Contribution des régions fronto-striatales dans les fonctions exécutives

Provost, Jean-Sébastien

08 1900

Des études récentes ont montré que le noyau caudé interagissait avec le cortex préfrontal et qu’il pourrait être impliqué dans les fonctions exécutives. Le but de cette thèse était d’étudier la contribution du noyau caudé dans les fonctions exécutives, plus précisément dans des tâches de monitoring et de changement de règle, et d’observer comment ces régions fronto-striatales interagissent avec le réseau par défaut (RPD). Dans un premier temps, nous avons étudié le rôle du noyau caudé dans les deux types de monitoring : le monitoring d’origine interne, consistant à effectuer un suivi sur l’état de l’information en mémoire de travail afin de pouvoir faire un choix subséquent, et dans le monitoring d’origine externe où le suivi sur l’état des items est effectué par l’individu, mais la sélection est exécutée par une source externe. Il a été montré que le cortex préfrontal dorsolatéral (CPFDL) est impliqué dans les deux types de monitoring. À l’aide de l’imagerie par résonance magnétique fonctionnelle (IRMf), nos résultats ont montré une augmentation significative du signal BOLD au niveau du CPFDL dans les contrastes des conditions de monitoring d’origine interne et monitoring d’origine externe par rapport à la condition contrôle. De manière plus importante, une augmentation significative de l’activité a été observée dans le noyau caudé seulement dans les soustractions impliquant le monitoring d’origine interne par rapport à la condition contrôle, et par rapport à la condition de monitoring d’origine externe. En deuxième lieu, des études ont montré une contribution spécifique des régions fronto-striatales dans l’exécution d’un changement de règle. Toutefois, l’effet d’un changement de règle sur l’activité cérébrale n’a jamais été étudié sur les essais subséquents. À l’aide de l’IRMf, le cortex préfrontal ventrolatéral (CPFVL) et le noyau caudé ont montré une augmentation significative de leur activité lors des changements de règle continus et lors des changements de règles sporadiques par rapport à la condition contrôle, et aussi lors des essais où le maintien d’une même règle devait être effectué pour une courte durée par opposition au contrôle. Cependant, aucune activité fronto-striatale n’a été observée lorsqu’une même règle devait être appliquée pour une plus longue période. De plus, une diminution significative de l’activité du noyau caudé a été observée lors de la répétition de l’exécution d’une même règle suggérant une meilleure intégration de cette dernière. Finalement, plusieurs études ont montré une déactivation du RPD lors de l’exécution de tâches. À l’aide de l’IRMf, nous avons posé l’hypothèse que le RPD serait corrélé négativement avec les régions fronto-striatales lors de l’exécution d’une tâche de changement de règle. Nos résultats montrent une augmentation significative de l’activité des régions fronto-striatales lors d’une augmentation du nombre d’essais de changement de règle consécutif, pendant que le RPD montre une déactivation continue. De façon intéressante, pendant que les régions fronto-striatales montrent une diminution de leur activité lors de l’exécution d’une même règle pour une longue période, le RPD augmente son activité de façon significative. On conclut donc que le noyau caudé joue un rôle important dans la planification d’une nouvelle action lorsque plusieurs possibilités doivent être considérées en mémoire de travail, et ce en même temps. Finalement, le RPD montre une corrélation négative avec les régions fronto-striatales suggérant sa participation dans l’intégration d’une tâche devenant de plus en plus familière. / Recent studies have shown that the caudate nucleus interacts with the prefrontal cortex, and that it is involved in executive processes. The goal of the thesis was to investigate the role of the caudate nucleus in executive processes, and to observe how the frontostriatal regions are interacting with the default mode network (DMN). Firstly, we studied the role of the caudate nucleus in self-ordered monitoring, which consist of keeping track of which stimuli have been selected and which remains to be selected, and externally-triggered monitoring, which refers to keeping track of one’s selection when an external source is performing the selection. It has been shown that de dorsolateral prefrontal cortex (DLPFC) was particularly involved in both types of monitoring. Using functional magnetic resonance imaging (fMRI), a significant increase of activity has been observed in the DLPFC during both monitoring conditions vs control condition. Importantly, significant increased activity in the caudate nucleus was observed only in subtractions involving self-ordered monitoring (the self-ordered vs control and self-ordered vs externally-triggered conditions). Secondly, previous studies have shown a specific contribution of frontostriatal regions during set-shifting. However, the effect of set-shifting on subsequent trials had yet to be determined. Using fMRI, significant increase of activity was observed in the ventrolateral prefrontal cortex (VLPFC) and the caudate nucleus during shifting trials versus control and in trials where the same rule was applied for a few trials before a set-shift occurred. However, no frontostriatal activity was observed when the same rule was applied for a longer period. Decreased activity in the caudate nucleus correlated with increasing trial position in trials where no set-shift occurred, suggesting that the more a rule is executed, the better it is established. Finally, several studies have shown a deactivation of the DMN during the execution of a goal-directed task. Using fMRI, we hypothesized that the DMN was negatively correlated with the frontostriatal regions during the execution of a set-shifting task. Our results showed a significant increase of activity in the frontostriatal regions as more set-shifts are being performed while the DMN gets more deactivated. Interestingly, as decreased activity was observed in the frontostriatal regions during the execution of the same rule for a long period, the DMN showed increasing activity. We concluded that the caudate nucleus is specifically involved during the planning of a novel action when several possibilities are available at the same time. Finally, the DMN shows a negative correlation with the frontostriatal regions suggesting its contribution to the execution of a more familiar task.

Cortex préfrontal

noyau caudé

fonctions exécutives

changement de règle

prefrontal cortex

caudate nucleus

functional magnetic resonance imaging

set-shifting

executive processes

三甲基甘胺酸和二甲基甘胺酸改善甲基安非他命所導致神經行為毒性 / N,N,N-Trimethylglycine and N,N-Dimethylglycine improve methamphetamine-induced neurobehavioral toxicity

陳映安

Unknown Date

甲基安非他命是一種被廣泛濫用的非法神經興奮劑，而且使用之後常伴隨著精神疾病的發生，動物研究也顯示，施打甲基安非他命所引起的神經毒性不僅會造成多巴胺神經元及血清素神經元的損傷，也引起認知功能和社交行為的缺失，同時對於產生迷幻作用的5-HT2A受體作用劑的行為反應增強。N,N,N-trimethylglycine (TMG)和N,N-dimethylglycine (DMG)是甘胺酸的甲基化衍生物，由於這兩種藥物具有治療神經系統疾病的潛力，因此本研究的目的為評估TMG及DMG是否可以預防或改善小鼠在甲基安非他命的暴露下所導致的行為缺失包括新位置辨識測試，新物體辨識測試，社交行為互動測試以及使用5-HT2A受體作用劑DOI 誘導小鼠頭部抽搐(head twitch )的行為。實驗方式為腹腔注射給予雄性ICR小鼠甲基安非他命，一天注射四劑（4 × 5mg/kg），每劑間隔兩小時。實驗一，小鼠在暴露甲基安非他命，先確認行為改變後，給予腹腔注射TMG及DMG (10或30 mg/kg)連續七天，評估TMG及DMG的治療效果。實驗二在施打每劑甲基安非他命30分鐘前給予TMG及DMG (100 mg/kg)，七天後進行行為評估，實驗三，評估TMG及DMG個別及混合劑量的治療效果，小鼠給予甲基安非他命之後，先確認行為改變，再給予腹腔注射TMG及DMG (20、5+5或是10+10 mg/kg) 連續七天，七天後進行行為測試。實驗四，檢測TMG及DMG的治療效果是否藉由活化NMDA受體glycine binding site，小鼠給予甲基安非他命七天之後，腹腔注射TMG及DMG (20 mg/kg)並在給予TMG及DMG前30分鐘給予glycine binding site 拮抗劑7-chlorokynurenic acid (7-CK) (1 mg/kg)，連續給藥七天，七天後進行行為評估。實驗結果發現連續給予七天TMG及DMG在個別劑量及混合劑量中都能夠恢復甲基安非他命所造成的認知功能缺損，社交退縮和降低由DOI 誘導小鼠頭部抽搐行為表現，以及在紋狀體中酪氨酸羥化酶的蛋白質表達減少情況。而前給予7-CK則阻斷TMG及DMG對甲基安非他命所造成的認知功能缺損，社交退縮的改善作用，但是對TMG及DMG對DOI 誘導小鼠頭部抽搐的行為的改善作用影響較小，顯示TMG及DMG可能都是經由活化NMDA 受體的glycine binding site改善甲基安非他命所造成的認知功能缺損，社交退縮，這些發現表示，TMG及DMG具有治療甲基安非他命成癮者所造成的精神分裂等異常症狀的潛力。 / Methamphetamine (METH) is a widely abused illicit psychostimulant. METH use is commonly associated with psychosis. A neurotoxic regimen of METH, which damages the dopaminergic and serotonergic neurons, causes cognitive dysfunction, social interaction deficits, and supersensitivity to hallucinogen in mice. N,N,N-trimethylglycine (TMG) and N,N-dimethylglycine (DMG) are methyl derivatives of amino acid glycine and naturally occur as intermediate metabolites in choline-to-glycine metabolism. Growing evidence shows that both compounds have potential to treat some neurological disorders. The aim of this study was to examine the protective and therapeutic effects of TMG and DMG on METH-induced behavioral aberrations. The novel location recognition test (NLRT), the novel objective recognition test (NORT), the social interaction and the hallucinogenic 2, 5-dimethoxy-4-iodoamphetamine (DOI)-induced head twitch response were evaluated. Male ICR mice received one day drug treatment with four injections of METH (4 × 5 mg/kg, i.p.) or saline at 2h interval. First, TMG or DMG (10 or 30 mg/kg, i.p.) were separately administered once daily for seven consecutive days after the behavioral impairment was confirmed in METH-treated mice. Seven days after final injection of TMG and DMG, the behavioral tests were monitored. Secondly, the preveting effects of TMG and DMG were examined by TMG and DMG (100 mg/kg, i.p.) pretreatment, 30 min prior to each dose of METH. Third, the lower dose (20 mg/kg) and combined effects of TMG and DMG (5+5 or 10+10 mg/kg i.p.) were evaluated. Fourth, in order to determine if the improving effects of TMG and DMG are mediated by NMDA receptor glycine binding site, the glycine binding site antagonist 7-CK (1 mg/kg, i.p.) was administered 30 min prior to each dose of TMG and DMG (20 mg/kg, i.p.), TMG and DMG dose-dependently improved, but not prevented the METH-induced cognition deficits, social withdrawal and hypersensitivity to hallucinogen with additional effect. Pretreatment of 7-CK, reversed the improving effects of TMG and DMG on behavioral deficits after METH exposure, yet had minor effect on hypersensitivity to hallucinogen. These results demonstrate that TMG and DMG might activate the glycine binding site of NMDA receptor to improve METH-induced cognition deficits and social withdrawal. TMG and DMG may be the novel therapeutic agents for psychiatric disorders related to METH abuse.

甲基安非他命

三甲基甘胺酸

二甲基甘胺酸

紋狀體

前額葉皮質區

METH

TMG

DMG

stratium

medial prefrontal cortex

Évaluation systématique des effets de la tDCS sur le DLPFC et applications en technologies de l'information

Dumont, Laurence

08 1900

No description available.

Neuropsychologie

évaluation cognitive

validation de traduction

cortex dorsolatéral préfrontal

fonctions exécutives

technologies de l'information

Neuropsychology

Cognitive evaluation

Translation validation

Dorsolateral prefrontal cortex

Transcranial direct current stimulation

Executive functions

Information systems

Anatomo-functional organization of adaptive manual, orofacial and vocal control in the human frontal cortex / L'organisation anatoma-fonctionnelle du contrôle adaptatif des réponses manuelles, orofaciales et vocales dans le cortex frontal humain

Loh, Kep Kee

01 October 2018

Ce travail de thèse explore l'organisation fonctionnelle du cortex frontal chez l'homme lors de l'apprentissage et l'utilisation de règles conditionnelles associées à des stimuli contextuels et demandant la réalisation d'actions manuelles, vocales et orofaciales. Ma première étude a démontré chez l'homme que 1) le cortex frontal latéral postérieur (pLFC) est organisé selon un gradient dorso-ventral, où le cortex prémoteur dorsal (PMd) et le cortex préfrontal dorsal (BA 44) sont impliqués respectivement dans les associations conditionnelles manuelles et vocal-orofaciales, et 2) que l'aire motrice cingulaire antérieure (RCZa) au sein du cortex cingulaire moyen (MCC), contribue à l'évaluation des feedback auditifs durant l'apprentissage par essai-erreur de ces associations. Ma seconde étude a révélé qu'au sein du MCC, les trois CMAs sont fonctionnellement couplées avec le cortex préfrontal latéral le long du gradient rostro- caudal où les régions les plus rostrales sont impliqués dans un contrôle comportemental de plus haut niveau. Ces résultats apportent de nouveaux éclaircissements aux théories actuelles concernant l'organisation cortico-frontal du contrôle comportemental. En réalisant une revue de la littérature, j'ai montré qu'au sein du réseau pLFD-MCC les aires BA 44 et RCZa font partie d'un réseau cérébral homologue qui pourrait jouer un rôle similaire dans le contrôle cognitif vocal/orofacial chez les primates - le contrôle adaptatif des actions vocales/orofaciales basés sur l'évaluation des feedback auditifs. Cette hypothèse a été validé chez l'homme dans ma première étude. Cette thèse a mis en évidence un important réseau neural aidant à comprendre comment le contrôle du langage a évolué au cours de l'évolution des primates. Pour finir, j'ai présenté des résultats préliminaires qui montre que la correspondance des profils de connectivité en état de repos est une approche prometteuse pour comparer l'organisation fonctionnelle cérébrale inter-espèces / This thesis primarily investigated how the human frontal cortex is organised to learn and use conditional rules linking contextual stimuli with manual, vocal and orofacial actions. My first study demonstrated that in humans: 1) the posterior lateral frontal cortex (pLFC) is organized along a dorso-ventral gradient, where the dorsal premotor cortex and ventral area 44 are involved in manual and vocal-orofacial conditional associations respectively, and 2) the anterior-most cingulate motor area (RCZa) within the mid-cingulate cortex (MCC), contributes to the evaluation of auditory feedback during the trial-and-error learning of the conditional associations. My second study showed that within the MCC, the three CMAs are functionally coupled with the lateral frontal cortex along a rostral-caudal gradient where more rostral regions are implicated in more abstracted levels of behavioral control. These findings provided important contributions to current theories about frontal cortical organization for behavioural control. Lastly, through an extensive review, I revealed that, within the pLFC-MCC network, area 44 and RCZa are part of a homologous brain network that might play a similar role in cognitive vocal/orofacial control across primates. My hypothesized role of this network in the adaptive control of vocal/orofacial actions based on auditory feedback monitoring had been validated, in humans, from my first study. Thus, my thesis had also revealed an important starting point - the area 44-RCZa, for future investigations into the potential neural changes that occurred across primate evolution to support the emergence of human speech abilities

Cortex préfrontal

Contrôle cognitif

Adaptation

Contrôle vocal

Cortex cingulaire moyen

Aire de Broca

Évolution du langage

Cerveau de primate

Prefrontal cortex

Cognitive control

Adaptation

Vocal control

Mid-cingulate cortex

Broca’s area

Speech evolution

Primate brain

612.8

Sensibilização cruzada entre anfetamina e nicotina: avaliação neuroquímica do núcleo acumbens e córtex préfrontal em ratos adolescentes e adultos

Oliveira, Paulo Eduardo Carneiro de

24 September 2009

Made available in DSpace on 2016-06-02T19:22:52Z (GMT). No. of bitstreams: 1 2640.pdf: 532825 bytes, checksum: 85901050327f52892439c98345181eee (MD5) Previous issue date: 2009-09-24 / Financiadora de Estudos e Projetos / Nicotine and psychostimulants are often abused in combination. Drug abuse often begins during adolescence. Exposure to drugs of abuse during adolescence can have long-term consequences. We have previously demonstrated that adolescent rats pretreated with amphetamine displayed behavioral sensitization to nicotine, which persisted until adulthood. Moreover, the pretreatment with nicotine during adolescence sensitized adolescent and adult animals to amphetamine-induced locomotor activation. In the present study we investigated whether the behavioral cross-sensitization between nicotine and amphetamine is related to changes in dopamine or serotonin neurotransmission. To this end adolescent rats (post-natal day 28) were treated with nicotine (0.4 mg/Kg), amphetamine (5.0 mg/Kg) or saline during seven days. Three or thirty days after the last injection animals received an acute injection of nicotine (0.4 mg/Kg), amphetamine (5.0 mg/Kg for adolescents or 1.0 mg/Kg for adults) or saline. Thirty minutes after challenge rats were sacrificed, decapitated and brains removed. Nucleus accumbens (NAcc) and prefrontal cortex (PFC) were dissected and prepared for HPLC (high performance liquid chromatography) analysis. Dopamine, DOPAC, HVA, serotonin and 5-HIAA were measured in these brain regions. Our results showed that: 1) repeated administration of nicotine attenuated the acute effect of amphetamine on NAcc dopamine levels of adolescent rats; 2) repeated administration of nicotine increased the acute effect of amphetamine on PFC dopamine levels of adolescent rats; 3) repeated administration of nicotine, during adolescence, increased the acute effect of amphetamine on PFC dopamine of adult rats. The behavioral cross-sensitization shown previously is not related to alterations in NAcc and PFC concentrations of neurotransmitters and its metabolites. However, neuroadaptations induced by repeated nicotine during adolescence endures until adulthood. / Uma característica comum das substâncias que causam dependência é o aumento gradual e progressivo da atividade locomotora observado após a administração repetida, esse fenômeno é denominado sensibilização comportamental. A sensibilização comportamental resulta de adaptações neuroquímicas e moleculares do sistema dopaminérgico mesocorticolímbico. Foi demonstrado anteriormente a sensibilização cruzada entre nicotina e anfetamina em animais adolescentes e que esse fenômeno permanece até a idade adulta. Nesse trabalho investigamos se a administração repetida com nicotina ou anfetamina, durante a adolescência, pode alterar o efeito agudo dessas substâncias e se essas neuroadaptações persistem até a idade adulta. Para tanto, administramos, por sete dias, nicotina (0,4 mg/Kg), anfetamina (5,0 mg/Kg) ou salina a ratos adolescentes. Três ou trinta dias após a última injeção os animais receberam injeção aguda de nicotina (0,4 mg/Kg), anfetamina (5,0 mg/Kg para adolescentes e 1,0 mg/Kg para adultos) ou salina. Trinta minutos após as injeções os ratos foram sacrificados, decapitados e seus encéfalos removidos. O núcleo acumbens (NAc) e o córtex pré-frontal (CPF) foram retirados e preparados para determinação de dopamina, serotonina e seus metabólitos por cromatografia líquida de alta resolução (HPLC). Os resultados encontrados mostram que: 1) o pré-tratamento com nicotina atenuou o efeito agudo da anfetamina sobre a concentração tecidual de dopamina no Nac de ratos adolescentes; 2) o prétratamento com nicotina aumentou o efeito agudo da anfetamina sobre a concentração tecidual de dopamina no CPF de ratos adolescentes; 3) o prétratamento com nicotina na adolescência aumentou o efeito agudo da anfetamina sobre a concentração tecidual de dopamina no CPF de ratos adultos. Estes resultados não se relacionam à sensibilização cruzada observada anteriormente, mas o tratamento repetido com nicotina promoveu alterações em animais adolescentes que podem ser observadas também na vida adulta.

Sensibilização comportamental

Nicotina

Anfetamina

Neuroquímica

Adolescentes

Sensibilização cruzada

Dopamina

HPLC

Núcleo acumbens

Córtex Pré-Frontal

Nicotine

Amphetamine

Cross-sensitization

Dopamine

Serotonin

Nucleus accumbens

Prefrontal cortex

Adolescents

CIENCIAS BIOLOGICAS::FISIOLOGIA

Tratamento do transtorno depressivo maior pós acidente vascular cerebral com Estimulação Transcraniana por Corrente Contínua (ETCC): ensaio-clínico, randomizado, duplo-cego / Transcranial direct current stimulation for the treatment of poststroke depression: results from a randomized, sham-controlled, double-blinded trial

Leandro da Costa Lane Valiengo

02 July 2015

A depressão pós Acidente Vascular Cerebral (AVC) é uma condição desabilitante que ocorre em um terço dos casos. Há uma dificuldade no tratamento farmacológico devido a efeitos adversos e eficácia limitada. Recentemente, a estimulação trasncraniana por corrente contínua (ETCC) tem demonstrado eficácia no tratamento da depressão unipolar, apesar dos seus efeitos em depressões secundárias serem desconhecidos. O objetivo do estudo foi avaliar a eficácia e segurança da ETCC, uma intervenção não farmacológica, para depressão pós AVC (DPA), através de um ensaio clínico, randomizado, duplo-cego, sham-controlado. Foram incluídos quarenta e oito pacientes sem uso de antidepressivos com DPA foram igualmente divididos em 2 grupos que não diferiram em gênero, idade, gravidade do AVC ou da depressão e nem em outras variáveis clínicas. Foram realiadas 12 sessões de 30 minutos de ETCC com 2mA de corrente com ânodo à esquerda e cátodo à direita em córtex pré-frontal dorsolateral. Para a ETCC sham foi feita um minuto de estimulação somente, seguida por desligamento da máquina até um total de 30 minutos. Foi feita uma análise por intenção de tratamento, na qual o desfecho primário foi mudança na Hamilton Depression Rating Scale na sexta-semana (final). Resposta clínica e remissão foram desfechos secundários. Segurança foi avaliada usando um questionário de efeitos adversos, avaliação da cognição e a escala de mania de Young. A ETCC ativa foi significantemente superior a sham no desfecho final (diferença de médias de 4.7 pontos, IC95% de 2.1 a 7.3, P < 0.001). Taxas de resposta e remissão também foram estatisticamente maior no grupo ativo (37.5% e 20.8%, respectivamente) em relação ao grupo sham (4.1% e 0). O número necessário para tratar para resposta e remissão foi, respectivamente, 3 e 5. A região ou lado do AVC não predisse resposta. Nenhum efeito adverso grave foi relatado e a frequência dos efeitos adversos foi semelhante em ambos grupos. Pacientes e avaliadores foram cegados de forma efetiva. Este é o primeiro estudo controlado que mostra a eficácia da ETCC na DPA. Dessa forma, a ETCC pode ser uma opção terapêutica para esses pacientes / Depression after a stroke is a disabling condition that occurs in up to one-third of cases. Pharmacological treatment is challenging due to adverse effects and presents limited efficacy. Recently, transcranial direct current stimulation (tDCS) has shown efficacy in the treatment of unipolar depression, although its antidepressant effects in secondary depressions are unknown. The objective of the study was to assess the efficacy and safety of tDCS, a nonpharmacological intervention, for post-stroke depression (PSD) in a prospective, randomized, double blind, sham-controlled trial. Forty-eight antidepressant-free patients with PSD were equally divided in two groups that did not differ in gender, age, stroke and depression severity and other clinical variables. Twelve 30-minute sessions of 2-mA anodal left/cathodal right dorsolateral prefrontal tDCS applied over 6 weeks. For sham tDCS we performed 1-min of stimulation only, followed by no stimulation during the remaining period. Intention-to-treat analysis, in which the primary outcome measure was the change in Hamilton Depression Rating scale score at 6 weeks (endpoint). Clinical response and remission were secondary outcomes. Safety was assessed using an adverse effects questionnaire, cognitive assessment and the Young mania rating scale. Active tDCS was significantly superior to sham at endpoint (mean difference, 4.7 points; 95% CI, 2.1 to 7.3; P <.001). Response and remission rates were also statistically higher in active (37.5% and 20.8%, respectively) vs. sham (4.1% and 0) groups. The number needed to treat for response and remission was, respectively, 3 and 5. Stroke region or side did not predict response. No serious adverse effects were reported and the frequency of common adverse effects was similar in both groups. Patients and raters were effectively blinded. This is the first controlled study that demonstrates the safety and clinically meaningful efficacy of tDCS in patients with PSD. Therefore, tDCS could be an option for the treatment of these patients

Acidente vascular cerebral

Córtex pré-frontal

Depressão

Ensaio clínico controlado aleatório

Neuropsiquiatria

Transtorno depressivo maior

Depressive disorder major

Neuropsychiatry

Prefrontal cortex

Randomized controlled trial, Depression

Stroke

Transcranial direct current stimulation

Padrão da atividade locomotora e expressão de EAAC1 e GLT1 no córtex pré-frontal e entorrinal de ratos criados em isolamento a partir do desmame / Pattern of locomotor activity and expression of EAAC1 and GLT1 in prefrontal and entorhinal cortex of rats reared in isolation from weaning

Nayanne Beckmann Bosaipo

20 July 2012

O estresse por isolamento social aplicado em ratos a partir do desmame e mantido durante o desenvolvimento encefálico tem sido utilizado como um modelo experimental de desordens psiquiátricas como a esquizofrenia. Tem sido demonstrado que o isolamento induz alterações morfológicas, comportamentais (como hiperatividade em um novo ambiente) e neuroquímicas semelhantes àquelas que ocorrem em humanos esquizofrênicos. Evidências sugerem que as sinapses glutamatérgicas sejam o sitio primário das anormalidades que ocorrem na esquizofrenia, sendo as alterações dopaminérgicas secundárias às glutamatérgicas. Nesse sentido, alterações nos mecanismos de regulação desta neurotransmissão pelos transportadores de glutamato podem contribuir para o desenvolvimento e/ou manutenção da esquizofrenia. Neste estudo analisamos o padrão de atividade locomotora e a expressão de transportadores de glutamato (EAAC1 e GLT1) no córtex pré-frontal e córtex entorrinal de ratos criados em isolamento a partir do desmame. Ratos Wistar machos (PND21) foram aleatoriamente alocados em 2 grupos (n=11-12): controle (agrupados, 3 animais/caixa) ou isolados (1 animal/caixa) por 10 semanas. Os animais foram testados no campo aberto (arena) durante 20 min. e registrados: números de cruzamentos (exploração horizontal), número de levantamentos (exploração vertical) e tempo despendido, tanto no centro como na periferia da arena. Os grupos foram comparados utilizando ANOVA ou teste t de Student (significante quando p 0.05). Os animais foram anestesiados (uretana-Sigma, 25%, 5ml/kg), perfundidos e os encéfalos retirados, congelados e posteriormente utilizados nos experimentos de imunoistoquímica. Secções (40m) do córtex pré-frontal (CPF) e córtex entorrinal (CE) foram utilizadas para o estudo da expressão de EAAC1 e GLT1. A criação em isolamento induziu hiperatividade, com um aumento no número total de cruzamentos em relação aos animais agrupados (F1,22=0,38; p<0,05), sendo mais consistente na periferia da arena e após 5 minutos de teste (73%, (F1,22=14,08; p<0,001). Em contraste, o isolamento induziu redução no número total de levantamentos (F1,22=0,27; p=0,05), principalmente no centro da arena (58%, F1,22=12,48; p<0,01), nos primeiros 15 minutos de teste e significante no 1° e 3° blocos de tempo (BT1 e BT3). Na periferia o isolamento induziu aumento significante no número de levantamentos em BT2 e BT3. O tempo despendido no centro e na periferia da arena pelos animais criados em isolamento foi, respectivamente, reduzido (54%; F1,22=11,11; p<0,001) e aumentado (65%; F1,22=11,20; p<0,01) quando comparados aos animais agrupados. A expressão de EAAC1 foi significantemente aumentada pelo isolamento no CPF (38%, t= 2,730, p=0,017). Em contraste, nenhuma diferença foi encontrada no CE (t= 1,892; p= 0,081). O isolamento não induziu alteração no número de células imunopositivas para GLT1 no CPF (t=-1,28; p=0,21). Entretanto, marcação fluorescente de GLT1 foi observada associada a células gliais e neuroniais do CPF e CE. Os resultados comportamentais sugerem: i) ratos Wistar criados em isolamento social apresentam hiperatividade em novo ambiente; ii) a hiperatividade locomotora somente é detectável após períodos maiores que cinco minutos de exposição a um novo ambiente; iii) o padrão de exploração apresentado pelos animais demonstra clara preferência pela periferia da arena. Os resultados moleculares fornecem evidências para a participação dos transportadores de glutamato na redução da neurotransmissão glutamatérgica no CPF de ratos criados em isolamento a partir do desmame. / Isolation rearing of rats from weaning has been used as an experimental model of psychiatric disorders like schizophrenia. It has been demonstrated that isolation induces morphological, behavioral (like hyperactivity in a novel environment) and neurochemical changes similar to those reported for humans with schizophrenia. Evidence suggest that glutamatergic synapses might be the site of primary abnormalities in this disorder with the dopaminergic changes being secundary to the glutamatergic ones. In this context, changes on the mechanisms of regulation of the glutamatergic neurotransmission through glutamate transporters may contribute to the development and/or maintenance of schizophrenia. In this study we analyzed the pattern of locomotor activity and the expression of glutamate transporters (EAAC1 and GLT1) in prefrontal cortex and entorhinal cortex of rats reared in social isolation from weaning. Male Wistar rats (PND 21) were randomly allocated in 2 groups (n=11-12): control (grouped, 3 animals/cage) or isolated (1 animal/cage) for 10 weeks. The animals were tested in the open field (arena) for 20min. and recorded: number of crossings (horizontal exploration), number of rearings (vertical exploration) and time spent either at the center or at the periphery of the arena. The groups were compared using ANOVA or Sudents \"t\" test (significance level was set at p 0.05). The animals were anesthetized (urethane-Sigma, 25%, 5ml/kg), perfused and the brains removed, frozen and further used on the experiments of immunohistochemistry. Sections (40m) of the prefrontal córtex (PFC) and entorhinal córtex (EC) were used for studying the expression of EAAC1 and GLT1. Isolation rearing induced hyperactivity, with an increase in the number of crossings related to grouped animals (F1,22=0,38; p<0,05), being more consistent at the periphery of the arena and after 5 minutes of test (F1,22=14,08; p<0,001). In contrast, isolation induced a decrease in the total number of rearings (F1,22=0,27; p=0,05), mainly in the center of the arena (58%, F1,22=12,48; p<0,01), in the first 15 minutes of test and significant on the 1st and 3rd blocks of time (BT1 e BT3). In the periphery isolation induced a significant increase in the number of rearings in BT2 and BT3. The time spent in both center and periphery of the arena by the rats reared in isolation was, respectively, decreased (54%; F1,22=11,11; p<0,01) and increased (65%; F1,22=11,20; p<0,01) when compared to grouped rats. The expression of EAAC1 was significantly increased by isolation in PFC (38%, t = 2,730, p = 0,017). In contrast, no change was found in EC (t = 1,892, p = 0,081). Isolation rearing did not induce alterations in the number of immunopositive cells for GLT1 in PFC (t= -1,28; p = 0,21). However, fluorescent labeling of GLT1 was seen associated to both glial cells and neuronal cells. The behavioral results suggest: i) Wistar rats reared in social isolation present hyperactivity in a novel environment; ii) the hyperactivity is only detectable after periods longer than 5 minutes; iii) the pattern of exploration showed by the animals demonstrate clear preference for the periphery of the arena. The molecular results provide evidence for the involvement of glutamate transporters on the reduction of glutamatergic neurotranmission in PFC of rats reared in isolation from weaning.

Atividade Locomotora

Campo aberto

Córtex entorrinal.

Córtex pré-frontal

EAAC1

Esquizofrenia

GLT1

Imunoistoquímica

Isolamento social

EAAC1

Entorhinal cortex.

GLT1

Immunohistochemistry

Isolation rearing

Locomotor activity

Open field.

Prefrontal cortex

Schizophrenia

Disfunção neuroquímica na depressão periparto / Neurochemistry dysfunction in peripartum depressive disorder

Carlos Eduardo Rosa

16 March 2016

A depressão periparto (PPD) é subtipo altamente prevalente e subdiagnosticado do transtorno depressivo maior (MDD), e causa um importante sofrimento para a mulher, sua família e seu filho. Uma interação complexa entre hormônios, neurotransmissores e fatores genéticos e ambientais pode estar envolvida na etiologia da PPD. Contudo, estudos de neuroimagem na PPD ainda são escassos, particularmente os que identificam alterações neuroquímicas. Sabe-se que a região do córtex pré frontal dorsolateral (dlPFC) está relacionada à funções executivas no circuito pré frontal, e juntamente com o giro do cíngulo anterior (ACG) faz parte das vias neuronais envolvidas no processamento emocional, desde a geração, regulação e reavaliação do estado afetivo. Existem evidências de que ambas as áreas estejam disfuncionais na MDD. A avaliação neuroquímica obtida pela espectroscopia de próton por ressonância magnética (MRS) permite inferir o metabolismo, a neurotransmissão e a viabilidade do tecido neuronal de interesse destas áreas fronto-límbicas. Objetivo: comparar puérperas com depressão periparto (grupo PPD) com puérperas saudáveis (grupo HP) quanto à avaliação neuroquímica no dlPFC esquerdo e no ACG bilateral. Métodos: 36 puérperas do grupo PPD e 25 puérperas do grupo HP foram submetidas à duas entrevistas psiquiátricas estruturadas e à aplicação de questionários e escalas psicométricas, sendo a segunda avaliação realizada seccionalmente à MRS. A MRS foi adquirida pro MRI com campo de 3 Tesla, estando o volume de interesse (VOI) posicionado no dlPFC esquerdo e no ACG bilateral e processada pelo software LCModel. Os resultados neuroquímicos expressos em valores absolutos e normalizados pela creatina (razão metabólito/creatina) foram analisados por ANCOVA, incluindo a idade, o tempo de puerpério e o tipo de contraceptivo, enquanto covariáveis. Resultados: No dlPFC, o grupo PPD apresentou menores valores de Glu/Cr (-0,17; p=0,05), Glx (-0,95 mM; p=0,04), Glx/Cr (-0,22; p=0,03), NAA (-0,60 mM; p<0,01), e NAA/Cr (-0,13; p=0,02) em relação ao grupo HP. No ACG, o uso de hormônios contraceptivos somente com progestágenos resultou em um aumento dos valores de Glu (2,18 mM; p=0,03), Glx (1,84 mM; p=0,03), e redução de Cho/Cr (-0,08; p=0,03) quando comparados ao grupo que não utilizou somente progestágenos, independentemente dos grupos HP e PPD. Conclusão: Os níveis reduzidos de Glu e NAA no grupo PPD estão relacionados, respectivamente, à disfunção metabólica glutamatérgica e neuroglial no dlPFC, o que pode explicar sintomas cognitivos também relacionados à PPD, tal como já verificado no MDD. O uso de hormônios contraceptivos com progestágenos isoladamente interferiu com a neuroquímica do ACG, mas não se relacionou com a PPD. Embora o aumento do glutamato possa sugerir uma hiperfuncionalidade do ACG, e a redução da Cho/Cr representar diminuição de \"turnover\" da membrana lipídica ou da transdução sináptica, seu significado clínico e fisiopatológico ainda é incerto. Estes resultados contribuem com a compreensão dos substratos neuroquímicos de PPD / Peripartum depression (PPD) is a highly prevalent subtype of major depressive disorder (MDD) related to a significant loss for mother, family and baby. An Interaction between hormones, genetic, and environmental factors must be involved in its etiology. However, neuroimaging studies on PPD are still rare, particularly those that identify neurochemical changes. However, neuroimaging studies in PPD are still rare, particularly those that identify neurochemical changes. It is known that the region of the dorsolateral prefrontal cortex (dlPFC) is related to executive functions in the prefrontal circuit, and together with the anterior cingulate gyrus (ACG) is part of the neural pathways involved in emotional processing, including the generation, regulation, and reappraisal of affective state. And, there is evidence that both areas are dysfunctional in MDD. The neurochemical evaluation obtained by spectroscopy of proton magnetic resonance (MRS) allows to infer metabolism, neurotransmission and the viability of the neuronal tissue of interest these frontal-limbic areas. Objective: Compare postpartum women with peripartum depression (PPD group) with healthy postpartum women (HP group) regarding the neurochemical evaluation in the left dlPFC and bilateral ACG. Methods: 36 postpartum women of PPD group and 25 postpartum women of the HP group were subjected to two structured psychiatric interviews and questionnaires and psychometric scales, with the second evaluation performed sectionally at MRS. The MRS was obtained by 3-T MRI system with the volume of interest (VOI) positioned on the left dlPFC and bilateral ACG and processed by LC Model software. The neurochemical results expressed in absolute values and normalized by creatine (reason metabolite/creatine) were analyzed using ANCOVA, including age, postpartum time, the type of contraceptive as covariates. Results: In the dlPFC, PPD group presented significantly lower values of Glu/Cr (-0.17; p=0.05), Glx (-0.95mM; p=0.04), Glx/Cr (-0.22; p=0.03), NAA (-0.60mM; p<0.01), and NAA/Cr (-0.13; p=0.02) than HP. In ACG, progestogens isolated contraceptive hormones use resulted in significantly increased Glu (2.18mM; p=0.03), Glx (1.84mM; p=0.03), and reduced Cho/Cr (-0.08; p=0.03), compared to women without use them, regardless of diagnostic groups. Conclusions: The reduced levels of Glu and NAA in the PPD group are related respectively to the glutamatergic and neuroglial metabolic dysfunction in the dlPFC, which may explain cognitive symptoms also related to PPD as already verified in MDD. Progestogens isolated contraceptive hormones use interfered with neurochemistry of ACG, but not associated with PPD. Although the increase of glutamate may suggest an overactive ACG, and lower Cho/Cr represent decrease of the lipid membrane turnover or synaptic transduction its clinical and pathophysiological significance remains uncertain. These results contribute to the understanding of the neurochemical substrates of PPD

Córtex Pré-frontal Dorsolateral

Depressão Periparto

Giro do Cíngulo Anterior

Transtorno Depressivo Maior

Anterior Cingulate Gyrus

Dorsolateral Prefrontal Cortex

Magnetic Resonance Spectroscopy

Major Depressive Disorder

Peripartum Depression

Ressonância magnética estrutural em pacientes com transtorno afetivo com características psicóticas avaliados no primeiro contato com serviço de saúde mental / Structural magnetic resonance in subjects with psychotic affective disorders assessed in the first contact with the health care system

Cintia de Azevedo Marques Périco

12 December 2007

Os transtornos afetivos são altamente prevalentes dentre os transtornos mentais, principalmente Transtorno Afetivo Bipolar (TAB) e Depressão Maior Unipolar (DMU), apresentando altas taxas de morbi-mortalidade. Estudos prévios de Ressonância Magnética (RM) têm identificado anormalidades estruturais cerebrais em indivíduos com TAB e DMU quando comparados a controles normais. Entretanto, nenhum destes estudos foi realizado a partir da comparação direta entre pacientes com DMU e TAB de início recente, nem comparou separadamente tais grupos com amostras representativas de controles assintomáticos provenientes de mesma região geográfica. No presente estudo, definimos a priori que regiões do circuito córtico-límbico-talâmico-estriatal estariam alteradas quando comparados indivíduos com TAB, DMU e controles normais diretamente entre si, em amostra de pacientes com quadros graves de sintomatologia psicótica e pareada com controles normais selecionados na mesma área geográfica dos pacientes. Foram selecionados 46 pacientes (20 com DMU e 26 com TAB) que tiveram contato pela primeira vez com serviço de saúde mental após início de sintomas psicóticos e 62 controles normais. Tanto pacientes quanto controles foram submetidos à RM em aparelho de 1,5 Tesla. Os diagnósticos foram baseados no DSM-IV e confirmados após 1 ano da realização da RM. As imagens foram analisadas pelo método automatizado de processamento denominado morfometria baseada no voxel (voxel-based morphometry). A comparação entre os grupos mostrou redução significativa de substância cinzenta regional em pacientes com DMU comparados aos controles (p<0,05, corrigido para comparações múltiplas) em duas regiões cerebrais selecionadas a priori: córtex pré-frontal dorsolateral (CPFDL) bilateralmente e giro parahipocampal posterior esquerdo. Na comparação direta entre pacientes com DMU e TAB encontramos uma redução de substância cinzenta de CPFDL direito em pacientes com DMU, como tendência a significância estatística (p<0,10, corrigido para comparações múltiplas). Nossos achados mostram que anormalidades volumétricas de CPFDL e região temporal medial estão presentes em pacientes com DMU em primeiro episódio psicótico, mas não em pacientes com TAB com gravidade de sintomas semelhante. / Affective disorders are highly prevalent mental disorders, mainly Major Depressive Disorder (MDD) and Bipolar Disorder (BD), with high morbidity and mortality rates. Previous morphometric magnetic resonance imaging (MRI) studies have identified brain volumetric abnormalities in samples of subjects suffering from MDD or BD. However, none of these have conducted direct brain volume comparisons between patients with recent-onset MDD and BD, nor contrasted them separately against representative groups of asymptomatic controls recruited from exactly the same environment. In the present study, we defined a priori that brain regions involved in cortico-limbic-thalamic-striatal circuits would present volume abnormalities when comparing subjects with MDD and BD with psychotic features, in their first contact with the health care system in Brazil, and a control sample of next-door asymptomatic neighbors. Forty-six patients (20 MDD and 26 BD) and 62 controls were examined with MRI, using an equipment of 1.5 Tesla. Diagnoses were based on DSM-IV, and confirmed one year after scanning. Image processing was conducted using voxel-based morphometry methods. Between-group comparisons showed significant regional gray matter deficits in MDD subjects relative to controls (p<0.05, corrected for multiple comparisons), involving two brain regions where abnormalities in mood disorder patients had been predicted a priori: the dorsolateral prefrontal cortex (DLPFC) bilaterally and the left posterior parahippocampal gyrus. In the direct comparison between MDD and BD patients, the right-sided finding of decreased DLPFC gray matter in the former group retained trend levels of significance (p<0.10 corrected). Our findings indicate that significant structural abnormalities of the DLPFC and medial temporal region are present in patients with MDD in their first episode with psychotic features, but not in BD subjects with symptoms of similar severity.

Córtex pré-frontal

Giro para-hipocampal.

Imagem por ressonância magnética

Transtorno bipolar

Transtorno depressivo

Transtornos psicóticos

Bipolar disorder

Depressive disorder

Magnetic ressonance imaging

Parahippocampal gyrus

Prefrontal cortex

Psychotic disorders

Papel do córtex pré-frontal medial na compreensão da linguagem figurada: experimento com eletroencefalografia e estimulação cerebral não-invasiva

Baptista, Nathalia Ishikawa

05 August 2014

Made available in DSpace on 2016-03-15T19:40:18Z (GMT). No. of bitstreams: 1 Nathalia Ishikawa Baptista.pdf: 1435875 bytes, checksum: 8415993ce2a61757efe0d96f926c9095 (MD5) Previous issue date: 2014-08-05 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior / Verbal irony is a figurative form of communication between human beings, to understand it a specific ability to infer and predict the ironist intention is essential called Theory of Mind. Currently researches using spatial correlation techniques showed activation of the Medial Prefrontal Cortex (MPFC) on irony comprehension tasks. Thus, this thesis aimed to investigate the role of this area irony comprehension. Therefore the Transcranial direct current stimulation (tDCS) was used, i.e. the induction of low intensity electric current on specific cortical structures. The effects of stimulation depend on the current polarity, and thus, it is possible to investigate how the modulation of target area affects the performance in a cognitive task. Thus, 60 participants were recruited; they were all right handed and match the inclusion criteria. They were allocated to one of three groups of stimulation (anode, cathode or placebo), and received the tDCS for twenty minutes over the MPFC. After, the participants performed a test of verbal irony comprehension, with 204 stories visually presented. This phase was conducted during the EEG recording of the participants. Thus, the effects of tDCS over MPFC were accessed by: i. the behavioral test performance (measured by total score and average reaction time); ii. the brain activity underlying the task (measured by event-related evoked potentials - ERP - N400 and P600). The results indicate the involvement of the MPFC in semantic integration of affective aspects of figurative language. The increased cortical excitability of the area (anodal stimulation) resulted in a decrease of cognitive demand to integrate these aspects; in addition, it decreased the reaction time for the semantic incongruences. Thus, our results indicate that irony comprehension depends on the integration of information: cognitive and affective. Hence for a true appreciation of it s meaning is necessary to develop language skills as well the Theory of Mind. / A ironia verbal é uma forma figurada de comunicação entre seres humanos, para compreendê-la é fundamental a habilidade de inferir e predizer a intenção daquele que emite a ironia a chamada Teoria da Mente. Atualmente as pesquisas com técnicas de correlação espacial evidenciaram a ativação do Córtex Pré-frontal Medial (CPFM) na compreensão de ironia. Sendo assim, a presente dissertação teve como objetivo investigar o papel dessa estrutura na compreensão da ironia. Para isso, foi utilizada a técnica de Estimulação transcraniana por corrente contínua (ETCC), ou seja, a indução de corrente elétrica de baixa intensidade sobre estruturas corticais específicas. Os efeitos dessa estimulação dependem da polaridade da corrente, e desta forma, é possível verificar como a modulação da área-alvo interfere no desempenho em uma tarefa cognitiva. Sendo assim, foram recrutados 60 participantes de pesquisa, que deveriam ser destros e estarem de acordo com os critérios de inclusão. Eles foram alocados em um dos três grupos de estimulação (anódica, catódica ou placebo), e receberam a ETCC por vinte minutos em CPFM. Após esta fase, os participantes realizaram um teste de compreensão de ironia verbal, com 204 histórias apresentadas visualmente. Esta fase foi realizada durante o registro eletroencefalográfico (EEG) dos participantes. Desta forma, os efeitos da ETCC em CPFM foram verificados: i. no desempenho comportamental no teste (mensurado pelo total de acertos e média de tempo de reação/resposta); ii. assim como na atividade cerebral subjacente a tarefa (mensurada pelos Potenciais evocados relacionados a evento ERP N400 e P600). Os resultados indicam o envolvimento do CPFM na integração semântica de aspectos afetivos da linguagem figurada. O aumento da excitabilidade cortical desta área (estimulação anódica) resultou em uma menor demanda cognitiva para integrar estes aspectos, além disso, diminuiu o tempo de resposta para as incongruências semânticas. Desta forma, entende-se que a compreensão da ironia depende da integração de informações: cognitivas e afetivas. E para que haja a verdadeira apreciação de seu significado é necessário o desenvolvimento de habilidades linguísticas e de Teoria da Mente.

ironia

Teoria da Mente

eletroencefalografia

ERP

córtex pré-frontal medial

irony

Theory of Mind

transcranial direct current stimulation

eletroencephalography

ERP

Medial Prefrontal Cortex