Global ETD Search

1	Efficacy of adjunctive exercise for the behavioral treatment of major depression Szuhany, Kristin 22 February 2018 (has links) Exercise alone is an efficacious intervention for depression, but few studies have identified the benefits of using exercise to augment other psychosocial treatments. The purpose of the current series of studies was to examine the feasibility, acceptability, efficacy, and potential mechanism of the augmentation of behavioral activation (BA) with exercise. The starting point for this series was a meta-analysis of the strength and reliability of brain-derived neurotrophic factor (BDNF) as a putative mechanism of the mood and cognitive effects of exercise. Evaluating 29 studies, I found: (1) a moderate effect for BDNF increases following acute exercise, (2) a moderate effect for the intensification of this effect following a program of exercise, and (3) a small effect on resting BDNF following a program of exercise. Given these effects, I hypothesized that exercise added to BA would improve mood beyond that for BA combined with a control condition and that changes in BDNF would mediate these effects. In a clinical trial, 32 sedentary, depressed patients received 9 sessions of BA over 12 weeks and were randomized to receive an exercise or control (stretching) augmentation. Assessments of depression, quality of life, distress intolerance, perceived stress, cognition (memory, attention), and amount of exercise were conducted across the treatment period. Results demonstrated strong credibility ratings and completion rates comparable to other exercise interventions. The randomized treatment failed to lead to differential exercise between groups; all participants exercised more over time. Similarly, participants, regardless of condition, significantly improved on all outcome measures over time. BDNF significantly increased following acute exercise. However, the amount of exercise completed over time was not significantly related to changes in BDNF across acute episodes, nor did resting BDNF significantly improve over time. Nonetheless, effect sizes for these changes were in the moderate range, reflecting values for the literature as a whole. Finally, contrary to my hypothesis, BDNF changes were not associated with subsequent improvement in depression symptoms. Results from this trial raise questions whether BA may be a powerful enough intervention to increase exercise, thus explicit exercise prescriptions may not be necessary for patients receiving this intervention. Clinical psychology Behavioral activation Brain-derived neurotrophic factor (BDNF) Depression Exercise Physical activity
2	Estudo do polimorfismo Val66Met na população brasileira e influência nos níveis plasmáticos de BDNF e reabilitação de pacientes pós-AVC / Study of Val66Met polymorphism on Brazilian population and the influence on plasmatic levels of BDNF and rehabilitation of post stroke patients Fontes, Daiane de Oliveira 29 November 2016 (has links) O número de pessoas acometidas por doenças cérebro vasculares, entre as quais, o acidente vascular cerebral (AVC), constitui um cenário alarmante nos dias atuais, fato que pode estar associado ao aumento da longevidade. A recuperação funcional de pessoas com sequelas de AVC requer a aplicação de técnicas de reabilitação que se baseiam em princípios de neuroplasticidade; no entanto, pouco se sabe quais são os benefícios morfofuncionais resultantes de diferentes abordagens terapêuticas. O presente estudo, portanto, teve como objetivos analisar a concentração plasmática de BDNF antes e após tratamento de reabilitação de indivíduos com AVC e correlacionar com o polimorfismo Val66Met; identificar e comparar a frequência do polimorfismo Val66Met na população brasileira e em pessoas que sofreram AVC. Os procedimentos experimentais foram aprovados pelo Comitê de Ética em Pesquisa da EACH/USP. O estudo foi dividido em duas abordagens experimentais: (i) caracterização genotípica de pessoas com diagnóstico de AVC e sua relação com diferentes protocolos de reabilitação e com o BDNF plasmático e (ii) estudo genético populacional para caracterização da frequência do polimorfismo Val66Met na população brasileira. Participaram deste estudo indivíduos saudáveis dos estados de Alagoas, Rio Grande do Sul e São Paulo (n=1558) e pacientes com sequelas de AVC (n=54). A análise do BDNF plasmático foi realizada por meio do teste imunoenzimático de ELISA e somente os indivíduos submetidos à terapia robótica tiveram níveis aumentados de BDNF circulante. As análises do polimorfismo Val66Met foram realizadas utilizando a técnica de PCR-RFLP (HRM). Não houve associação entre o polimorfismo e os níveis plasmáticos de BDNF. As frequências genotípicas e alélicas do polimorfismo Val66Met dos indivíduos saudáveis e com AVC foram muito semelhantes. Os dados de gênero apontou aumento nos níveis de BDNF em mulheres, entretanto, a idade não interferiu nos níveis de BDNF. Considerando-se os resultados, podemos concluir que o polimorfismo não apresenta relação com a ocorrência de AVC e não interfere nos níveis plasmáticos de BDNF plasmático. No que concerne às técnicas de reabilitação, a terapia robótica pode ser mais efetiva para desencadear eventos de neuroplasticidade considerando o aumento de BDNF circulante após o tratamento. Através do estudo populacional foi possível verificar que o perfil da miscigenação mudou ao longo de três gerações analisadas e confirmamos a presença rara do polimorfismo em pessoas de cor/raça preta e indígena / The number of people affected by cerebrovascular diseases, including the stroke, is an alarming scenario nowadays, which may be associated with the increment of the longevity. Functional recovery of people with stroke sequelae requires the application of rehabilitation techniques based on principles of neuroplasticity, however, the knowledge about how the morphological and functional benefits of different therapeutic approaches is insipient. This study, therefore, aimed to analyze the plasma concentration of BDNF before and after rehabilitation program of patients with stroke and correlate with Val66Met polymorphism; to identify and to compare the frequency of Val66Met polymorphism in the Brazilian population and in the patients who have suffered strokes. The experimental procedures were approved by the Research Ethics Committee of EACH/USP. The study was divided into two experimental approaches: (i) genotypic characterization of people diagnosed with stroke and their relation to different rehabilitation protocols and plasma BDNF and (ii) populational genetic study to characterize the frequency of Val66Met polymorphism in the Brazilian population. The study included healthy individuals in the states of Alagoas, Rio Grande do Sul and São Paulo (n = 1558) and patients with stroke sequelae (n = 54). The analysis of plasma BDNF was performed by immunoenzymatic test ELISA, and only those individuals undergoing robotic therapy had increased levels of circulating BDNF. The analysis of the polymorphism Val66Met was performed using PCR-RFLP (HRM). There was no association between the polymorphism and the plasma levels of BDNF. The genotypic and allelic frequencies of the Val66Met polymorphism of healthy individuals and stroke were similar. The gender data showed an increase in BDNF levels in women, but age did not interfere with BDNF levels. Considering the results, we can conclude that the polymorphism is not related to the occurrence of stroke and does not affect the plasma levels of serum BDNF. As regards the rehabilitation techniques, robotic therapy may be more effective to trigger neuroplasticity events considering the increase of circulating BDNF after treatment. Through the study population was possible to verify that the profile of miscegenation has changed over the three generations examined and confirmed the presence of the rare polymorphism in black and indigenous people Acidente Vascular Cerebral (AVC) Brain-Derived Neurotrophic Factor (BDNF) Polimorfismo Polymorphism Reabilitação Rehabilitation Stroke
3	Neurotrofinas como possíveis biomarcadores e alvos terapêuticos em leucemias pediátricas Gil, Mirela Severo January 2016 (has links) As leucemias correspondem a 30% dos tumores pediátricos, e constituem as neoplasias mais frequentes em indivíduos com menos de 15 anos. Apesar da elevada taxa de cura, frequentemente a ela está associada resistência à quimioterapia e efeitos colaterais tardios. Por isso, novas estratégias de tratamento, diagnóstico e prognóstico são necessárias. O fator neurotrófico derivado do cérebro (BDNF) e seus receptores de quinase relacionados à tropomiosina (tropomyosin related kinase, ou Trk) estão envolvidos com muitos processos na medula óssea (MO). Entretanto, o papel do BDNF em leucemias agudas (LA) pediátricas ainda não é bem conhecido. O objetivo desse estudo foi analisar os níveis de BDNF em amostras de MO ou sangue periférico (SP) de crianças com LA, e iniciar a caracterização dos efeitos de agonistas e antagonistas de neurotrofinas sobre culturas primárias de leucemias linfóides agudas em diferentes momentos terapêuticos Foram coletadas amostras de MO ou SP de crianças e adolescentes com leucemia linfóide aguda (LLA), crianças e adolescentes com leucemia mielóide aguda (LMA), e indivíduos saudáveis (IS) da mesma faixa etária. Para análise dos níveis séricos de BDNF utilizou-se kit de imuno-ensaio enzimático tipo sanduíche. Quando comparados aos IS os níveis de BDNF de pacientes com LA, ao diagnóstico, foram significativamente menores. Resultados similares foram observados nos pacientes durante indução, consolidação, diagnóstico e tratamento de recidiva. Da mesma forma, os níveis de BDNF foram inferiores em pacientes que receberam transfusão de plaquetas e, ao diagnóstico naqueles pacientes que foram a óbito. Para a caracterização dos efeitos de agonistas e antagonistas de neurotrofinas em cultura de células, amostras de pacientes ao momento do diagnóstico e no momento de indução do tratamento foram utilizadas. Os linfócitos foram extraídos e, após plaqueamento, as células foram tratadas com BDNF (Sigma, B3795), NGF (Sigma, SRP3015) e K252a (Sigma, 05288) por 72 horas. A viabilidade foi avaliada pelo método de exclusão por azul de Tripan. Devido às dificuldades no cultivo das células, esses dados ainda estão em análise. / Leukemias account for 30% of pediatric tumors and are the most frequent cancers in people under 15 years. Despite the high cure rate, often it is associated with resistance to chemotherapy and late side effects. Therefore, new strategies for treatment, diagnosis and prognosis are necessary. The brain-derived neurotrophic factor (BDNF) and their kinase receptor related tropomyosin (tropomyosin related kinase, and Trk) are involved in many processes in bone marrow (BM), however, the role of BDNF in acute leukemias (AL) pediatric it is not well known. The aim of this study was to analyze the BDNF levels in BM samples or peripheral blood (PB) of children with AL, and start the characterization of the effects of agonists and antagonists on neurotrophin primary cultures of acute lymphoblastic leukemias in different therapeutic moments. BM or PB samples were collected from children and adolescents with acute lymphoblastic leukemia (ALL), children and adolescents with acute myeloid leukemia (AML), and healthy individuals (HI) of the same age. For analysis of serum levels of BDNF was used sandwich enzyme immunoassay kit. When compared to HI, BDNF levels in patients with AL at diagnosis were significantly lower. Similar results were observed in patients during induction, consolidation, diagnosis and treatment of relapse. Similarly, BDNF levels were lower in patients receiving platelet transfusion and at diagnosis in patients that died. To characterize the effects of agonists and antagonists for neurotrophin in cell culture, samples of patients at diagnosis and at the time of induction treatment were used. Lymphocytes were extracted and, after plating, cells were treated with BDNF (Sigma B3795), NGF (Sigma, SRP3015) and K252a (Sigma, 05288) for 72 hours. Viability was assessed by exclusion of trypan blue method. Due to difficulties in cell culture, these data are still under analysis. Leucemia Neoplasias Fatores de crescimento neural Biomarcadores Criança Adolescente Neurotrophin, Childhood leukemia Brain derived neurotrophic factor (BDNF)
4	Translational assessment of cognitive impairments in depression models Martis, Lena-Sophie January 2018 (has links) Major depressive disorder (MDD) affects 300 million people worldwide and is a major contributor to the global burden of disease. The aetiology of depression, emerging through a gene x environment interaction, is still incompletely understood which prevents tailoring of treatment approaches. In addition to MDD core symptoms, such as anhedonia (a diminished anticipation or experience of pleasure), depressed patients suffer from a plethora of manifestations including cognitive impairments, which occur primarily in the domains of executive function, attention and memory. Patients remitted from affective symptoms of MDD often continue to display cognitive impairments. These cognitive deficits are the longest present residual symptom, predict treatment response and increase risk of relapse. Consequently, cognitive impairments need to be targeted more effectively by antidepressants for complete remission from MDD. Clinically relevant animal models are essential for developing, tailoring and testing such novel, pro-cognitive antidepressants. This PhD project aimed to establish a preclinical screening platform for the testing of pro-cognitive antidepressants, to improve understanding of MDD risk factors and consequent symptom development, and finally, to focus on clinical relevance of the applied techniques. The chronic mild stress (CMS) rodent model of depression was used, known for displaying the core symptom anhedonia, but also for a high construct, face and predictive validity. The environmental MDD risk factor 'stress' induces an anhedonic-like phenotype in a subgroup of exposed rats, whereas another subgroup of rats is resilient, as determined by the sucrose consumption test. The cognitive performance of different rat strains, including CMS anhedonic-like and resilient rats, was assessed employing the touchscreen operant platform, which was developed based on the Cambridge neuropsychological test automated battery (CANTAB) for assessing cognition in humans. Furthermore, a group of anhedonic-like rats was treated with the antidepressant vortioxetine, which acts as both a pro-cognitive and antidepressant treatment. Our results showed that stress exposure induced anhedonia in albino and pigmented rat strains, although stress did not affect cognitive performance of pigmented rats in a simple pairwise discrimination touchscreen task. Applying a more complex pairedassociates learning touchscreen task revealed impaired cognitive performance in the CMS anhedonic-like but not in the resilient phenotype. Furthermore, vortioxetine treatment reversed anhedonia in the CMS model and altered executive functions in treated rats. The expression of genes involved in the stress response, affective disorders and neuronal plasticity was altered in the prefrontal cortex and hippocampus owned to treatment and hedonic state. Thus, we have demonstrated that the CMS model exhibits both stress-induced cognitive alterations and depression-associated cognitive impairments in touchscreen tasks. Furthermore, touchscreen testing was sufficiently sensitive to detect alterations in cognitive performance due to pharmacological intervention. Overall, we established a potential platform for pro-cognitive antidepressant drug screening. Furthermore, brain derived neurotrophic factor (BDNF), involved in learning and memory, was examined in the context of depression. BDNF is reduced in MDD patients as well as in preclinical models in response to stress. Although this suggests that BDNF contributes to the aetiology of depression, studies including mice heterozygous for BDNF (BDNF+/-) have generated conflicting results. BDNF+/- rats may provide a more suitable model as (1) rats have a greater behavioural repertoire than mice, (2) classical behaviour tests are designed for rats, and (3) rats, like humans, produce peripheral BDNF. We found anhedonia and mild signs of anxiety in BDNF+/- rats, accompanied by prefrontal and hippocampal changes in expression of genes relevant in psychiatric disorders and underpinning learning. Thus, behavioural and molecular findings in BDNF+/- rats complement existing literature and suggest that rats are a more suitable model in BDNF research than mice. Overall, the project uncovered environmental and genetic manifestations of risk factors in translational models and established a novel tool for translational pro-cognitive antidepressant drug screening.
5	Neurotrofinas como possíveis biomarcadores e alvos terapêuticos em leucemias pediátricas Gil, Mirela Severo January 2016 (has links) As leucemias correspondem a 30% dos tumores pediátricos, e constituem as neoplasias mais frequentes em indivíduos com menos de 15 anos. Apesar da elevada taxa de cura, frequentemente a ela está associada resistência à quimioterapia e efeitos colaterais tardios. Por isso, novas estratégias de tratamento, diagnóstico e prognóstico são necessárias. O fator neurotrófico derivado do cérebro (BDNF) e seus receptores de quinase relacionados à tropomiosina (tropomyosin related kinase, ou Trk) estão envolvidos com muitos processos na medula óssea (MO). Entretanto, o papel do BDNF em leucemias agudas (LA) pediátricas ainda não é bem conhecido. O objetivo desse estudo foi analisar os níveis de BDNF em amostras de MO ou sangue periférico (SP) de crianças com LA, e iniciar a caracterização dos efeitos de agonistas e antagonistas de neurotrofinas sobre culturas primárias de leucemias linfóides agudas em diferentes momentos terapêuticos Foram coletadas amostras de MO ou SP de crianças e adolescentes com leucemia linfóide aguda (LLA), crianças e adolescentes com leucemia mielóide aguda (LMA), e indivíduos saudáveis (IS) da mesma faixa etária. Para análise dos níveis séricos de BDNF utilizou-se kit de imuno-ensaio enzimático tipo sanduíche. Quando comparados aos IS os níveis de BDNF de pacientes com LA, ao diagnóstico, foram significativamente menores. Resultados similares foram observados nos pacientes durante indução, consolidação, diagnóstico e tratamento de recidiva. Da mesma forma, os níveis de BDNF foram inferiores em pacientes que receberam transfusão de plaquetas e, ao diagnóstico naqueles pacientes que foram a óbito. Para a caracterização dos efeitos de agonistas e antagonistas de neurotrofinas em cultura de células, amostras de pacientes ao momento do diagnóstico e no momento de indução do tratamento foram utilizadas. Os linfócitos foram extraídos e, após plaqueamento, as células foram tratadas com BDNF (Sigma, B3795), NGF (Sigma, SRP3015) e K252a (Sigma, 05288) por 72 horas. A viabilidade foi avaliada pelo método de exclusão por azul de Tripan. Devido às dificuldades no cultivo das células, esses dados ainda estão em análise. / Leukemias account for 30% of pediatric tumors and are the most frequent cancers in people under 15 years. Despite the high cure rate, often it is associated with resistance to chemotherapy and late side effects. Therefore, new strategies for treatment, diagnosis and prognosis are necessary. The brain-derived neurotrophic factor (BDNF) and their kinase receptor related tropomyosin (tropomyosin related kinase, and Trk) are involved in many processes in bone marrow (BM), however, the role of BDNF in acute leukemias (AL) pediatric it is not well known. The aim of this study was to analyze the BDNF levels in BM samples or peripheral blood (PB) of children with AL, and start the characterization of the effects of agonists and antagonists on neurotrophin primary cultures of acute lymphoblastic leukemias in different therapeutic moments. BM or PB samples were collected from children and adolescents with acute lymphoblastic leukemia (ALL), children and adolescents with acute myeloid leukemia (AML), and healthy individuals (HI) of the same age. For analysis of serum levels of BDNF was used sandwich enzyme immunoassay kit. When compared to HI, BDNF levels in patients with AL at diagnosis were significantly lower. Similar results were observed in patients during induction, consolidation, diagnosis and treatment of relapse. Similarly, BDNF levels were lower in patients receiving platelet transfusion and at diagnosis in patients that died. To characterize the effects of agonists and antagonists for neurotrophin in cell culture, samples of patients at diagnosis and at the time of induction treatment were used. Lymphocytes were extracted and, after plating, cells were treated with BDNF (Sigma B3795), NGF (Sigma, SRP3015) and K252a (Sigma, 05288) for 72 hours. Viability was assessed by exclusion of trypan blue method. Due to difficulties in cell culture, these data are still under analysis. Leucemia Neoplasias Fatores de crescimento neural Biomarcadores Criança Adolescente Neurotrophin, Childhood leukemia Brain derived neurotrophic factor (BDNF)
6	Neurotrofinas como possíveis biomarcadores e alvos terapêuticos em leucemias pediátricas Gil, Mirela Severo January 2016 (has links) As leucemias correspondem a 30% dos tumores pediátricos, e constituem as neoplasias mais frequentes em indivíduos com menos de 15 anos. Apesar da elevada taxa de cura, frequentemente a ela está associada resistência à quimioterapia e efeitos colaterais tardios. Por isso, novas estratégias de tratamento, diagnóstico e prognóstico são necessárias. O fator neurotrófico derivado do cérebro (BDNF) e seus receptores de quinase relacionados à tropomiosina (tropomyosin related kinase, ou Trk) estão envolvidos com muitos processos na medula óssea (MO). Entretanto, o papel do BDNF em leucemias agudas (LA) pediátricas ainda não é bem conhecido. O objetivo desse estudo foi analisar os níveis de BDNF em amostras de MO ou sangue periférico (SP) de crianças com LA, e iniciar a caracterização dos efeitos de agonistas e antagonistas de neurotrofinas sobre culturas primárias de leucemias linfóides agudas em diferentes momentos terapêuticos Foram coletadas amostras de MO ou SP de crianças e adolescentes com leucemia linfóide aguda (LLA), crianças e adolescentes com leucemia mielóide aguda (LMA), e indivíduos saudáveis (IS) da mesma faixa etária. Para análise dos níveis séricos de BDNF utilizou-se kit de imuno-ensaio enzimático tipo sanduíche. Quando comparados aos IS os níveis de BDNF de pacientes com LA, ao diagnóstico, foram significativamente menores. Resultados similares foram observados nos pacientes durante indução, consolidação, diagnóstico e tratamento de recidiva. Da mesma forma, os níveis de BDNF foram inferiores em pacientes que receberam transfusão de plaquetas e, ao diagnóstico naqueles pacientes que foram a óbito. Para a caracterização dos efeitos de agonistas e antagonistas de neurotrofinas em cultura de células, amostras de pacientes ao momento do diagnóstico e no momento de indução do tratamento foram utilizadas. Os linfócitos foram extraídos e, após plaqueamento, as células foram tratadas com BDNF (Sigma, B3795), NGF (Sigma, SRP3015) e K252a (Sigma, 05288) por 72 horas. A viabilidade foi avaliada pelo método de exclusão por azul de Tripan. Devido às dificuldades no cultivo das células, esses dados ainda estão em análise. / Leukemias account for 30% of pediatric tumors and are the most frequent cancers in people under 15 years. Despite the high cure rate, often it is associated with resistance to chemotherapy and late side effects. Therefore, new strategies for treatment, diagnosis and prognosis are necessary. The brain-derived neurotrophic factor (BDNF) and their kinase receptor related tropomyosin (tropomyosin related kinase, and Trk) are involved in many processes in bone marrow (BM), however, the role of BDNF in acute leukemias (AL) pediatric it is not well known. The aim of this study was to analyze the BDNF levels in BM samples or peripheral blood (PB) of children with AL, and start the characterization of the effects of agonists and antagonists on neurotrophin primary cultures of acute lymphoblastic leukemias in different therapeutic moments. BM or PB samples were collected from children and adolescents with acute lymphoblastic leukemia (ALL), children and adolescents with acute myeloid leukemia (AML), and healthy individuals (HI) of the same age. For analysis of serum levels of BDNF was used sandwich enzyme immunoassay kit. When compared to HI, BDNF levels in patients with AL at diagnosis were significantly lower. Similar results were observed in patients during induction, consolidation, diagnosis and treatment of relapse. Similarly, BDNF levels were lower in patients receiving platelet transfusion and at diagnosis in patients that died. To characterize the effects of agonists and antagonists for neurotrophin in cell culture, samples of patients at diagnosis and at the time of induction treatment were used. Lymphocytes were extracted and, after plating, cells were treated with BDNF (Sigma B3795), NGF (Sigma, SRP3015) and K252a (Sigma, 05288) for 72 hours. Viability was assessed by exclusion of trypan blue method. Due to difficulties in cell culture, these data are still under analysis. Leucemia Neoplasias Fatores de crescimento neural Biomarcadores Criança Adolescente Neurotrophin, Childhood leukemia Brain derived neurotrophic factor (BDNF)
7	Estudo do polimorfismo Val66Met na população brasileira e influência nos níveis plasmáticos de BDNF e reabilitação de pacientes pós-AVC / Study of Val66Met polymorphism on Brazilian population and the influence on plasmatic levels of BDNF and rehabilitation of post stroke patients Daiane de Oliveira Fontes 29 November 2016 (has links) O número de pessoas acometidas por doenças cérebro vasculares, entre as quais, o acidente vascular cerebral (AVC), constitui um cenário alarmante nos dias atuais, fato que pode estar associado ao aumento da longevidade. A recuperação funcional de pessoas com sequelas de AVC requer a aplicação de técnicas de reabilitação que se baseiam em princípios de neuroplasticidade; no entanto, pouco se sabe quais são os benefícios morfofuncionais resultantes de diferentes abordagens terapêuticas. O presente estudo, portanto, teve como objetivos analisar a concentração plasmática de BDNF antes e após tratamento de reabilitação de indivíduos com AVC e correlacionar com o polimorfismo Val66Met; identificar e comparar a frequência do polimorfismo Val66Met na população brasileira e em pessoas que sofreram AVC. Os procedimentos experimentais foram aprovados pelo Comitê de Ética em Pesquisa da EACH/USP. O estudo foi dividido em duas abordagens experimentais: (i) caracterização genotípica de pessoas com diagnóstico de AVC e sua relação com diferentes protocolos de reabilitação e com o BDNF plasmático e (ii) estudo genético populacional para caracterização da frequência do polimorfismo Val66Met na população brasileira. Participaram deste estudo indivíduos saudáveis dos estados de Alagoas, Rio Grande do Sul e São Paulo (n=1558) e pacientes com sequelas de AVC (n=54). A análise do BDNF plasmático foi realizada por meio do teste imunoenzimático de ELISA e somente os indivíduos submetidos à terapia robótica tiveram níveis aumentados de BDNF circulante. As análises do polimorfismo Val66Met foram realizadas utilizando a técnica de PCR-RFLP (HRM). Não houve associação entre o polimorfismo e os níveis plasmáticos de BDNF. As frequências genotípicas e alélicas do polimorfismo Val66Met dos indivíduos saudáveis e com AVC foram muito semelhantes. Os dados de gênero apontou aumento nos níveis de BDNF em mulheres, entretanto, a idade não interferiu nos níveis de BDNF. Considerando-se os resultados, podemos concluir que o polimorfismo não apresenta relação com a ocorrência de AVC e não interfere nos níveis plasmáticos de BDNF plasmático. No que concerne às técnicas de reabilitação, a terapia robótica pode ser mais efetiva para desencadear eventos de neuroplasticidade considerando o aumento de BDNF circulante após o tratamento. Através do estudo populacional foi possível verificar que o perfil da miscigenação mudou ao longo de três gerações analisadas e confirmamos a presença rara do polimorfismo em pessoas de cor/raça preta e indígena / The number of people affected by cerebrovascular diseases, including the stroke, is an alarming scenario nowadays, which may be associated with the increment of the longevity. Functional recovery of people with stroke sequelae requires the application of rehabilitation techniques based on principles of neuroplasticity, however, the knowledge about how the morphological and functional benefits of different therapeutic approaches is insipient. This study, therefore, aimed to analyze the plasma concentration of BDNF before and after rehabilitation program of patients with stroke and correlate with Val66Met polymorphism; to identify and to compare the frequency of Val66Met polymorphism in the Brazilian population and in the patients who have suffered strokes. The experimental procedures were approved by the Research Ethics Committee of EACH/USP. The study was divided into two experimental approaches: (i) genotypic characterization of people diagnosed with stroke and their relation to different rehabilitation protocols and plasma BDNF and (ii) populational genetic study to characterize the frequency of Val66Met polymorphism in the Brazilian population. The study included healthy individuals in the states of Alagoas, Rio Grande do Sul and São Paulo (n = 1558) and patients with stroke sequelae (n = 54). The analysis of plasma BDNF was performed by immunoenzymatic test ELISA, and only those individuals undergoing robotic therapy had increased levels of circulating BDNF. The analysis of the polymorphism Val66Met was performed using PCR-RFLP (HRM). There was no association between the polymorphism and the plasma levels of BDNF. The genotypic and allelic frequencies of the Val66Met polymorphism of healthy individuals and stroke were similar. The gender data showed an increase in BDNF levels in women, but age did not interfere with BDNF levels. Considering the results, we can conclude that the polymorphism is not related to the occurrence of stroke and does not affect the plasma levels of serum BDNF. As regards the rehabilitation techniques, robotic therapy may be more effective to trigger neuroplasticity events considering the increase of circulating BDNF after treatment. Through the study population was possible to verify that the profile of miscegenation has changed over the three generations examined and confirmed the presence of the rare polymorphism in black and indigenous people Acidente Vascular Cerebral (AVC) Polimorfismo Reabilitação Brain-Derived Neurotrophic Factor (BDNF) Polymorphism Rehabilitation Stroke
8	EGR3 Immediate Early Gene and the Brain-Derived Neurotrophic Factor in Bipolar Disorder Pfaffenseller, Bianca, Kapczinski, Flavio, Gallitano, Amelia L., Klamt, Fábio 05 February 2018 (has links) Bipolar disorder (BD) is a severe psychiatric illness with a consistent genetic influence, involving complex interactions between numerous genes and environmental factors. Immediate early genes (IEGs) are activated in the brain in response to environmental stimuli, such as stress. The potential to translate environmental stimuli into long-term changes in brain has led to increased interest in a potential role for these genes influencing risk for psychiatric disorders. Our recent finding using network-based approach has shown that the regulatory unit of early growth response gene 3 (EGR3) of IEGs family was robustly repressed in postmortem prefrontal cortex of BD patients. As a central transcription factor, EGR3 regulates an array of target genes that mediate critical neurobiological processes such as synaptic plasticity, memory and cognition. Considering that EGR3 expression is induced by brain-derived neurotrophic factor (BDNF) that has been consistently related to BD pathophysiology, we suggest a link between BDNF and EGR3 and their potential role in BD. A growing body of data from our group and others has shown that peripheral BDNF levels are reduced during mood episodes and also with illness progression. In this same vein, BDNF has been proposed as an important growth factor in the impaired cellular resilience related to BD. Taken together with the fact that EGR3 regulates the expression of the neurotrophin receptor p75NTR and may also indirectly induce BDNF expression, here we propose a feed-forward gene regulatory network involving EGR3 and BDNF and its potential role in BD. immediate early genes early growth response gene 3 (EGR3) brain-derived neurotrophic factor (BDNF) bipolar disorder neuroplasticity regulatory network
9	Influência da dieta vegetariana no estado nutricional, em parâmetros bioquímicos e na expressão de BDNF circulante em adultos na cidade São Paulo / The influence of vegetarian diets on the nutritional status, biochemical parameters and the expression of circulating brain-derived neurotrophic factor (BDNF) among adults in the city of São Paulo Pimentel, Carolina Vieira de Mello Barros 19 September 2014 (has links) Introdução - Os efeitos na saúde de dietas vegetarianas (DV) apontam principalmente para a diminuição do risco de Doenças Crônicas Não Transmissíveis (DCNT), uma vez que modula positivamente parâmetros bioquímicos, particularmente aqueles relacionados ao controle da glicemia e lipemia, além de ser uma medida para o controle de peso. Estudos recentes em adultos demonstram que a dieta possa também modular parâmetros moleculares. Nesse cenário, atenta-se para o papel do Fator Neurotrófico Derivado do Encéfalo (BDNF) o qual parece estar relacionado com a DV em relação à redução de triglicerídeos e colesterol e aumento da sensibilidade à insulina. Objetivo - Avaliar adultos que adotaram uma DV, em relação ao estado nutricional, aos parâmetros bioquímicos e moleculares comparados aos adultos com dieta onívora. Métodos - A população avaliada foi constituída por 96 indivíduos, 56 vegetarianos e 40 onívoros, adultos e de ambos os sexos, em um estudo do tipo transversal. Para o levantamento dos dados sociodemográficos e de estilo de vida foi aplicado questionário e aferidas às medidas de peso corporal (PC) e altura, para posterior cálculo de Índice de Massa Corporal (IMC) e circunferência de cintura (CC). Foi realizada também coleta de sangue para estudos bioquímicos e expressão de BDNF plasmático. Os índices de Castelli 1 e 2 (razões lipídicas) são indicadores de risco cardiovascular (RCV) com maior valor preditivo do que parâmetros isolados, por isso, também foram calculados. A resistência à insulina (IR) foi avaliada pelo índice HOMA_IR. As análises foram conduzidas pelo software SPSS (Statistical Package for Social Sciences) versão 20.0 e para todas foi considerado um nível de significância de 5 por cento .Foi realizada análise de regressão logística para identificar se a DV e outros fatores podem prever a redução da chance de ter RCV, determinado pelos índices de Castelli 1 e 2.Resultados Em relação às variáveis de estilo de vida, os VEG têm uma tendência a praticar mais atividade física (64,3 por cento vs 42,5 por cento , p = 0,056) e ingerir suplementos alimentares (48,1 por cento vs 20,5 por cento , p = 0,012), embora o número de fumantes se apresente semelhante em ambos os grupos. Não houve diferença estatisticamente significante para as variáveis: idade, sexo, prática de fumar, triglicerídeos (TG), Colesterol Total (CT) e lipoproteína de baixa densidade (LDL- c) entre os dois grupos. Já os valores dos índices de Castelli 1 (3,23 ± 0,84 vs 3,90 ± 0,99, p =0,001)e 2 (1,91 ± 0,69 vs 2,42 ± 0,79, p = 0,001) foram menores em vegetarianos (VEG) do que em onívoros (ONV). O grupo VEG tinha significativamente menor PC (63,9 ± 10,4 vs 69,4 ± 14,6 kg, p = 0,032); IMC (22,5 ± 2,6 vs 25,0 ± 3,9 kg/m2, p = 0,001); CC( 81,8 ± 8,2 vs 87,8 ± 10,9 cm, p = 0,003 ) e maior lipoproteína de alta densidade (HDL-c) (54,88 ± 14,44 vs 47,30 ± 12,27 mg / dl , p = 0,008) . Os VEG também apresentaram menor HOMA-IR (1,17 ± 0,70 vs 1,48 ± 0,8, p = 0,02) em comparação com ONV. Quanto a variável BDNF, não houve diferença entre os grupos VEG e ONV (662,8 + 276,5pg/ml vs 698,1 + 314,9 pg/ml, p=0,563). Conclusão - Sugere-se, portanto, que a DV pode ter efeitos protetores na saúde cardiovascular e no metabolismo desses indivíduos. / Introduction - The effects of vegetarian diets (VD) on health points out mainly to a decrease in the risk for noncomunnicable chronic disease (NCDs) once it positively modulates the biochemical parameters, particularly those related to the control of glicemic and lipemia being also a way of controlling weight. Recent studies have shown that diet can also modulate molecular parameters. In this scenario, one must pay attention to the role of the brain-derived neurotrophic factor (BDNF) which seems to be related to the VG in what regards the reduction of triacylglycerol and cholesterol, and the increase of insulin sensitivity. Objective - To assess adults that adopted a VD in what regards their nutritional status, biochemical and molecular parameters, in comparison to adults that adopted an omnivorous diet. Methods- A cross-sectional study assessed a population composed of 96 individuals, 56 vegetarians and 40 omnivores, adults of both genders. A questionnaire was administered in order to gather sociodemographic and life-style related data, body weight (BW), height and waist circumference (WC) were surveyed. In order to carry out the biochemical study and the expression of plasmatic BDNF, blood was collected. The Castelli indexes 1 and 2 (lipid ratios) are indicators of cardiovascular risk (CVR) with a higher predictive value than isolated parameters and therefore were calculated. Insulin resistance (IR) was calculated by the HOMA_IR index. The analyses were carried out through the SPSS (Statistical Package for Social Sciences) software, 20.0 version, taking into account a 5 per cent significance level. An analysis of logistic regression was done in order to identify if the VD and other factors are able to prevent the reduction of CVR, determined by the Castelli indexes 1 and 2. Results - There was no statistically significant difference between both groups regarding the following variables: age, gender, smoking habits, triglyceride (TG), Total Cholesterol (TC) low-density lipoprotein cholesterol (LDL- col). On the other hand, the values of the Castelli indexes 1 (3,23 ± 0,84 vs 3,90 ± 0,99, p =0,001) and 2 (1,91 ± 0,69 vs 2,42 ± 0,79, p = 0,001) were lower in vegetarians (VEG) than in omnivores (OMV). The VEG-groups showed significant lower BW (63,9 ± 10,4 vs 69,4 ± 14,6 kg, p = 0,032); BMI (22,5 ± 2,6 vs 25,0 ± 3,9 kg/m2, p = 0,001); WC ( 81,8 ± 8,2 vs 87,8 ± 10,9 cm, p = 0,003 ) and more high-density lipoprotein cholesterol (HDL col) (54,88 ± 14,44 vs 47,30 ± 12,27 mg / dl , p = 0,008). The VEG-group also presented lower HOMA-IR (1,17 ± 0,70 vs 1,48 ± 0,8, p = 0,02) in comparison to the OMV-group. Regarding life-style parameters, the individuals of the VEG-group displayed a tendency for practicing more physical activity (64,3 per cent vs 42,5 per cent , p = 0,056) and for ingesting food supplement (48,1 per cent vs 20,5 per cent , p = 0,012), although the number of smokers was quite similar between both groups. Regarding the BDNF variable, there was no difference between the VEG-group and the OMVGroup (662,8 + 276,5 pg/ml vs 698,1 + 314,9 pg/ml, p=0,563).Conclusion - In relation to these results it is to be suggested that a VD may exert protective effects on cardiovascular health and on the metabolism of the individuals that adopt it. Brain-Derived Neurotrophic Factor (BDNF) Cardiovascular Diseases Dieta Vegetariana Doenças Cardiovasculares Estado Nutricional Nutritional Status Vegetarian Diet
10	The Effects of Nicotine in the Neonatal Quinpirole Rodent Model of Psychosis: Neural Plasticity Mechanisms and Nicotinic Receptor Changes Peterson, Daniel J., Gill, Wesley Drew, Dose, John M., Hoover, Donald B., Pauly, James R., Cummins, Elizabeth D., Burgess, Katherine C., Brown, Russell W. 15 May 2017 (has links) Neonatal quinpirole (NQ) treatment to rats increases dopamine D2 receptor sensitivity persistent throughout the animal’s lifetime. In Experiment 1, we analyzed the role of α7 and α4β2 nicotinic receptors (nAChRs) in nicotine behavioral sensitization and on the brain-derived neurotrophic factor (BDNF) response to nicotine in NQ- and neonatally saline (NS)-treated rats. In Experiment 2, we analyzed changes in α7 and α4β2 nAChR density in the nucleus accumbens (NAcc) and dorsal striatum in NQ and NS animals sensitized to nicotine. Male and female Sprague-Dawley rats were neonatally treated with quinpirole (1mg/kg) or saline from postnatal days (P)1-21. Animals were given ip injections of either saline or nicotine (0.5mg/kg free base) every second day from P33 to P49 and tested on behavioral sensitization. Before each injection, animals were ip administered the α7 nAChR antagonist methyllycaconitine (MLA; 2 or 4mg/kg) or the α4β2 nAChR antagonist dihydro beta erythroidine (DhβE; 1 or 3mg/kg). Results revealed NQ enhanced nicotine sensitization that was blocked by DhβE. MLA blocked the enhanced nicotine sensitization in NQ animals, but did not block nicotine sensitization. NQ enhanced the NAcc BDNF response to nicotine which was blocked by both antagonists. In Experiment 2, NQ enhanced nicotine sensitization and enhanced α4β2, but not α7, nAChR upregulation in the NAcc. These results suggest a relationship between accumbal BDNF and α4β2 nAChRs and their role in the behavioral response to nicotine in the NQ model which has relevance to schizophrenia, a behavioral disorder with high rates of tobacco smoking. adolescence brain-derived neurotrophic factor (BDNF) dopamine D2 receptor nicotine sensitization α4β2 nicotinic receptor α7 nicotinic receptor Biomedical Sciences Neurosciences Substance Abuse and Addiction

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