Global ETD Search

161	NEURAL ACTIVITY WITHIN SOLID BREAST TUMORS AND THE IMPLICATIONS ON METASTASIS Suciu, Diana J. 31 August 2018 (has links) No description available. Biomedical Engineering Biomedical Research breast cancer neural recording metastasis metastatic solid tumors neural activity vagus nerve 4T1 D2A1 neural activity during metastasis lidocaine nerve stimulation autonomic nervous system
162	The study of pain with blood oxygen level dependant functional magnetic resonance imaging Ibinson, James W. 29 September 2004 (has links) No description available. Functional magnetic resonance imaging Pain Physiologic noise General linear modeling Electrical nerve stimulation Autonomic nervous system End tidal carbon dioxide Respiration Cardiovascular function
163	Étude des effets de la stimulation électrique transcutanée sur le réflexe-H des muscles du triceps sural Goulet, Caroline January 1995 (has links) Thèse numérisée par la Direction des bibliothèques de l'Université de Montréal. Muscle contraction Electric stimulation Electrophysiology Muscles -- Contraction Triceps Stimulation électrique Électrophysiologie Neurostimulation transcutanée TENS Spasticité Blessés médullaires Réadaptation
164	Mapeamento metabólico cortical por espectroscopia funcional em sujeitos saudáveis submetidos a estimulação elétrica do nervo acessório Bandeira, Janete Shatkoski January 2017 (has links) A estimulação elétrica periférica (PES), que abrange diversas técnicas com respostas fisiológicas diversas, tem apresentado em alguns casos resultados clínicos promissores para o tratamento da dor e reabilitação clínica. No entanto, as respostas encontradas são heterogêneas, principalmente porque há uma falta de compreensão em relação ao seu mecanismo de ação. Neste estudo, buscamos avaliar os efeitos da PES através da medição da ativação cortical cerebral utilizando a espectroscopia funcional por infravermelho (fNIRS). A fNIRS é um método de imagem óptica funcional que avalia mudanças hemodinâmicas nas concentrações de hemoglobina oxigenada (HbO) e desoxigenada (HbR), relacionadas à atividade cortical. Nós hipotetizamos que a PES do nervo acessório espinal (ASN) pode promover a ativação do córtex motor (MC) e do córtex pré-frontal dorsolateral (DLPFC), relacionados ao processamento da dor. Quinze voluntários saudáveis receberam estimulação elétrica ativa e sham em um ensaio clínico randomizado cruzado. A resposta hemodinâmica à estimulação elétrica unilateral direita do nervo acessório com 10 Hz foi medida pela espectroscopia funcional por um sistema de 40 canais. A variação de HbO nas áreas corticais de interesse mostrou ativação do DLPFC direito (p=0,025) e do MOTOR esquerdo (p=0,042) no grupo ativo comparado com sham. Em relação ao DLPFC esquerdo (p=0,610) e ao MOTOR direito (p=0,154), não houve diferença estatística entre os grupos. Como na modulação top-down, a estimulação bottom-up do nervo acessório parece ativar as mesmas áreas corticais, relacionadas às dimensões sensório-discriminativas e afetivo-motivacionais da dor. Esses resultados fornecem evidência adicional para desenvolver e otimizar o uso clínico da estimulação elétrica periférica. / Peripheral electrical stimulation (PES), which encompasses several techniques with heterogeneous physiological responses, has shown in some cases remarkable outcomes for pain treatment and clinical rehabilitation. However, results are still mixed, mainly because there is a lack of understanding regarding its neural mechanisms of action. In this study, we aimed to assess its effects by measuring cortical activation as indexed by functional near infrared spectroscopy (fNIRS). fNIRS is a functional optical imaging method to evaluate hemodynamic changes in oxygenated (HbO) and de-oxygenated (HbR) blood hemoglobin concentrations in cortical capillary networks that can be related to cortical activity. We hypothesized that PES of accessory spinal nerve (ASN) can promote cortical activation of motor cortex (MC) and dorsolateral prefrontal cortex (DLPFC) pain processing cortical areas. Fifteen healthy volunteers received both active and sham ASN electrical stimulation in a crossover design. The hemodynamic response to unilateral right ASN burst electrical stimulation with 10 Hz was measured by a 40- channel fNIRS system. The effect of ASN electrical stimulation over HbO concentration in cortical areas of interest was observed through the activation of right- DLPFC (p=0.025) and left-MOTOR (p=0.042) in the active group but not in sham group. Regarding left-DLPFC (p=0.610) and right-MOTOR (p=0.174) there was no statistical difference between groups. As in non-invasive brain stimulation (NIBS) topdown modulation, bottom-up electrical stimulation to the accessory spinal nerve seems to activate the same critical cortical areas on pain pathways related to sensorydiscriminative and affective-motivational pain dimensions. These results provide additional mechanistic evidence to develop and optimize the effects of peripheral neural electrical stimulation. Excitabilidade cortical Nervo acessório Eletroacupuntura Dor crônica Estimulacao eletrica Cortical Activation (CA) Clinical Trials NCT 03295370 Accessory Spinal Nerve (ASN) Electroacupuncture (EA) Electrical Nerve Stimulation (ENS) Peripheral Nerve Stimulation (PNS) Near infrared spectroscopy (NIRS) Cortical Excitability (CE)
165	La stimulation du nerf vague pour le traitement de la dépression réfractaire : les résultats après un an de suivi LaGarde, Elise 08 1900 (has links) La stimulation du nerf vague (SNV) a reçu l’approbation de Santé Canada en 2001, comme en Europe, pour le traitement de la dépression réfractaire et en 2005 aux États-Unis. Les études européennes et américaines rapportent un taux de réponse de 50% et de rémission de 30% après un an de traitement. La sélection des patients, encadrée par la recherche de marqueurs biologiques et des critères de résistance, pourrait contribuer à améliorer les taux de réponse. Cette étude décrit le suivi des patients ambulatoires souffrant de dépression réfractaire, d’un spectre unipolaire ou bipolaire (n=13) sous SNV. Une révision exhaustive de l’histoire médicale et thérapeutique précède une évaluation clinique intensive. Si un consensus d’équipe est obtenu, une investigation clinique à la recherche des marqueurs biologiques est effectuée. Ceci inclut une tomographie par émission de photons simples (SPECT), une tomographie par émission de positrons (TEP), une formule sanguine complète, un test de suppression à la dexaméthasone (DST), une collecte d’urine 24h (catécholamines et cortisol), une polysomnographie et une évaluation neuropsychologique abrégée. Après 1 an de traitement, 61,5% (8/13) des patients ont atteint le seuil de réponse (diminution de 50% des symptômes), dont 87.5% (7/8) en rémission. Les patients diagnostiqués d’un trouble bipolaire, présentant un DST anormal et/ou avec déficits cognitifs ont répondu au traitement et poursuivent leur rémission après 2 ans. Une sélection minutieuse des patients pour le SNV serait une méthode efficace pour traiter les dépressions réfractaires, notamment pour prévenir les rechutes, amenant un état euthymique durable pour la plupart des patients. / Since 2001, Vagus Nerve Stimulation (VNS) has been used in treatment-resistant depression (TRD) in Europe and Canada, and in 2005 in the USA. European and American studies have shown a 50% response rate and 30% remission rate respectively after one year. Patient selection, driven by biological correlates and resistance criteria, may contribute to improved response and remission rates. This naturalistic study describes the follow-up of outpatients with TRD in individuals with unipolar or bipolar spectrum disorder (type 1 or 2) (n=13) treated with VNS. An exhaustive review of the medical and treatment history precedes an intensive clinical evaluation consisting of an individual evaluation and a subsequent team evaluation. A consensus is pursued, and if reached, an investigation of putative biological correlates of depression follows. This include a single photon emission computed tomography (SPECT) and a positron emission tomography (PET), a brain magnetic resonance imaging (MRI), a complete blood count, a dexamethasone suppression test (DST), a 24h urine collection; a polysomnography, and a limited neuropsychological evaluation. After one year of treatment, 61,5% (8/13) responded to treatment with at least a 50% reduction of their symptoms. Of those who responded 87.5% (7/8) are in remission. All patients with bipolar disorder, and/or abnormal baseline DST and/or baseline memory deficit responded to VNS therapy and continue to be in remission at the 24 months mark. Careful selection of patients for VNS treatment can be a very effective method of treatment of TRD and subsequent prevention of relapse, resulting in a sustained normothymic state in most responders. Stimulation du nerf vague, dépression réfractaire maladie bipolaire bipolarité neuromodulation dépression réfractaire vagus nerve stimulation, treatment-resistant depression bipolar disorder neuromodulation depression
166	La stimulation du nerf vague pour le traitement de la dépression réfractaire : les résultats après un an de suivi LaGarde, Elise 08 1900 (has links) La stimulation du nerf vague (SNV) a reçu l’approbation de Santé Canada en 2001, comme en Europe, pour le traitement de la dépression réfractaire et en 2005 aux États-Unis. Les études européennes et américaines rapportent un taux de réponse de 50% et de rémission de 30% après un an de traitement. La sélection des patients, encadrée par la recherche de marqueurs biologiques et des critères de résistance, pourrait contribuer à améliorer les taux de réponse. Cette étude décrit le suivi des patients ambulatoires souffrant de dépression réfractaire, d’un spectre unipolaire ou bipolaire (n=13) sous SNV. Une révision exhaustive de l’histoire médicale et thérapeutique précède une évaluation clinique intensive. Si un consensus d’équipe est obtenu, une investigation clinique à la recherche des marqueurs biologiques est effectuée. Ceci inclut une tomographie par émission de photons simples (SPECT), une tomographie par émission de positrons (TEP), une formule sanguine complète, un test de suppression à la dexaméthasone (DST), une collecte d’urine 24h (catécholamines et cortisol), une polysomnographie et une évaluation neuropsychologique abrégée. Après 1 an de traitement, 61,5% (8/13) des patients ont atteint le seuil de réponse (diminution de 50% des symptômes), dont 87.5% (7/8) en rémission. Les patients diagnostiqués d’un trouble bipolaire, présentant un DST anormal et/ou avec déficits cognitifs ont répondu au traitement et poursuivent leur rémission après 2 ans. Une sélection minutieuse des patients pour le SNV serait une méthode efficace pour traiter les dépressions réfractaires, notamment pour prévenir les rechutes, amenant un état euthymique durable pour la plupart des patients. / Since 2001, Vagus Nerve Stimulation (VNS) has been used in treatment-resistant depression (TRD) in Europe and Canada, and in 2005 in the USA. European and American studies have shown a 50% response rate and 30% remission rate respectively after one year. Patient selection, driven by biological correlates and resistance criteria, may contribute to improved response and remission rates. This naturalistic study describes the follow-up of outpatients with TRD in individuals with unipolar or bipolar spectrum disorder (type 1 or 2) (n=13) treated with VNS. An exhaustive review of the medical and treatment history precedes an intensive clinical evaluation consisting of an individual evaluation and a subsequent team evaluation. A consensus is pursued, and if reached, an investigation of putative biological correlates of depression follows. This include a single photon emission computed tomography (SPECT) and a positron emission tomography (PET), a brain magnetic resonance imaging (MRI), a complete blood count, a dexamethasone suppression test (DST), a 24h urine collection; a polysomnography, and a limited neuropsychological evaluation. After one year of treatment, 61,5% (8/13) responded to treatment with at least a 50% reduction of their symptoms. Of those who responded 87.5% (7/8) are in remission. All patients with bipolar disorder, and/or abnormal baseline DST and/or baseline memory deficit responded to VNS therapy and continue to be in remission at the 24 months mark. Careful selection of patients for VNS treatment can be a very effective method of treatment of TRD and subsequent prevention of relapse, resulting in a sustained normothymic state in most responders. Stimulation du nerf vague dépression réfractaire maladie bipolaire bipolarité neuromodulation dépression réfractaire vagus nerve stimulation treatment-resistant depression bipolar disorder neuromodulation depression
167	Analysis of intrinsic cardiac neuron activity in relation to neurogenic atrial fibrillation and vagal stimulation Salavatian, Siamak 08 1900 (has links) La fibrillation auriculaire est le trouble du rythme le plus fréquent chez l'homme. Elle conduit souvent à de graves complications telles que l'insuffisance cardiaque et les accidents vasculaires cérébraux. Un mécanisme neurogène de la fibrillation auriculaire mis en évidence. L'induction de tachyarythmie par stimulation du nerf médiastinal a été proposée comme modèle pour étudier la fibrillation auriculaire neurogène. Dans cette thèse, nous avons étudié l'activité des neurones cardiaques intrinsèques et leurs interactions à l'intérieur des plexus ganglionnaires de l'oreillette droite dans un modèle canin de la fibrillation auriculaire neurogène. Ces activités ont été enregistrées par un réseau multicanal de microélectrodes empalé dans le plexus ganglionnaire de l'oreillette droite. L'enregistrement de l'activité neuronale a été effectué continument sur une période de près de 4 heures comprenant différentes interventions vasculaires (occlusion de l'aorte, de la veine cave inférieure, puis de l'artère coronaire descendante antérieure gauche), des stimuli mécaniques (toucher de l'oreillette ou du ventricule) et électriques (stimulation du nerf vague ou des ganglions stellaires) ainsi que des épisodes induits de fibrillation auriculaire. L'identification et la classification neuronale ont été effectuées en utilisant l'analyse en composantes principales et le partitionnement de données (cluster analysis) dans le logiciel Spike2. Une nouvelle méthode basée sur l'analyse en composante principale est proposée pour annuler l'activité auriculaire superposée sur le signal neuronal et ainsi augmenter la précision de l'identification de la réponse neuronale et de la classification. En se basant sur la réponse neuronale, nous avons défini des sous-types de neurones (afférent, efférent et les neurones des circuits locaux). Leur activité liée à différents facteurs de stress nous ont permis de fournir une description plus détaillée du système nerveux cardiaque intrinsèque. La majorité des neurones enregistrés ont réagi à des épisodes de fibrillation auriculaire en devenant plus actifs. Cette hyperactivité des neurones cardiaques intrinsèques suggère que le contrôle de cette activité pourrait aider à prévenir la fibrillation auriculaire neurogène. Puisque la stimulation à basse intensité du nerf vague affaiblit l'activité neuronale cardiaque intrinsèque (en particulier pour les neurones afférents et convergents des circuits locaux), nous avons examiné si cette intervention pouvait être appliquée comme thérapie pour la fibrillation auriculaire. Nos résultats montrent que la stimulation du nerf vague droit a été en mesure d'atténuer la fibrillation auriculaire dans 12 des 16 cas malgré un effet pro-arythmique défavorable dans 1 des 16 cas. L'action protective a diminué au fil du temps et est devenue inefficace après ~ 40 minutes après 3 minutes de stimulation du nerf vague. / Atrial fibrillation is the most frequent sustained rhythm disorder in humans and often leads to severe complications such as heart failure and stroke. A neurogenic mechanism of atrial fibrillation has been hypothesized. Tachyarrhythmia induction by mediastinal nerve stimulation has been proposed as a model to study neurogenic atrial fibrillation. In this thesis, we studied the activity of intrinsic cardiac neurons and their interactions inside the right atrium ganglionated plexus in a canine model of neurogenic atrial fibrillation. These activities were recorded by a multichannel microelectrode array that was paled into the right atrium ganglionated plexus. The recording was done for up to 4 hours and it covered the neuronal activity during different interventions such as vascular (aorta occlusion, inferior vena cava occlusion, left anterior descending coronary artery occlusion), mechanical (touching atrium and ventricle) and electrical (stimulating of vagus nerve or stellate ganglion) stimuli as well as atrial fibrillation induction. Neuronal identification and classification were done using the principal component analysis and cluster on measurements analysis in Spike2 software. New method based on principal component analysis was proposed to cancel superimposed atrial activity on neuronal signal to increase the accuracy of the neuronal response identification and classification. Based on the neuronal response, we defined subtypes of neurons (afferent, efferent and local circuit neurons) and their related activity to different stressors which provided a more detailed description of the intrinsic cardiac nervous system. The majority of recorded neurons reacted to episodes of atrial fibrillation by becoming more active. This hyperactivity of intrinsic cardiac neurons during atrial fibrillation suggested that controlling that activity might help preventing neurogenic atrial fibrillation. Since low-level vagus nerve stimulation obtunds the intrinsic cardiac neuronal activity (especially for afferent and convergent local circuit neurons), we investigated whether this intervention could be applied as a therapy for atrial fibrillation. Our results showed that right vagus nerve stimulation was able to mitigate atrial fibrillation in 12 of 16 cases and showed an adverse pro-arrhythmic effect in 1 of 16 cases. The protective action however decreased over time and became ineffective after ~40 minutes for 3 minutes vagus nerve stimulation. Arythmies auriculaires Les neurones de circuit local La stimulation du nerf vague Interactivité neuronal stochastique Atrial arrhythmias Intrinsic cardiac nervous system Local circuit neurons Vagus nerve stimulation Stochastic neuronal interactivity
168	Estabilização segmentar lombar e TENS na hérnia discal lombar: um ensaio clínico randomizado / Lumbar segmental stabilization and TENS in lumbar disc herniation: a randomized controlled trial França, Fabio Jorge Renovato 01 October 2013 (has links) INTRODUÇÃO: A hérnia de disco lombar (HDL) acomete cerca de 5% dos pacientes com de dor lombar e o tratamento cirúrgico nestes casos é cada vez menos indicado, optando-se, na maior parte dos casos, pelo conservador. Embora o método estabilização lombar (EL) e a estimulação elétrica nervosa transcutânea (TENS) tenham mostrado bons resultados em indivíduos portadores de dor lombar inespecífica, há escassa literatura que tenha verificado a eficácia destes tratamentos isoladamente em sujeitos acometidos por hérnia de disco lombar. OBJETIVO: Comparar a eficácia dos exercícios de estabilização lombar e da TENS na dor, incapacidade funcional, e capacidade de ativação do músculo transverso do abdome (TrA) de indivíduos com hérnia de disco lombar. METODOLOGIA: Participaram da pesquisa 40 indivíduos com idade variando de 25 a 58 anos com dor lombar e hérnia de disco, e foram randomizados em dois grupos: Grupo estabilização lombar (EL) (exercícios específicos para os músculos TrA e multífido lombar(ML)) (n=20) e Grupo TENS (GT) (n=20) que receberam atendimento com corrente de estimulação elétrica nervosa transcutânea. Foram avaliados quanto à dor (Escala Visual Analógica e Questionário McGill de Dor), incapacidade funcional (Índice de Incapacidade de Oswestry), e capacidade de recrutamento do TrA (Unidade de Biofeedback Pressórico-UBP). Os grupos foram tratados em duas sessões semanais com duração de 60 minutos por oito semanas. Cada indivíduo foi avaliado antes e após o tratamento. O nível de significância estabelecido foi de alfa=0,05. RESULTADOS: Após oito semanas, o grupo estabilização lombar mostrou melhora significativa na dor (p < 0,001), incapacidade funcional (p < 0,001), e capacidade de ativação do TrA (p < 0,001). O grupo TENS apresentou diferença estatisticamente significante apenas na dor (p < 0,012). A estabilização foi superior à TENS na melhora na dor (p < 0,001), incapacidade funcional (p < 0,001), e capacidade de ativação do TrA (p < 0,001). CONCLUSÃO: Os resultados indicam que a estabilização é efetiva na melhora da dor, incapacidade funcional, e capacidade da ativação do TrA, e a TENS apenas na dor. A estabilização foi superior à TENS em todas as variáveis / INTRODUCTION: Lumbar disc herniation (LDH) affects about 5% of low back pain (LBP) patients. Surgical treatment in these cases is increasingly less suitable, opting, in most cases, for the conservative. Although lumbar stabilization method and transcutaneous electric nerve stimulation (TENS) have shown good results in patients with nonspecific low back pain, there is scarce literature that has verified the effectiveness of these treatments alone in subjects suffering from lumbar disc herniation.OBJECTIVE: To compare the effectiveness of lumbar stabilization exercises and transcutaneous electrical nerve stimulation (TENS), on pain, functional disability and activation of the transversus abdominis muscle (TrA), in individuals with lumbar disc herniation (LDH). METHODS: This study involved 40 patients (age range 25-58 years) with lumbar disc herniation randomized into two groups: Stabilization group (SG: n=20); which received of stabilization exercises (transversus abdominis and lumbar multifidus muscles) and TENS group (TG: n=20), which received electrotherapy. The following instruments were used: visual analogue pain scale and McGill Pain Questionnaire for pain, Oswestry Disability Index for functional disability, and pressure biofeedback unit (PBU) for ability to contract the TrA. Analyses within and between groups were performed after treatment. Groups underwent 16 sessions, for 60 minutes, twice a week and they were evaluated before and after eight weeks. Significance level was set at alfa= 0.05. RESULTS: After eight weeks, lumbar stabilization group showed significant improvements in pain (p < 0.001), functional disability (p < 0.001), and the ability to contract the TrA (p < 0.001). There were no significant differences in TENS group in terms of disability (p < 0.264) or ability to contract the TrA muscle (p < 0.181), however, improvement in pain was demonstrated (p < 0.012). The stabilization was superior to TENS in terms of improvements in pain (p < 0.001), functional disability (p < 0.001), and ability to contract the TrA (p < 0.001). CONCLUSION: The results indicate that stabilization is effective in improving pain, functional disability, and the ability to contract the TrA in individuals with LDH. In the TENS group, the only improvement after treatment was in terms of pain. Stabilization was superior to TENS in all outcomes Clinical trial Deslocamento do disco intervertebral Dor lombar/reabilitação Ensaio clínico Estabilização Exercise therapy Intervertebral disc displacement Low back pain/rehabilitation Modalidades de fisioterapia Physical therapy modalities Stabilization Terapia por exercício
169	Interação da atividade autonômica e resposta imunomoduladora na fase aguda do infarto do miocárdio experimental / Interaction of autonomic activity and immunomodulatory response in acute experimental myocardial infarction Rocha, Juraci Aparecida 12 November 2013 (has links) INTRODUÇÃO: A atuação do sistema nervoso parassimpático em células imunes é conhecida como \"Via Anti-inflamatória Colinérgica\". Trabalhos prévios demonstraram que a estimulação vagal reduz a inflamação e melhora a sobrevida em modelos experimentais com sepse. Neste estudo avaliamos se o uso do anticolinesterásico piridostigmina: altera o número de linfócitos T (CD4+ e CD8+) convencionais (CD25+Foxp3-) e reguladores (CD25+Foxp3+) no sangue periférico, no baço e no miocárdio; modifica a concentração de citocinas (interleucina 1, interleucina 6, TNFalfa) no miocárdio; e influencia a função ventricular após infarto agudo do miocárdio experimental (IAM) em ratos. MÉTODOS: Utilizamos ratos machos adultos da linhagem Wistar, com peso variando entre 200 e 250 g, divididos em 3 grupos de 20 animais cada: grupo controle (GC), grupo infartado sem tratamento (IC) e grupo infartado tratado com piridostigmina (IP). O infarto agudo do miocárdio (IAM) foi obtido com a técnica da ligadura da artéria coronária esquerda, e o grupo IP recebeu piridostigmina na dose de 40mg/kg/dia na água de beber, iniciada 4 dias antes do IAM. Todos os animais foram submetidos à canulação da artéria femoral no dia seguinte ao IAM para registro das curvas de pressão arterial, e posterior análise dos componentes da variabilidade da freqüência cardíaca (VFC), domínio do tempo (SDNN e RMSSD) e da freqüência (componentes LF e HF); o estudo ecocardiográfico foi realizado no segundo dia pós IAM. No terceiro dia pós IAM, os ratos foram divididos em subgrupos de 10 animais, e sacrificados de forma específica para coleta de materiais: 500 ul de sangue periférico e baço fresco para realização da técnica de citometria de fluxo; ventrículo esquerdo para dosagem de citocinas pela técnica de ELISA; e ventrículo esquerdo para realização de imunohistoquímica. Foram usadas as técnicas padronizadas e de uso corrente nos laboratórios. Os resultados foram avaliados por análise de variância (ANOVA) multifatorial, usando o programa GraphPad Prism com teste post hoc de Tukey. RESULTADOS: O grupo IC comparado ao grupo controle apresentou queda significativa da pressão arterial e aumento da freqüência cardíaca. O grupo IP, comparado ao grupo IC, apresentou maior atividade vagal, caracterizada pela significante redução da FC e aumento da VFC (SDNN, 9,2±1,5 vs 5,2±0,5 p < 0,05). Os parâmetros ecocardiográficos avaliados evidenciaram presença de área hipo/acinética e redução da fração de ejeção do ventrículo esquerdo nos grupos infartados, de igual magnitude. Com relação ao número de linfócitos T, verificamos que o grupo IC, comparado ao grupo controle, apresentou número significativamente menor de linfócitos reguladores (CD25+Foxp3+) no sangue periférico (CD4+: 63,5 ±1,4 vs 70,6 ±3,2%, e CD8+: 68,3 ±1,9 vs 76,1 ± 2,8%). O grupo IP, comparado ao grupo IC, apresentou significativa redução do número de linfócitos T convencionais no sangue periférico (respectivamente, CD4+: 1,5 ±0,2 vs 2,2 ± 0,2 %; CD8+: 1,1 ± 0,1 vs 1,8 ± 0,9%), e no baço houve redução somente do tipo CD4+ (respectivamente, 1,4 ± 0,2 vs 2,2 ± 0,2%), com aumento do tipo CD8+ (respectivamente, 1,2 ± 0,1 vs 0,7 ± 0,1 %). O grupo IP também apresentou significativo aumento de linfócitos reguladores (CD25+Foxp3+) no sangue periférico (respectivamente, CD4+: 76,5 ± 2,9 vs 63,5 ± 1,4 %; CD8+: 75,1 ± 1,0 vs 68,3 ± 1,9 %), e não apresentou diferenças significativas no número dessas células no baço. O grupo IC comparado ao grupo controle apresentou significativa marcação de anticorpos para CD4 e CD8 nas áreas infartada e peri-infarto por meio da análise de imunohistoquímica. O grupo IP comparado ao grupo IC, apresentou significativo aumento de CD4+ (respectivamente, 20,9 ± 6,5 vs 12,2 ± 2,5, p < 0,05) e de CD8+ (respectivamente, 17,9 ± 2,8 vs 5,8 ± 1,1%, p < 0,05) na área infartada; observamos redução significativa na marcação de CD4+ (respectivamente, 6,0 ±1,2 vs 12,5 ±4,8) na área peri-infarto, sem alterações significativas na marcação de CD8+. CONCLUSÃO: O tratamento com piridostigmina em ratos com IAM está associado a aumento da atividade vagal, aumento do número de linfócitos reguladores (CD25+Foxp3+) no sangue periférico e maior mobilização de células inflamatórias (CD4+ e CD8+) para a área infartada no miocárdio, com redução de CD4+ na área peri-infarto, no entanto sem mudança de CD8+ nesta região. A mudança do perfil inflamatório decorrente do aumento da atividade vagal na fase aguda do IAM, pode ser um possível mecanismo para explicar os benefícios detectados no remodelamento cardíaco após o IAM, em especial, na redução da área de lesão e na melhora da função ventricular, com uso de anticolinesterásicos / INTRODUTION: The role of the parasympathetic nervous system in immune cells is known as \"Cholinergic anti-inflammatory pathway\". In previous work has demonstrated that vagal stimulation reduces inflammation and improves survival in experimental sepsis models. The aim of the present study evalued the use of anticholinesterase pyridostigmine: change the number of T lymphocytes (CD4+ and CD8+) conventional (CD25+Foxp3-) and regulatory (CD25+Foxp3+) in peripheral blood, spleen, and myocardium: modifies the concentration of cytokines (interleukin-1, interleukin-6, TNFalfa) in the myocardium, and influences ventricular function after experimental myocardial infarction (MI) in rats. METHODS: Adult male rats of Wistar strain, weighing between 200 and 250 g were divided into 3 groups of 20 animals each: control group (GC); untreated group without treatment (IC) and infarcted group treated with pyridostigmine (IP). Acute myocardial infarction (AMI) was obtained with the technique of ligation of the left coronary artery, and the IP group received pyridostigmine dose of 40 mg/Kg/day in drinking water starting 4 days before the AMI. All animals underwent cannulation of the femoral artery on the day following AMI to record the blood pressure curves, and subsequent analysis of the components of heart rate variability (HRV), the time domain (SDNN and RMSSD) and frequency (components LF and HF), the echocardiografic study was performed on the second day after AMI. On the third day post-MI, mice were divided into subgroups of 10 animals, and were sacrificed in order to collet specific materials: 500 ul of fresh peripheral blood and spleen technique for performing flow cytometry left ventricle for measurement of cytokine ELISA, and the left ventricle to perform immunohistochemistry. Techniques used were standardized and commonly used in laboraties. The results were evaluated by analysis of variance (ANOVA) multifactorial, using the GraphPad Prism with Tukey post hoc test RESULTS: The HF group compared to the control group showed a significant drop in blood pressure and increased heart rate. The IP group compared to the IC group showed higher vagal activity, characterized by a significant reduction in HR and increase HVR (SDNN, 9.2 ± 1.5 vs 5.2 ± 0.5, p < 0.05). The echocardiography parameters evaluated showed presence of area hypo/acinetic and reduced ejection fraction of the left ventricle in infracted groups of equal magnitude. Regarding the number of T lymphocytes, we found that the IC group compared with the control group showed significantly fewer lymphocytes regulators (CD25+Foxp3+) in peripheral blood (CD4+:63.5 ± 1.4 vs 70.6 ± 3.2% and CD8+ cells: 68.3 ± 1.9 vs 76.1 ± 2.8%). The IP group compared to the IC group showed a significant reduction in the number of conventional T lymphocytes in peripheral blood (CD4+:1.5 ± 0.2 vs 2.2 ± 0.2%; CD8+: 1.1 ± 0.1 vs 1.8 ± 0.9%) and was reduced only in the spleen of the type CD4+(1.4 ± 0.2 vs 2.2 ± 0,2%) with increased CD8+(1.2 ± 0.1 vs 0.7 ± 0.1%). The IP group also showed a significant increase of lymphocytes regulators (CD25+Foxp3+) in peripheral blood (CD4+: 76.5 ± 2.9 vs 63.5 ± 1.4%; CD8+:75.1 ± 1.0 vs 68.3 ± 1.9%), and no significant differences in the number of these cells in the spleen. The IC group compared to the control group showed significant labeling antibodies to CD4 and CD8 areas infarcted and peri-infarction by immunohistochemical analysis. The IP group compared to the IC group showed a significant increase in CD4 (20.9 ± 6.5 vs 12.2 ± 2.5, p < 0.05) and CD8 (17.9 ± 2.8 vs 5.8 ± 1.1%, p < 0.05) in the infarcted area, and we observed a significant reduction in the labeling of CD4 (6.0 ± 1.2 vs 12.5± 4.8) in the peri-infraction without significant changes in the marking of CD8. CONCLUSION: The treatment with pyridostigmine in rats with acute myocardial infarction is associated with increased vagal activity, increased number of regulatory lymphocytes (CD25+Foxp3+) in peripheral blood and increased mobilization of inflammatory cells (CD4 and CD8) to the infarcted myocardium, with reduction of these cells in the peri-infarction. The change of the inflammatory profile due to increased vagal activity may be a possible mechanism to explain the benefits in the evolution of myocardial infarction, especially in the improvement of cardiac remodeling and maintenance of ventricular function with anticholinesterase drugs Brometo de piridostigmina Cholinergic anti-inflammatory pathway Estimulação nervo vago Infarto do miocárdio Inflamação/imunologia Linfócitos T reguladores Linfócitos-T Myocardial infarction Neuroimmunomodulation Neuroimunomodulação Piridostigmina Pyridostigmine Ratos Wistar Receptor alpha 7 nicotinico T-lymphocytes Vagal nerve stimulation Via anti-inflamatória colinérgica
170	Eficácia analgésica da estimulação elétrica cerebral e periférica na dor lombar crônica inespecífica: ensaio clínico aleatorizado, duplo-cego, fatorial / Analgesic efficacy of cerebral and peripheral electrical stimulation in chronic nonspecific low back pain: a randomized, double-blind, factorial clinical trial Hazime, Fuad Ahmad 02 December 2015 (has links) Recentes evidências sugerem que a dor lombar crônica está associada a alterações plásticas no cérebro, que podem ser modificadas por estratégias de neuromodulação. Neste ensaio clínico investigamos a eficácia analgésica de 12 sessões não consecutivas de estimulação transcraniana por corrente contínua (ETCC), estimulação elétrica periférica (EEP), ETCC+EEP e estimulação simulada (sham) em 92 pacientes com dor lombar crônica inespecífica. A intensidade, aspecto sensorial e afetivo da dor, incapacidade e percepção global de recuperação foram avaliadas antes do tratamento e quatro semanas, três e seis meses pós-randomização. Efeitos adversos, satisfação do paciente com o tratamento e fatores de confusão como ansiedade e depressão também foram avaliados. Os resultados demonstraram efeitos analgésicos clinicamente importantes da ETCC+EEP (MD = -2,6 IC95% = -4,4 a -0,9) e EEP isolada (MD = -2,2 IC95% = -3,9 a -0,4) comparada ao grupo sham, mas não da ETCC isolada (MD = -1,7 IC95% = -3,4 a -0,0). Além da manutenção do efeito analgésico por até três meses a ETCC+EEP obteve maior proporção de respondedores em diferentes pontos de corte. Os resultados sugerem que tanto a ETCC+EEP quanto EEP isolada são eficazes em curto prazo para o alívio da dor lombar crônica inespecífica. No entanto o efeito analgésico mais duradouro aliado a maior proporção de respondedores indicam um possível efeito aditivo e sinérgico da ETCC+EEP no alívio da dor em pacientes com dor lombar crônica não específica. Os nossos resultados não apoiam o uso da ETCC no regime de tratamento utilizado / Recent evidence suggests that chronic low back pain is associated with plastic changes in the brain that can be modified by neuromodulation strategies. In this clinical trial we have investigated the analgesic efficacy of 12 non-consecutive sessions of transcranial direct current stimulation (tDCS), peripheral electrical stimulation (PES), tDCS+PES and sham stimulation in 92 patients with chronic nonspecific low back pain. Intensity, the sensory and affective aspect of pain, disability, and overall perception of recovery were assessed before treatment and four weeks, three and six months post-randomization. Adverse effects, patient satisfaction with treatment and confounding factors such as anxiety and depression were also evaluated. The results showed clinically significant analgesic effects of tDCS+PES (Mean Reduction (MR) = -2.6; CI95% = -4.4 to - 0.9) and PES alone (MD = -2.2, CI95% = -3.9 to -0.4) compared to sham group, but not tDCS alone (MD = -1.7, CI95% = -3.4 to -0.0). In addition to maintaining the analgesic effect for up to three months, tDCS+PES treatment had a higher proportion of responders in different cutoff points. The results suggest that both tDCS+PES and PES alone are effective in relieving chronic nonspecific low back pain in the short term. However the most lasting analgesic effect, combined with a higher proportion of responders, indicates a possible additive and synergistic effect of tDCS+PES in relieving low back pain. Our findings do not support the use of tDCS alone in this condition Back pain Chronic pain Dor crônica Dor lombar Ensaio clínico controlado randomizado Randomized controlled trial Transcranial direct current stimulation

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