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Sleep and Alzheimer’s disease: A critical examination of the risk that Sleep Problems or Disorders particularly Obstructive Sleep Apnea pose towards developing Alzheimer’s diseaseBubu, Omonigho A. Michael 17 November 2017 (has links)
This dissertation is a critical examination of the relationship between sleep problems and/or disorders, particularly Obstructive Sleep Apnea (OSA) and Alzheimer Disease (AD). First, I conducted an exhaustive systematic review of existing literature, and identified gaps in research that led to specific research aims. For the first aim, I conducted the first ever-published meta-analysis examining sleep, cognitive decline and AD, providing an aggregate effect of sleep on AD. Second, focusing on OSA, I conducted a study examining OSA’s effect on longitudinal changes on AD biomarkers in cognitive normal, MCI and AD subjects, using data from the Alzheimer Disease Neuroimaging Initiative (ADNI). Lastly, I conducted a review, integrating over 3 decades of research examining OSA and cognition; OSA and subsequent cognitive decline; and OSA and AD; with particular focus in appreciating the heterogeneity of OSA and its outcomes in distinct age groups.
Results and implications from my research indicate that ample evidence exists linking sleep impairments and circadian regulating mechanisms directly to clinical symptoms in AD. Sleep problems and/or disorders increases your risk of cognitive decline and AD. OSA is associated with increased AD biomarker burden over time, and effects longitudinal changes in these biomarkers, such that OSA subjects progress faster than non-OSA subjects do. OSA may be age-dependent in older adults (60 – 70 years old) and the elderly (70 years and above) and is associated with neurodegenerative diseases particularly, cognitive decline and AD. Intermittent hypoxia and sleep fragmentation are two main processes by which OSA induces neurodegenerative changes. Therefore, clinical interventions aimed at OSA, such as treatment with CPAP or dental appliances, in cognitive normal and MCI patients, could possibly slow the progression of cognitive impairment to AD.
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Vaskulární změny a atrofie hipokampů v Enhanced Cued Recall testu / Vascular changes and hippocampal atrophy in Enhanced Cued Recall testVaníčková, Monika January 2016 (has links)
Memory structure, memory assessment, Grober-Buschke paradigm, Alzheimer disease, and vascular dementia were discussed in the first part of the present thesis. Present study aims to examine the relationship between white matter changes, hippocampal atrophy and the performance in Enhanced Cued Recall test in nondemented geriatric population (n = 104). Partial neparametric correlations were used while controlling for age and Fazekas score. Medium correlations were found between left/right hippocampal volumes and free and total recall. No correlations were found between Fazekas score and ECR scores while controlling for age and left and right hippocampal volumes. Keywords: hippocampal atrophy, white matter changes, cued recall, ECR
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Associação dos níveis de BDNF com volume do hipocampo no comprometimento cognitivo leve e na doença de AlzheimerBorba, Ericksen Mielle January 2016 (has links)
Introdução: Perda de memória é um dos sintomas mais comuns em pacientes nos estágios iniciais da doença de Alzheimer; esses déficits são um reflexo do envolvimento da formação do hipocampo. O BDNF tem sido relacionado com a plasticidade do hipocampo. Neste sentido, as combinações de biomarcadores, como, por exemplo, a volumetria do hipocampo, pode apresentar um maior valor preditivo para diferenciar doença de Alzheimer do envelhecimento normal em pacientes com comprometimento cognitivo leve. Objetivo: A presente tese de doutorado teve como objetivo avaliar os níveis séricos do BDNF e o volume do hipocampo em pacientes com demência devido à doença de Alzheimer, Comprometimento Cognitivo Leve (CCL) e idosos saudáveis. Métodos: Para realização do estudo foram selecionados 10 idosos saudáveis, 10 CCL e 13 pacientes com demência devido à doença de Alzheimer pelos critérios NIA-AA. Todos participantes foram submetidos a uma avaliação cognitiva. Para as análises do BDNF, foi utilizado método de ELISA e para as análises de volumetria do hipocampo as imagens foram obtidas por meio de equipamento de ressonância de 1.5T e os volumes obtidos por meio do programa NeuroQuant®. Resultados: Idosos saudáveis apresentaram níveis séricos mais elevados de BDNF do que os CCL e pacientes com demência. O grupo de pacientes com demência apresentou menor volume total do hipocampo do que os idosos saudáveis e os CCL. Não houve correlação significativa do BDNF sérico com volume do hipocampo. Conclusão: Considerando nossos resultados em conjunto (baixos níveis de BDNF nos grupos CCL e demência devido à DA e menor volume do hipocampo na demência devido à AD), podemos supor que a diminuição dos níveis de BDNF ocorre antes da lesão neuronal expressa pela redução do hipocampo. / Introduction: Memory impairment is the most common symptom in patients in the early stages of Alzheimer's disease; this deficit is a reflection of the involvement of the hippocampal formation. BDNF has been linked to the hippocampal plasticity. Combinations of biomarkers, such as the hippocampal volumetry may have higher predictive value for differentiating Alzheimer's disease from normal aging in patients with mild cognitive impairment. Objective: The objective of present thesis was to evaluate serum levels of BDNF and hippocampal volume in patients with Mild Cognitive Impairment (MCI) and dementia due to Alzheimer's disease, and healthy elderly participants. Method: Ten healthy elderly subjects, 10 MCI and 13 patients with dementia due to Alzheimer's Disease (NIA-AA criteria) were selected for the study. All participants were assessed cognitively. The ELISA method was used for BDNF analysis, and the analysis of hippocampal volumetric images were acquired with 1.5T magnetic resonance equipment and volumes obtained with NeuroQuant® program. Results: Healthy elderly had higher BDNF serum levels than MCI and dementia due to AD patients. The group of dementia patients had lower total hippocampal volume than MCI and healthy elderly participants. No significant correlation between serum BDNF and hippocampal volume was observed. Conclusion: Taking our results together (lower BDNF levels in MCI and dementia due to AD and smaller hippocampal volume in dementia due to AD) we can hypothesize that the decrease of BDNF may start before the establishment of neuronal injury expressed by the hippocampal reduction.
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Avaliação dos efeitos das medicações antiepilépticas na conectividade cerebral de pacientes com epilepsia do lobo temporal por meio da neuroimagem / Analysis of the antiepileptic medications effects on the cerebral connectivity of patients with temporal lobe epilepsy through neuroimagingBellentani, Fernanda Furlanetto [UNESP] 17 February 2017 (has links)
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Previous issue date: 2017-02-17 / A conectividade funcional é anormal na epilepsia do lobo temporal mesial (ELTm). O objetivo deste estudo foi investigar os efeitos de fármacos antiepilépticos (FAES) na conectividade funcional de pacientes com ELTm. Para isso, 31 pacientes com ELTm (16 à direita e 15 à esquerda) e 36 controles foram investigados. Sequências 3D volumétricas T1 e imagens funcionais a partir de sinal BOLD foram adquiridas em um equipamento 3T. Os dados da ressonância magnética funcional (RMf) em repouso foram processados e analisados utilizando o programa CONN. Para cada sujeito, duas formas de análise foram realizadas: uma de correlação entre as várias regiões de interesse e outra de região interesse para todos os voxels. A análise de grupos foi feita utilizando um modelo linear geral com nível de significância de p < 0,05 corrigido para múltiplas comparações. Foram realizadas comparações entre pacientes com ELTm (direita ou esquerda) e controles, seguidas de comparações de acordo com a carga de FAEs. A partir dessas análises, foi constatado uma redução de conectividade com volume total de 9092 mm3 (p<0,0001), em pacientes com ELTm esquerda e 5234 mm3 (p<0,0001), em pacientes com ELTm direita . Quando considerada a carga de medicação, pacientes com ELTm esquerda, recebendo doses altas, apresentaram redução de conectividade nas regiões temporais. Nos pacientes que recebiam doses baixas, essa redução atingiu uma área total mais extensa, no córtex frontal medial, na região posterior do cíngulo e pré-cúneo. Para o lado direito, em pacientes recebendo doses altas, a redução de conectividade foi observada apenas na área do cótex frontal medial. Nos que receberam doses baixas, 2 áreas com redução foram observadas (córtex frontal medial e região posterior do cíngulo) e com uma extensão maior. A análise de correlação envolvendo regiões de interesse mostrou, para ambos os lados, que o circuito amígdalo-hipocampal e a rede de modo padrão apresentaram maior conectividade quando utilizadas maiores doses de FAEs. Com base nesses resultados, foram confirmadas áreas de conectividade funcional anormal em pacientes com ELTm e que se apresentam mais difusas em pacientes com ELTm esquerda. Conclui-se também que as doses de medicamentos podem influenciar nestas observações, uma vez que o aumento de dose tende a normalizar a conectividade funcional cerebral. / The functional connectivity is abnormal in mesial temporal lobe epilepsy (MTLE). The objective of this study was to investigate the effects of antiepileptic drugs (AED) laterality and medication effect in the functional connectivity of MTLE. For this, 31 patients with MTLE (16 right and 15 left) and 36 controls were investigated. 3D volumetric sequences T1 and functional images from BOLD signal were acquired in a 3T equipment. Functional magnetic resonance imaging (fMRI) data were processed and analyzed using the CONN program. Two forms of analysis were performed for each patient: one of correlation between the various regions of interest and other of region of interest for all the voxels. The group analyzes was done following a general linear model with a level of significance of p < 0,05 corrected for the multiple comparisons. Comparisons were made between patients with MTLE (right or left) and controls, following of comparisons according to the AED. From these analysis, it was observed that in patients with left MTLE, there was a reduction in connectivity with total volume of 9092 mm³ (p<0,0001) and in patients with right MTLE, the areas of decreased connectivity totaled 5234 mm³ (p<0,0001). When considering the medication load, patients with left MTLE receiving high doses presented reduced connectivity in the temporal regions and in patients receiving low doses, this reduction reached a more extensive total area, in the medial frontal cortex, in the posterior region of the cingulate and pre-cuneous. To the right side, in patients receiving high doses, a reduced connectivity was observed only in the area of the medial frontal cortex, whereas in those receiving low doses, 2 areas with reduction were observed (medial frontal cortex and posterior cingulate region). The analysis of correlation involving regions of interest showed, to both sides that the amygdalo-hippocampal circuit and the network pattern mode presented greater connectivity when higher doses of AED. Based on these results were confirmed areas of abnormal functional connectivity in patients with MTLE and are more difuse in patients with left MTLE. It was also concluded that drug doses can influence these observations, once the doses increase tends to normalize functional brain connectivity.
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Associação dos níveis de BDNF com volume do hipocampo no comprometimento cognitivo leve e na doença de AlzheimerBorba, Ericksen Mielle January 2016 (has links)
Introdução: Perda de memória é um dos sintomas mais comuns em pacientes nos estágios iniciais da doença de Alzheimer; esses déficits são um reflexo do envolvimento da formação do hipocampo. O BDNF tem sido relacionado com a plasticidade do hipocampo. Neste sentido, as combinações de biomarcadores, como, por exemplo, a volumetria do hipocampo, pode apresentar um maior valor preditivo para diferenciar doença de Alzheimer do envelhecimento normal em pacientes com comprometimento cognitivo leve. Objetivo: A presente tese de doutorado teve como objetivo avaliar os níveis séricos do BDNF e o volume do hipocampo em pacientes com demência devido à doença de Alzheimer, Comprometimento Cognitivo Leve (CCL) e idosos saudáveis. Métodos: Para realização do estudo foram selecionados 10 idosos saudáveis, 10 CCL e 13 pacientes com demência devido à doença de Alzheimer pelos critérios NIA-AA. Todos participantes foram submetidos a uma avaliação cognitiva. Para as análises do BDNF, foi utilizado método de ELISA e para as análises de volumetria do hipocampo as imagens foram obtidas por meio de equipamento de ressonância de 1.5T e os volumes obtidos por meio do programa NeuroQuant®. Resultados: Idosos saudáveis apresentaram níveis séricos mais elevados de BDNF do que os CCL e pacientes com demência. O grupo de pacientes com demência apresentou menor volume total do hipocampo do que os idosos saudáveis e os CCL. Não houve correlação significativa do BDNF sérico com volume do hipocampo. Conclusão: Considerando nossos resultados em conjunto (baixos níveis de BDNF nos grupos CCL e demência devido à DA e menor volume do hipocampo na demência devido à AD), podemos supor que a diminuição dos níveis de BDNF ocorre antes da lesão neuronal expressa pela redução do hipocampo. / Introduction: Memory impairment is the most common symptom in patients in the early stages of Alzheimer's disease; this deficit is a reflection of the involvement of the hippocampal formation. BDNF has been linked to the hippocampal plasticity. Combinations of biomarkers, such as the hippocampal volumetry may have higher predictive value for differentiating Alzheimer's disease from normal aging in patients with mild cognitive impairment. Objective: The objective of present thesis was to evaluate serum levels of BDNF and hippocampal volume in patients with Mild Cognitive Impairment (MCI) and dementia due to Alzheimer's disease, and healthy elderly participants. Method: Ten healthy elderly subjects, 10 MCI and 13 patients with dementia due to Alzheimer's Disease (NIA-AA criteria) were selected for the study. All participants were assessed cognitively. The ELISA method was used for BDNF analysis, and the analysis of hippocampal volumetric images were acquired with 1.5T magnetic resonance equipment and volumes obtained with NeuroQuant® program. Results: Healthy elderly had higher BDNF serum levels than MCI and dementia due to AD patients. The group of dementia patients had lower total hippocampal volume than MCI and healthy elderly participants. No significant correlation between serum BDNF and hippocampal volume was observed. Conclusion: Taking our results together (lower BDNF levels in MCI and dementia due to AD and smaller hippocampal volume in dementia due to AD) we can hypothesize that the decrease of BDNF may start before the establishment of neuronal injury expressed by the hippocampal reduction.
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Associação dos níveis de BDNF com volume do hipocampo no comprometimento cognitivo leve e na doença de AlzheimerBorba, Ericksen Mielle January 2016 (has links)
Introdução: Perda de memória é um dos sintomas mais comuns em pacientes nos estágios iniciais da doença de Alzheimer; esses déficits são um reflexo do envolvimento da formação do hipocampo. O BDNF tem sido relacionado com a plasticidade do hipocampo. Neste sentido, as combinações de biomarcadores, como, por exemplo, a volumetria do hipocampo, pode apresentar um maior valor preditivo para diferenciar doença de Alzheimer do envelhecimento normal em pacientes com comprometimento cognitivo leve. Objetivo: A presente tese de doutorado teve como objetivo avaliar os níveis séricos do BDNF e o volume do hipocampo em pacientes com demência devido à doença de Alzheimer, Comprometimento Cognitivo Leve (CCL) e idosos saudáveis. Métodos: Para realização do estudo foram selecionados 10 idosos saudáveis, 10 CCL e 13 pacientes com demência devido à doença de Alzheimer pelos critérios NIA-AA. Todos participantes foram submetidos a uma avaliação cognitiva. Para as análises do BDNF, foi utilizado método de ELISA e para as análises de volumetria do hipocampo as imagens foram obtidas por meio de equipamento de ressonância de 1.5T e os volumes obtidos por meio do programa NeuroQuant®. Resultados: Idosos saudáveis apresentaram níveis séricos mais elevados de BDNF do que os CCL e pacientes com demência. O grupo de pacientes com demência apresentou menor volume total do hipocampo do que os idosos saudáveis e os CCL. Não houve correlação significativa do BDNF sérico com volume do hipocampo. Conclusão: Considerando nossos resultados em conjunto (baixos níveis de BDNF nos grupos CCL e demência devido à DA e menor volume do hipocampo na demência devido à AD), podemos supor que a diminuição dos níveis de BDNF ocorre antes da lesão neuronal expressa pela redução do hipocampo. / Introduction: Memory impairment is the most common symptom in patients in the early stages of Alzheimer's disease; this deficit is a reflection of the involvement of the hippocampal formation. BDNF has been linked to the hippocampal plasticity. Combinations of biomarkers, such as the hippocampal volumetry may have higher predictive value for differentiating Alzheimer's disease from normal aging in patients with mild cognitive impairment. Objective: The objective of present thesis was to evaluate serum levels of BDNF and hippocampal volume in patients with Mild Cognitive Impairment (MCI) and dementia due to Alzheimer's disease, and healthy elderly participants. Method: Ten healthy elderly subjects, 10 MCI and 13 patients with dementia due to Alzheimer's Disease (NIA-AA criteria) were selected for the study. All participants were assessed cognitively. The ELISA method was used for BDNF analysis, and the analysis of hippocampal volumetric images were acquired with 1.5T magnetic resonance equipment and volumes obtained with NeuroQuant® program. Results: Healthy elderly had higher BDNF serum levels than MCI and dementia due to AD patients. The group of dementia patients had lower total hippocampal volume than MCI and healthy elderly participants. No significant correlation between serum BDNF and hippocampal volume was observed. Conclusion: Taking our results together (lower BDNF levels in MCI and dementia due to AD and smaller hippocampal volume in dementia due to AD) we can hypothesize that the decrease of BDNF may start before the establishment of neuronal injury expressed by the hippocampal reduction.
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Avaliação dos efeitos das medicações antiepilépticas na conectividade cerebral de pacientes com epilepsia do lobo temporal por meio da neuroimagem.Bellentani, Fernanda Furlanetto. January 2017 (has links)
Orientador: Luiz Eduardo Gomes Garcia Betting / Resumo: A conectividade funcional é anormal na epilepsia do lobo temporal mesial (ELTm). O objetivo deste estudo foi investigar os efeitos de fármacos antiepilépticos (FAES) na conectividade funcional de pacientes com ELTm. Para isso, 31 pacientes com ELTm (16 à direita e 15 à esquerda) e 36 controles foram investigados. Sequências 3D volumétricas T1 e imagens funcionais a partir de sinal BOLD foram adquiridas em um equipamento 3T. Os dados da ressonância magnética funcional (RMf) em repouso foram processados e analisados utilizando o programa CONN. Para cada sujeito, duas formas de análise foram realizadas: uma de correlação entre as várias regiões de interesse e outra de região interesse para todos os voxels. A análise de grupos foi feita utilizando um modelo linear geral com nível de significância de p < 0,05 corrigido para múltiplas comparações. Foram realizadas comparações entre pacientes com ELTm (direita ou esquerda) e controles, seguidas de comparações de acordo com a carga de FAEs. A partir dessas análises, foi constatado uma redução de conectividade com volume total de 9092 mm3 (p<0,0001), em pacientes com ELTm esquerda e 5234 mm3 (p<0,0001), em pacientes com ELTm direita . Quando considerada a carga de medicação, pacientes com ELTm esquerda, recebendo doses altas, apresentaram redução de conectividade nas regiões temporais. Nos pacientes que recebiam doses baixas, essa redução atingiu uma área total mais extensa, no córtex frontal medial, na região posterior do cíngulo e p... (Resumo completo, clicar acesso eletrônico abaixo) / Doutor
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Análise das descargas epileptiformes interictais na epilepsia de lobo temporal mesial utilizando análise quantitativa do eletroencefalograma e da neuroimagem / Analysis of interictal epileptiform discharges (IED) in mesial temporal lobe epilepsy using quantitative EEG and neuroimagingFujisao, Elaine Keiko [UNESP] 23 February 2018 (has links)
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Previous issue date: 2018-02-23 / FUJISAO, E.K. Análise das descargas epileptiformes interictais (IED) na epilepsia de lobo temporal mesial utilizando análise quantitativa do eletroencefalograma e da neuroimagem. Doutorado – Faculdade de Medicina de Botucatu, Universidade Estadual Paulista ―Júlio de Mesquita Filho‖, Botucatu, 2018. Objetivos: Investigar áreas de correlação entre a substância cinzenta e mapas de fonte interictal nos subtipos de epilepsia de lobo temporal mesial (ELTM). Introdução: Na ELTM, os eletroencefalogramas (EEG) de rotina de escalpo interictais mostram descargas epileptiformes na região temporal anterior revelando a circuitaria epileptiforme. Os geradores anatômicos precisos destas descargas ainda não foram identificados. Métodos: Setenta e um pacientes e trinta e seis controles foram submetidos à ressonância magnética (RM) de3T. Imagens de alta resolução T1 foram utilizadas para análise estrutural. A segmentação do hipocampo foi realizada com o pacote Freesurfer e utilizada para confirmar a atrofia do hipocampo (AH). O software SPM foi utilizado para segmentação da matéria cinzenta, registro e análise estatística. Os pacientes também foram submetidos à EEG de rotina com eletrodos temporais anteriores adicionais. Para cada paciente, as descargas epileptiformes foram selecionadas, promediadas e a fonte foi extraída com o algoritmo CLARA incluído no software BESA. Finalmente, a análise de correlação voxel-wise foi realizada entre a matéria cinzenta suavizada e os mapas de origem EEG em subtipos ELTM distintos. Resultados: 16 pacientes apresentaram ELTM sem AH, foram avaliadas 154 descargas (67 à esquerda e 87 à direita), 10826 mm³ correlacionadas envolvendo regiões extra-temporais (lobos frontal e parietal, r = -0,78, x = 19, y = 61, z = 6). 22 pacientes tinham AH esquerda, 839 descargas foram avaliadas (818 à esquerda e 21 à direita), 2700 mm3 foram correlacionadas envolvendo o lobo temporal esquerdo (r = -0,56, x = -28, y = -5, z = -19). 21 pacientes tinham AH direita, foram avaliadas 910 descargas (139 à esquerda e 771 à direita), 3625 mm3 foram correlacionadas envolvendo o giro frontal inferior direito (r = -0,70, x = 32, y = 33, z = 8). 12 pacientes apresentaram AH bilateral, 343 descargas foram avaliadas (264 à esquerda e 79 à direita), 4932 mm3 foram correlacionadas envolvendo principalmente a ínsula direita (r = -0,87, x = 29, y = 0, z = 8). Conclusão: Correlações negativas foram encontradas entre volumes de matéria cinzenta e imagens de origem EEG. Os geradores neuroanatômicos de IED são heterogêneos e variam de acordo com o subtipo ELTM. / FUJISAO, E.K. Analysis of interictal epileptiform discharges (IED) in mesial temporal lobe epilepsy using quantitative EEG and neuroimaging. PhD - Medical School of Botucatu City, State University of São Paulo "Júlio de Mesquita Filho", Botucatu, 2018. Aims: To investigate areas of correlation between gray matter and interictal EEG source maps in subtypes of mesial temporal lobe epilepsy (MTLE). Background: In MTLE, routine interictal scalp EEG typically shows epileptiform discharges over the anterior temporal region disclosing the epileptogenic circuitry. The precise anatomical generators of these discharges have not yet been identified. Methods: 71 patients and 36 controls underwent to 3T MRI. High resolution T1 images were used for structural analysis. Hippocampal segmentation was performed with Freesurfer package and used to confirm hippocampal atrophy (HA). SPM software was used for segmentation of the gray matter, registration and statistical analysis. Patients were also submitted to routine EEG with additional anterior temporal electrodes. For each patient, epileptiform discharges were selected, averaged and the source was extracted with CLARA algorithm included in the BESA´s software. Finally, voxel-wise correlation analysis was conducted between the smoothed gray matter and EEG source maps in distinct mTLE subtypes. Results: 16 patients had mTLE without HA, 154 discharges were evaluated (67 left and 87 right), 10826mm³ were correlated involving extra-temporal regions (frontal and parietal lobes; r=-0.78, x=19, y=61, z=6). 22 patients had left HA, 839 discharges were evaluated (818 left and 21 right), 2700mm3 were correlated involving the left temporal lobe (r=-0.56, x=-28, y=-5, z=-19). 21 patients had right HA, 910 discharges were evaluated (139 left and 771 right), 3625mm3 were correlated involving the right inferior frontal gyrus (r=-0.70, x=32, y=33, z=8). 12 patients had bilateral HA, 343 discharges were evaluated (264 left and 79 right), 4932mm3 were correlated mainly involving the right insula (r=-0.87, x=29, y=0, z=8). Conclusion: Negative correlations were disclosed between gray matter volumes and EEG source imaging. Neuroanatomical generators of interictal discharges are heterogeneous and vary according to mTLE subtype.
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Análise das descargas epileptiformes interictais na epilepsia de lobo temporal mesial utilizando análise quantitativa do eletroencefalograma e da neuroimagemFujisao, Elaine Keiko January 2018 (has links)
Orientador: Luiz Betting / Resumo: FUJISAO, E.K. Análise das descargas epileptiformes interictais (IED) na epilepsia de lobo temporal mesial utilizando análise quantitativa do eletroencefalograma e da neuroimagem. Doutorado – Faculdade de Medicina de Botucatu, Universidade Estadual Paulista ―Júlio de Mesquita Filho‖, Botucatu, 2018. Objetivos: Investigar áreas de correlação entre a substância cinzenta e mapas de fonte interictal nos subtipos de epilepsia de lobo temporal mesial (ELTM). Introdução: Na ELTM, os eletroencefalogramas (EEG) de rotina de escalpo interictais mostram descargas epileptiformes na região temporal anterior revelando a circuitaria epileptiforme. Os geradores anatômicos precisos destas descargas ainda não foram identificados. Métodos: Setenta e um pacientes e trinta e seis controles foram submetidos à ressonância magnética (RM) de3T. Imagens de alta resolução T1 foram utilizadas para análise estrutural. A segmentação do hipocampo foi realizada com o pacote Freesurfer e utilizada para confirmar a atrofia do hipocampo (AH). O software SPM foi utilizado para segmentação da matéria cinzenta, registro e análise estatística. Os pacientes também foram submetidos à EEG de rotina com eletrodos temporais anteriores adicionais. Para cada paciente, as descargas epileptiformes foram selecionadas, promediadas e a fonte foi extraída com o algoritmo CLARA incluído no software BESA. Finalmente, a análise de correlação voxel-wise foi realizada entre a matéria cinzenta suavizada e os mapas de origem EEG em su... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: FUJISAO, E.K. Analysis of interictal epileptiform discharges (IED) in mesial temporal lobe epilepsy using quantitative EEG and neuroimaging. PhD - Medical School of Botucatu City, State University of São Paulo "Júlio de Mesquita Filho", Botucatu, 2018. Aims: To investigate areas of correlation between gray matter and interictal EEG source maps in subtypes of mesial temporal lobe epilepsy (MTLE). Background: In MTLE, routine interictal scalp EEG typically shows epileptiform discharges over the anterior temporal region disclosing the epileptogenic circuitry. The precise anatomical generators of these discharges have not yet been identified. Methods: 71 patients and 36 controls underwent to 3T MRI. High resolution T1 images were used for structural analysis. Hippocampal segmentation was performed with Freesurfer package and used to confirm hippocampal atrophy (HA). SPM software was used for segmentation of the gray matter, registration and statistical analysis. Patients were also submitted to routine EEG with additional anterior temporal electrodes. For each patient, epileptiform discharges were selected, averaged and the source was extracted with CLARA algorithm included in the BESA´s software. Finally, voxel-wise correlation analysis was conducted between the smoothed gray matter and EEG source maps in distinct mTLE subtypes. Results: 16 patients had mTLE without HA, 154 discharges were evaluated (67 left and 87 right), 10826mm³ were correlated involving extra-temporal regions... (Complete abstract click electronic access below) / Doutor
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Toxicité neuronale du cholestérol et physiopathologie de la maladie d’Alzheimer : analyse in vivo des conséquences de l’inhibition de la cholestérol-24-hydroxylase / Toxicity of neuronal cholesterol accumulation and Alzheimer’s disease : in vivo consequence of cholesterol-24-hydroxylaseDjelti, Fathia 30 September 2013 (has links)
Le vieillissement normal s’accompagne d’une diminution du contenu du cholestérol cérébral. Au contraire, une accumulation de cholestérol est associée aux processus toxiques dans plusieurs pathologies dégénératives (maladie d’Huntington, maladie de Parkinson, épilepsie, maladie de Niemann Pick de type C, maladie d’Alzheimer). De plus, les parallèles étroits existent entre la physiopathologie moléculaire de la maladie d’Alzheimer et celle de la maladie de Niemann Pick de type C, maladie de l’homéostasie du cholestérol. Ainsi on retrouve dans ces deux pathologies une hyperphosphorylation de la protéine Tau, associée à une augmentation des endosomes élargis et à la production de peptides A. L’ensemble de ces éléments évoque le rôle potentiel de la surcharge en cholestérol cérébral comme facteur favorisant le développement de la maladie d’Alzheimer. L’objectif de mon travail de doctorat a été de déterminer si une surcharge en cholestérol in vivo dans les neurones de l’hippocampe, région précocement touchée par la maladie d’Alzheimer, pouvait être à l’origine de processus neurotoxiques et de modifications biochimiques et neuropathologiques proches de ceux qui sont observés dans cette pathologie. La quasi-totalité du cholestérol cérébral est synthétisée in situ, la barrière hémato-encéphalique ne permettant qu’un apport minime du cholestérol périphérique. L’excès de cholestérol est exporté de la circulation sanguine sous la forme du 24-hydroxycholestérol, un métabolite produit exclusivement dans les neurones par la cholestérol-24-hydroxylase codée par le gène Cyp46a1.La surcharge en cholestérol a été induite in vivo par inhibition de la cholestérol-24-hydroxylase, dans l’hippocampe par une stratégie d’ARN interférence délivré par une injection stéréotaxique d’un vecteur AAV5. Nous avons étudié, d’une part la capacité d’une accumulation de cholestérol à induire chez la souris normale, un phénotype clinique et neuropathologique proche de la maladie d’Alzheimer et d’autre part si cette même accumulation de cholestérol neuronal pouvait aggraver ou compléter le phénotype Alzheimer d’un modèle murin de la maladie, la souris APP23. L’injection du vecteur AAV5-shCYP46A1 dans la stratum lacunosum moleculare de l’hippocampe conduit à une inhibition significative de l'expression du gène Cyp46a1, associée à une diminution de la concentration du 24-hydroxycholestérol et une augmentation du contenu en cholestérol dans les neurones de l’hippocampe, 3 semaines après l’injection. En réponse à cet excès de cholestérol, des mécanismes régulateurs permettent de diminuer, d’une part l’import et d’augmenter l’export du cholestérol de la cellule et d’autre part d’augmenter le contenu en phosphatidylcholine afin de rétablir un ratio phospholipide/cholestérol physiologique. Cependant, l'accumulation majeure de cholestérol intracellulaire conduit, 3 semaines après l’injection, à une activation de la réponse UPR (Unfolded Protein Response ou stress du réticulum endoplasmique) caractérisée par l'expression des gènes codant les facteurs XBP1s, ATF6, GRP78 associée à celles des protéines PERK phosphorylée, CHOP et caspase 12, entraînant l'activation des caspases 9 et 3. Elle est associée à la phosphorylation des protéines GSK3 (Tyr216) et Tau (Thr231). En parallèle, l’augmentation du cholestérol induit, 3 semaines après l’injection, une augmentation de l’expression de la protéine Rab5 (marqueur des endosomes précoces) et une relocalisation de la protéine APP dans les fractions de radeaux lipidiques associées à l'activation de la voie amyloïdogénique (production des fragments-CTF et des peptides A42). L’étude lipidomique met en évidence, 4 semaines après l’injection, une augmentation du contenu en céramide à longues chaînes et à une augmentation des gangliosides. Tous ces éléments aboutissent à un processus de perte neuronale associée à un recrutement des astrocytes dès la quatrième semaine après l’injection.... / An increasing number of arguments suggest a close and complex link between cholesterol metabolism and neurodegenerative diseases, particularly with Alzheimer’s disease. Normal ageing is associated with a decrease of brain cholesterol content. Conversly, accumulation of brain cholesterol is associated with several neurodegenerative diseases (Huntington disease, Parkinson disease, epilepsy, Niemann Pick C disease, Alzheimer’s disease). Moreover, close connections exist between molecular physiopathology of AD and that of Niemann Pick, a disease of cholesterol homeostasis. Altogether, these results suggest that cholesterol overload might play a role, as an initiating factor for the development of AD.In the brain, cholesterol metabolism is tightly controlled. In adults, cholesterol is mainly synthetized by astrocytes, then shuttles to neurons where it is used. All cholesterol excess must be eliminated. Cholesterol cannot cross freely the blood-brain-barrier. To be metabolized, brain cholesterol must be converted in 24-hydroxy-cholesterol by the cholesterol-24 hydroxylase enzyme, coded by CYP46A1 gene. The objective of my PhD project was to determine if cholesterol accumulation in vivo in hippocampal neurons, a region early involved in AD pathology, could trigger neurotoxic processes with biochemical and neuropathological modifications close to what is observed in AD. Cholesterol overload in vivo was induced by inhibiting cholesterol 24-hydroxylase enzyme activity, using an RNA interference strategy. Stereotactic injection of an AAV5- shCYP46A1 vector in the stratum lacunosum moleculare of the hippocampus led to significant and rapid (as soon as 3 weeks after injection) inhibition of the Cyp46a1 gene in the hippocampus with an absence of RNA interference off-target effect. This inhibition was associated with a decrease of 24-hydroxycholesterol content and an increase of the cholesterol content. In response to this cholesterol excess, cell control mechanisms were initiated leading to decrease import and increase export of cholesterol, accompanied with an increase of phosphatidylcholine content to restore a physiological ratio of phospholipide/cholesterol. However, major accumulation of cholesterol led to neuronal death with activation of caspases 9 et 3, suggesting an apoptotic process. The cholesterol overload drives to an endoplasmic reticulum stress, with activation of the unfolded protein response (UPR) and expression of spliced XBP1, ATF6, GRP78, phosphorylated PERK, CHOP and caspase 12. These modifications were associated with phosphorylation of GSK3 (Tyr 216) and tau (Thr 231) proteins. In parallel, cholesterol accumulation led to increased expression of Rab5 (early endosome marker) and relocalization of APP in rafts domains associated to activation of amyloid pathway (production of -CTF fragments and A42 peptides). Lipidomic analysis showed an increase of ceramides and gangliosides content. All these modifications were associated with neuronal death 4 weeks after injection and astrocytosis, leading to an EEG theta rhythm accelerated to beta frequencies, memory deficits and hippocampal atrophy. In a mouse model of Alzheimer disease, the APP23 mouse, cholesterol accumulation led to major aggravation of the phenotype, with increased production of A peptides, occurring of tau phosphorylation and UPR response, leading to accelerated neuronal death. Altogether, these results suggest a direct link between cholesterol accumulation in the brain and Alzheimer’s disease. Brain cholesterol accumulation could seed the sows to the development of Alzheimer’s pathology. Reducing cerebral cholesterol could thus be a relevant therapeutic strategy to prevent the development, or at least slow down the evolution of the pathology in Alzheimer’s disease.
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