom in die Präsynapse eine langanhaltende Erhöhung der Transmitterausschüttung herbeizuführen. Ebenso zeigten sich abhängig von der Zielzelle Hinweise auf eine unterschiedliche Aktivierung der präsynaptischen Adenylylcyclase-cAMP Kaskade. In Pilokarpin-behandelten Tieren ließ sich nach hochfrequenter Reizung keine langanhaltende Potenzierung der synaptischen Antworten nachweisen. Stattdessen scheinen polysynaptisch latente Verbindungen mittels tetanischer Stimulation aktivierbar zu sein. In einigen Fällen waren diese polysynaptisch latenten Verbindungen per se, in anderen Fällen nach Blockade der GABAergen Neurotransmission aktiv. In Hirnschnittpräparaten von Patienten mit pharmakoresistenter Temporallappenepilepsie konnte im Subikulum spontane rhythmische Aktivität mit einer Frequenz von 0,75 bis 3 Hz aufgezeichnet werden. Diese Aktivität, bestehend aus EPSP/IPSP Sequenzen, wurde sowohl in sklerotischem als auch in nicht sklerotischem Gewebe gefunden. In beiden Gruppen korrelierte die in vitro Aktivität sehr gut mit dem präoperativen Auftreten elektroenzephalografisch detektierter interiktaler Aktivität. Die Blockade GABAerger oder glutamaterger Neurotransmission hob die inhibitorische bzw. exzitatorische Aktivität auf. Dies legt den Schluss nahe, dass sowohl Interneurone wie Pyramidalzellen an der spontanen rhythmischen Aktivität beteiligt sind. / The subiculum plays a key role in processing memory information from the hippocampus to different cortical and subcortical brain regions. Subicular pyramidal cells are classified as regular firing or bursting cells according to their responses to supra-threshold depolarizing current pulses. Synaptic terminals arising from CA1 pyramidal cells do not function as a single compartment but show a specialized synaptic plasticity onto subicular pyramidal cells depending on the discharge properties of the synaptic target. Tetanic stimulation of CA1 axons caused a significantly stronger long-term potentiation (LTP) in bursting cells than in regular firing cells. Postsynaptic bursting was not necessary for the enhanced synaptic potentiation in bursting cells. The LTP in bursting neurons was independent of postsynaptic calcium, induced by presynaptic NR2B-containing autoreceptors and mediated via a adenylyl cylcase-cAMP-dependent signaling cascade. In pilocarpine-treated animals subicular LTP was impaired. A long-lasting increase in synaptic transmission could not be observed after titanic stimulation neither in regular firing cells nor in bursting cells. In human brain slices resected from patients from with drug-resistant temporal lobe epilepsy the subiculum displayed spontaneous rhythmic activity. In sclerotic but also in non-sclerotic hippocampal tissue the subiculum showed cellular and synaptic changes which suffice to generate spontaneous rhythmic activity that is correlated with the occurrence and frequency of interictal discharges recorded in the electroencephalograms of the corresponding patients.
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Plasticidade sináptica no córtex pré-frontal induzida por estimulação do tálamo mediodorsal de ratos in vivo: efeitos da modulação colinérgica muscarínica e nicotínica / Prefrontal cortical synaptic plasticity induced by stimulation of the rat mediodorsal thalamus in vivo: effects of cholinergic muscarinic and nicotinic modulationBueno Junior, Lézio Soares 17 August 2012 (has links)
O núcleo talâmico mediodorsal (Tmd) e o córtex pré-frontal (CPF) comunicam-se mutuamente, formando um circuito envolvido em funções executivas e transtornos psiquiátricos. As funções executivas estão sujeitas aos níveis de alerta gerados pela atividade oscilatória talamocortical, que por sua vez é controlada pela transmissão colinérgica. Possivelmente, a plasticidade sináptica do circuito Tmd-CPF é sensível tanto aos padrões oscilatórios do próprio circuito quanto à modulação colinérgica. Porém, esta possibilidade ainda não foi testada, muito menos dissociando-se a participação dos receptores muscarínicos e nicotínicos. Assim, nosso objetivo foi examinar como a plasticidade Tmd-CPF é modulada sob estados oscilatórios globais mediados pelo sistema colinérgico, e se esta modulação varia com os tipos de receptores recrutados. Anestesiamos ratos com uretana e implantamos um eletrodo de estimulação no Tmd, um eletrodo de registro no CPF e uma cânula de microinjeção acima do ventrículo. Emitimos 90 pulsos elétricos no Tmd (0,05 Hz) para evocação de potenciais pós-sinápticos de campo (PPSCs) basais no CPF por 30 min. Em seguida, aplicamos injeção intraventricular do agonista muscarínico pilocarpina (PILO), do agonista nicotínico nicotina (NIC), ou veículo-controle (VEIC). Os efeitos das substâncias sobre potenciais de campo locais (eletrencefalograma) foram monitorados através dos mesmos eletrodos. PILO e NIC induziram aumento das oscilações rápidas (4-80 Hz) e proporcional redução das oscilações lentas mantidas pela anestesia (0,5-4 Hz) e tais efeitos duraram ~10-15 min, conforme padronização prévia das concentrações das drogas. Justamente durante este período, aplicamos estimulação em alta frequência (EAF) ou baixa frequência (EBF) para indução de, respectivamente, potencialização (PLD) ou depressão (DLD) de longa duração, que são modelos bem conhecidos de plasticidade sináptica. Em grupos-controle, a injeção de PILO, NIC ou VEIC foi desacompanhada de EAF/EBF. Por fim, retomamos a coleta de PPSCs a 0,05 Hz por 240 min. Os resultados mostraram que a EAF não afetou os PPSCs quando aplicada após VEIC. Porém, nos ratos PILO e NIC, os PPSCs tiveram amplitude aumentada a partir de 150 min após EAF, indicando que a pré-ativação colinérgica foi necessária à indução de uma PLD tardia. Inversamente, quando a EBF foi aplicada após VEIC, a amplitude dos PPSCs foi reduzida de modo estável por 240 min. Isto não ocorreu quando a EBF foi aplicada após PILO e NIC, sugerindo que a modulação colinérgica suprimiu a DLD. Nos grupos-controle, PILO, NIC e VEIC sozinhos não afetaram os PPSCs em longo prazo, confirmando que os resultados de PLD e DLD são devidos a uma interação entre a pré-ativação colinérgica e mecanismos sinápticos desencadeados pela EAF/EBF.Portanto,as oscilações rápidas induzidas pela transmissão colinérgica favorecem a PLD no circuito Tmd-CPF, enquanto dificultam sua DLD. Além disto, os efeitos muscarínicos e nicotínicos sobre a plasticidade de longo prazo são iguais, apesar de os mecanismos celulares destes receptores serem diferentes. Nossos achados ajudam a esclarecer a regulação do sinal talâmico no CPF sob modulação colinérgica fisiológica (atenção e sono paradoxal) e disfuncional (esquizofrenias e doença de Alzheimer). / The mediodorsal thalamic nucleus (MD) and the prefrontal cortex (PFC) communicate with each other, constituting a circuit involved in executive functions and psychiatric disorders. Executive functions are subject to arousal levels driven& by the thalamocortical oscillatory activity, which in turn is controlled by the cholinergic neurotransmission. Possibly, the MD-PFC synaptic plasticity is susceptible to both the oscillatory patterns within the MD-PFC circuit and the cholinergic modulation. However, this likelihood is still untested, as well as the specific roles of muscarinic and nicotinic receptors. Thus, our aim was to evaluate whether and how the MD-PFC plasticity is modulated under cholinergic system-dependent oscillatory states of the forebrain, and if such modulation varies with the subtypes of activated cholinergic receptors. For that, we anesthetized rats with urethane to implant a stimulating electrode into the MD, a recording electrode into the PFC, and a microinjection cannula above the ventricle. We applied 90 monophasic square pulses into the MD (0.05 Hz) for recording of basal field postsynaptic potentials (fPSPs) in the PFC for 30 min. Then, we did an intraventricular injection of either the muscarinic agonist pilocarpine (PILO), the nicotinic agonist nicotine (NIC), or a control vehicle (Veh). The drug effects on local field potentials (electroencephalogram) were monitored through the same electrodes. PILO and NIC induced an increase in theta, beta and gamma oscillations (4-80 Hz) with proportional reduction of urethane-driven delta waves (0.5-4 Hz), and these effects survived approximately 10-15 min according to pilot-experiments on PILO and NIC concentrations. During this period, we applied either high-frequency (HFS) or low-frequency stimulation (LFS) for induction of respectively long-term potentiation (LTP) or depression (LTD), which are well-known synaptic plasticity models. In control groups, the injection of PILO, NIC or Veh was not followed by the HFS/LFS. Lastly, we resumed the evoking of fPSP at 0.05 Hz for an additional 240 min. The results showed that the HFS did not affect the fPSPs when applied after the Veh. However, in PILO and NIC rats the fPSP had their amplitudes increased from 150 min after HFS, indicating that the cholinergic pre-activation was required for the induction of a late-phase LTP. On the other hand, when the LFS was applied after the Veh, the fPSP amplitudes were stably decreased for 240 min, which did not occur when the LFS was applied after PILO and NIC, suggesting that the cholinergic modulation suppressed the LTD. In the control groups, PILO, NIC, and Veh by themselves did not change fPSPs in the long term, reinforcing that the LTP and LTD were due to an interaction between the cholinergic pre-activation and synaptic mechanisms triggered by the HFS/LFS. Therefore, the rapid oscillations induced by the cholinergic transmission favor LTP in the MD-PFC loop, while occlude its LTD. Moreover, the muscarinic and nicotinic effects on long-term plasticity were equal, although their quite distinct cell mechanisms. Our findings might help clarify the regulation of thalamic signals on the PFC both under physiological (attention and rapid-eye-movement sleep) and dysfunctional (schizophrenia symptoms and Alzheimer\'s) cholinergic drive.
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Mécanismes traductionnels impliqués dans la potentialisation à long-terme de la transmission synaptique des cellules pyramidales de l’hippocampe chez le rongeur.Gobert, Delphine 04 1900 (has links)
La mémoire et l’apprentissage sont des phénomènes complexes dont on ne comprend pas encore bien l’origine au niveau cellulaire et moléculaire. Cependant, il est largement admis que des changements plus simples au niveau synaptique, tels que la potentialisation à long-terme (long-term potentiation ou LTP) pourraient constituer la base cellulaire de la formation des nouveaux souvenirs. Ces mécanismes sont couramment étudiés au niveau de l’hippocampe, une région du lobe temporal reconnue comme étant nécessaire à la formation de la mémoire explicite chez les mammifères. La LTP est classiquement définie comme un renforcement durable de l’efficacité de connexions synaptiques ayant été stimulées de façon répétée et soutenue. De plus, on peut distinguer deux formes de LTP: une LTP précoce, qui repose sur la modification de protéines déjà formées, et une LTP tardive, qui requiert, elle, la synthèse de nouvelles protéines. Cependant, bien que de nombreuses études se soient intéressées au rôle de la traduction pour la maintenance de la LTP, les mécanismes couplant l’activité synaptique à la machinerie de synthèse protéique, de même que l’identité des protéines requises sont encore peu connus.
Dans cette optique, cette thèse de doctorat s’est intéressée aux interactions entre l’activité synaptique et la régulation de la traduction. Il est par ailleurs reconnu que la régulation de la traduction des ARNm eukaryotiques se fait principalement au niveau de l’initiation. Nous avons donc étudié la modulation de deux voies majeures pour la régulation de la traduction au cours de la LTP : la voie GCN2/eIF2α et la voie mTOR.
Ainsi, nos travaux ont tout d’abord démontré que la régulation de la voie GCN2/eIF2α et de la formation du complexe ternaire sont nécessaires à la maintenance de la plasticité synaptique et de la mémoire à long-terme. En effet, l’activité synaptique régule la phosphorylation de GCN2 et d’eIF2α, ce qui permet de moduler les niveaux du facteur de transcription ATF4. Celui-ci régule à son tour la transcription CREB-dépendante et permet ainsi de contrôler les niveaux d’expression génique et la synthèse de protéines nécessaires pour la stabilisation à long-terme des modifications synaptiques.
De plus, la régulation de la voie mTOR et de la traduction spécifique des ARNm 5’TOP semble également jouer un rôle important pour la plasticité synaptique à long-terme. La modulation de cette cascade par l’activité synaptique augmente en effet spécifiquement la capacité de traduction des synapses activées, ce qui leur permet de traduire et d’incorporer les protéines nécessaires au renforcement durable des synapses.
De telles recherches permettront sans doute de mieux comprendre la régulation des mécanismes traductionnels par l’activité synaptique, ainsi que leur importance pour la maintenance de la potentialisation à long-terme et de la mémoire à long-terme. / Learning and memory are complex processes that are not yet fully understood at the cellular and molecular levels. It is however widely accepted that persistent modifications of synaptic connections, like long-term potentiation (LTP), could be responsible for the encoding of new memories. These changes are frequently studied in the hippocampus, a temporal lobe structure that as been shown to be necessary for explicit memory in mammals. Long-term potentiation is classically defined as a persistent and stable modification of synaptic connections that have been repeatedly stimulated. Moreover, there are two different phases of LTP: an early-LTP, that only requires the modification of pre-existing proteins, and a late-LTP, that requires the synthesis of new proteins. Numerous studies have evaluated the role of new protein synthesis for the persistence of LTP, however, the mechanisms coupling synaptic activity and the translational machinery, as well as the identity of the necessary proteins are not yet fully understood.
From this perspective, this Ph.D. thesis has evaluated the interactions between synaptic activity and the regulation of translation. As it is widely accepted that the regulation of translation is primarily at the initiation level, we therefore investigated the modulation of two major pathways for the regulation of translation during LTP: the GCN2/eIF2α pathway and the mTOR pathway.
First, our studies have shown that the regulation of the GCN2/eIF2α pathway and of the ternary complex formation are necessary for the long-term maintenance of synaptic plasticity and memory. Indeed, synaptic activity regulates GCN2 and eIF2α phosphorylation, which modulates the transcription factor ATF4 levels. ATF4 in turn regulates CREB-dependent transcription, and therefore controls the levels of genetic expression and the synthesis of new proteins necessary for the long-term stabilization of synaptic modifications.
Moreover, the regulation of the mTOR pathway and of the specific translation of 5’TOP mRNAs likely also play an important role for long-term synaptic plasticity. Modulation of this cascade by synaptic activity specifically increases the translational capacity of activated synapses, allowing them to translate and incorporate the necessary proteins for the lasting reinforcement of synapses.
These studies will undoubtedly help to understand the regulation of translational mechanisms by synaptic activity and their significance for the maintenance of long-term potentiation and long-term memory.
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Modulation cholinergique à long terme des potentiels évoqués visuels dans le cortex visuel chez le ratKang, Jun Il January 2007 (has links)
Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal
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Impact of N-terminally truncated Aß4-42 on memory and synaptic plasticity - Tg4-42 a new mouse model of Alzheimer's diseaseDietrich, Katharina 17 December 2014 (has links)
No description available.
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