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Apathy and impulsivity in frontotemporal lobar degeneration syndromesLansdall, Claire Jade January 2017 (has links)
There has been considerable progress in the clinical, pathological and genetic fractionation of frontotemporal lobar degeneration syndromes in recent years, driving the development of novel diagnostic criteria. However, phenotypic boundaries are not always distinct and syndromes converge with disease progression, limiting the insights available from traditional diagnostic classification. Alternative transdiagnostic approaches may provide novel insights into the neurobiological underpinnings of symptom commonalities across the frontotemporal lobar degeneration spectrum. In this thesis, I illustrate the use of transdiagnostic methods to investigate apathy and impulsivity. These two multifaceted constructs are observed across all frontotemporal lobar degeneration syndromes, including frontotemporal dementia, progressive supranuclear palsy and corticobasal syndrome. They cause substantial patient morbidity and carer distress, often coexist and are undertreated. Using data from the Pick’s disease and Progressive supranuclear palsy Prevalence and INcidence (PiPPIN) Study, I examine the frequency, characteristics and components of apathy and impulsivity across the frontotemporal lobar degeneration spectrum. A principal component analysis of the neuropsychological data identified eight distinct components of apathy and impulsivity, separating patient ratings, carer ratings and behavioural tasks. Apathy and impulsivity measures were positively correlated, frequently loading onto the same components and providing evidence of their overlap. The data confirmed that apathy and impulsivity are common across the spectrum of frontotemporal lobar degeneration syndromes. Voxel based morphometry revealed distinct neural correlates for the components of apathy and impulsivity. Patient ratings correlated with white matter changes in the corticospinal tracts, which may reflect retained insight into their physical impairments. Carer ratings correlated with grey and white matter changes in frontostriatal, frontotemporal and brainstem systems, which have previously been implicated in motivation, arousal and goal directed behaviour. Response inhibition deficits on behavioural tasks correlated with focal frontal cortical atrophy in areas implicated in goal-directed behaviour and cognitive control. Diffusion tensor imaging was highly sensitive to the white matter changes underlying apathy and impulsivity in frontotemporal lobar degeneration syndromes. Diffusion tensor imaging findings were largely consistent with voxel-based morphometry, with carer ratings reflecting widespread changes while objective measures showed changes in focal, task-specific brain regions. White matter abnormalities often extended beyond observed grey matter changes, providing supportive evidence that white matter dysfunction represents a core pathophysiology in frontotemporal lobar degeneration. Apathy was a significant predictor of death within two and a half years from assessment, consistent with studies linking apathy to poor outcomes. The prognostic importance of apathy warrants more accurate measurement tools to facilitate clinical trials. Although causality remains unclear, the influence of apathy on survival suggests effective symptomatic treatments may also prove disease-modifying. These findings have several implications. First, clinical studies for apathy/impulsivity in frontotemporal lobar degeneration syndromes should target patients who present with these symptoms, irrespective of their diagnostic category. Second, data-driven approaches can inform the choice of assessment tools for clinical trials, and their link to neural drivers of apathy and impulsivity. Third, the components and their neural correlates provide a principled means to measure (and interpret) the effects of novel treatments in the context of frontotemporal lobar degeneration.
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Vers un marqueur biochimique des dégénérescences lobaires fronto-temporales : variations quantitatives et profils protéiques de la protéine TDP43 dans différentes matrices biologiques / Towards a biochemical marker of fronto temporal lobar degeneration : quantitative variations and qualitative patterns of TDP43 protein in different biological matricesFourier, Anthony 30 November 2018 (has links)
Les dégénérescences lobaires frontotemporales (DLFT) représentent la deuxième étiologie neurodégénérative chez l’adulte de moins de 65 ans. Les DLFT sont constituées d’un ensemble hétérogène de phénotypes cliniques et sont fréquemment héréditaires. Leurs particularités neuropathologiques communes reposent sur une atrophie des lobes frontaux et/ou temporaux associée à la présence d’inclusions de protéines agrégées parmi lesquelles la protéine TAR DNA binding protein 43 (TDP43). Actuellement, aucun marqueur protéique n’est validé pour diagnostiquer les DLFT du vivant du patient.Une cohorte de cas certains DLFT-TDP43 a été constituée grâce au développement d’outils spécifiques de diagnostic moléculaire. Une analyse des concentrations pondérales de protéine TDP43 dans le liquide cérébrospinal (LCS) a été réalisée dans cette cohorte, puis comparée à des cohortes bien caractérisées sur le plan clinique et neuropathologique. Finalement, les profils qualitatifs de la protéine TDP43 ont été étudiés dans différents compartiments accessibles du vivant du patient : les profils des formes solubles (LCS et plasma) et des formes intracellulaires (éléments figurés du sang) de la protéine TDP43 ont été comparés aux profils protéiques obtenus sur des tissus cérébraux présentant des inclusions de protéine TDP43. Les profils protéiques des culots plaquettaires présentent des similitudes avec le tissu cérébral et pourraient devenir un marqueur candidat pour le diagnostic probabiliste des DLFT / Frontotemporal lobar degeneration (FTLD) syndrome is the second most common of presenile dementia. FTLD is a clinically heterogeneous syndrome and comprises many hereditary cases. Common neuropathological features rely on a degeneration of the frontal and/or anterior temporal lobes, associated to specific inclusions of aggregated proteins including TAR DNA binding protein 43 (TDP43). Unfortunately, no practical protein marker is currently validated to improve FTLD diagnosis in living patients.A cohort of FTLD patients with definite TDP43 pathology was defined with the development of specific genetic testing. An analysis of TDP43 concentrations in cerebrospinal fluid (CSF) was performed in this cohort and then compared to other cohorts well-characterized on clinical and neuropathological features. Finally, qualitative patterns of TDP43 were studied in compartments accessible from the patient’s living: profiles of soluble TDP43 protein (in CSF or in plasma) and intracellular TDP43 protein (in the formed elements of blood) were compared to protein patterns observed in brain tissues with TDP43 protein inclusions. Platelet samples exhibit similar characteristics to brain tissue and could become a candidate biomarker for FTLD probabilistic diagnosis
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Contribution of FDG-PET and MRI to improve Understanding, Detection and Differentiation of DementiaDukart, Jürgen 22 March 2011 (has links) (PDF)
Progression and pattern of changes in different biomarkers of Alzheimer’s disease (AD) and frontotemporal lobar degeneration (FTLD) like [18F]fluorodeoxyglucose positron emission tomography (FDG-PET) and magnetic resonance imaging (MRI) have been carefully investigated over the past decades. However, there have been substantially less studies investigating the potential of combining these imaging modalities to make use of multimodal information to further improve understanding, detection and differentiation of various dementia syndromes. Further the role of preprocessing has been rarely addressed in previous research although different preprocessing algorithms have been shown to substantially affect diagnostic accuracy of dementia. In the present work common preprocessing procedures used to scale FDG-PET data were compared to each other. Further, FDG-PET and MRI information were jointly analyzed using univariate and multivariate techniques. The results suggest a highly differential effect of different scaling procedures of FDG-PET data onto detection and differentiation of various dementia syndromes. Additionally, it has been shown that combining multimodal information does further improve automatic detection and differentiation of AD and FTLD.
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Perfil neurolinguístico comparativo das demências tipo Alzheimer e não AlzheimerSoares, Cândida Dias 14 September 2010 (has links)
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Previous issue date: 2010-09-14 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / The national surveys of dementia and its implications for language, although in small numbers, line up with the international literature in the early trends of research. The articles presented were intended to draw a profile comparison between the differential Neurolinguistics degenerative dementia of Alzheimer type and non-Alzheimer's and dementia compare the two groups with a control group. The study was conducted from March 2008 to December 2009 were evaluated in 90 participants in the Dementia Clinic of the Hospital das Clinicas, Federal University of Goias The sample consisted of 30 patients with frontotemporal lobar degeneration (DLF), 30 patients with AD and 30 subjects with no dementia. We applied the following tests neurolinguistic: Boston Diagnostic Aphasia Examination (BDAE), Boston Naming Test (Boston Naming Test - BNT), Verbal Fluency Category for Semantics and Semantic and Phonemic Fluency (FAS), Token Test, subtest of Vocabulary / WAIS-R Similarities subtest of and / WAIS-R. To compare the performance of the group used the Mann-Whitney. All groups showed substantial linguistic differences. The APP group stood out from the other groups when compared to DA, showing that fluency, vocabulary, abstraction of ideas, understanding, reading and writing are more impaired. The FTD group reinforced the presence of dysfunction in semantic and phonemic verbal fluency DS group showed a statistically significant abstractive capacity with respect to the AD group. The DLF group is the group where the oral expression was shown to be noticeably compromised compared to the AD group. The language is therefore an indispensable tool to aid in the differential diagnosis of dementia. / As investigações nacionais das demências e suas implicações na linguagem, embora ainda em pequeno número, alinham-se com a literatura internacional, nas primeiras tendências de investigação. Os artigos apresentados tiveram como objetivo traçar um perfil diferencial neurolinguístico comparativo entre as demências degenerativas do tipo Alzheimer e não Alzheimer e comparar os dois grupos demenciais com um grupo controle. Foi realizado o estudo no período de março de 2008 a dezembro de 2009 em que foram avaliados 90 participantes do Ambulatório de Demências do Hospital das Clínicas da Universidade Federal de Goiás. A amostra foi constituída por 30 pacientes com Degenerações Lobares Frontotemporais (DLF); 30 pacientes com DA e 30 indivíduos com ausência de demência. Foram aplicados os seguintes testes neurolinguísticos: Teste de Boston para Diagnóstico da Afasia (BDAE), Teste de Nomeação de Boston (Boston Naming Test – BNT), Fluência Verbal por Categoria Semântica e Fluência Fonêmica e Semântica (F.A.S.),Token Test, Subteste de Vocabulário / WAIS-R e Subteste de Semelhanças / WAIS-R. Para comparar o desempenho dos grupo utilizou-se o teste de Mann-Whitney. Todos os grupos avaliados mostraram diferenças lingüísticas significativas. O grupo APP destacou-se dos demais grupos quando comparado ao grupo DA, demonstrando que a fluência, o vocabulário, a abstração de idéias, a compreensão, a leitura e a escrita encontram-se mais comprometidas. O grupo DFT reforçou a presença da disfunção na fluência verbal fonêmica semântica e o grupo DS demonstrou significância estatística na capacidade abstrativa com relação ao grupo DA. O grupo DLF foi o grupo em que a expressão oral mostrou-se visivelmente mais comprometida comparada ao grupo DA. A linguagem é, portanto, um instrumento indispensável para auxiliar no diagnóstico diferencial das demências.
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Banco de Cérebros do Brasil Central (BCBC): prevalência de demências e correlação clínico-patológica / Brains Bank of Central of Brazil (BBCB): prevalence dementias correlation and climical pathologySilva, Wesley Gomes da 29 January 2016 (has links)
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Previous issue date: 2016-01-29 / The diagnosis of dementia is made through autopsy. The histopathological and immunohistochemical technique makes it possible to differentiate the subtypes of dementia by pre-established macroscopic and microscopic criteria. Banks brain, although recent, provide biological material quality for multidisciplinary research in normal subjects and with dementia. Objectives: To correlate clinical findings with neuropathological cases with dementia from the Brains Bank of Central of Brazil (BBCB); establish morphological patterns in macroscopic focal dementias; determine the prevalence of diagnosis of other types of dementia. Materials and Methods: Brain Study from autopsies of patients with neurodegenerative diseases of dementia clinic of the HC-UFG (Ethics Committee of the Protocol on research 0692007). The brains were processed following dissection and measurement protocol. Appropriate external and macroscopic morphological descriptions and coronal and sagittal sections were performed. Results: 15 brains, 9 female patients were studied, aged 10 to 89 years. The types of dementias found in BCBC were 5 cases of frontotemporal dementia (FTD), 3 Alzheimer's disease (AD), 3 patients had primary progressive aphasia (PPA) and corticobasal degeneration (CBD), 1 Huntington's disease, 1 disease Creutzfeldt-Jakob 1, Rasmussen's encephalitis and 1 depressive pseudodementia (Cotard’s syndrome). Described frontal gyrus supernumerary in 3 cases of CBD and 2 cases of FTD. Discussion: Most cases presented morphological pattern of the respective type of dementia according to the literature, except PPA with CBD. In BCBC material only 20% of AD cases were 27% and frontotemporal lobar degeneration (FTLD). Conclusion: The higher prevalence of dementia in BCBC was the type FTLD. The frontotemporal focal atrophy was the most observed type of change. The cases with FTD showed classic morphological patterns, while the PPA CBD was different standard literature. The BCBC will enable studies in various research areas. / O diagnóstico definitivo das demências é feito através de necropsia. Os exames anatomopatológico e imunoistoquímico possibilitam diferenciar os subtipos de demência por critérios macroscópicos e microscópicos pré-estabelecidos. Os bancos de cérebros, apesar de recentes, fornecem material biológico de qualidade para pesquisas multidisciplinares de indivíduos normais e com demência. Objetivos: Correlacionar aspectos clínicos com alterações neuropatológicas de casos com demências provenientes do Banco de Cérebros do Brasil Central (BCBC); estabelecer padrões morfológicos macroscópicos nas demências focais; verificar a prevalência do diagnóstico de outros tipos de demências. Materiais e Métodos: Estudo de cérebros provenientes de necropsias de pacientes com doenças neurodegenerativas do ambulatório de demências do HC-UFG (protocolo do Comitê de ética em pesquisa 0692007). Os cérebros foram processados seguindo protocolo de dissecção e mensuração. Foram realizadas as devidas descrições morfológicas e macroscópicas externas e dos cortes coronais e sagitais. Resultados: Foram estudados 15 cérebros, 9 de pacientes do sexo feminino, com idade entre 10 a 89 anos. Os tipos de demências encontrados no BCBC foram: 5 casos de demência frontotemporal (DFT), 3 de doença de Alzheimer (DA), 3 casos com afasia progressiva primaria (APP) e degeneração corticobasal (DCB), 1 de doença de Huntington, 1 de doença de Creutzfeldt-Jakob, 1 de encefalite de Rasmussen e 1 de pseudodemência depressiva (síndrome de Cotard). Foi observado giro frontal supranumerário nos 3 casos de DCB e em 2 casos de DFT. Discussão: A maioria dos casos apresentou padrão morfológico do respectivo tipo de demência de acordo com a literatura, exceto APP com DCB. No material do BCBC apenas 20% dos casos foram de DA e 27% degeneração lobar frontotemporal (DLFT). Conclusão: A maior prevalência de demências no BCBC foi do tipo DLFT. A atrofia focal frontotemporal foi o tipo de alteração mais observada. Os casos com DFT apresentaram padrões morfológicos clássicos, enquanto que os de APP com DCB apresentaram padrão diferente da literatura. O BCBC possibilitará a realização de estudos em várias linhas de pesquisa.
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Dégénérescences lobaires frontotemporales : vers une nouvelle classification, vers de nouveaux marqueurs / Frontotemporal lobar degeneration : to a new classification, to new markersPapegaey, Anthony 19 December 2016 (has links)
Le terme dégénérescence lobaire frontotemporale ou FTLD définit un groupe hétérogène de maladies neurodégénératives caractérisé par des troubles du langage, du comportement et/ou moteurs qui résultent principalement d’une dégénérescence du cortex frontal et temporal. Cette hétérogénéité tant au niveau clinique, génétique que neuropathologique rend cette pathologie très complexe et il existe aujourd’hui un véritable problème de diagnostic différentiel des FTLD. Le diagnostic final des FTLD repose ainsi sur l’examen neuropathologique, la nature des lésions observées et leurs constituants moléculaires. La caractérisation de ces lésions a permis d’établir une classification des FTLD qui ne cesse d’évoluer avec la découverte de nouveaux acteurs moléculaires. À l’instar de nombreuses maladies neurodégénératives, les FTLD sont caractérisées par la présence de protéines agrégées dans les régions cérébrales affectées. Cependant, contrairement à la maladie d’Alzheimer (MA), ces agrégats ne sont pas toujours constitués des mêmes protéines. Ainsi, approximativement 40% des cas de FTLD présentent des agrégats composés de protéines Tau hyper et anormalement phosphorylées, et forment le groupe FTLD-Tau. Lorsqu’aucune pathologie Tau n’est détectée, les patients présentent généralement des inclusions neuronales cytoplasmiques ou intranucléaires immunoréactives pour la protéine TDP-43 (transactive response DNA binding protein 43), et constituent la sous-classe FTLD-TDP. Plus rarement, la protéine FUS (Fused in Sarcoma, FTLD-FUS) ou des protéines liées au système ubiquitine protéasome peuvent également s’agréger (FTLD-UPS). La génétique représente également une composante majeure des FTLD avec 10 à 15% des cas correspondant à des formes héréditaires dominantes. Les premières mutations furent découvertes sur le gène MAPT. Le gène de la progranuline (GRN) fut ensuite identifié comme fréquemment associé aux FTLD. Plus récemment, une répétition anormale d’héxanucléotides GGGGCC au sein du gène C9ORF72 (chromosome 9 open reading frame 72) a été montrée comme étant responsable d’un grand nombre de cas familiaux de FTLD. De manière moins fréquente, d’autres gènes tels que VCP (valosin containing protein) ou CHMP2B (charged multivesicular body protein 2B) peuvent aussi être associés à des cas familiaux de FTLD. Des années avant la découverte des principaux acteurs moléculaires des FTLD, des études ont décrit une perte partielle ou totale des protéines Tau physiologiques dans le tissu cérébral. A l’origine, ce phénomène fut observé dans un groupe de démences appelées DLDH pour démences sans signe histopathologique distinctif (plus tard appelé FTLD-ni pour no inclusion). En 2006, la majorité de ces cas a été reclassée en tant que FTLD-U (présence de lésions immunoréactives pour l’ubiquitine). En revanche, aucune étude ne s’est intéressée à cette perte de Tau depuis celle de Zhukareva et collègues en 2003. Au regard des récentes avancées sur la compréhension de la base moléculaire et génétique des FTLD, la pertinence de cette perte de Tau reste ainsi encore à déterminer. Dans ce contexte, ce travail de recherche a pour principal objectif d’étudier l’expression des protéines Tau au sein du tissu cérébral d’individus sains ou atteints de différents troubles neurodégénératifs (MA, FTLD-Tau, FTLD-TDP-GRN, FTLD-TDP-C9ORF72, FTLD-TDP et FTLD-FUS sporadiques) en utilisant la technique d’immunoempreinte. De manière remarquable, nous avons mis en évidence une réduction significative de Tau, et ce, spécifiquement chez les patients FTLD-TDP-GRN. Ainsi, nos résultats démontrent que ces cas, appelés FTLD-TDP-GRNltau (pour low Tau protein level), caractérisés par une altération synaptique et une astrogliose très importante, pourraient constituer un groupe distinct dans la classification des FTLD [...] / FTLD is a clinical syndrome mainly characterized by progressive deterioration in behavior, personality and/or language resulting from progressive frontal and temporal degeneration. In addition, movement disorder can also be frequently observed. Given this phenotype variability, FTLD clinical diagnosis remains difficult and uneasy to establish with certainty.The final diagnosis relies on neuropathological examination of the brain, the characteristics of these brain lesions and their molecular basis. Indeed, as many neurodegenerative diseases, FTLD are characterized by the presence of protein aggregates in the affected brain regions. However, in contrast to the well-characterized nature of protein inclusions in Alzheimer’s disease (AD), proteinaceous aggregates in FTLD can be composed of different proteins. Thus, approximatively 40% of FTLD cases display aggregates made of abnormally and hyperphosphorylated Tau proteins and constitute the FTLD-Tau subclass. However, most of FTLD brains are negative for Tau inclusions and exhibit neuronal cytoplasmic and/or nuclear inclusions immunoreactive for transactive response DNA binding protein 43 (TDP-43) and constitute the FTLD-TDP subclass). To a lesser extent, another protein called FUS (Fused in Sarcoma protein) is found in aggregates that are Tau and TDP-43 negative. This subclass is thus named FTLD-FUS. Finally, inclusions negative for Tau, TDP-43 or FUS are observed in rare cases of FTLD and associated with ubiquitin-proteasome system related proteins (FTLD-UPS).Gene mutations also play an important role in FTLD with 30 to 50% of patients reporting a positive family history of FTD and 10 to 15% of patients corresponding to dominantly inherited form. Firstly described are the MAPT mutations. Mutations in the progranulin gene GRN were then found to be the most frequent mutations associated with FTLD. More recently, two studies demonstrated that expanded hexanucleotide GGGGCC repeats in a noncoding region of the chromosome 9 open reading frame 72 (C9ORF72) gene was responsible for a large proportion of FTLD. Less frequently mutations in the valosin containing protein (VCP) gene or charged multivesicular body protein 2B (CHMP2B) gene are also found associated with FTLD.Prior to the discovery of the main molecular actors of FTLD, studies described a partial or total loss of soluble or physiological Tau protein expression in both grey and white matter. This loss of Tau was originally found in a subset of dementia called DLDH for Dementia Lacking Distinctive Histopathology (renamed later FTLD-ni for FTLD with no inclusion). In 2006, most of these cases were reclassified as FTLD-U (presenting with ubiquitin positive inclusions). However, additional investigation with specific regards to this loss of Tau expression has not been reported since Zhukareva et al. in 2003. With the progress in genetics and neuropathology of FTLD, the question of whether this reduction of Tau expression is seldom remains ill-defined.This work takes place in this context whose primary goal was to investigate human brain Tau protein expression in Control, AD, FTLD-Tau, FTLD-TDP-GRN, FTLD-TDP-C9ORF72, sporadic FTLD-TDP and sporadic FTLD-FUS brains using western blot analysis. Remarkably, we demonstrated a huge reduction of all six human brain Tau isoforms only in a subset of FTLD-TDP brains with mutation on the GRN gene. Thus, our data clearly suggest that these specific cases, referred to as FTLD-TDP-GRNltau (for low levels of Tau protein), could be part of the current classification as a distinct entity with more severe synaptic dysfunction and astrogliosis. Beside this, we also performed a comparative proteomic study between the different FTLD sub-classes in order to find common physiopathological mechanisms.
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Pesquisa de mutações do gene GRN e dosagem plasmática de progranulina em casuística brasileira de degeneração lobar frontotemporal / Mutations in GRN and plasma progranulin levels in a Brazilian cohort of Frontotemporal Lobar DegenerationTakada, Leonel Tadao 29 June 2015 (has links)
Introdução: A demência frontotemporal (DFT) inclui a variante comportamental da demência frontotemporal (vcDFT), a variante semântica da afasia progressiva primária (vsAPP), e a variante não fluente da APP (vnfAPP). Os genes em que são encontradas mutações causadoras de DFT mais frequentemente são: GRN (que codifica a progranulina), MAPT (que codifica a proteína tau) e C9orf72. Métodos: Foram incluídos probandos diagnosticados com vcDFT, vsAPP ou vnfAPP, com base com os critérios diagnósticos mais recentes, e um grupo de indivíduos cognitivamente normais. Os éxons 2-12 de GRN e os éxons 1, 9-13 de MAPT foram sequenciados pelo método de Sanger, e foi realizada dosagem de progranulina no plasma. Resultados: foram incluídos 62 probandos, sendo 44 com vcDFT, 9 com vsAPP, e 9 com vnfAPP. Antecedente familiar de demência foi positivo em 45,1% dos probandos, e de DFT, em 24,1%. Os 60 indivíduos do grupo controle tinham idade média de 60,8±8,5 anos. Foram identificadas seis mutações nulas em GRN (p.Q130X, p.V200Gfs*18, p.Q257Pfs*26, p.Q300X, p.S301Cfs*60 e p.D317Afs*11) e uma mutação patogênica em MAPT (p.N279K). A dosagem média de progranulina plasmática nos pacientes com mutações de GRN foi de 29,8±11,9ng/ml Conclusões: A frequência de mutações patogênicas em GRN nesta casuística foi de 9,6%, e a de mutações em MAPT foi de 1,6%. Entre casos familiais de DFT, a frequência de mutações em GRN foi de 33,3%, e em MAPT foi de 6,7%. Duas das mutações encontradas em GRN (p.Q130X e p.D317Afs*11) ainda não foram descritas em casos de DFT. O valor de corte de 70ng/ml identificou as mutações nulas de GRN com sensibilidade e especificidade de 100% / Introduction: Frontotemporal dementia (FTD) encompasses behavioral variant of frontotemporal dementia (bvFTD), semantic variant of primary progressive aphasia (svPPA), and nonfluent variant PPA (nfvPPA). The genes in which FTD-causing mutations are most frequently found are: GRN (which encodes progranulin), MAPT (which encodes tau protein) and C9orf72. Methods: We included probands diagnosed with bvFTD, svPPA or nfvPPA, based on the most recent diagnostic criteria, and a group of cognitively normal individuals. GRN exons 2-12 and MAPT exons 1, 9-13 were sequenced by the Sanger method, and plasma progranulin levels were measured. Results: we included 62 probands (44 with bvFTD, 9 with svPPA, and 9 with nfvPPA). Family history of dementia was positive in 45.1% of probands, and of DFT, in 24.1%. The control group of 60 individuals had a mean age of 60.8±8.5 years. Six null GRN mutations were identified in (p.Q130X, p.V200Gfs*18, p.Q257Pfs*26, p.Q300X, p.S301Cfs*60 e p.D317Afs*11) and one MAPT pathogenic mutation (p.N279K). The mean plasma progranulin level in patients with GRN mutations was 29.8±11,9ng/ml. Conclusions: The frequency of pathogenic mutations in GRN was 9.6%, and of MAPT mutations was 1.6%. Among cases of familial FTD, the frequency of GRN mutations was 33.3%, and of MAPT mutations was 6.7%. Two of the mutations found in GRN (p.Q130X and p.D317Afs*11) are novel. The cutoff value of 70ng/ml identified null GRN mutations with sensitivity and specificity of 100%
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Análise da presença de mutação no gene TARDBP em pacientes com degeneração lobar frontotemporal e implementação de metodologia para determinação dos polimorfismos do gene APOE em pacientes com Doença de Alzheimer em São Paulo - SP / Analysis of the presence of mutation in TARDBP gene in patients with frontotemporal lobar degeneration and implementation of APOE gene methodology for polymorphism determination in patients with Alzheimer\'s disease in São Paulo - SPCosta, Thaís Virgínia Moura Machado 15 August 2012 (has links)
Atualmente, as demências tornam-se mais prevalentes e constituem-se como um importante problema de saúde pública mundial. A Degeneração Lobar Frontotemporal (DLFT) e a Doença de Alzheimer (DA) são as de maior incidência. A investigação dos fatores de risco para as demências degenerativas inscreve-se entre os temas mais relevantes das neurociências e a avaliação dos fatores de risco de natureza genética tem produzido contribuições importantes. Na DLFT, mutações no gene TARDBP, codificador da proteína nuclear TDP-43, estão entre as ocorrências genéticas mais descritas, enquanto que para a DA, o alelo 4 do gene da apolipoproteína E (APOE) é o principal fator de risco. Pacientes com diagnóstico clínico de DLFT (n=47) e de DA provável (n=30) recebidos do ambulatório do Grupo de Neurologia Cognitiva e do Comportamento (GNCC) da Clínica Neurológica do HC-FMUSP foram convidados a participar do estudo. Amostras de sangue foram coletadas para a realização da extração de DNA linfocitário. Os éxons de 1-6 do gene TARDBP foram amplificados por PCR e seus produtos foram sequenciados em sequenciador automático. Os polimorfismos do gene APOE foram determinados através da técnica de PCR em tempo real. A análise do gene da TDP-43 em pacientes com DLFT mostrou a presença de uma mutação na região do éxon 6 do TARDBP (g.14935A>G) em um paciente do sexo masculino, com idade de 54 anos e diagnóstico de demência semântica. Na genotipagem dos pacientes de DA, foi observado que a metodologia utilizada, através de PCR em tempo real mostrou-se eficiente em detectar os polimorfismos do gene APOE, fornecendo resultados compatíveis quando comparados aos demais estudos brasileiros publicados anteriormente / Brazil is one of the developing countries that are undergoing a process of demographic transition in which the elderly represents a significant proportion of the total population. Neurodegenerative illnesses most commonly appear at such ages. Frontotemporal lobar degeneration (FTLD) and Alzheimers disease (AD) are the most frequent causes for dementia. The investigation of risk factors for degenerative dementia is a relevant subject of neurosciences and the evaluation of the nature of genetic risk factors has produced the most important contributions. Mutations in TARDBP gene, the encoder of the TDP-43 nuclear protein, appear as the most frequent genetic occurrences for FTLD, whereas, in DA, the 4 allele of the apolipoprotein E (APOE) is the major genetic risk factor. Patients with clinical diagnosis of FTLD types of families and sporadic (n=47) and probable AD (n=30) from the ambulatory of Cognitive Neurology Group and Behavior (CNGB) of Neurological Clinic of HC-FMUSP were invited to participate in this study. Blood samples were collected for lymphocytic DNA extraction. The APOE gene polymorphisms are being determined through the real time PCR technique. The 1-6 exons of TARDBP gene were amplified by PCR and their products were sequenced in automated sequencer. The TDP-43 gene analysis in patients with FTLD showed the presence of one mutation in the region of exon 6 TARDBP gene in a male patient of 54 years old, with diagnoses of semantic dementia. Regarding DA patients genotyping, the real time methodology has been shown as an efficient approach to detect APOE polymorphisms, presenting data similar to those observed in other Brazilian studies
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Validação da escala de estadiamento e progressão da demência frontotemporal (FTD-FRS) / Validation of the frontotemporal dementia staging and progression scale (FTD-FRS)Silva, Thais Bento Lima da 22 February 2018 (has links)
Introdução: No Brasil há carência de instrumentos validados para a análise do curso da Demência Frontotemporal (DFT). Dessa forma, torna-se relevante a validação da Escala de Estadiamento e Progressão da Demência Frontotemporal (FTD-FRS). Em nosso meio, as escalas de estadiamento das demências, como a Clinical Dementia Rating (CDR), foram elaboradas para graduar a doença de Alzheimer (DA) e não incluem os sintomas específicos da DFT. Objetivos: 1. Realizar a tradução, adaptação transcultural e validação da FTD-FRS para o contexto brasileiro. 2. Avaliar a capacidade da FTD-FRS detectar alterações em pacientes com DFTvc, afasia progressiva primária (APP) e DA após 12 meses da avaliação inicial, em comparação com a escala CDR para DLFT, e com a CDR original. Métodos: Participaram do estudo 101 indivíduos com idade igual ou superior a 40 anos, com escolaridade formal acima de dois anos, sendo 31 pacientes com diagnóstico de DFT variante comportamental (DFTvc), doze pacientes com afasia progressiva primária (APP), 28 pacientes com doença de Alzheimer (DA), oito com comprometimento cognitivo leve (CCL) e 22 controles normais (CN). Foram entrevistados os familiares ou cuidadores que tinham contato frequente com o paciente. Os pacientes com DA, e com os subtipos de DFT foram pareados quanto à gravidade da doença, segundo a CDR. Resultados: Foi realizado o processo de adaptação transcultural da FTD-FRS. Consistiu em: tradução, retrotradução (realizadas por tradutores independentes), discussão com especialistas sobre a versão em português e equivalência com a versão original, e desenvolvimento da versão final. A consistência interna da FTD-FRS, estimada pelo alfa de Cronbach foi 0,975, e o coeficiente de correlação intra-classe, para a estabilidade no teste e reteste em seis meses foi de 0,977. A análise fatorial revelou a existência de quatro fatores que se correlacionaram significativamente com os domínios da CDR-DLFT. Os pacientes com DFTvc apresentaram progressão mais rápida em 12 meses do que os demais subtipos de demência na FTD-FRS, na CDR-DLFT e na CDR-original. Considerações finais: A FTD-FRS tem propriedades psicométricas adequadas para seu uso clínico no Brasil. Este instrumento pode auxiliar na caracterização de sintomas clínicos relevantes para o diagnóstico e estadiamento da DFT. Também pode documentar os resultados relacionados à intervenção terapêutica. Este estudo fornece aos clínicos e pesquisadores um instrumento válido para estadiamento e acompanhamentode de pacientes diagnosticados com DFT / Introduction: In Brazil there is a shortage of validated instruments for the analysis of the course of Frontotemporal Dementia (FTD). Thus, the validation of the Frontotemporal Dementia Staging and Progression Scale (FTD-FRS) becomes relevant. In our setting, dementia staging scales, such as the Clinical Dementia Rating (CDR), were designed to stage Alzheimer\'s disease (AD) and did not include the specific symptoms of FTD. Objectives: 1. To perform the translation, cross-cultural adaptation and validation of the FTD-FRS for the Brazilian context. 2. Evaluate the ability of the FTD-FRS to detect changes in patients with bvFTD, primary progressive aphasia (PPA) and AD after 12 months of the initial evaluation, compared to the CDR scale for FTLD, and with the original CDR. Methods: A total of 101 individuals aged 40 years and older, with formal schooling above two years of age, were included in the study. Twenty-one patients were diagnosed with bvFTD, twelve patients with PPA, 28 AD, eight with mild cognitive impairment (MCI) and 22 normal controls (NC). Family members or caregivers who had frequent contact with the patient were interviewed. Patients with AD and with FTD subtypes were matched for disease severity, according to CDR. Results: The process of cross-cultural adaptation of the FTD-FRS was carried out. It consisted of: translation, back-translation (carried out by independent translators), discussion with experts about the Portuguese version and equivalence with the original version, and development of the final version. The internal consistency of the FTD-FRS, estimated by the Cronbach\'s alpha was 0.975, and the intra-class correlation coefficient for the test and retest stability at six months was 0.977. Factor analysis revealed the existence of four factors that correlated significantly with the CDR-DLFT domains. Patients with bvFTD showed faster progression at 12 months than the other dementia subtypes in the FTD-FRS, CDR-DLFT and CDR-original version scales. Final considerations: FTD-FRS has psychometric properties suitable for clinical use in Brazil. This instrument may aid in the characterization of clinical symptoms relevant to the diagnosis and staging of FTD. It can also document the results related to therapeutic interventions. This study provides clinicians and researchers with a valid instrument for staging and follow-up of patients diagnosed with FTD
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Análise da presença de mutação no gene TARDBP em pacientes com degeneração lobar frontotemporal e implementação de metodologia para determinação dos polimorfismos do gene APOE em pacientes com Doença de Alzheimer em São Paulo - SP / Analysis of the presence of mutation in TARDBP gene in patients with frontotemporal lobar degeneration and implementation of APOE gene methodology for polymorphism determination in patients with Alzheimer\'s disease in São Paulo - SPThaís Virgínia Moura Machado Costa 15 August 2012 (has links)
Atualmente, as demências tornam-se mais prevalentes e constituem-se como um importante problema de saúde pública mundial. A Degeneração Lobar Frontotemporal (DLFT) e a Doença de Alzheimer (DA) são as de maior incidência. A investigação dos fatores de risco para as demências degenerativas inscreve-se entre os temas mais relevantes das neurociências e a avaliação dos fatores de risco de natureza genética tem produzido contribuições importantes. Na DLFT, mutações no gene TARDBP, codificador da proteína nuclear TDP-43, estão entre as ocorrências genéticas mais descritas, enquanto que para a DA, o alelo 4 do gene da apolipoproteína E (APOE) é o principal fator de risco. Pacientes com diagnóstico clínico de DLFT (n=47) e de DA provável (n=30) recebidos do ambulatório do Grupo de Neurologia Cognitiva e do Comportamento (GNCC) da Clínica Neurológica do HC-FMUSP foram convidados a participar do estudo. Amostras de sangue foram coletadas para a realização da extração de DNA linfocitário. Os éxons de 1-6 do gene TARDBP foram amplificados por PCR e seus produtos foram sequenciados em sequenciador automático. Os polimorfismos do gene APOE foram determinados através da técnica de PCR em tempo real. A análise do gene da TDP-43 em pacientes com DLFT mostrou a presença de uma mutação na região do éxon 6 do TARDBP (g.14935A>G) em um paciente do sexo masculino, com idade de 54 anos e diagnóstico de demência semântica. Na genotipagem dos pacientes de DA, foi observado que a metodologia utilizada, através de PCR em tempo real mostrou-se eficiente em detectar os polimorfismos do gene APOE, fornecendo resultados compatíveis quando comparados aos demais estudos brasileiros publicados anteriormente / Brazil is one of the developing countries that are undergoing a process of demographic transition in which the elderly represents a significant proportion of the total population. Neurodegenerative illnesses most commonly appear at such ages. Frontotemporal lobar degeneration (FTLD) and Alzheimers disease (AD) are the most frequent causes for dementia. The investigation of risk factors for degenerative dementia is a relevant subject of neurosciences and the evaluation of the nature of genetic risk factors has produced the most important contributions. Mutations in TARDBP gene, the encoder of the TDP-43 nuclear protein, appear as the most frequent genetic occurrences for FTLD, whereas, in DA, the 4 allele of the apolipoprotein E (APOE) is the major genetic risk factor. Patients with clinical diagnosis of FTLD types of families and sporadic (n=47) and probable AD (n=30) from the ambulatory of Cognitive Neurology Group and Behavior (CNGB) of Neurological Clinic of HC-FMUSP were invited to participate in this study. Blood samples were collected for lymphocytic DNA extraction. The APOE gene polymorphisms are being determined through the real time PCR technique. The 1-6 exons of TARDBP gene were amplified by PCR and their products were sequenced in automated sequencer. The TDP-43 gene analysis in patients with FTLD showed the presence of one mutation in the region of exon 6 TARDBP gene in a male patient of 54 years old, with diagnoses of semantic dementia. Regarding DA patients genotyping, the real time methodology has been shown as an efficient approach to detect APOE polymorphisms, presenting data similar to those observed in other Brazilian studies
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