Master's Dissertation
DOI
https://doi.org/10.11606/D.5.2012.tde-02102012-084400
Document
Author
Full name
Thaís Virgínia Moura Machado Costa
E-mail
Institute/School/College
Knowledge Area
Date of Defense
Published
São Paulo, 2012
Supervisor
Committee
Chadi, Gerson (President)
Bahia, Valéria Santoro
Nitrini, Ricardo
Bahia, Valéria Santoro
Nitrini, Ricardo
Title in Portuguese
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
Keywords in Portuguese
APOE
Degeneração lobar frontotemporal
Doença de Alzheimer
Metanálise
Mutação
Polimorfismo genético
Proteinopatias TDP-43
TARDBP
Degeneração lobar frontotemporal
Doença de Alzheimer
Metanálise
Mutação
Polimorfismo genético
Proteinopatias TDP-43
TARDBP
Abstract in Portuguese
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
Title in English
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 - SP
Keywords in English
Alzheimers disease
APOE
Frontotemporal lobar degeneration
Genetic polymorphism
Meta-analysis
Mutation
TARDBP
TDP-43 proteinopathies
APOE
Frontotemporal lobar degeneration
Genetic polymorphism
Meta-analysis
Mutation
TARDBP
TDP-43 proteinopathies
Abstract in English
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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Publishing Date
2012-10-02
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