Representation of object-in-context within mouse hippocampal neuronal activity

Unknown Date

The rodent hippocampus is critical for processing spatial memory but its contribution to non-spatial, specifically object memory is debated. The cognitive map theory of hippocampal function states that the hippocampus stores relationships of goal locations (places) to discrete items (objects) encountered within environments. Dorsal CA1 place cells were recorded in male C57BL/6J mice performing three variations of the novel object recognition paradigm to define "object-in-context" representation of hippocampal neuronal activity that may support object memory. Results indicate, (i) that place field stability is higher when polarizing environmental cues are provided during object recognition; (ii) hippocampal place fields remain stable throughout the novel object recognition testing without a polarizing cue; and (iii) time dependent effects on stability when objects were dissociated from the context. These data indirectly support that the rodent hippocampus processes object memory, and challenge the view that "object-in-context" representations are formed when mice perform novel object recognition task. / by Herborg Nanna âAsgeirsdâottir. / Thesis (M.A.)--Florida Atlantic University, 2013. / Includes bibliography. / Mode of access: World Wide Web. / System requirements: Adobe Reader.

Mice as laboratory animals

Hippocampus (Brain)

Neurotransmitter receptors

Cellular control mechanisms

Cellular signal transduction

Selective Activation of the SK1 Subtype of Small Conductance Ca2+ Activated K+ Channels by GW542573X in C57BL6J Mice Impairs Hippocampal-dependent Memory

Unknown Date

SK channels are small conductance Ca2+-activated K+ channels expressed throughout the CNS. SK channels modulate the excitability of hippocampal CA1 neurons by affecting afterhyperpolarization and shaping excitatory postsynaptic responses. Such SK-mediated effects on activity-dependent neuronal excitability and synaptic strength are thought to underlie the modulatory influence of SK channels on memory encoding. Here,the effect of a new SK1 selective activator, GW542573X, on hippocampal-dependent object memory, contextual and cued conditioning, and trace fear conditioning was examined. The results demonstrated that pre- but not post-training systemic administration of GW542573X impaired object memory and trace fear memory in mice 24 h after training. Contextual and cued fear memory were not disrupted. These current data suggest that activation of SK1 subtype-containing SK channels impairs long-term memory. These results are consistent with converging evidence that SK channel activation suppressed behaviorally triggered synaptic plasticity necessary for encoding hippocampal-dependent memory. / Includes bibliography. / Thesis (M.S.)--Florida Atlantic University, 2015. / FAU Electronic Theses and Dissertations Collection

Cellular control mechanisms

Cognitive neuroscience

Cognitive psychology

Hippocampus (Brain)

Mice as laboratory animals

Neurotransmitter receptors

Participação dos glicocorticoides na progressão e no prejuízo cognitivo da encefalomielite autoimune experimental em camundongos C57BL/6. / Glucocorticoid involvement in the progression and cognitive impairment of experimental autoimmune encephalomyelitis in C57BL/6 mice.

Santos, Nilton Barreto dos

16 March 2017

A esclerose multipla (EM) é uma doença neurodegenerativa autoimune. As células da glia contribuem para o agravamento da EAE. Este trabalho objetiva mostrar a influência da dexametasona, na progressão da doença e nos défcits cognitivos da EAE. Foram utilizados camundongos C57BL/6, fêmeas, divididos em 4 grupos (CONT, DEX, EAE, EAE+DEX) imunizadas com MOG e Bordetella Pertussis, tratados com dexametasona (50mg/kg). Antes e após o aparecimento dos sintomas, os animais foram submetidos a testes comportamentais de campo aberto, labirinto em cruz elevado, contexto aversivo e reconhecimento de objetos. Os animais tratados com dexametasona (EAE+DEX) apresentaram diminuição do escore clínico em relação ao grupo EAE e apresentaram comportamento do tipo ansioso. Entretanto, o tratamento com DEX promoveu diminuição da memória de trabalho. Houve aumento marcadores inflamatórios e aumento do número de astrócitos no hipocampo do grupo EAE+DEX no 26o dia. Estes dados sugerem que a dexametasona diminui a aquisição da memória e aumenta o número e reatividade astrocitária na EAE. / Multiple sclerosis (MS) is an autoimmune neurodegenerative disease. The glial cells contribute to the aggravation of EAE. This work aims to show an influence of dexamethasone, the progression of the disease and the cognitive deficits of EAE. Female C57BL/6 mice were divided into 4 groups (CONT, DEX, EAE, EAE+DEX) immunized with MOG and Bordetella Pertussis, treated with dexamethasone (50mg/kg). Before and after the onset of symptoms, the animals were submitted to behavioral tests open field, the elevated plus maze, the aversive context and the object recognition test. The animals treated with dexamethasone (EAE+DEX) presented a decrease in the clinical score in relation to the EAE group and presented an anxious type behavior. However, treatment with DEX promoted a decrease in the work memory. There were increased inflammatory markers and increased number of hippocampal astrocytes from the EAE+DEX group on the 26th day. These data suggest that dexamethasone decreases memory acquisition and increases the astrocytic number and reactivity in EAE.

Animal memory

Astrócitos

Astrocytes

Esclerose múltipla

Glicocorticoides

Glucocorticoids

Hipocampo

Hippocampus

Memória animal

Multiple sclerosis

Interactions between the hippocampus and prefrontal cortex in context-dependent overlapping memory retrieval

Cohen, Justine E.

15 November 2018

Activation in the hippocampus (HC) and prefrontal cortex (PFC) is critical to accurately retrieve overlapping sequences. Experiments 1 and 2 tested the hypotheses that activation in and interaction between HC and PFC increases as overlap between sequences increases in a non-spatial task. Experiment 3 tested the hypothesis that theta oscillations are involved in orchestrating interactions between HC and PFC in a spatial task with overlapping elements. In the first two studies, 17 participants (aged 18-34; 11 female) learned sequences consisting of a picture frame, face, and scene. Conditions varied by degree of overlap. Using fMRI, Experiment 1 tested how degree of overlap affected HC and PFC activation. In overlapping sequences, middle and posterior HC were active when predictability of the correct response increased, dorsolateral PFC was active when participants were able to ascertain the correct set of sequences, and ventrolateral PFC was active when inhibition of interfering associations was required. Experiment 2 examined functional connectivity of HC and PFC during disambiguation. Low- and high-overlap conditions were associated with increased connectivity in separate regions at different times indicating that retrieval under the two conditions used different neural networks and strategies. Low-overlap trials were associated with increased connectivity between HC and prefrontal and parietal regions. High-overlap trials showed increased connectivity between lateral PFC and visual areas, indicating that imagery may be necessary for accurate performance. Using EEG recording, Experiment 3 examined theta activity during retrieval of well-learned, overlapping and non-overlapping mazes in 17 participants (aged 18-34, 11 female). Theta activity increased in overlapping mazes during the first of four hallways, suggesting participants were looking ahead to upcoming turns in the maze. Theta activity increased at the beginning and choice point of the third overlapping hallway, possibly in response to interference from the paired, overlapping maze. These studies provide evidence that (1) overlapping associations in non-spatial sequences elicit interactions between hippocampus and lateral prefrontal cortex, (2) increasing the degree of overlap changes the neural processes required to perform the task, and (3) theta power increases in response to increased cognitive demand and maintenance of sequence information needed to differentiate between overlapping spatial routes.

Cognitive psychology

EEG

Episodic memory retrieval

Functional MRI

Context-dependent

Hippocampus

Prefrontal cortex

Clorfeniramina microinjetada no hipocampo dorsal reverte e efeito ansiolítico da L-histidina e prejudica a memória emocional de camundongos / Dorsal hippocampal microinjections of chlorpheniramine reverses anxiolitic-like effect of L-histidine and impairs mice emotional memory.

Lucas Canto de Souza

30 September 2011

O nosso grupo tem investigado os efeitos da Clorfeniramina (CPA), antagonista H1, e da L-histidina (LH), uma droga precursora da síntese de histamina, sobre a ansiedade e a memória emocional. Diante disso, os objetivos desse estudo foram investigar os efeitos LH administrada i.p. e da CPA microinjetada no hipocampo dorsal sobre a ansiedade e a memória emocional de camundongos submetidos ao labirinto em cruz elevado (LCE). O experimento foi realizado em dois dias consecutivos. No primeiro dia (T1) 71 camundongos machos da cepa Suíço-Albino pesando 25-35g foram pré-tratados i.p. com salina (SAL) ou LH (500mg/Kg). Após duas horas, os sujeitos receberam microinjeção de SAL ou CPA (0,016nmol; 0,052nmol; 0,16nmol/0,1l) no hipocampo dorsal. Após cinco minutos, os animais foram expostos ao LCE por cinco minutos. Vinte quatro horas depois, o mesmo protocolo experimental foi adotado na reexposição (T2). Os animais foram distribuídos aleatoriamente em 8 grupos de acordo com o tratamento farmacológico: SAL/SAL (n=9), SAL/CPA1 (n=9), SAL/CPA2 (n=10), SAL/CPA3 (n=8), LH/SAL (n=10), LH/CPA1 (n=8), LH/CPA2 (n=8) e LH/CPA3 (n=9). As três doses de CPA microinjetadas no hipocampo dorsal não alteraram a porcentagem de tempo gasto nos braços abertos (%TBA) na exposição ao LCE: T1 SAL/CPA1 (46,13±4,45); SAL/CPA2 (47,59±4,89); SAL/CPA3 (44,30±6,65) quando comparados com o grupo controle SAL/SAL (35,84±2,77) e não alteraram o número de entradas nos braços fechados (EBF) SAL/CPA1 (8,56±1,06); SAL/CPA2 (9,70±1,10); SAL/CPA3 (9,38±1,25) - quando comparados com o grupo controle SAL/SAL (10,56±1,11). A administração i.p. de LH aumentou a %TBA em T1 para o grupo LH/SAL (59,79±4,71), quando comparado ao grupo controle SAL/SAL (35,84±2,77), mas não alterou o EBF: LH/SAL (9,20±1,78) e SAL/SAL (10,56±1,11). Os animais do grupo LH/CPA3 diminuíram %TBA (32,25±4,81) em T1 quando comparados com o grupo LH/SAL (59,79±4,71). Os animais do grupo SAL/CPA1 não apresentaram diminuição da %TBA em T2 (T1: 46,13±4,45; T2: 39,38±6,53). O mesmo foi observado para os sujeitos dos grupos LH/CPA2 (T1: 50,10±3,99; T2: 40,97±8,22) e LH/CPA3 (T1: 32,25±4,81; T2: 32,16±6,93). Nós concluímos que: a CPA microinjetada no hipocampo dorsal de camundongos não apresenta efeito sobre a ansiedade; a administração intraperitoneal de LH apresenta efeito ansiolítico em camundongos expostos ao LCE e que esse efeito é revertido pela maior dose de CPA (0,16nmol/0,1l); são necessárias maiores doses de CPA para que haja prejuízo na memória emocional de camundongos reexpostos ao LCE quando os níveis de histamina no hipocampo dorsal estão elevados. / Our group has been investigating the effects of Chlorpheniramine (CPA), a histaminergic H1 antagonist, and of L-Histidine (LH), a histamine precursor, on anxiety-related behaviors and emotional memory. Thus the aim of this study was to investigate the effects of LH i.p. injections and of dorsal intra-hippocampal microinjections of Chlorpheniramine (CPA) on anxiety-related behaviors and emotional memory in male mice using elevated plus-maze (EPM). The experiment was performed in two days. On the first day (T1) 71 male Swiss Albino mice of body weight 25- 35g were pre-treated with saline (SAL) i.p. or LH (500mg/Kg) i.p. After two hours they were treated with dorsal intra-hippocampal microinjections of SAL or CPA (0.016nmol; 0.052nmol; 0.16nmol/0,1l). Five minutes after intra-hippocampal microinjections the animals were exposed to EPM for 5 minutes. Twenty four hours later the same protocol was repeated (T2). The animals were randomly assigned to 8 groups based on drug treatment: SAL/SAL (n=9), SAL/CPA1 (n=9), SAL/CPA2 (n=10), SAL/CPA3 (n=8), LH/SAL (n=10), LH/CPA1 (n=8), LH/CPA2 (n=8) and LH/CPA3 (n=9). All three doses of intra-hippocampal microinjections of CPA did not change the percentage of time spent in the open-arms (%OAT) on T1 SAL/CPA1 (46.13±4.45); SAL/CPA2 (47.59±4.89); SAL/CPA3 (44.30±6.65) when compared to control group SAL/SAL (35.84±2.77) and did not change the enclosed arm entries (EAE) SAL/CPA1 (8.56±1.06); SAL/CPA2 (9.70±1.10); SAL/CPA3 (9.38±1.25) when compared to control group SAL/SAL (10.56±1.11). Intraperitoneal injections of LH increased %OAT on T1 on LH/SAL group (59.79±4.71), when compared to control group SAL/SAL (35.84±2.77), but not EAE LH/SAL (9.20±1.78) and SAL/SAL (10.56±1.11). Animals treated with LH and CPA3 (LH/CPA3) decreased %OAT (32.25±4.81) on T1 when compared to LH/SAL (59.79±4.71) group. SAL/CPA1 animals did not decreased %OAT on T2 (T1: 46.13±4.45; T2: 39.38±6.53). The same happened to LH/CPA2 (T1: 50.10±3.99; T2: 40.97±8.22) and LH/CPA3 (T1: 32.25±4.81; T2: 32.16±6.93) groups. Thus, we conclude that: dorsal intra-hippocampal microinjection of Chlorpheniramine has no effect on anxiety-related behaviors in male mice; intraperitoneal injection of L-Histidine has an anxiolytic-like effect in male mice exposed to elevated plus-maze, that is reversed by the higher dose of Chlorpheniramine (0.16nmol/0,1l); higher doses of CPA are necessary to impair emotional memory when the levels of hippocampal histamine are elevated.

Ansiedade

Clorfeniramina

Hipocampo dorsal

L-histidina

Memória emocional

anxiety

Chlorpheniramine

dorsal hippocampus

emotional memory

L-histidine

Efeitos comportamentais e bioquímicos da dieta intermitente na vigência de um estímulo inflamatório no hipocampo de ratos. / Behavioral and biochemical effects of intermittent fasting in the presence or absence of an inflammatory stimulus (LPS) in rat hippocampus.

Vasconcelos, Andréa Rodrigues

18 October 2011

A dieta intermitente (DI), quando não causa desnutrição, expõe os organismos a um estresse nutricional moderado que estimula as proteínas de estresse e os mecanismos de defesa do organismo, tornando-o mais resistente a estímulos tóxicos. A DI atua em vias associadas à sobrevivência celular e à inflamação, envolvendo com isso a modulação do NF-<font face=\"Symbol\">kB. Porém, pouco se sabe sobre os mecanismos moleculares associados a estes efeitos, assim como o envolvimento de vias como a do CREB e da WNT, além de sua correlação com a sinalização inflamatória. Este projeto tem como objetivo avaliar os efeitos da DI na cognição e hipocampo de ratos na ausência ou presença de LPS. Os resultados mostraram que a DI melhora o desempenho dos animais nos testes comportamentais labirinto de Barnes e esquiva inibitória. Ainda, a DI induz um aumento de pCREB e da sinalização canônica da WNT e promove o aumento da razão IL-10 / TNF e a diminuição dos níveis de RNAm do Tlr-4, Nosi e Cox-2 no hipocampo. Os dados sugerem que a DI induz um predomínio das vias de sinalização protetoras no SNC de ratos. / The intermittent fasting (IF) protocol, when it does not cause malnutrition, induces a moderate nutritional stress to the organism which stimulates the stress proteins and the body\'s defense mechanisms, making it more resistant to toxic stimuli. The IF seems to act by mechanisms associated with cell survival and inflammation, thereby involving NF-<font face=\"Symbol\">kB modulation. However, little is known about the molecular mechanisms involved, as well as the participation of CREB and WNT pathways and its correlation with inflammatory signaling. This study investigates the effects of IF on cognition and on rat hippocampus in absence or presence of LPS. The results showed that IF improved performance in Barnes maze and inhibitory avoidance behavioral tests. Also, IF induced both increase of pCREB and canonical WNT signaling pathway, and decrease in inflammatory mRNA markers levels, such as Tlr-4, iNos and Cox-2. In addition, IF can also increase IL-10 / TNF ratio levels. Our results suggest that IF induces a prevalence of protective signaling pathways in the central nervous system.

Animal hippocampus

Cognição

Cognition

Hipocampo de animal

Inflamação

Inflammation

Mice

Neurofarmacologia

Neuropharmacology

Ratos

RNA

RNA

Avaliação temporal da expressão gênica e proteica de S100b no encéfalo de ratos neonatos submetidos à anóxia. / Assessment of S100b gene and protein expression over time in the brain of newborn rats subjected to anoxia.

Hamasaki, Mike Yoshio

27 January 2014

O presente trabalho objetivou explorar a eventual variação da expressão do mRNA e da proteína S100b no hipocampo, cerebelo e córtex cerebral de ratos neonatos em condições de anóxia, comparativamente à condições controle. Este estudo foi desenvolvido em ratos albinos, divididos em dois grupos: o grupo Experimental Anóxia (EA) e o grupo Experimental Controle (EC), que por sua vez foram subdivididos em tempos de 2, 4, 6, 12 e 24 horas no que se refere à coleta de amostras após a aplicação dos estímulos pré-estabelecidos para cada grupo. Dos períodos avaliados, nossos resultados indicaram que a anóxia proporcionou um pico na expressão gênica de S100b após duas horas e proteica após 4 horas nas áreas do hipocampo e cerebelo. O córtex cerebral do grupo EA quando comparado ao grupo EC, não apresentou nenhum aumento significante de S100b nos períodos avaliados. Os resultados obtidos contribuem de forma crucial para elucidação do papel da proteína S100b como biomarcadora na EHI, bem como no esclarecimento parcial da função deste gene com relação à fisiopatologia da doença. / The aim of the present study was to investigate the temporal variation in the expression of S100b mRNA and protein in the hippocampus, cerebellum, and cerebral cortex of newborn rats under conditions of anoxia compared with control rats. The study was performed using two groups albino rats: Experimental Anoxia (EA) and Experimental Control (EC). The animals in both EA and EC were distributed in the following subgroups relative to the time elapsed since the application of the stimuli predefined for each group: two, four, six, 12, and 24 hours. Anoxia induced a peak in the S100b gene expression after two hours and protein expression after 4 hours in the hippocampus and cerebellum. With respect to the cerebral cortex, S100b never exhibited a significant increase in the EA group compared with the EC group. The results of the present study represent a crucial contribution to the elucidation of the role protein S100b plays as a biomarker in HIE, as well as a contribution to the elucidation of the role the corresponding gene plays in the physiopathology of the disease.

Biomarcador

Biomarker

Cerebellum

Cerebelo

Cerebral cortex

Córtex cerebral

Encefalopatia hipóxico-isquêmica

Hipocampo

Hippocampus

Hypoxic-ischemic encephalopathy

Expressão dos microRNAs miR-629-3p, miR-1202 e miR-1225-5p em amígdalas, hipocampos e sangue de pacientes com epilepsia do lobo temporal mesial / Expression of microRNAs miR-629-3p, miR-1202 and miR-1225 in amygdala, hippocampus and blood of patients with mesial temporal lobe epilepsy

Gattás, Daniela

06 September 2017

INTRODUÇÃO: Epilepsia do lobo temporal (ELTM) é a forma mais comum de epilepsia parcial, ocorrendo em cerca de 40% dos pacientes. Na ELTM as crises epilépticas podem ter origem na região cortical, o que é menos comum, porém ocorrem frequentemente em estruturas mesiais do lobo temporal, representadas basicamente pelo hipocampo e/ou amígdala. Com intuito de incluir novas possibilidades de tratamento e diagnóstico, torna-se necessário uma maior compreensão das bases moleculares da ELMT. Dentro desta perspectiva, um dos grandes desafios para a Neurociências na atualidade é o desenvolvimento de biomarcadores que facilitem o diagnóstico e prognóstico para a epilepsia. Recentemente, com o desenvolvimento de algumas pesquisas e novas técnicas no campo da biologia molecular demonstram que microRNAs circulantes no sangue são biomarcadores sensíveis e específicos para várias doenças, incluindo doenças neurológicas, podendo ser obtido de forma não invasiva, representando assim um método de eficiente detecção e custo baixo. OBJETIVOS: Analisar o perfil de expressão dos microRNAs miR-629-3p, miR-1202, miR1225-5p na amígdala, hipocampo e sangue de pacientes submetidos a cirurgia para tratamento da epilepsia do lobo temporal mesial refratários ao tratamento medicamentoso e investigar se os mesmos podem auxiliar como biomarcadores de diagnóstico e prognóstico para a epilepsia. PACIENTES E MÉTODOS: Foram utilizadas amostras de amígdalas, hipocampos e sangue de 20 pacientes com ELTM, sendo 10 com boa evolução pós-operatória (Engel I) e 10 com evolução pós-operatória insatisfatória (Engel III e IV), e para controle foram utilizados 10 amostras de amígdalas e 10 de hipocampos de necrópsias, assim como 10 amostras de sangue de indivíduos saudáveis. A análise de expressão dos miRNAs foi feita utilizando a técnica de RQPCR. RESULTADOS e CONCLUSÕES: Os miRNAs miR-629-3p, miR-1202 e miR- 1225-5p apresentaram-se hiperexpressos no sangue de pacientes com ELTM, podendo sugerir um possível papel de biomarcadores auxiliando no diagnóstico da ELTM. Os miRNAs-629-3p, 1202 e 1225-5p apresentaram aumento nos níveis de expressão sanguíneos progressivos entre os grupos controle, Engel I e Engel III e IV respectivamente, apresentando também possível potencial de biomarcadores no prognóstico cirúrgico entre Engel I e Engel III e IV. / INTRODUCTION: Epilepsy of the temporal lobe is the most common form of partial epilepsy, occurring in about 40% of patients. In TLE epileptic seizures may originate in the cortical region, which is less common. However they occur more frequently in temporal lobe mesial structures, represented primarily by the hippocampus and / or amygdala. A greater understanding of the epilepsy molecular basis is necessary when aiming to implement new treatments possibilities. Within this field of study, one of the major challenges for neuroscience today is the development of biomarkers that facilitate the diagnosis and prognosis for epilepsy. Recently, with the development of some researches and new techniques in the field of molecular biology, it demonstrate that microRNAs circulating in the blood are sensitive and specific biomarkers for various diseases, including neurological diseases and they can be obtained noninvasively, thus representing a low cost method of efficient detection. OBJECTIVES: To analyze the expression profile of miR-629-3p, miR-1202, miR1225-5p microRNAs in the amygdala, hippocampus and blood of patients operated to treat the mesial temporal lobe epilepsy refractory to drug treatment and investigate whether they can be used as biomarkers for epilepsy diagnosis and prognosis. PATIENTS AND METHODS: Amygdala, hippocampus and blood samples of 20 patients with MTLE were used; 10 with good postoperative outcome (Engel I) and 10 with poor postoperative outcome (Engel III and IV), and for the control group 10 amygdalas and 10 hippocampus of necropsy, as well as, 10 samples blood from healthy individuals. The analysisof the expression of miRNAs was performed using RQ-PCR. RESULTS AND CONCLUSION: MiRNAs miR-629-3P, miR-1202 and miR- 1225-5P were hyper-expressed in the blood of patients with MTLE, and may suggest a possible role of biomarkers in the diagnosis of MTLE. miR-629-3p, miR-1202 and miR-1225-5p were progressively expressed in the blood of patients in the control, Engel I and Engel III and IV groups respectively, representing also potential biomarkers for surgical prognosis between Engel I and Engel III and IV.

Amígdala

Amygdala

Epilepsia do Lobo Temporal Mesial

Hipocampo

Hippocampus

microRNAs

microRNAs

Temporal Lobe Epilepsy

"Avaliação da doença de Alzheimer através da espectroscopia de prótons por ressonância magnética: comparação entre os achados no cíngulo posterior e nos hipocampos" / Evaluation of Azheimer's Disease using Magnetic Resonance Spectroscopy : comparation of findings in the posterior cingulate and hippocampi

Lee, Hae Won

26 October 2005

Foi realizada a comparação entre os achados de espectroscopia de prótons por ressonância magnética utilizando a sequência PRESS (point resolved spectroscopy), com TE curto (35ms) no cíngulo posterior e hipocampos de 29 pacientes com doença de Alzheimer (leve e moderada) e 15 controles. As relações de metabólitos com melhor sensibilidade e especificidade na diferenciação entre os grupos foram em ordem decrescente: Naa/Cr do cíngulo, mI/Naa do cíngulo, mI/Naa dos hipocampos e mI/Cr dos hipocampos. Não houve vantagens, nesta casuística, na realização da espectroscopia de prótons nos hipocampos, um local tecnicamente mais difícil e demorado em relação ao cíngulo posterior. Observou-se correlação positiva da relação Naa/Cr e negativa da relação mI/Naa do cíngulo posterior com o MMSE / The objective of this study is to compare the findings on Magnetic Resonance Spectroscopy using PRESS (point resolved spectroscopy) technique with short TE (35ms) in the posterior cingulate and hippocampi of 29 patients with Alzheimer's disease (mild and moderate) and 15 controls. The metabolic ratios with highest sensitivity and specificity were (in a decreasing order): posterior cingulate Naa/Cr, posterior cingulate mI/Naa, hippocampi mI/Naa and hippocampi mI/Cr. In the group analised it seems there is no advantage in performing MRS in the hippocampi instead of posterior cingulate, a technically challenging location, usually leading to a longer examination time. In the posterior cingulate we observed a positive correlation with Naa/Cr ratio and a negative correlation with mI/Naa ratio and the MMSE

Alzheimer disease

Doença de Alzheimer

Giro do cíngulo

Gyrus cinguli

Hipocampo

Hippocampus

Magnetic resonance spectroscopy

Effets comportementaux et neurogéniques des antidépresseurs dans un nouveau modèle d'anxiété/dépression chez la souris adulte / Behavioural neurogenic effects of antidepressants in a new model of anxiety/depression in adult Mouse

Rainer, Quentin

07 March 2011

Les pathologies dépressives se caractérisent par des symptômes hétérogènes impliquant de nombreuses régions cérébrales. L’une d’entre elles, l’hippocampe, est le siège d’un processus physiologique, appelé neurogenèse, qui, chez l’adulte, serait impliqué dans l’étiologie de la dépression et la réponse au traitement antidépresseur.L’objectif de ce travail a été d’étudier le rôle des 4 étapes du processus de neurogenèse hippocampique dans l’action des antidépresseurs dans un modèle physiopathologique de la dépression, chez la Souris adulte. / Depression is characterized by heterogeneous symptoms in several brain regions. One of them, the hippocampus, is related to a phenomenon called neurogenesis, which seems to be linked to the etiology of depression and to the response of antidepressants. The main goal of this work was to study the relationships between all the 4 steps of hippocampal neurogenesis and antidepressants action in a model of depression in adult mouse.

Neurogenèse

Sérotonine

Agomélatine

Corticostérone

Modèle animal

Depression

Anxiety

Neurogenesis

Hippocampus

Serotonine

Antidépressant

Agomelatine

Corticosterone

Animal model