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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
91

Rôle des récepteurs P2X4 dans la dégradation d’ApoE : implication dans la maladie d’Alzheimer / Involvement of P2X4 receptors in ApoE degradation : implication in Alzheimer disease

Hua, Jennifer 06 November 2019 (has links)
Les récepteurs purinergiques P2X4 (P2X4R) sont des récepteurs canaux exprimés par lesneurones et les microglies du système nerveux central et sont impliqués dans de nombreuxprocessus physiologiques et pathologiques. Des études préliminaires, menées au sein dulaboratoire, ont permis de mettre en évidence une interaction entre P2X4R etl’Apolipoprotéine E (ApoE), ainsi qu’une augmentation d’ApoE dans les macrophages et lesmicroglies provenant de souris déficientes pour P2X4R. Basée sur ces observations, lapremière partie de cette thèse a cherché à caractériser les mécanismes impliquant P2X4R danscet effet. ApoE étant un facteur de risque majeur dans la maladie d’Alzheimer, la deuxièmepartie de cette thèse a été consacrée à étudier l’implication de P2X4R dans cette pathologie.Les résultats présentés montrent que P2X4R module l’activité de la cathepsine B, enzymeresponsable de la dégradation lysosomale d’ApoE. L’utilisation de souris APP/PS1 a permisde montrer que l’absence de P2X4R conduit à une amélioration des capacités mnésiques, unediminution de la concentration de peptide Aβ soluble ainsi qu’à une augmentation d’ApoEmicrogliale.Ces résultats indiquent que P2X4R régule la dégradation d’ApoE par un mécanismedépendant de la cathepsine B, et que son invalidation permet d’améliorer les symptômescognitifs de la maladie d’Alzheimer. / P2X4 receptors (P2X4R) are purinergic ion channels expressed on neurons and microglia inthe central nervous system. They have been widely studied and have been implicated in manyphysiological and pathological processes. Previous studies conducted in the laboratoryrevealed an interaction between P2X4R and the Apolipoprotein E (ApoE), as well as anincrease in ApoE level in primary macrophages and microglia obtained from mice lackingP2X4R. Based on these results, this thesis aimed to decipher the mechanisms underlyingP2X4R regulation of ApoE levels. In addition, ApoE being a major risk factor forAlzheimer’s disease, part of this work investigated potential implications of P2X4R in thispathology.Results show that P2X4R modulates cathepsin B activity, which in turn promotes ApoElysosomal degradation. APP/PS1 mice lacking P2X4R show an increase in cognitiveperformances, a decrease in soluble Aβ peptide and an increase of microglia ApoE level.These results support that P2X4R modulates ApoE degradation in a cathepsin B-dependantmanner and that its invalidation leads to an improvement in Alzheimer’s pathology.
92

Prévention du phénomène de nucléation et de la propagation des tauopathies par immunothérapie passive utilisant un anticorps ciblant une région centrale de la protéine tau / Prevention of nucleation and spread of tauopathies by passive immunotherapy using an antibody targeting a central region of the tau protein

Albert, Marie 10 December 2018 (has links)
Dans les tauopathies, telle la maladie d'Alzheimer, la protéine tau devient anormalement hyperphosphorylée ce qui conduit à son accumulation et à son agrégation intracellulaire. Ce processus aboutit progressivement à une perte neuronale et un déclin cognitif. L'immunothérapie anti-tau est de plus en plus considérée comme un traitement potentiel en vue de bloquer la progression des tauopathies.Récemment, l’entreprise UCB BioPharma a montré que l’anticorps D, anticorps ciblant la protéine tau en un épitope central (aa 235 à 250), était en mesure de bloquer, in vitro, l'agrégation intracellulaire de protéines tau, induite par des PHFs purifiés au départ de cerveaux Alzheimer. L’anticorps A, de même isotype, associé à des propriétés de liaison comparables mais reconnaissant la protéine tau en son extrémité N-terminale (aa 15 à 24), n’est pas en mesure de prévenir l’agrégation dans ce même modèle, ce qui souligne l’importance du choix de l’épitope en vue de neutraliser les amorces pathologiques issues de cerveaux Alzheimer.En vue d’étudier les propriétés de l’anticorps D in vivo, nous avons développé deux modèles murins de tauopathies. Premièrement, un modèle étudiant les phénomènes de recrutement et nucléation, basé sur l'injection unilatérale d’un homogénat de cerveau Alzheimer dans l'hippocampe de jeunes souris transgéniques (Tg30tau). Deuxièmement, un modèle permettant l’étude de la propagation intercellulaire de formes pathologiques de tau, par injection unilatérale de fibrilles P301L-K18 dans l’hippocampe de souris transgéniques (hTauP301L). Les tauopathies induites par ces injections intracérébrales ont été quantifiées dans l'hippocampe ipsi et controlatéral, en présence de traitements immunothérapeutiques utilisant les anticorps anti-tau A et D ou un anticorps témoin négatif de même isotype. La quantification des formes hyperphosphorylées et agrégées de tau a été réalisée par des approches immunohistochimique ou biochimique.Dans le modèle de nucléation, l’anticorps D est en mesure de prévenir significativement l’apparition des formes hyperphosphorylées et agrégées de tau à la fois dans l’hippocampe ipsilatéral (injecté avec l’homogénat Alzheimer) et contralatéral. A l’opposé, l’anticorps A n’est pas en mesure de prévenir l’apparition de la tauopathie dans ce modèle. Dans le modèle de propagation, basé sur l'injection unilatérale hippocampique de fibrilles P301L-K18, le traitement immunothérapeutique utilisant l’anticorps D réduit significativement la propagation d’espèces pathologiques de la protéine tau dans l'hippocampe controlatéral.De par l’utilisation de ces deux modèles murins de tauopathies, nous avons pu confirmer in vivo, la capacité de l’anticorps D à neutraliser les espèces pathologiques contenues dans un homogénat de cerveau Alzheimer et avons démontré sa capacité à s’opposer à la propagation intercellulaire de la tauopathie in vivo. Dans le modèle de nucléation, l’anticorps A n’a pas été en mesure de s’opposer à l’apparition de la tauopathie. Les résultats obtenus confirment ceux décrits par l’entreprise UCB BioPharma dans leur modèle d’agrégation in vitro et confirme l’importance considérable du choix de l’épitope en vue de prévenir efficacement le développement de tauopathies in vivo. / In tauopathies, such as Alzheimer's disease, tau protein becomes abnormally hyperphosphorylated which leads to its accumulation and intracellular aggregation. This process gradually leads to neuronal loss and cognitive decline. Anti-tau immunotherapy is increasingly considered as a potential treatment to block tauopathies’s progression.UCB BioPharma recently showed that antibody D, targeting an epitope in the central region of tau (aa 235-250), is able to block, in vitro, the intracellular seeding of tau proteins induced by PHFs purified from the brain of Alzheimer's patients. The antibody A, same isotype and associated with similar binding properties but recognizing the N-terminal region of tau (aa 15 to 24) is not able to prevent tau seeding in this cell based assay. This observation underlines the importance of the targeted epitope on tau protein in order to neutralize pathological species contained in Alzheimer's brains (Courade et al., 2018).In order to study the properties of antibody D in vivo, we developed two murine models of tauopathies. First, a seeding model based on a unilateral injection of Alzheimer's brain homogenate into the hippocampus of young Tg30tau mice. Secondly, a spreading model to study the propagation of pathological tau seeds, based on unilateral hippocampal injection of P301L-K18 fibrils in hTauP301L transgenic mice. Tauopathies induced in these models were quantified in the ipsi and contralateral hippocampus in the presence of immunotherapeutic treatments with anti-tau antibodies (D, A) or a negative control antibody. Quantification of hyperphosphorylated and aggregated tau was performed by immunohistochemical or biochemical analyses.In the seeding model, antibody D significantly reduces the appearance of hyperphosphorylated and aggregated tau both in the ipsi and contralateral CA1 regions of hippocampus. In contrast, antibody A is not able to prevent the appearance of pathological tau in this model. In the spreading model, immunotherapeutic treatments with antibody D significantly reduces the spread of pathological tau seeds in the contralateral hippocampus.From these two murine models of tauopathies, we confirmed in vivo the ability of antibody D to neutralize the pathological tau species contained in an Alzheimer's brains homogenate and demonstrated its capacity to reduce the intercellular propagation of tauopathies. In the seeding model, antibody A wasn’t able to affect the onset of tauopathy. These results confirm those described by UCB BioPharma based on their in vitro aggregation assay and confirm the importance of the targeted epitope in order to effectively prevent the development of tauopathies in vivo.
93

Representación social del Alzheimer desde la perspectiva de la familia, Chiclayo 2012

Díaz Bernabé, Dánae Angélica, Pérez Paz, Alma Rosaura, Pérez Paz, Alma Rosaura, Díaz Bernabé, Dánae Angélica January 2013 (has links)
El Alzheimer es una epidemia silenciosa que genera mitos y creencias que influyen en el comportamiento y actitud de la sociedad y por ende en la familia, la cual adopta conductas, que afectan a estas personas, estigmatizándolas y generando en ellas poco a poco la pérdida de su identidad o muerte social; en ese sentido, este trabajo se justifica, porque logra conocer y profundizar la construcción social de la imagen del Alzheimer, a partir de la información generada por el censo común, teniendo como objetivos caracterizar, analizar y discutir la representación social del Alzheimer desde la perspectiva de la familia. Los presupuestos teóricos que respaldan la investigación son: Sergio Moscovici (1979) y Jodelet (1984) para los conceptos de representación social, De la Cuesta (2004) y Feria (2005) para los conceptos de Alzheimer, y finalmente Marta Aja Abelán (1998) y Karol Wojtyla (1999) para los conceptos de familia. La metodología utilizada fue cualitativa con enfoque de representación social. Los sujetos de estudio fueron comprendidos por los familiares de los adultos mayores diagnosticados con Alzheimer que están inscritos en la Asociación “Ayudémonos”. Para la recolección de datos se utilizó como instrumentos el cuestionario sociodemográfico y la entrevista semiestructurada. Y para su análisis se utilizó el método asociación de contenido. Las tres categorías que emergieron del tratamiento de datos son: El Alzheimer representado como enfermedad progresiva-crónica, deterioro físico-mental y dependencia; El Alzheimer como etiqueta desaprobatoria, pérdida de identidad, estigma y muerte social y El Alzheimer ancorado como sufrimiento, estrés y necesidad de cuidado. Se tuvo en cuenta los principios éticos personalistas de Elio Sgreccia y los criterios de cientificidad. / Tesis
94

Changes in gene expression of brain insulin system in STZ icv - damaged rats - relevance to Alzheimer disease

Osmanovic, Jelena January 2008 (has links) (PDF)
Ratten, die intrazerebroventricular (icv) mit Streptozotocin (STZ) behandelt werden, eignen sich gut als Tiermodelle für die sporadische Alzheimererkrankung (sAD). In der hier vorgelegten Arbeit wurden Veränderungen bezüglich der Insulinkonzentration sowie einiger Bestandteile der Insulinrezeptor (IR) – Signalkaskade in Rattengehirnen, welche icv mit STZ behandelt wurden, zu verschiedenen Zeitpunkten untersucht. Die Auswirkungen von STZ auf die zerebrale IR-Signalkaskade wurden dann mit denen von chronisch erhöhten Corticosteronkonzentrationen verglichen. In dieser Studie wurde im Hippocampus eine verminderte mRNA-Expression von Insulin, der IR sowie des insulinabbauenden Enzyms (IDE) nachgewiesen; bezüglich der tau-mRNA-Expression konnten jedoch in diesem Gehirnareal der mit STZ behandelten Ratten keine Veränderungen beobachtet werden. Die Resultate der Insulin-, IR- und IDE-mRNA-Expression fielen bei den mit Corticosteron behandelten Ratten ähnlich aus Im Gegensatz hierzu nahm die tau-mRNA-Expression bei Ratten, die mit Corticosterone behandelt wurden, zu, was auch für eine sAD kennzeichnend ist. Sowohl bei den mit STZ als auch bei den mit Corticosteronen behandelten Ratten konnten Verhaltensanomalien beobachtet werden. Die in dieser Arbeit erzielten Resultate deuten darauf hin, dass viele Merkmale einer sAD experimentell durch eine Beeinträchtigung des Insulin/IR-Signalwegs sowie eine chronische Erhöhung der Corticosteronkonzentration hervorgerufen werden können. Dies untermauert wiederum unsere Hypothese, dass es sich bei sAD um eine neuroendokrine Störung handelt, die mit gehirnspezifischen Fehlfunktionen in der Insulin/IR-Signalkaskade einhergeht, welche zum Teil durch erhöhte Corticosteronkonzentrationen ausgelöst werden können. Auf Grund der in dieser Arbeit erzielten Resultate stellt sich die Frage, ob -Amyloid (A) ein Auslöser oder eine Konsequenz einer sAD darstellt. Die hier vorgelegte Arbeit last den Schlus zu, dass bei sAD-Tiermodellen ein Zusammenhang zwischen primären Fehlfunktionen im zerebralen Insulinsystem und dadwol sekundär ausgeloster A-Pathologie besteht. Weiterfübende Untersuchungen wird aber notwendig um diese Aussagen zu bestätigen. / This research was aimed to evaluate the time-course of changes in the brain insulin and some elements of the insulin receptor (IR) signalling cascade in the streptozotocin-intracerebroventricullarly (STZ-icv) treated rats representing experimental model of sporadic Alzheimer’s disease (sAD) and to compare them with effects of chronically increased corticosterone on the brain insulin system. This study shows down-regulation in mRNA expression of insulin, insulin receptor (IR), and insulin degrading enzyme (IDE) but no changes were observed in the expression of tau mRNA in hippocampus of STZ-icv treated rats. Comparing these results to the ones found in corticosterone treated rats similarities at the level of insulin, IR and IDE mRNA expression can be assumed. In contrast tau mRNA expression in corticosterone treated rats were increased, data which are in line with sAD. Behavioural deficits were found in both STZ-icv and corticosterone treated rats. In conclusion, these results demonstrate that many of the characteristic features of sporadic Alzheimer’s disease (sAD) can be produced experimentally by impairing the insulin/IR signaling pathway combined with a chronic increase of corticosterone. This supports our hypothesis that sAD represents a neuro-endocrine disorder associated with brain-specific disregulation in insulin and IR signaling, caused in part by increased level of corticosterone. In line with that our study puts a question on the classical amyloid β (Aβ) hypothesis, supporting the view of brain insulin system dysfunction as a trigger for the Aβ pathology in an experimental sAD model.
95

Investigating therapeutic strategies in a preclinical model for Alzheimer's disease

Jackson, Joshua D. January 2017 (has links)
Alzheimer's disease (AD) is a worldwide, incurable disease, and the most common form of dementia. Numbers of cases are rising, and since its discovery the only approved medications have treated only the symptoms, not the pathological cause. With the cost to society rising, the debilitating nature of the disease and the pressure put on the family members and support network of patients, disease modifying therapies are in dire need. Current models have proven an invaluable tool with which to study certain aspects of the disease and the genetics behind it, however the lack of clinically approved medications in the last 20 years suggests new models are needed. Based on the amyloid cascade hypothesis, this thesis initially characterises two models of β-Amyloid oligomer (Aβo) induced cognitive deficits. Both models are created by ICV injection of soluble Aβo into the brain of rat. The models differ only by the molecular weight of the Aβo 1-42, one, referred to as low molecular weight (LMW) Aβo, with stable dimers, trimers and tetramers, the other, referred to as high molecular weight (HMW) Aβo, consisting of assemblies ranging from ~50 to ~150 kDa. It was found that behavioural deficits were similar between the two, with a robust object recognition deficit, but no working memory deficit. Both models also showed a deficit in the synaptic marker PSD-95; however the LMW Aβo caused a deficit in the frontal cortex, whereas the HMW Aβo caused a hippocampal deficit. The role of the cellular prion protein (PrPC) was explored, by blocking its binding to Aβo with the antibody 6D11. Interestingly the two models showed different results. The HMW Aβo deficits were completely blocked by the 6D11 application, however the LMW Aβo deficits were only partially prevented. Finally, Fasudil, a vasodilator approved in parts of Asia, was used to inhibit Rho-kinase, showing a prevention of the cognitive deficits in the HMW Aβo model. The results of this thesis show the ICV administration of Aβo to be a useful model for investigating the effects of Aβo, provides a platform with which to study the differing effects of Aβo with different oligomeric assemblies, and a model to test therapeutic strategies with relevance to AD.
96

Characterizing the symmetry of amyloid beta protein retention in Alzheimer's disease using florbetapir positron emission tomography - a study using data from the Alzheimer's disease neuroimaging initiative

Nguyen, Hoan 22 January 2016 (has links)
Progression of Alzheimer's disease has been associated with the deposition of aggregated amyloid beta (Aβ) protein in the brain. Though first described in post-mortal tissue, the development of Aβ specific tracers for positron emission tomography (PET) permits in-vivo mapping of its distribution in the brain. One of the well-known and early-developed tracers is the Pittsburgh Compound B (PiB) (Klunk et al., 2004). However, the challenge with PiB lies in the stability of the radioisotope 11C. 11C's short half-life of only 20 minutes hinders its transportation and usage at imaging facilities that are not in close proximity with the radioisotopes manufacturer. Recently, an alternative Aβ tracer has been developed, Florbetapir (Wong et al, 2010.), with a half-life of 110 minutes that should allow wider accessibility to imaging sites while improve the detection of Aβ. To define better the specificity and utility of Florbetapir, we propose to utilize existing PET data acquired with the radioactive tracer Florbetapir from the Alzheimer's disease Neuroimaging Initiative (ADNI). Our goal is to characterize the symmetry of Aβ protein deposition in the brain of patients with Alzheimer's disease. While a previous study has investigated this issue using PiB, Florbetapir has not been used. Our project will involve data post-processing by segmenting out non-brain tissues. Segmented data is then normalized by the pixel intensity and a distribution curve is created using MathCad program. In addition, we will calculate the asymmetry score for Regions of Interest. This will permit comparison of the uptakes of tracer between brain hemispheres to be made. Results from our project can provide insight into Florbetapir's binding affinity for Aβ. In addition, Florbetapir's potential as a better alternative to PiB can also be evaluated.
97

Um modelo híbrido aplicado ao diagnóstico da doença de Alzheimer / A HYBRID MODEL APPLIED TO THE DIAGNOSIS OF ALZHEIMER'S DISEASE (Inglês)

Castro, Ana Karoline Araujo de 29 December 2008 (has links)
Made available in DSpace on 2019-03-29T23:13:00Z (GMT). No. of bitstreams: 0 Previous issue date: 2008-12-29 / This work presents a hybrid model, combining Influence Diagrams and the Multicriteria Method, for aiding to discover, from a battery of tests, which are the most attractive questions, in relation to the stages of CDR (Clinical Dementia Rating) in decision making for the diagnosis of Alzheimer's disease. Due to the increase in life expectancy there is higher incidence of dementias. Alzheimer's disease is the most common dementia (alone or together with other dementias), accounting for 50% of the cases. Because of this and due to limitations in treatment at late stages of the disease early diagnosis is fundamental because it improves quality of life for patients and their families. Influence Diagram is implemented using GeNie tool. Next, the judgment matrixes are constructed to obtain cardinal value scales which are implemented through MACBETH Multicriteria Methodology. The modeling and evaluation processes were carried out through a battery of standardized assessments for the evaluation of cases with Alzheimer's disease developed by Consortium to Establish a Registry for Alzheimer's Disease (CERAD). Keywords: Alzheimer's Disease, Diagnosis, Multicriteria Method, Bayesian Network, Influence Diagram. / Devido à elevação da expectativa de vida, ocorre como conseqüência, o aumento da prevalência de demências. A doença de Alzheimer, dentre as demências, é a mais freqüente e responde (isoladamente ou em associação) por cerca de 50% dos casos. Por conta deste quadro e das limitações terapêuticas nos estágios mais avançados da doença, o diagnóstico nas fases iniciais torna-se fundamental, pois pode proporcionar melhores condições de vida aos pacientes e seus familiares. Apresenta-se um modelo híbrido, estruturado em Diagramas de Influência e Multicritério, objetivando descobrir, a partir de uma bateria de testes, quais são as questões mais atrativas, em relação aos estágios da CDR (Clinical Dementia Rating), na tomada de decisão do diagnóstico da doença de Alzheimer. O Diagrama de Influência é apresentado aplicando-se a ferramenta GeNie, em seguida são construídas as matrizes de juízos de valor e obtenção das escalas de valor cardinal através da metodologia MACBETH. Os processos de modelagem e avaliação foram realizados através de uma bateria neuropsicológica de avaliação padronizada, desenvolvida pelo CERAD (Consortium to Establish a Registry for Alzheimer's Disease). Palavras-chave: Doença de Alzheimer, Diagnóstico, Multicritério, Redes Bayesianas, Diagramas de Influência.
98

Modelo de doença de Alzheimer pela infusão intracerebroventricular de estreptozotocina : influência do tempo de administração e do sexo dos animais sobre parâmetros neurogliais

Biasibetti, Regina January 2016 (has links)
Muitos trabalhos têm demonstrado a correlação existente entre gênero e prevalência da doença de Alzheimer (DA), sendo que as mulheres compreendem dois terços dos pacientes afetados. A estreptozotocina (STZ) é uma substância que vem sendo muito utilizada, por administração intracerebroventricular, para produzir um modelo de doença de Alzheimer esporádica com características neuroquímicas e fisiopatológicas semelhantes à DA, em roedores. Dessa forma, essa tese teve como objetivo avaliar as alterações comportamentais cognitivas e parâmetros neuroquímicos (ChAT, S100B, GFAP, GSH e captação de glicose) em hipocampo e cerebelo de ratos e ratas expostas ao modelo de doença de Alzheimer por STZ. Para um melhor entendimento das alterações, as avaliações foram realizadas em três diferentes tempos após a indução do modelo: duas, quatro e oito semanas. Como resultado, encontramos declínio cognitivo e alterações neuroquímicas hipocampais e cerebelares. Interessantemente, machos e fêmeas apresentaram distintas respostas frente ao insulto por STZ, mostrando ser este um campo interessante para caracterização e aprofundamento do modelo que utilizamos. Este trabalho confirma o comprometimento cognitivo e as alterações neuroquímicas presentes no modelo e estes se somam às variações funcionais encontradas nos astrócitos. Tais alterações também estão presentes na DA, apontando a interação neuroglial como um importante alvo de estudo na doença e, consequentemente, na busca por alternativas terapêuticas. / Many studies have demonstrated the correlation between gender and prevalence of Alzheimer's disease (AD), with women comprising two thirds of the affected patients. Streptozotocin (STZ) is a substance that has been widely used by intracerebroventricular administration to produce a model of sporadic Alzheimer's disease with neurochemical and pathophysiological characteristics similar to AD, in rodents. Thus, this thesis aimed to evaluate cognitive behavioral changes and neurochemical parameters (ChAT, S100B, GFAP, GSH and glucose uptake) in the hippocampus and cerebellum of rats (males and females) exposed to the model of sporadic Alzheimer's disease by STZ. For the best comprehension of the changes, the evaluations were performed at three different times after the induction of the model: two, four and eight weeks. As a result, we found cognitive decline and hippocampal and cerebellar neurochemical changes. Interestingly, males and females presented different responses to STZ damage, showing that this is an interesting field for characterization and deepening of the model we use. This work confirms the cognitive impairment and the neurochemical changes present in the model and these are added to the functional shifts found in the astrocytes. These alterations are also present in AD, pointing to neuroglial interaction as an important target for the study of the disease and, consequently, the search for therapeutic alternatives.
99

A escrita autobiográfica com portadores da doença de alzheimer na clínica da terapia ocupacional

Carvalho, Elcyana Bezerra 30 April 2003 (has links)
Made available in DSpace on 2019-04-05T23:01:42Z (GMT). No. of bitstreams: 0 Previous issue date: 2003-04-30 / A doença de Alzheimer (DA) é uma patologia neurodegenerativa progressiva, irreversível que compromete as áreas do cérebro responsáveis pela memória, pensamento e linguagem. A presente dissertação se propõe a discorrer sobre o uso dos escritos autobiográficos na clínica da Terapia Ocupacional com portadores da doença de Alzheimer. Esses escritos podem se constituir mobilizadores de atividades a serem realizados na clínica da Terapia Ocupacional, uma vez que propiciam a valorização do sujeito pelo resgate de sua historicidade e identidade, bem como da memória e da manutenção das funções cognitivas, promovendo assim laços sociais. Daí a relação entre escritos autobiográficos e a D.A. A escrita autobiográfica como gênero da história de vida foi o escolhido, já que permite ao sujeito narrar sua própria vida, realizando uma articulação entre a dimensão do passado às circunstancias do presente e as projeções em relação ao futuro. A pesquisa foi do tipo qualitativa a partir de três casos clínicos, cujos atendimentos em Terapia Ocupacional a escrita autobiográfica ocupou um lugar de destaque. Foram realizados relatos dos casos clínicos, investigação dos escritos em termos de forma e conteúdo e repercussão no portador da Doença de Alzheimer. Os dados para a análise dos escritos autobiográficos foram classificados nas seguintes categorias temáticas: identificação de si e descrição de si; relações familiares; figura do pai e da mãe; irmãos; marido e mulher; filhos; histórico escolar; histórico profissional e memória coletiva. Ressaltamos os resultados referentes aos escritos autobiográficos como um espaço de atribuição de sentido às vivencias do paciente, como promotor do resgate da memória e identidade do paciente, como forma de redimensionar sua posição frente à doença e reconfiguração dos elos familiares, e , o mais importante, a partir dos escritos autobiográficos houve a produção de novos escritos como textos, contos, cartas que organizam, constróem e expressam a vida cotidiana.
100

Funktionelle Aktivierungen im Verlauf eines Jahres bei Patienten mit Alzheimer-Erkrankung und gesunden Kontrollen / Functional Brain Activation in Patients suffering from Alzheimer's disease and healthy Controls over a one-year Interval

Zeller, Julia January 2011 (has links) (PDF)
Hintergrund: Die Alzheimer-Erkrankung ist die häufigste neurodegenerative Erkrankung. Da es zurzeit für sie noch keine Heilung gibt, richtet sich das Hauptaugenmerk auf eine möglichst frühe Diagnose und die Behandlung mit krankheitsverzögernden Medikamenten. Vor allem die funktionelle Bildgebung gilt im Bereich der Frühdiagnose als vielversprechend. Neben dem Gedächtnis werden die visuell-räumliche Informationsverarbeitung, exekutive Funktionen und Aufmerksamkeitsprozesse untersucht. Hierbei zeigen sich zentralnervöse Aktivierungsauffälligkeiten in kortikalen Zielregionen etwa im präfrontalen und im parietalen Kortex. Verlaufsuntersuchungen konzentrieren sich vor allem darauf aus der Gehirnaktivierung Vorhersagen über kognitive Veränderungen bei älteren Personen mit und ohne Gedächtnisstörung treffen zu können. Nur wenige Studien erfassen dabei jedoch die Gehirnaktivierung zu mehreren Messzeitpunkten. Gerade für große Stichproben und wiederholte Messungen könnte die funktionelle Nahinfrarotspektroskopie (fNIRS) sich als Alternative zur Magnetresonanztomographie anbieten. Ziel: Ziel der Studie war es, mit fNIRS und ereigniskorrelierten Potentialen funktionelle Unterschiede zwischen Alzheimer-Patienten und gleichaltrigen Kontrollen in mehreren Funktionsbereichen darzustellen und ihre Veränderung über den Zeitraum eines Jahres zu verfolgen. Zum ersten Mal sollte im Rahmen einer prospektiven Untersuchung mit fNIRS geprüft werden ob kortikale Aktivierungen zur Vorhersage von neuropsychologischen Testwerten genutzt werden können. Zusätzlich stellte sich die Frage, ob fNIRS für Verlaufsuntersuchungen an älteren Stichproben geeignet ist. Methoden: Im Rahmen der vorliegenden Arbeit wurden zum ersten Messzeitpunkt (T1) 73 Patienten und 71 Kontrollen mit vier Paradigmen in den drei Funktionsbereichen visuell-räumliche Informationsverarbeitung, exekutive Funktionen und zentralnervöse Filtermechanismen mit fNIRS und ereigniskorrelierten Potentialen gemessen. Die Probanden durchliefen eine Line Orientation Aufgabe, zwei Versionen einer Wortflüssigkeitsaufgabe (phonologisch und semantisch) und das P50-Doppelklickparadigma. Zielparameter waren dabei die aufgabenbezogene Aktivierung im parietalen Kortex, im dorsolateralen Präfrontalkortex (DLPFC) und das sensorische Gating, gemessen durch die P50-Supression nach wiederholter Reizdarbietung. Zusätzlich wurden zwei typische Tests zur Demenzdiagnostik (MMST und DemTect) erhoben. Die zweite Messung (T2) fand nach 12 Monaten statt und lief identisch zur ersten Untersuchung ab. Zu T2 konnten 14 Patienten und 51 Kontrollen erneut rekrutiert werden. Ergebnisse: Zu T1 konnte mit fNIRS ein Aktivierungsdefizit für Patienten im DLPFC während der phonologischen Wortflüssigkeitsaufgabe und im rechten Parietalkortex während der Line Orientation Aufgabe festgestellt werden. Für die semantische Wortflüssigkeitsaufgabe und das sensorische Gating zeigten sich keine zentralnervösen Unterschiede. Über das Jahr hinweg nahm die aufgabenbezogene Aktivierung der Patienten im linken DLPFC für beide Versionen der Wortflüssigkeitsaufgabe deutlich ab, während gleichaltrige Kontrollpersonen keine kortikalen Veränderungen zeigten. Zu T2 war das sensorische Gating der Patienten außerdem deutlich schlechter im Vergleich zu gesunden Kontrollen. Die Veränderungen der Oxygenierung während der Wortflüssigkeitsaufgabe konnten für gesunde Kontrollen Verschlechterungen im MMST und im DemTect vorhersagen. Vor allem ein Verlust der Lateralisierung ging mit einem Abfall in den kognitiven Tests einher. Schlussfolgerung: Spezifische Defizite in der kortikalen Aktivierung konnten bei Alzheimer-Patienten mit fNIRS beobachtet und genauer beschrieben werden. Auch die Veränderung im Verlauf eines Jahres ließ sich mit dieser Methode verfolgen. Für Längsschnittuntersuchungen, die sich mit der kortikalen Aktivierung als Prädiktor für dementielle Entwicklungen beschäftigen, bietet sich fNIRS somit als praktische Alternative zur fMRT an, zumal die gemessenen Veränderungen in der Oxygenierung auch prognostischen Wert für ältere Kontrollpersonen besaßen. Vor allem die funktionelle Lateralisierung in frontalen Kortexbereichen scheint als Prädiktor kognitiver Leistungen im Alter von Bedeutung zu sein. / Background: Alzheimer’s disease is the most common form of neurodegenerative disorder. Since as of yet no cure exists, one important aim is the development of methods for the early detection of cerebral changes. Functional imaging is an especially promising approach as functional changes might occur even before neural atrophy in certain brain areas. While episodic memory is the main objective of research, other studies focus visual-spatial processing, executive function and attention. Patients suffering from Alzheimer’s disease display deviant cortical activation in prefrontal and parietal areas during tasks targeting these domains. Prospective studies try to predict cognitive decline using brain activations as predictors for future test scores. Only a few studies record functional activations repeatedly however. Functional near infrared spectroscopy (fNIRS) might be a good alternative to functional magnet resonance imaging (fMRI) when it comes to monitoring large populations in longitudinal studies. Objective: The aim of the present study was to detect and describe functional differences between patients suffering from Alzheimer’s disease and healthy elderly controls via fNIRS and event-related potentials and track them over an interval of 12 months. This is the first prospective study using fNIRS: Functional changes in oxygenated and deoxygenated haemoglobin during the first measurement will be employed to predict neuropsychological decline after one year. Methods: During the first measurement (T1) 73 AD patients and 71 age-matched controls without cognitive complaints or other neurological or psychiatric disorders completed four tasks in three cognitive domains: A line orientation task (visual-spatial processing), a phonological and a semantic verbal fluency task (executive functions) and a dual-click paradigm resulting in auditory sensory gating (attention and filter mechanisms). Regions of interest were the parietal and the dorsolateral prefrontal cortex (DLPFC) as well as the gating ratio measured via the P50 suppression in paired click stimuli. Additionally subjects underwent two common tests for cognitive functioning of dementia patients (MMSE and DemTect). The second measurement (T2) was conducted 12 months after the first and followed exactly the same protocol. At T2 14 AD-patients and 51 controls could be tested again. Results: At T1, patients suffering from Alzheimer’s disease displayed deficient activations in the right parietal cortex during Line Orientation and in the DLPFC during the phonological version of the verbal fluency task. No group differences could be found in the semantic verbal fluency paradigm and in sensory gating. Over the course of one year, patients’ activation in the left DLPFC significantly declined during both versions of the verbal fluency task whereas controls showed no cortical changes. After 12 months, the sensory gating differed between the groups with patients displaying worse values. Changes of oxygenation during the verbal fluency tasks predicted the decline in neuropsychological tests in elderly controls. The prefrontal lateralization held the best prognostic value with a positive prognosis for stronger left-sided activation. Conclusion: The present study succeeded in describing specific deficits in cortical activation concerning patients suffering from Alzheimer’s disease and healthy age-matched controls using fNIRS. Changes over the course of 12 months could also be observed. The results indicate that fNIRS is well suited as an alternative to fMRI in longitudinal studies targeting cortical changes as predictors of cognitive decline. This is underlined by the fact that cortical activations during the verbal fluency task could be used to predict neuropsychological changes in elderly controls. Therefore the functional lateralization of prefrontal activations should become a new focus in prospective studies.

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