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221	Evaluation du systeme nerveux autonome dans l'hypertension arterielle essentielle Yacine, Amine 06 1900 (has links) L’analyse spectrale de la fréquence cardiaque, de la pression artérielle systolique, de la pression artérielle diastolique ainsi que de la respiration par la transformée de Fourier rapide, est considérée comme une technique non invasive pour la détermination de l’activité du système nerveux autonome (SNA). Dans une population de sujets normaux volontaires, nous avons obtenu à l’état basal, des oscillations de basses fréquences (0,05-0,15Hz) reliées au système nerveux sympathique autonome et des oscillations de hautes fréquences (0,2Hz) représentant sur les intervalles entre chaque ondes R de l’électrocardiogramme (RR), l’arythmie sinusale respiratoire correspondant à une activité vagale. Nous avons comparé les tests de stimulation du système nerveux sympathique autonome déclenché par le passage de la position de repos (en décubitus dorsal), à la position orthostatique volontaire et le passage de la position de repos à la position orthostatique avec la table basculante à 60o. Nous avons également comparé un groupe normotendu à un groupe hypertendu qui a été soumis au passage du repos à l’orthostation volontaire et pour lesquels nous avons évalué la sensibilité du baroréflexe et la réponse sympathique par la mesure des catécholamines circulantes. Dans un groupe de sujets ayant une hypertension artérielle essentielle, nous avons évalué l’effet de la thérapie hypotensive, par le Trandolapril qui est un Inhibiteur de l’enzyme de conversion (IEC) de l`angiotensine. Dans ce groupe hypertendu, nous avons procédé, en plus de la stimulation sympathique par l’orthostation volontaire, à un exercice isométrique de trois minutes à 30 % de la force maximale. Nous avons également complété notre évaluation par la mesure de la densité de récepteurs ß2 adrénergiques sur lymphocytes et par la mesure des indices de contractilité à l’aide de l’échocardiographie en M mode. Les résultats ont montré, dans les groupes normaux volontaires, dans les deux types de stimulation du système nerveux sympathique par la position orthostatique, une augmentation significative des catécholamines plasmatiques avec une augmentation de la fréquence cardiaque et des basses fréquences de RR, confirmant ainsi que l’on est en état de stimulation sympathique. On observe en même temps une diminution significative des hautes fréquences de RR, suggérant un retrait vagal lors de cette stimulation. On a observé au test de la table basculante six cas d’hypotension orthostatique. On a comparé la position orthostatique volontaire entre le groupe de sujets normaux et le groupe de sujets hypertendus. L’analyse spectrale croisée de RR et de la pression artérielle systolique a permis d’évaluer dans l’hypertension artérielle (HTA), essentielle une sensibilité du baroréflexe atténuée, accompagnée d’une réactivité vagale réduite en présence d’une activité et d’une réactivité sympathique augmentées suggérant une altération sympathovagale dans l’HTA. Dans le groupe de sujets hypertendus traités (Trandolapril 2mg/jour), nous avons identifié un groupe de répondeurs au traitement par le Trandolapril et un groupe de non répondeurs à ce type de thérapie anti-hypertensive. Le groupe répondeur avait un profil hyper-adrénergique avec une hyper-réactivité sympathique, une fréquence cardiaque et des pressions artérielles diastolique et systolique plus élevées au repos. Dans le groupe total traité au Trandolapril, la densité des récepteurs ß2 adrénergiques a doublé, après thérapie, alors que la réactivité des basses fréquences obtenues à l’analyse spectrale a augmenté. Nous avons montré dans notre étude qu’un IECA a pu inhiber le mécanisme facilitateur de l’angII sur les terminaisons nerveuses sympathiques et a permis ainsi de réduire l’hyperactivité sympathique et le mécanisme de « down regulation » des récepteurs ß2 adrénergiques rendant ainsi l’expression de l’influence du SNA post synaptique plus efficace. Dans l’ensemble de nos protocoles cliniques, par l’utilisation de l’analyse spectrale des signaux RR, de la pression artérielle systolique,de la pression artérielle diastolique et de la respiration, nous avons montré que cette technique non invasive permet de décrire et de mieux comprendre les mécanismes physiologiques, physiopathologiques et pharmacologiques reliés au système nerveux autonome et à l’hypertension artérielle essentielle. / The spectral analysis of the heart rate, the systolic blood pressure, the diastolic blood pressure and the respiration with the Fast Fourier Transform, is considered as a non-invasive technique for the determination of the autonomic nervous system activity. In a population of normal volunteer subjects, we obtained in the basal state, low-frequency oscillations related to the sympathetic autonomous nervous system (0.05-0.15Hz) and the high-frequency oscillations (0.2Hz), which represent, on RR intervals, the respiratory sinus arrhythmia corresponding to vagal activity. We compared the sympathetic nervous system stimulation tests triggered by the transition from resting to voluntary orthostatic positions and the transition from resting to orthostatic position using tilt table at 60o. We also compared a normal blood pressure group to a hypertensive group which were both subject to the transition from resting to voluntary orthostation and for whom we evaluated the baroreflex sensitivity and the sympathetic response by measuring circulating catecholamines. In a group of subjects having an essential arterial hypertension, we have evaluated the effect of hypotensive therapy, by the Trandolapril which is an Angiotensin Converting Enzyme Inhibitor. In the hypertensive group, we evaluated the sympathetic stimulation using the voluntary orthostation, and we have also proceeded to a 3 minutes isometric exercise at 30% of maximum force. We have also completed our evaluation by measuring both the ß2 adrenergic receptor density on isolated lymphocytes and the contractility index using the echocardiography in M mode. In both sympathetic nervous system stimulation types by orthostatic position, the results have shown, for normal blood pressure volunteer subject groups, a significant increase in concentration of plasma catecholamines with an increase of heart rate (HR) and the low frequency RR, confirming therefore that we are in the presence of a sympathetic stimulation state. At the same time, we observed a significant decrease of high frequency of RR, suggesting a vagal withdrawal during the stimulation. We observed six cases of orthostatic hypotension from the tilt table test. We compared the voluntary orthostatic position between normal and hypertension subject groups. The results with combined spectral analysis of RR and the systolic blood pressure allowed to evaluate in the essential high blood pressure a reduced baroreflex sensitivity along with a reduced vagal reactivity in presence of increased sympathetic activity and reactivity suggesting a sympatho-vagal alteration in essential arterial hypertension. In hypertensive subjects treated with Trandolapril 2mg/day, we have identified a group responding to Trandolapril treatment and a group of non-responders to this type of anti-hypertensive therapy. The responding group has an hyper-adrenergic profile with higher sympathetic reactivity, heart rate and arterial diastolic and systolic pressures at rest. In the total group treated with Trandolapril, the ß2 adrenergic receptor density has doubled after therapy, while the reactivity of low frequencies obtained from spectral analysis has increased. We have shown in this study that Angiotensin Converting Enzyme Inhibitor could inhibit the facilitatory mechanism of angII on sympathetic nerve terminals and therefore allowed the reduction of the sympathetic hyperactivity and the cause of a beta2 adrenergic “down regulation”. Thus it allowed us to obtain an increased density of the receptors and the expression of more effective influence of post synaptic Sympathetic nervous system. In all of our clinical protocols, using spectral analysis of RR, systolic blood pressure, diastolic blood pressure and breathing signals, we have shown that this non-invasive technique has helped to describe and to better understand the physiological and pharmacological mechanisms related to the autonomic nervous system in normotensive and hypertensive subjects. Variabilité RR Variabilité de la pression artérielle Système nerveux autonome Sensibilité du barorécepteur Hypertension artérielle essentielle RR variability Blood pressure variability Autonomic nervous system Baroreceptor sensitivity Essential hypertension Angiotensin-converting Enzyme inhibitors
222	Diagnóstico da cardiomiopatia na distrofia muscular progressiva por ressonância magnética cardiovascular - correlação com tratamento, prognóstico e preditores genéticos / Diagnosis of cardiomyopathy in progressive muscular dystrophy by cardiovascular magnetic resonance - correlation with treatment, prognosis and genetic predictors Silva, Marly Conceição 08 August 2013 (has links) Introdução: Distrofia muscular progressiva nas formas de Duchenne (DMD) e Becker (DMB) são doenças caracterizadas por progressiva degeneração musculoesquelética e substituição por tecido fibrogorduroso. O envolvimento cardíaco está presente em 80% dos pacientes, apresenta curso clínico silencioso e é diagnosticado tardiamente pelos métodos tradicionais. Objetivos: 1. Investigar a progressão da fibrose miocárdica pela ressonância magnética cardíaca (RMC), em ensaio clínico randomizado para tratamento ou não com IECA, de pacientes com DMD e DMB e fração de ejeção ventricular esquerda (FEVE) preservada, por um período de 02 anos. 2. Investigar se há mutações genéticas específicas que sejam preditoras do acometimento miocárdico diagnosticado pela RMC. 3. Comparar os achados do ECG, radiografia de tórax e ecocardiograma com os da RMC. Métodos: Entre 1/6/2009 e 1/6/2012 foram incluídos 76 pacientes com diagnóstico de DMD e DMB. Todos os pacientes realizaram duas RMCs com intervalo médio de 2,05±0,11 anos, com técnicas de cine ressonância para avaliação da função ventricular e realce tardio miocárdico para avaliação da fibrose miocárdica. A fibrose miocárdica foi quantificada por software específico para obtenção do percentual da massa de fibrose do VE com análise semi automática, utilizando os desvios padrões da média dos valores de intensidade do sinal do miocárdio normal. Os valores acima de 5 desvios padrões da média do miocárdio normal foram considerados como fibrose miocárdica. Os 42 pacientes com fibrose miocárdica e FEVE normal foram randomizado em 2 grupos, com 21 deles recebendo tratamento com IECA e 21 sem qualquer tratamento para cardiomiopatia. Após 2 anos, novas RMCs foram realizadas para avaliar a evolução da fibrose e a FEVE. Resultados: Notou-se fibrose miocárdica em 72,3% dos pacientes, sendo que 55,6 % não apresentavam disfunção sistólica. Verificou-se uma correlação positiva significativa entre idade e percentual de fibrose na RMC basal (r=0,338, p=0,014) e seguimento (r=0,315, p=0,006). Os pacientes randomizados e tratados com IECA apresentaram menor evolução do percentual de fibrose do que os randomizados não tratados (3,1±7,4% versus 10,0±6,2% respectivamente, p=0,001). Na análise linear multivariada, verificamos que pertencer ao grupo tratado diminui a progressão do percentual de fibrose (y=-4,51x+29,63 ajustado por idade, CK e percentual de fibrose basal, p=0,039) e indica uma tendência de menor probabilidade de apresentar fração de ejeção do VE < 50% na RMC seguimento (OR= 3,18, p= 0,102, por regressão logística). Os pacientes com mutação nos exons menores que 45 do gene da distrofina apresentaram maior percentual de fibrose que os com mutação dos exons maiores ou iguais ao 45 na RMC basal (27,9±18,4% versus 12,1±13,4%, respectivamente, p=0,006) e seguimento (33,1±21,1% versus 18,8±16,9%, respectivamente, p=0,024). A avaliação conjunta por métodos tradicionais (radiografia de tórax, ECG e ecocardiografia) apresentou baixa sensibilidade de 47,3% e valor preditivo negativo de 34,1% para o diagnóstico do envolvimento cardíaco na DMD e DMB, em pacientes com FEVE normal e fibrose miocárdica na RMC. Conclusões: O ensaio clínico randomizado, por um período de 2 anos, em pacientes com DMD e DMB, com fibrose miocárdica diagnosticada pela RMC e FEVE preservada, demonstrou significativa maior progressão da fibrose miocárdica nos pacientes que não fizerem uso de IECA. Existe uma correlação significativa entre o local de mutação no gene da distrofina e o acometimento cardíaco. O ECG, o eco e radiografia de tórax apresentaram baixa sensibilidade e baixo valor preditivo negativo para detecção do envolvimento cardíaco precoce nos pacientes com DMD e DMB / Introduction: Duchenne and Becker muscular dystrophies (DMD and BMD) are diseases characterized by progressive skeletal muscle degeneration and replacement by fibro fatty tissue. Cardiac involvement is frequent, as high as 70 - 80% of patients, and often develops clinically silent, without any evident early clinical signs. Traditional diagnostic methods (ECG, chest x-ray and echocardiography) are only able to diagnose cardiac involvement at a later stage. Objectives: 1. To investigate the progression of myocardial fibrosis by cardiac magnetic resonance (CMR), in a randomized clinical trial for treatment with ACE inhibitors, in patients with DMD or BMD and preserved left ventricular ejection fraction (LVEF), for a period of 02 years. 2. To investigate whether there are specific genetic mutations that are predictive of myocardial involvement detected by CMR. 3. To compare the findings of ECG, chest radiography and echocardiography with those found by CMR. Methods: Between 01/06/2009 and 01/06/2012 76 patients with DMD and BMD were included. All patients underwent two CMRs with a mean interval of 2.05±0.11 years, using cine resonance for function evaluation and myocardial delayed enhancement technique for myocardial fibrosis detection. Myocardial fibrosis was quantified by specific software for obtaining fibrosis mass, as percentage of LV mass, using semi-automatic fibrosis analysis and standard deviations of the mean values of signal intensity of the normal myocardium. A value of five standard deviations above the mean of a normal myocardium were considered myocardial fibrosis. The 42 patients with myocardial fibrosis and normal LVEF were randomized into 2 groups, with 21 of them receiving ACE inhibitor treatment and 21 no treatment for cardiomyopathy. After 2 years, new CMRs were performed to evaluate fibrosis extent and LVEF. Results: Myocardial fibrosis was noted in 72.3% of the patients, 55.6% showed no systolic dysfunction. There was a significant positive correlation between age and myocardial fibrosis at the CMR baseline (r=0.338, p=0.014) and follow-up (r=0.315, p=0.006). Patients randomized and treated with ACE inhibitors had lower evolution of myocardial fibrosis than those who were randomized and untreated (3.1±7.4% vs.10.0±6.2%, respectively, p=0.001). Using multivariate regression analysis, we found that belonging to the treated group decreases the progression of myocardial fibrosis (y=-4.51x+29.63 adjusted for age, CK and baseline myocardial fibrosis, p=0.039) and indicated a trend for lower probability of presenting LVEF<50% at follow-up CMR (OR= 3.18, p= 0.102, by logistic regression). Patients with mutations in exons less than 45 had greater extent of myocardial fibrosis than patients with mutations in exons greater than or equal to 45 in CMR at baseline (27.9±18.4% vs. 12.1±13.4%, respectively, p=0.006) and at follow-up (33.1±21.1% vs. 18.8±16.9%, respectively, p=0.024). Conclusions: In this 2-year follow-up randomized clinical trial in patients with DMD and BMD with preserved LVEF, myocardial fibrosis diagnosed by CMR, showed significantly greater progression in patients not receiving ACE inhibitors therapy. There was a significant correlation between the site of mutation in the dystrophin gene and cardiac involvement. ECG, echocardiography and chest radiography showed low sensitivity and low negative predictive value for early detection of cardiac involvement (myocardial fibrosis by CMR) in patients with DMD and BMD Angiotensin-converting enzyme inhibitors Cardiomiopatias/diagnóstico Cardiomiopatias/etiologia Cardiomiopatias/fisiopatologia Cardiomyopathies/diagnosis Cardiomyopathies/etiology Cardiomyopathies/physiopathology Creatina quinase Creatine kinase Fibrose/diagnóstico Fibrosis/diagnosis Função ventricular Imagem por ressonância magnética Magnetic resonance imaging Miocárdio/patologia Mutação/genética Mutation/genetics Myocardium/pathology Ventricular function
223	Sobrecarga de sal durante o período perinatal: efeito sobre a modulação do sistema renina-angiotensina em resposta à variação no consumo de sal na prole adulta / Dietary salt load during perinatal period: effects on the reninangiotensin system in response to sodium intake in the adult offspring rat Costa, Nauilo Lima 09 February 2009 (has links) O objetivo deste estudo foi avaliar se a sobrecarga de sal durante a gestação interfere na liberação de renina renal e circulante e a sua relação com a COX-2 e nNOS no rim após estimulo ou inibição do sistema renina angiotensina (SRA) nas proles femininas adultas. Ratas fêmeas Wistar receberam dieta normossódica (1,3%), hipersódica 4,0% ou hipersódica 8,0%NaCl durante a gestação. Ao nascimento, as proles receberam dieta normossódica. As proles com 12 semanas de vida foram submetidas ao teste de restrição (0,15%) ou a sobrecarga de sódio (8,0%NaCl). Foram avaliados pesos corpóreos, a pressão arterial, atividades da renina plasmática e renal; porcentagem de ramos vasculares com grânulos de renina, nitrito sérico; expressão do mRNA e protéica de renina, COX-2 e nNOS no córtex e medula renal. A pressão arterial, peso corpóreo, atividade da renina plasmática e renal não foram diferentes entre os grupos. A prole HR1 apresentou modulação do SRA, enquanto que prole HR2 não apresentou modulação adequada frente à restrição ou sobrecarga de sódio. Além disso, a expressão do mRNA da renina, COX-2 e nNOS foi estimulada na medula, e diminuída no córtex renal das proles HR1 diante da restrição ou sobrecarga de sódio. Em conclusão, a sobrecarga de sódio durante a gestação modifica as respostas do sistema renina-angiotensina, da COX-2 e da nNOS diante de subseqüente restrição e sobrecarga de sódio nas proles femininas adultas. / The objective was to evaluate whether mother high salt diet interferes in circulating and local renin release and its relation to kidney COX-2 and nNOS under RAS stimulation or inhibition by sodium in female offspring. Female rats were fed a normal (1,3%NaCl, NSD) or high 1 (4,0%, HSD1) or high 2 (8,0%, HSD2) diet throughout pregnancy. Mating occurred on the 12th week of age. From birthday, the offspring received normal salt diet. In adult offspring; plasma, renal renin activity, granulated renin cell, serum Nox, medullar and cortical renin, COX-2 and nNOS mRNA and protein expression were measured in basal condition and after one week of RAS stimulation or inhibition by sodium. Results: In basal condition, renin activity was not different among groups; however HSD1 offspring was more responsive to RAS stimulation or inhibition. Medulla COX-2 and nNOS mRNA of HSD1 offspring were decreased in basal conditions and they were more responsive to RAS stimulation or inhibition. Enhanced responses of circulating and local renin, COX-2 and nNOS to RAS stimulation or inhibition by sodium in offspring from maternal high salt diet during pregnancy lead to activation of renin angiotensin system, prostaglandin and nitric oxide pathways, and could be origin of hypertension in late life. Angiotensin-conversive enzyme inhibitors Ciclooxigenase 2 Cloreto de sódio na dieta Cyclooxygenase 2 Diet sodium-restricted Dieta hipossódica Gravidez Hipertensão Hypertension Nitric oxide synthase Type 1 Óxido nítrico sintase Tipo 1 Pregnancy Renin-angiotensin system Sistema renina-angiotensina Sodium chloride dietary
224	Evaluation du systeme nerveux autonome dans l'hypertension arterielle essentielle Yacine, Amine 06 1900 (has links) L’analyse spectrale de la fréquence cardiaque, de la pression artérielle systolique, de la pression artérielle diastolique ainsi que de la respiration par la transformée de Fourier rapide, est considérée comme une technique non invasive pour la détermination de l’activité du système nerveux autonome (SNA). Dans une population de sujets normaux volontaires, nous avons obtenu à l’état basal, des oscillations de basses fréquences (0,05-0,15Hz) reliées au système nerveux sympathique autonome et des oscillations de hautes fréquences (0,2Hz) représentant sur les intervalles entre chaque ondes R de l’électrocardiogramme (RR), l’arythmie sinusale respiratoire correspondant à une activité vagale. Nous avons comparé les tests de stimulation du système nerveux sympathique autonome déclenché par le passage de la position de repos (en décubitus dorsal), à la position orthostatique volontaire et le passage de la position de repos à la position orthostatique avec la table basculante à 60o. Nous avons également comparé un groupe normotendu à un groupe hypertendu qui a été soumis au passage du repos à l’orthostation volontaire et pour lesquels nous avons évalué la sensibilité du baroréflexe et la réponse sympathique par la mesure des catécholamines circulantes. Dans un groupe de sujets ayant une hypertension artérielle essentielle, nous avons évalué l’effet de la thérapie hypotensive, par le Trandolapril qui est un Inhibiteur de l’enzyme de conversion (IEC) de l`angiotensine. Dans ce groupe hypertendu, nous avons procédé, en plus de la stimulation sympathique par l’orthostation volontaire, à un exercice isométrique de trois minutes à 30 % de la force maximale. Nous avons également complété notre évaluation par la mesure de la densité de récepteurs ß2 adrénergiques sur lymphocytes et par la mesure des indices de contractilité à l’aide de l’échocardiographie en M mode. Les résultats ont montré, dans les groupes normaux volontaires, dans les deux types de stimulation du système nerveux sympathique par la position orthostatique, une augmentation significative des catécholamines plasmatiques avec une augmentation de la fréquence cardiaque et des basses fréquences de RR, confirmant ainsi que l’on est en état de stimulation sympathique. On observe en même temps une diminution significative des hautes fréquences de RR, suggérant un retrait vagal lors de cette stimulation. On a observé au test de la table basculante six cas d’hypotension orthostatique. On a comparé la position orthostatique volontaire entre le groupe de sujets normaux et le groupe de sujets hypertendus. L’analyse spectrale croisée de RR et de la pression artérielle systolique a permis d’évaluer dans l’hypertension artérielle (HTA), essentielle une sensibilité du baroréflexe atténuée, accompagnée d’une réactivité vagale réduite en présence d’une activité et d’une réactivité sympathique augmentées suggérant une altération sympathovagale dans l’HTA. Dans le groupe de sujets hypertendus traités (Trandolapril 2mg/jour), nous avons identifié un groupe de répondeurs au traitement par le Trandolapril et un groupe de non répondeurs à ce type de thérapie anti-hypertensive. Le groupe répondeur avait un profil hyper-adrénergique avec une hyper-réactivité sympathique, une fréquence cardiaque et des pressions artérielles diastolique et systolique plus élevées au repos. Dans le groupe total traité au Trandolapril, la densité des récepteurs ß2 adrénergiques a doublé, après thérapie, alors que la réactivité des basses fréquences obtenues à l’analyse spectrale a augmenté. Nous avons montré dans notre étude qu’un IECA a pu inhiber le mécanisme facilitateur de l’angII sur les terminaisons nerveuses sympathiques et a permis ainsi de réduire l’hyperactivité sympathique et le mécanisme de « down regulation » des récepteurs ß2 adrénergiques rendant ainsi l’expression de l’influence du SNA post synaptique plus efficace. Dans l’ensemble de nos protocoles cliniques, par l’utilisation de l’analyse spectrale des signaux RR, de la pression artérielle systolique,de la pression artérielle diastolique et de la respiration, nous avons montré que cette technique non invasive permet de décrire et de mieux comprendre les mécanismes physiologiques, physiopathologiques et pharmacologiques reliés au système nerveux autonome et à l’hypertension artérielle essentielle. / The spectral analysis of the heart rate, the systolic blood pressure, the diastolic blood pressure and the respiration with the Fast Fourier Transform, is considered as a non-invasive technique for the determination of the autonomic nervous system activity. In a population of normal volunteer subjects, we obtained in the basal state, low-frequency oscillations related to the sympathetic autonomous nervous system (0.05-0.15Hz) and the high-frequency oscillations (0.2Hz), which represent, on RR intervals, the respiratory sinus arrhythmia corresponding to vagal activity. We compared the sympathetic nervous system stimulation tests triggered by the transition from resting to voluntary orthostatic positions and the transition from resting to orthostatic position using tilt table at 60o. We also compared a normal blood pressure group to a hypertensive group which were both subject to the transition from resting to voluntary orthostation and for whom we evaluated the baroreflex sensitivity and the sympathetic response by measuring circulating catecholamines. In a group of subjects having an essential arterial hypertension, we have evaluated the effect of hypotensive therapy, by the Trandolapril which is an Angiotensin Converting Enzyme Inhibitor. In the hypertensive group, we evaluated the sympathetic stimulation using the voluntary orthostation, and we have also proceeded to a 3 minutes isometric exercise at 30% of maximum force. We have also completed our evaluation by measuring both the ß2 adrenergic receptor density on isolated lymphocytes and the contractility index using the echocardiography in M mode. In both sympathetic nervous system stimulation types by orthostatic position, the results have shown, for normal blood pressure volunteer subject groups, a significant increase in concentration of plasma catecholamines with an increase of heart rate (HR) and the low frequency RR, confirming therefore that we are in the presence of a sympathetic stimulation state. At the same time, we observed a significant decrease of high frequency of RR, suggesting a vagal withdrawal during the stimulation. We observed six cases of orthostatic hypotension from the tilt table test. We compared the voluntary orthostatic position between normal and hypertension subject groups. The results with combined spectral analysis of RR and the systolic blood pressure allowed to evaluate in the essential high blood pressure a reduced baroreflex sensitivity along with a reduced vagal reactivity in presence of increased sympathetic activity and reactivity suggesting a sympatho-vagal alteration in essential arterial hypertension. In hypertensive subjects treated with Trandolapril 2mg/day, we have identified a group responding to Trandolapril treatment and a group of non-responders to this type of anti-hypertensive therapy. The responding group has an hyper-adrenergic profile with higher sympathetic reactivity, heart rate and arterial diastolic and systolic pressures at rest. In the total group treated with Trandolapril, the ß2 adrenergic receptor density has doubled after therapy, while the reactivity of low frequencies obtained from spectral analysis has increased. We have shown in this study that Angiotensin Converting Enzyme Inhibitor could inhibit the facilitatory mechanism of angII on sympathetic nerve terminals and therefore allowed the reduction of the sympathetic hyperactivity and the cause of a beta2 adrenergic “down regulation”. Thus it allowed us to obtain an increased density of the receptors and the expression of more effective influence of post synaptic Sympathetic nervous system. In all of our clinical protocols, using spectral analysis of RR, systolic blood pressure, diastolic blood pressure and breathing signals, we have shown that this non-invasive technique has helped to describe and to better understand the physiological and pharmacological mechanisms related to the autonomic nervous system in normotensive and hypertensive subjects. Variabilité RR Variabilité de la pression artérielle Système nerveux autonome Sensibilité du barorécepteur Hypertension artérielle essentielle RR variability Blood pressure variability Autonomic nervous system Baroreceptor sensitivity Essential hypertension Angiotensin-converting Enzyme inhibitors
225	Diagnóstico da cardiomiopatia na distrofia muscular progressiva por ressonância magnética cardiovascular - correlação com tratamento, prognóstico e preditores genéticos / Diagnosis of cardiomyopathy in progressive muscular dystrophy by cardiovascular magnetic resonance - correlation with treatment, prognosis and genetic predictors Marly Conceição Silva 08 August 2013 (has links) Introdução: Distrofia muscular progressiva nas formas de Duchenne (DMD) e Becker (DMB) são doenças caracterizadas por progressiva degeneração musculoesquelética e substituição por tecido fibrogorduroso. O envolvimento cardíaco está presente em 80% dos pacientes, apresenta curso clínico silencioso e é diagnosticado tardiamente pelos métodos tradicionais. Objetivos: 1. Investigar a progressão da fibrose miocárdica pela ressonância magnética cardíaca (RMC), em ensaio clínico randomizado para tratamento ou não com IECA, de pacientes com DMD e DMB e fração de ejeção ventricular esquerda (FEVE) preservada, por um período de 02 anos. 2. Investigar se há mutações genéticas específicas que sejam preditoras do acometimento miocárdico diagnosticado pela RMC. 3. Comparar os achados do ECG, radiografia de tórax e ecocardiograma com os da RMC. Métodos: Entre 1/6/2009 e 1/6/2012 foram incluídos 76 pacientes com diagnóstico de DMD e DMB. Todos os pacientes realizaram duas RMCs com intervalo médio de 2,05±0,11 anos, com técnicas de cine ressonância para avaliação da função ventricular e realce tardio miocárdico para avaliação da fibrose miocárdica. A fibrose miocárdica foi quantificada por software específico para obtenção do percentual da massa de fibrose do VE com análise semi automática, utilizando os desvios padrões da média dos valores de intensidade do sinal do miocárdio normal. Os valores acima de 5 desvios padrões da média do miocárdio normal foram considerados como fibrose miocárdica. Os 42 pacientes com fibrose miocárdica e FEVE normal foram randomizado em 2 grupos, com 21 deles recebendo tratamento com IECA e 21 sem qualquer tratamento para cardiomiopatia. Após 2 anos, novas RMCs foram realizadas para avaliar a evolução da fibrose e a FEVE. Resultados: Notou-se fibrose miocárdica em 72,3% dos pacientes, sendo que 55,6 % não apresentavam disfunção sistólica. Verificou-se uma correlação positiva significativa entre idade e percentual de fibrose na RMC basal (r=0,338, p=0,014) e seguimento (r=0,315, p=0,006). Os pacientes randomizados e tratados com IECA apresentaram menor evolução do percentual de fibrose do que os randomizados não tratados (3,1±7,4% versus 10,0±6,2% respectivamente, p=0,001). Na análise linear multivariada, verificamos que pertencer ao grupo tratado diminui a progressão do percentual de fibrose (y=-4,51x+29,63 ajustado por idade, CK e percentual de fibrose basal, p=0,039) e indica uma tendência de menor probabilidade de apresentar fração de ejeção do VE < 50% na RMC seguimento (OR= 3,18, p= 0,102, por regressão logística). Os pacientes com mutação nos exons menores que 45 do gene da distrofina apresentaram maior percentual de fibrose que os com mutação dos exons maiores ou iguais ao 45 na RMC basal (27,9±18,4% versus 12,1±13,4%, respectivamente, p=0,006) e seguimento (33,1±21,1% versus 18,8±16,9%, respectivamente, p=0,024). A avaliação conjunta por métodos tradicionais (radiografia de tórax, ECG e ecocardiografia) apresentou baixa sensibilidade de 47,3% e valor preditivo negativo de 34,1% para o diagnóstico do envolvimento cardíaco na DMD e DMB, em pacientes com FEVE normal e fibrose miocárdica na RMC. Conclusões: O ensaio clínico randomizado, por um período de 2 anos, em pacientes com DMD e DMB, com fibrose miocárdica diagnosticada pela RMC e FEVE preservada, demonstrou significativa maior progressão da fibrose miocárdica nos pacientes que não fizerem uso de IECA. Existe uma correlação significativa entre o local de mutação no gene da distrofina e o acometimento cardíaco. O ECG, o eco e radiografia de tórax apresentaram baixa sensibilidade e baixo valor preditivo negativo para detecção do envolvimento cardíaco precoce nos pacientes com DMD e DMB / Introduction: Duchenne and Becker muscular dystrophies (DMD and BMD) are diseases characterized by progressive skeletal muscle degeneration and replacement by fibro fatty tissue. Cardiac involvement is frequent, as high as 70 - 80% of patients, and often develops clinically silent, without any evident early clinical signs. Traditional diagnostic methods (ECG, chest x-ray and echocardiography) are only able to diagnose cardiac involvement at a later stage. Objectives: 1. To investigate the progression of myocardial fibrosis by cardiac magnetic resonance (CMR), in a randomized clinical trial for treatment with ACE inhibitors, in patients with DMD or BMD and preserved left ventricular ejection fraction (LVEF), for a period of 02 years. 2. To investigate whether there are specific genetic mutations that are predictive of myocardial involvement detected by CMR. 3. To compare the findings of ECG, chest radiography and echocardiography with those found by CMR. Methods: Between 01/06/2009 and 01/06/2012 76 patients with DMD and BMD were included. All patients underwent two CMRs with a mean interval of 2.05±0.11 years, using cine resonance for function evaluation and myocardial delayed enhancement technique for myocardial fibrosis detection. Myocardial fibrosis was quantified by specific software for obtaining fibrosis mass, as percentage of LV mass, using semi-automatic fibrosis analysis and standard deviations of the mean values of signal intensity of the normal myocardium. A value of five standard deviations above the mean of a normal myocardium were considered myocardial fibrosis. The 42 patients with myocardial fibrosis and normal LVEF were randomized into 2 groups, with 21 of them receiving ACE inhibitor treatment and 21 no treatment for cardiomyopathy. After 2 years, new CMRs were performed to evaluate fibrosis extent and LVEF. Results: Myocardial fibrosis was noted in 72.3% of the patients, 55.6% showed no systolic dysfunction. There was a significant positive correlation between age and myocardial fibrosis at the CMR baseline (r=0.338, p=0.014) and follow-up (r=0.315, p=0.006). Patients randomized and treated with ACE inhibitors had lower evolution of myocardial fibrosis than those who were randomized and untreated (3.1±7.4% vs.10.0±6.2%, respectively, p=0.001). Using multivariate regression analysis, we found that belonging to the treated group decreases the progression of myocardial fibrosis (y=-4.51x+29.63 adjusted for age, CK and baseline myocardial fibrosis, p=0.039) and indicated a trend for lower probability of presenting LVEF<50% at follow-up CMR (OR= 3.18, p= 0.102, by logistic regression). Patients with mutations in exons less than 45 had greater extent of myocardial fibrosis than patients with mutations in exons greater than or equal to 45 in CMR at baseline (27.9±18.4% vs. 12.1±13.4%, respectively, p=0.006) and at follow-up (33.1±21.1% vs. 18.8±16.9%, respectively, p=0.024). Conclusions: In this 2-year follow-up randomized clinical trial in patients with DMD and BMD with preserved LVEF, myocardial fibrosis diagnosed by CMR, showed significantly greater progression in patients not receiving ACE inhibitors therapy. There was a significant correlation between the site of mutation in the dystrophin gene and cardiac involvement. ECG, echocardiography and chest radiography showed low sensitivity and low negative predictive value for early detection of cardiac involvement (myocardial fibrosis by CMR) in patients with DMD and BMD Cardiomiopatias/diagnóstico Cardiomiopatias/etiologia Cardiomiopatias/fisiopatologia Creatina quinase Fibrose/diagnóstico Função ventricular Imagem por ressonância magnética Miocárdio/patologia Mutação/genética Angiotensin-converting enzyme inhibitors Cardiomyopathies/diagnosis Cardiomyopathies/etiology Cardiomyopathies/physiopathology Creatine kinase Fibrosis/diagnosis Magnetic resonance imaging Mutation/genetics Myocardium/pathology Ventricular function
226	Sobrecarga de sal durante o período perinatal: efeito sobre a modulação do sistema renina-angiotensina em resposta à variação no consumo de sal na prole adulta / Dietary salt load during perinatal period: effects on the reninangiotensin system in response to sodium intake in the adult offspring rat Nauilo Lima Costa 09 February 2009 (has links) O objetivo deste estudo foi avaliar se a sobrecarga de sal durante a gestação interfere na liberação de renina renal e circulante e a sua relação com a COX-2 e nNOS no rim após estimulo ou inibição do sistema renina angiotensina (SRA) nas proles femininas adultas. Ratas fêmeas Wistar receberam dieta normossódica (1,3%), hipersódica 4,0% ou hipersódica 8,0%NaCl durante a gestação. Ao nascimento, as proles receberam dieta normossódica. As proles com 12 semanas de vida foram submetidas ao teste de restrição (0,15%) ou a sobrecarga de sódio (8,0%NaCl). Foram avaliados pesos corpóreos, a pressão arterial, atividades da renina plasmática e renal; porcentagem de ramos vasculares com grânulos de renina, nitrito sérico; expressão do mRNA e protéica de renina, COX-2 e nNOS no córtex e medula renal. A pressão arterial, peso corpóreo, atividade da renina plasmática e renal não foram diferentes entre os grupos. A prole HR1 apresentou modulação do SRA, enquanto que prole HR2 não apresentou modulação adequada frente à restrição ou sobrecarga de sódio. Além disso, a expressão do mRNA da renina, COX-2 e nNOS foi estimulada na medula, e diminuída no córtex renal das proles HR1 diante da restrição ou sobrecarga de sódio. Em conclusão, a sobrecarga de sódio durante a gestação modifica as respostas do sistema renina-angiotensina, da COX-2 e da nNOS diante de subseqüente restrição e sobrecarga de sódio nas proles femininas adultas. / The objective was to evaluate whether mother high salt diet interferes in circulating and local renin release and its relation to kidney COX-2 and nNOS under RAS stimulation or inhibition by sodium in female offspring. Female rats were fed a normal (1,3%NaCl, NSD) or high 1 (4,0%, HSD1) or high 2 (8,0%, HSD2) diet throughout pregnancy. Mating occurred on the 12th week of age. From birthday, the offspring received normal salt diet. In adult offspring; plasma, renal renin activity, granulated renin cell, serum Nox, medullar and cortical renin, COX-2 and nNOS mRNA and protein expression were measured in basal condition and after one week of RAS stimulation or inhibition by sodium. Results: In basal condition, renin activity was not different among groups; however HSD1 offspring was more responsive to RAS stimulation or inhibition. Medulla COX-2 and nNOS mRNA of HSD1 offspring were decreased in basal conditions and they were more responsive to RAS stimulation or inhibition. Enhanced responses of circulating and local renin, COX-2 and nNOS to RAS stimulation or inhibition by sodium in offspring from maternal high salt diet during pregnancy lead to activation of renin angiotensin system, prostaglandin and nitric oxide pathways, and could be origin of hypertension in late life. Ciclooxigenase 2 Cloreto de sódio na dieta Dieta hipossódica Gravidez Hipertensão Óxido nítrico sintase Tipo 1 Sistema renina-angiotensina Angiotensin-conversive enzyme inhibitors Cyclooxygenase 2 Diet sodium-restricted Hypertension Nitric oxide synthase Type 1 Pregnancy Renin-angiotensin system Sodium chloride dietary
227	Analyse pharmacologique comparative de l'action vasculaire du ramipril et d'inhibiteurs de l'HMG-COA réductase sur l'aorte isolée de rat: perspectives d'applications cliniques / Comparative pharmacological analysis of the vascular mechanisms of Ramipril and HMGCoa reductase inhibitors in isolated rat aorta: clinical perspectives Fontaine, David 10 May 2004 (has links) La prévention des maladies cardiovasculaires constitue actuellement une approche capitale dans la diminution de la mortalité au sein de nos pays industrialisés. Tous les facteurs de risques étant associés à une dysfonction endothéliale, nous nous sommes intéressés à deux classes de médicaments dont l’action bénéfique se situe, du moins en partie, au niveau de l’endothélium vasculaire :les inhibiteurs de l’enzyme de conversion de l’angiotensine (IECA) et les inhibiteurs de l’hydroxy-3-méthyl-3-glutaryl-Coenzyme A (HMG-CoA) réductase (statines).<p> Le présent travail contribue à l’étude in vitro des effets protecteurs vasculaires de l’administration chronique, chez le rat, de deux statines (la pravastatine et l’atorvastatine) vis-à-vis de la toxicité aiguë des LDL humaines oxydées et vis-à-vis de la tolérance à la nitroglycérine. Une comparaison est menée par rapport au ramipril dans ces deux modèles expérimentaux.<p>Les effets de ces médicaments se manifestent au niveau vasculaire par une amélioration de la disponibilité du NO. Toutefois, dans nos modèles, des mécanismes singulièrement différents ont été identifiés entre les agents étudiés :alors que le ramipril engendre une augmentation de l’expression de la eNOS, enzyme synthétisant le NO, les statines permettent une meilleure disponibilité de ce radical par un mécanisme post-traductionnel. Outre cette action, elles semblent agir directement sur des enzymes oxydatives comme les NAD(P)H oxydases.<p>Une action antioxydante des statines pourrait expliquer tous les effets observés, ce qui n’est pas le cas pour le ramipril. Vu que le stress oxydatif intervient dans tous les facteurs de risques cardiovasculaires, diverses perspectives cliniques sont envisagées afin d’améliorer l’approche thérapeutique de la maladie athéroscléreuse.<p> / Doctorat en sciences pharmaceutiques / info:eu-repo/semantics/nonPublished Sciences pharmaceutiques Statins (Cardiovascular agents) Ramipril Statines Ramipril atorvastatine pravastatine endothélium ramipril angiotensine tolérance aux nitrés rat LDL oxydées
228	Small molecule compounds targeting DNA binding domain of STAT3 for inhibition of tumor growth and metastasis Huang, Wei January 2014 (has links) Indiana University-Purdue University Indianapolis (IUPUI) / Signal transducer and activator of transcription 3 (STAT3) is constitutively activated in malignant tumors, and its activation is associated with high histological grade and advanced cancer stage. STAT3 has been shown to play important roles in multiple aspects of cancer aggressiveness including proliferation, survival, self-renewal, migration, invasion, angiogenesis and immune response by regulating the expression of diverse downstream target genes. Thus, inhibiting STAT3 promises to be an attractive strategy for treatment of advanced tumors with metastatic potential. We firstly identified a STAT3 inhibitor, inS3-54, by targeting the DNA-binding site of STAT3 using an in-silico screening approach; however, inS3-54 was finally found not to be appropriate for further studies because of low specificity on STAT3 and poor absorption in mice. To develop an effective and specific STAT3 inhibitor, we identified 89 analogues for the structure-activity relationship analysis. By using hematopoietic progenitor cells isolated from wild-type and STAT3 conditional knockout mice, further studies showed that three analogues (A18, A26 and A69) only inhibited STAT3-dependent colony formation of hematopoietic progenitor cells, indicating a higher selectivity for STAT3 than their parental compound, inS3-54. These compounds were found to (1) inhibit STAT3-specific DNA binding activity; (2) bind to STAT3 protein; (3) suppress proliferation of cancer cells harboring aberrant STAT3 signaling; (4) inhibit migration and invasion of cancer cells and (5) inhibit STAT3-dependent expression of downstream targets by blocking the binding of STAT3 to the promoter regions of responsive genes in cells. In addition, A18 can reduce tumor growth in a mouse xenograft model of lung cancer with little effect on body weight. Taken together, we conclude that it is feasible to inhibit STAT3 by targeting its DNA-binding domain for discovery of anticancer therapeutics. STAT3 DNA binding domain Inhibitor Structure-based drug discovery Signaling pathway Cancer Chemoprevention -- Research Cancer -- Chemotherapy Pathology, Molecular Genetic transcription -- Regulation Mobile genetic elements Drug development Carcinogenesis Enzyme inhibitors -- Therapeutic use
229	MSK1 regulates homeostatic and experience-dependent synaptic plasticity Corrêa, Sonia A.L., Hunter, C.J., Palygin, O., Wauters, S.C., Martin, K.J., McKenzie, C., McKelvey, K., Morris, R.G., Pankratov, Y., Arthur, J.S., Frenguelli, B.G. January 2012 (has links) No / The ability of neurons to modulate synaptic strength underpins synaptic plasticity, learning and memory, and adaptation to sensory experience. Despite the importance of synaptic adaptation in directing, reinforcing, and revising the behavioral response to environmental influences, the cellular and molecular mechanisms underlying synaptic adaptation are far from clear. Brain-derived neurotrophic factor (BDNF) is a prime initiator of structural and functional synaptic adaptation. However, the signaling cascade activated by BDNF to initiate these adaptive changes has not been elucidated. We have previously shown that BDNF activates mitogen- and stress-activated kinase 1 (MSK1), which regulates gene transcription via the phosphorylation of both CREB and histone H3. Using mice with a kinase-dead knock-in mutation of MSK1, we now show that MSK1 is necessary for the upregulation of synaptic strength in response to environmental enrichment in vivo. Furthermore, neurons from MSK1 kinase-dead mice failed to show scaling of synaptic transmission in response to activity deprivation in vitro, a deficit that could be rescued by reintroduction of wild-type MSK1. We also show that MSK1 forms part of a BDNF- and MAPK-dependent signaling cascade required for homeostatic synaptic scaling, which likely resides in the ability of MSK1 to regulate cell surface GluA1 expression via the induction of Arc/Arg3.1. These results demonstrate that MSK1 is an integral part of a signaling pathway that underlies the adaptive response to synaptic and environmental experience. MSK1 may thus act as a key homeostat in the activity- and experience-dependent regulation of synaptic strength. Analysis of Variance Animals Brain-derived neurotrophic factor Cells Cytoskeletal proteins Dendritic spines Environment Enzyme inhibitors Excitatory postsynaptic potentials Female Gene expression regulation Green fluorescent proteins Hippocampus Homeostasis Male Mice Inbred C57BL Transgenic Nerve tissue proteins Neuronal plasticity Neurons Patch-clamp techniques Point mutation Receptors AMPA Ribosomal protein S6 kinases Signal transduction Sodium channel blockers Synapses Tetrodotoxin Time factors REF 2014
230	Biguanide metformin acts on tau phosphorylation via mTOR/protein phosphatase 2A (PP2A) signaling Kickstein, E., Krauss, S., Thornhill, P., Rutschow, D., Zeller, R., Sharkey, J., Williamson, Ritchie, Fuchs, M., Kohler, A., Glossmann, H., Schneider, R., Sutherland, C., Schweiger, S. January 2010 (has links) No / Hyperphosphorylated tau plays an important role in the formation of neurofibrillary tangles in brains of patients with Alzheimer's disease (AD) and related tauopathies and is a crucial factor in the pathogenesis of these disorders. Though diverse kinases have been implicated in tau phosphorylation, protein phosphatase 2A (PP2A) seems to be the major tau phosphatase. Using murine primary neurons from wild-type and human tau transgenic mice, we show that the antidiabetic drug metformin induces PP2A activity and reduces tau phosphorylation at PP2A-dependent epitopes in vitro and in vivo. This tau dephosphorylating potency can be blocked entirely by the PP2A inhibitors okadaic acid and fostriecin, confirming that PP2A is an important mediator of the observed effects. Surprisingly, metformin effects on PP2A activity and tau phosphorylation seem to be independent of AMPK activation, because in our experiments (i) metformin induces PP2A activity before and at lower levels than AMPK activity and (ii) the AMPK activator AICAR does not influence the phosphorylation of tau at the sites analyzed. Affinity chromatography and immunoprecipitation experiments together with PP2A activity assays indicate that metformin interferes with the association of the catalytic subunit of PP2A (PP2Ac) to the so-called MID1-alpha4 protein complex, which regulates the degradation of PP2Ac and thereby influences PP2A activity. In summary, our data suggest a potential beneficial role of biguanides such as metformin in the prophylaxis and/or therapy of AD. Adenylate Kinase Metabolism Alzheimer Disease Pathology Physiopathology Animals Cells Cultured Enzyme Inhibitors Pharmacology Epitopes HeLa cells Humans Hypoglycemic agents Metformin Mice Transgenic Multiprotein complexes Neurofibrillary Tangles Neurons Cytology Okadaic acid Phosphorylation Protein Phosphatase 2 Proteins Signal Transduction Drug effects TOR Serine-Threonine Kinases Tau Proteins REF 2014

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