Epilepsia generalizada idiopatica : aspectos etnicos, eletroencefalograficos e de neuroimagem l / Idiopathic generalized epilepsy : clinical, electroencephalographic and neuroimagem features

Betting, Luiz Eduardo Gomes Garcia

12 December 2006

Orientadores: Fernando Cendes, Li Li Min / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-08-10T05:20:09Z (GMT). No. of bitstreams: 1 Betting_LuizEduardoGomesGarcia_D.pdf: 9629246 bytes, checksum: a5717d51675609b6835960db129c8d3b (MD5) Previous issue date: 2006 / Resumo: Epilepsias generalizadas idiopáticas (EGI) constituem de 20-40% das epilepsias e de forma oposta às epilepsias parciais, anormalidades estruturais não são esperadas. De acordo com a idade de início e o tipo principal de crise, as EGI são divididas principalmente em epilepsia ausência infantil e juvenil (EA), epilepsia mioclônica juvenil (EMJ) e epilepsia com crises tônico-clônicas generalizadas (CTCG). Os limites entre estas subsíndromes são imprecisos e a classificação muitas vezes é difícil. Devido às características semelhantes, alguns autores consideram a EGI como uma única patologia com múltiplos fenótipos (continuum biológico). O eletroencefalograma (EEG) auxilia no diagnóstico das EGI especialmente quando evidencia descargas do tipo espícula onda-lenta generalizadas com atividade de base normal. Entretanto, o EEG pode ser normal e até mesmo mostrar focalidades dificultando o diagnóstico. A ressonância magnética (RM) não é realizada de forma rotineira em pacientes com EGI. Contudo, novas técnicas de aquisição e processamento de imagens vêm detectando anormalidades sutis nestes indivíduos. O objetivo deste estudo foi investigar a fisiopatologia das EGI através da análise de características clínicas, eletroencefalográficas e de neuroimagem. Inicialmente, as características dos EEGs de 180 pacientes com diagnóstico clínico de EGI foram avaliadas. 493 exames foram analisados. Em 33% dos pacientes o EEG inicial foi característico e em 22% o exame evidenciou focalidades. Após a identificação de focalidades utilizamos a neuroimagem convencional (análise visual) na avaliação de 134 pacientes com EGI. Observamos anormalidades na RM de 27 (20%) pacientes. A maioria das anormalidades não apresentou relação direta com as crises. Utilizamos a técnica da morfometria baseada em voxel (MBV) para investigar lesões discretas eventualmente não identificadas na neuroimagem de rotina. Esta técnica permite a comparação entre grupos de imagens aumentando a chance de detecção de anormalidades. Observamos aumento na concentração de substância cinzenta (CSC) localizada no córtex frontal de pacientes com EMJ (n=44) e EA (n=24). Observamos também uma maior CSC na região anterior do tálamo nos pacientes com crises de ausência (n=47). Avaliando as focalidades clínicas e de EEG de 22 pacientes com EGI utilizando a MBV, observamos áreas de aumento da CSC em 8 dos 9 (89%) pacientes com EMJ, 5 dos 6 (83%) pacientes com EA e 5 dos 7 (71%) pacientes com CTCG ao despertar. A volumetria do tálamo foi realizada para investigar o aumento de CSC sugerido pela MBV. A comparação entre 147 pacientes e um grupo controle evidenciou um maior volume da região anterior do tálamo nos pacientes com crises de ausência. Nossos resultados revelam que a fisiopatologia das EGI envolve o tálamo e o córtex cerebral. As diversas alterações na neuroimagem quantitativa apresentadas por cada subsíndrome sugerem um diferente mecanismo para as EGI. Este achado fortalece o conceito de diferentes doenças com fenótipos semelhantes. Mais do que isso, nossos achados indicam, uma alteração estrutural no cérebro destes indivíduos. Os diversos fenótipos estão relacionados a diferentes mecanismos fisiopatológicos. As focalidades observadas no EEG e na RM refletem a patogênese das crises em pacientes com EGI / Abstract: Idiopathic generalized epilepsies (IGE) represent 20-40% of all epilepsies and opposed to partial epilepsies, structural abnormalities are not expected. According to the age of onset and the main seizure type, IGE are divided mainly in childhood and juvenile absence epilepsy (AE), juvenile myoclonic epilepsy (JME) and generalized tonic-clonic seizures (GTCS). The limits between these subsyndromes are unclear and sometimes classification is difficult. Because of the similar characteristics, some authors consider IGE as a single pathology with multiple phenotypes (biological continuum). Electroencephalogram (EEG) helps the IGE diagnosis specially when it shows the generalized spike and wave discharges with normal background. However, the EEG may be normal or even disclose focalities difficulting the diagnosis. Magnetic resonance imaging (MRI) is not routinely performed in patients with IGE. In spite of this, new techniques of acquisition and processing of the images are detecting subtle abnormalities in these individuals. The objective of this study was to investigate the pathophysiology of the IGE using the clinical, EEG and neuroimaging features. Initially, the characteristics of the EEGs of 180 patients with clinical diagnosis of IGE were evaluated. 493 exams were analyzed. In 33% of the patients the initial EEG was characteristic and in 22% the exam revealed focalities. After the identification of the focalities, we used conventional neuroimaging (visual analysis) on the evaluation of 134 patients with IGE. We observed abnormalities in the MRI of 27 (20%) patients. Most of the abnormalities were not directly related to the seizures. We used the voxel base morphometry (VBM) technique to evaluate the images. This technique allows comparisons between groups of images increasing the chances of detecting abnormalities. We observed increased gray matter concentration (GMC) localized in the frontal cortex of patients with JME (n=44) and AE (n=24). We also observed increased GMC in the anterior thalamic region of patients with absence seizures (n=47). Evaluating the clinical and EEG focalities of 22 patients with IGE using VBM, we observed areas of increased GMC in 8 of 9 (89%) patients with JME, 5 of 6 (83%) patients with AE and 5 of 7 (71%) patients with GTCS on awakening. The volumetry of the thalamus was performed to investigate the increased GMC suggested by the VBM. The comparison between 147 patients with a control group showed increased volume of the anterior thalamic region in patients with absence seizures. Our results revealed that the pathophysiology of the IGE involves the thalamus and the cerebral cortex. The several abnormalities on the neuroimage presented by each subsyndrome suggest a different mechanism for the IGE. This finding strengths the concept of multiple diseases with similar phenotypes. Furthermore, our findings indicate a structural abnormality in the brain of these individuals. The several phenotypes are related with different pathophysiological mechanisms. The focalities present on the EEG and in the MRI reflect the pathogenesis of the seizures in patients with IGE / Doutorado / Neurociencias / Doutor em Fisiopatologia Medica

Epilepsia generalizada idiopática

Neuroimagem

Ressonância magnética

Electroencefalograma

Idiopathic generalized epilepsy

Neuroimaging

Magnetic resonance imaging

Electroencephalogram

Association Between Gamma Aminobutyric Acid (gaba) Type B Receptors Gene Polymorphisms And Idiopathic Generalized Epilepsy

Eroglu, Ezgi

01 February 2012

Epilepsy is neurological disorder affecting 0.5 to 1% of the population all around the world. It is characterized by the seizures, which are the sudden alterations of behavior due to a temporary change in electrical functioning of the brain. Idiopathic generalized epilepsy (IGE) accounts for one-fifth of all the other epilepsy types, and several gene mutations were identified as the causes of IGE. In general, voltage-gated and ligand-gated ion channel mutations are linked with seizure formation. Gamma amino butyric acid (GABA), the most important inhibitory neurotransmitter of the central nervous system, and its receptors are commonly mentioned in the pathophysiology of epilepsies. Decrease in the inhibitory effect of GABA in neurons causes epileptic discharges resulting in seizure development. The study population consisted of a total of 176 idiopathic generalized epilepsy (IGE) patients, 83 subjects having psychogenic non-epileptic seizures (PNES), 86 non-epileptic control subjects from Turkey. Total blood samples were obtained from G&uuml / lhane Military Medical Academy Hospital Neurology Department, Ankara. There was no statistically difference between the patient and control groups in terms of age. Genomic DNA isolations were performed and genotyping of G1465A and C59T polymorphisms of GABAB1 gene / rs1999501, rs967932, rs3780428 and rs944688 polymorphisms of GABAB2 gene were determined by PCR-RFLP technique. In this study, GABAB1 G1465A polymorphic allele was not observed in Turkish population. For GABAB1 C59T polymorphism, polymorphic allele frequencies were found as 0.097 in IGE patients / 0.072 in PNES subjects and 0.105 in non-epileptic control subjects. No significant difference is identified for C59T polymorphism in all three groups. Four SNPs of GABAB2 were studied / rs967932 was found to increase the risk of IGE 3.6-fold (P=0.031) compared to PNES subjects, polymorphic allele frequencies were found as 0.060 in IGE patients / 0.018 in PNES subjects and 0.035 in non-epileptic control subjects. For rs1999501 polymorphism, polymorphic allele frequencies were found as 0.077 in IGE patients / 0.048 in PNES subjects and 0.093 in non-epileptic control subjects. For rs3780428 polymorphism, polymorphic allele frequencies were found as 0.267 in IGE patients / 0.235 in PNES subjects and 0.256 in non-epileptic control subjects. For rs944688 polymorphism, polymorphic allele frequencies were found as 0.196 in IGE patients / 0.260 in PNES subjects and 0.227 in non-epileptic control subjects. No significant difference was identified for rs1999501, rs3780428 and rs944688 polymorphisms among IGE patients, PNES subjects and non-epileptic control groups. IGE risk was 6.54-fold higher for subjects having combined GA genotype for rs967932 and GG genotype for rs3780428 when compared with PNES subjects (P=0.042). The combination of CC genotype for rs1999501, GG genotype for rs967932 and TT genotype for rs944688 had around 9-fold protective effect against IGE when both compared with PNES subjects (P=0.038) and non-epileptic control subjects (P=0.041).

QH Genetics 426-470

Molekulargenetische Kartierung von genetischen Determinanten bei idiopathisch generalisierten Epilepsien

Sander, Thomas

06 March 2001

Ziel unserer molekulargenetischen Studien ist es, Gene der genetisch komplexen idiopathisch generalisierten Epilepsien (IGE) im Genom des Menschen zu lokalisieren und die verantwortlichen Genstörungen durch die Mutationsanalyse von positionell und funktionell plausiblen Kandidatengenen zu identifizieren. Unsere Kopplungsanalysen konnten einen IGE-Locus (Locus-Symbol: EJM1) in der chromosomalen Region 6p21.3 bestätigen und die Kandidatengenregion auf ein chromosomales Segment von 10 centiMorgan (cM) eingrenzen. Ein positionell und funktionell plausibles Kandidatengen ist das Gen einer Untereinheit des heterodimeren GABAB Rezeptors (Gen-Symbol: GABA-BR1). Die systematische Mutationsanalyse des GABA-BR1 Gens und eine Assoziationsstudie mit drei Sequenzpolymorphismen in den Exonen 1a1, 7 und 11 ergaben keinen Anhalt für eine Beteiligung des GABA-BR1 Gens bei der Epileptogenese der IGE. Kopplungshinweise in den chromosomalen Regionen 20q13, 8q24 und 15q14 konnten wir in unserem Familienkollektiv nicht bestätigen. Die Mutationsanalyse der Kandidatengene CHRNA4 und KCNQ2 in der Kandidatengenregion 20q13 und von zwei Kalziumkanal-Genen (CACNA1A, CACNB4) ergaben keinen Hinweis auf disponierende Sequenzvarianten bei IGE-Patienten. Unsere systematische Genomanalyse bei 130 Familien mit mehreren IGE-Angehörigen zielte auf die positionelle Eingrenzung von Genstörungen, die an der Disposition eines breiten IGE-Spektrums beteiligt sind. Bei 360 der 694 Familienangehörigen lag ein IGE-Phänotyp vor. Bei 617 Familienangehörigen wurden für die systematische Genomanalyse insgesamt 416 Mikrosatelliten-Polymorphismen mit einem durchschnittlichen Abstand von 10 cM genotypisiert. Die parameter-freien Kopplungsanalysen ergaben einen signifikanten Kopplungsbefund in der chromosomalen Region 3q26 (P = 1,7 x 10-5 bei D3S3725) sowie zwei Kopplungshinweise in den chromosomalen Regionen 2q36.1 (P = 5,4 x 10-4 bei D2S1371) und 14q23 (P = 5,6 x 10-4 bei D14S63). Positionell und funktionell plausible Kandidatengene sind die Gene des Kalium-Kanals KCNA1B und des Chlorid-Kanals CLCN2 in der Region 3q26, das Gen des Chlorid-Bikarbonat Austauschers SLC4A3 in der Region 2q36, und das Gen des Natrium-Kalzium Austauschers SLC8A3 in der Region 14q23. Der molekulargenetische Nachweis von Genmutationen für die IGE wird konkrete Einblicke in die molekularen Mechanismen der Epileptogenese eröffnen und die Voraussetzungen dafür schaffen, rational begründete Therapieansätze zu entwickeln. / The aim of our molecular genetic studies is to map genes of the genetically complex idiopathic generalized epilepsies on the human genome and to identify the causative gene variants by mutation analyses of positional and functional plausible candidate genes. Our linkage studies confirmed an IGE-locus (locus symbol: EJM1) in the chromosomal region 6p21.3 and to refine the candidate region to a chromosomal segment of 10 centiMorgan (cM). A positional and functional candidate gene is the gene encoding a subunit of the heterodimeric GABAB receptor (gene symbol: GABA-BR1). The systematic mutation screening of the GABA-BR1 gene and an association analysis with three sequence polymorphisms in exons 1a1, 7 and 11 provided no evidence that the GABA-BR1 gene confers susceptibility to the epileptogenesis of IGE. We failed to replicate previous linkage findings in the chromosomal regions 20q13, 8q24 and 15q14 in our family sample. Mutation analysis of the candidate genes CHRNA4 and KCNQ2 and two genes encoding calcium channel subunits (CACNA1A, CACNB4) did not detect common susceptibility alleles in IGE patients. Our systematic genome scan was designed to identify susceptibility loci that predispose to a broad spectrum of common IGE syndromes. Our study included 130 families with two or more siblings affected by an IGE. In total, 360 out of 694 family members were affected by an IGE-trait. 617 family members were genotyped for 416 microsatellite polymorphisms with an average distance of 10 cM. Non-parametric linkage analysis provided significant evidence for a novel IGE susceptibility locus on chromosome 3q26 (ZNPL = 4.19 at D3S3725; P = 0.000017) and suggestive evidence for two IGE loci on chromosome 14q23 (ZNPL = 3.28 at D14S63; P = 0.000566), and chromosome 2q36 (ZNPL = 2.98 at D2S1371; P = 0.000535). Positional and functional candidate genes include the potassium channel gene KCNA1B and the chloride channel gene CLCN2 in the region 3q26, the chloride-bicarbonate anion exchanger gene SLC4A3 in the region 2q36, and the sodium-calcium exchanger gene SLC8A3 in the region 14q23. The molecular genetic detection of susceptibility genes for IGE will provide clues to elucidate the complex molecular pathways of epileptogenesis, and, finally, will help to develop rational treatment strategies.

Molekulargenetik

Idiopathisch generalisierte Epilepsie

Genomanalyse

Kandidatengene

molecular genetics

Idiopathic generalized epilepsy

genome scan

candidate genes

610 Medizin

33 Medizin

YH 6300

ddc:610

Análise quantitativa das descargas epileptiformes generalizadas e da neuroimagem de pacientes com epilepsia generalizada idiopática / Quantitative analysis of generalized epileptiform discharges and neuroimage of patients with generalized idiopathic epilepsy

Braga, Aline Marques da Silva [UNESP]

18 February 2016

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Agradecemos a compreensão. on 2016-04-27T16:55:50Z (GMT) / Submitted by ALINE MARQUES DA SILVA BRAGA null (aline.sms@gmail.com) on 2016-05-16T12:39:41Z No. of bitstreams: 1 Tese Aline.pdf: 9957836 bytes, checksum: 6bc924ddc7c437583c8bda4fb0a99ab3 (MD5) / Approved for entry into archive by Juliano Benedito Ferreira (julianoferreira@reitoria.unesp.br) on 2016-05-16T14:36:42Z (GMT) No. of bitstreams: 1 braga_ams_dr_bot.pdf: 9957836 bytes, checksum: 6bc924ddc7c437583c8bda4fb0a99ab3 (MD5) / Made available in DSpace on 2016-05-16T14:36:42Z (GMT). No. of bitstreams: 1 braga_ams_dr_bot.pdf: 9957836 bytes, checksum: 6bc924ddc7c437583c8bda4fb0a99ab3 (MD5) Previous issue date: 2016-02-18 / Fundação de Amparo à Pesquisa do Estado de Mato Grosso (FAPEMAT) / Fundamento: Evidências experimentais de modelos animais de crises de ausência sugerem focalidades no início das descargas generalizadas. Estudos clínicos indicam que pacientes com o diagnóstico de epilepsia generalizada idiopática (EGI) exibem anormalidades focais que envolvem o circuito tálamo-cortical no eletroencefalograma (EEG) e na neuroimagem. Objetivos: Investigar a presença de características focais nas descargas generalizadas interictais usando análise quantitativa do EEG (EEGq) e avaliar o córtex do giro do cíngulo usando múltiplas abordagens quantitativas de neuroimagem. Métodos: 75 EEGs de 64 pacientes foram analisados. A primeira espícula generalizada inequívoca foi marcada para cada descarga. Três métodos de análise de fonte geradora da atividade observada foram aplicados: transformação do dipolo em imagem (dipole source imaging-DSI), abordagem LORETA aplicada iterativamente (CLARA), e análise de dipolo equivalente de componentes independentes com análise de agrupamentos. Após processamento do EEG, 32 pacientes (18 mulheres, 32 ± 11) fizeram ressonância magnética. Foram utilizados três métodos para comparar o giro do cíngulo de pacientes e controles: morfometria baseada em voxel (VBM), análise cortical e análise de formato. Resultados: 753 descargas generalizadas foram analisadas. Usando as três técnicas, o lobo frontal foi a principal fonte das descargas (70%), seguido pelos lobos parietal e occipital (14%) e, por fim, os núcleos da base (12%). As principais fontes anatômicas das descargas generalizadas foram o córtex da porção anterior do giro do cíngulo (36%) e giro frontal medial (23%). A VBM mostrou atrofia de substância cinzenta na porção anterior do giro do cíngulo (972 mm3) e no istmo (168 mm3). Análises individuais do córtex do giro do cíngulo mostraram resultados semelhantes. Comparações de superfície mostraram anormalidades principalmente na porção posterior do giro do cíngulo (718.12 mm2). A análise de formato demonstrou uma predominância de anormalidades nas porções anterior e posterior do giro do cíngulo. Discussão: A análise de fonte não mostrou uma fonte única comum a todas as descargas generalizadas mas indicou predominância do giro do cíngulo e lobo frontal. Além disso, o estudo sugere a existência de anormalidades estruturais sutis no giro do cíngulo, principalmente nas porções anterior e posterior. / Background: Experimental evidence from animal models of absence seizures suggests a focal source for the initiation of generalized spike-and-wave (GSW) discharges. Clinical studies indicate that patients diagnosed with idiopathic generalized epilepsy (IGE) exhibit focal electroencephalographic and subtle structural abnormalities, which involve the thalamo-cortical circuitry. Aims: The objectives of the current investigation were to investigate whether interictal generalized discharges exhibit focal characteristics using qEEG analysis and to perform a comprehensive analysis of the cingulate cortex using multiple quantitative structural neuroimaging techniques. Methods: 75 EEG recordings from 64 patients were analyzed. The first unequivocally confirmed generalized spike was marked for each discharge. Three methods of source imaging analysis were applied: dipole source imaging (DSI), classical LORETA analysis recursively applied (CLARA), and equivalent dipole of independent components with cluster analysis. After EEG analysis, 32 patients (18 women, 30± 10 years) and 36 controls (18 women, 32 ±11 years) were imaged by 3 Tesla magnetic resonance (MRI). We used three models to compare cingulate gyrus of patients and the control group: voxel-based morphometry (VBM), cortical analyses and shape analyses. Results: A total of 753 GSW discharges were spatiotemporally analyzed. Source analysis using all three techniques revealed that the frontal lobe was the principal source of GSW discharges (70%), followed by the parietal and occipital lobes (14%), and the basal ganglia (12%). The main anatomical sources of the generalized discharges were the anterior cingulate cortex (36%) and the medial frontal gyrus (23%). VBM analyses of cingulate gyrus showed areas of gray matter atrophy, mainly in the anterior cingulate gyrus (972 mm3) and the isthmus (168 mm3). Individual analyses of the cingulate cortex were similar between patients with IGE and controls. Surface- based comparisons revealed abnormalities located mainly in the posterior cingulate cortex (718.12 mm2). Shape analyses demonstrated a predominance of abnormalities in the anterior and posterior portions of cingulate gyrus abnormalities. Discussion: Source analysis did not reveal a common focal source of generalized discharges. However, there was a predominance of GSW discharges originating from the cingulate gyrus and the frontal lobe. Furthermore, this study suggests that patients with IGE have structural abnormalities in the cingulate gyrus mainly localized at the anterior and posterior portions. This finding is subtle and variable among patients. / FAPEMAT: 11/16452-2

Epilepsia generalizada idiopática

Paroxismos epileptiformes generalizados

Eletroencefalograma quantitativo

Giro do cíngulo

Neuroimagem

Análise de formato

Morfometria baseada em voxel

Idiopathic generalized epilepsy

Generalized discharges

Quantitative electroencephalography

Cingulate cortex

Neuroimaging

Shape analysis

Voxel-based morphometry

Análise quantitativa das descargas epileptiformes generalizadas e da neuroimagem de pacientes com epilepsia generalizada idiopática

Braga, Aline Marques da Silva

January 2016

Orientador: Luiz Eduardo Gomes Garcia Betting / Resumo: Fundamento: Evidências experimentais de modelos animais de crises de ausência sugerem focalidades no início das descargas generalizadas. Estudos clínicos indicam que pacientes com o diagnóstico de epilepsia generalizada idiopática (EGI) exibem anormalidades focais que envolvem o circuito tálamo-cortical no eletroencefalograma (EEG) e na neuroimagem. Objetivos: Investigar a presença de características focais nas descargas generalizadas interictais usando análise quantitativa do EEG (EEGq) e avaliar o córtex do giro do cíngulo usando múltiplas abordagens quantitativas de neuroimagem. Métodos: 75 EEGs de 64 pacientes foram analisados. A primeira espícula generalizada inequívoca foi marcada para cada descarga. Três métodos de análise de fonte geradora da atividade observada foram aplicados: transformação do dipolo em imagem (dipole source imaging-DSI), abordagem LORETA aplicada iterativamente (CLARA), e análise de dipolo equivalente de componentes independentes com análise de agrupamentos. Após processamento do EEG, 32 pacientes (18 mulheres, 32 ± 11) fizeram ressonância magnética. Foram utilizados três métodos para comparar o giro do cíngulo de pacientes e controles: morfometria baseada em voxel (VBM), análise cortical e análise de formato. Resultados: 753 descargas generalizadas foram analisadas. Usando as três técnicas, o lobo frontal foi a principal fonte das descargas (70%), seguido pelos lobos parietal e occipital (14%) e, por fim, os núcleos da base (12%... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Background: Experimental evidence from animal models of absence seizures suggests a focal source for the initiation of generalized spike-and-wave (GSW) discharges. Clinical studies indicate that patients diagnosed with idiopathic generalized epilepsy (IGE) exhibit focal electroencephalographic and subtle structural abnormalities, which involve the thalamo-cortical circuitry. Aims: The objectives of the current investigation were to investigate whether interictal generalized discharges exhibit focal characteristics using qEEG analysis and to perform a comprehensive analysis of the cingulate cortex using multiple quantitative structural neuroimaging techniques. Methods: 75 EEG recordings from 64 patients were analyzed. The first unequivocally confirmed generalized spike was marked for each discharge. Three methods of source imaging analysis were applied: dipole source imaging (DSI), classical LORETA analysis recursively applied (CLARA), and equivalent dipole of independent components with cluster analysis. After EEG analysis, 32 patients (18 women, 30± 10 years) and 36 controls (18 women, 32 ±11 years) were imaged by 3 Tesla magnetic resonance (MRI). We used three models to compare cingulate gyrus of patients and the control group: voxel-based morphometry (VBM), cortical analyses and shape analyses. Results: A total of 753 GSW discharges were spatiotemporally analyzed. Source analysis using all three techniques revealed that the frontal lobe was the principal ... (Complete abstract click electronic access below) / Doutor

Epilepsia generalizada idiopática

Paroxismos epileptiformes generalizados

Eletroencefalograma quantitativo

Giro do cíngulo

Neuroimagem.

Análise de formato

Morfometria baseada em voxel

Idiopathic generalized epilepsy

Generalized discharges

Quantitative electroencephalography

Cingulate cortex

Neuroimaging

Shape analysis

Voxel-based morphometry