Avaliação da combinação de BDNF e quimioterapia em células de câncer de ovário (OVCAR-3)

Anjos, Gabriel Marques dos

January 2012

Introdução: O câncer de ovário é o mais prevalente e letal câncer ginecológico. A quimioterapia é um componente importante do tratamento sistêmico clássico com uma combinação de um agente platinado e um taxano, usualmente. Invariavelmente, câncer de ovário avançado torna-se resistente à quimioterapia. Objetivos: Com base em dados recentes que demonstram um possível papel das neurotrofinas na regulação de quimiosensibilidade, decidimos estudar o impacto do fator neurotrófico derivado de cérebro (BDNF) sobre a atividade antitumoral de diferentes classes de agentes antineoplásicos. Métodos: Para avaliar um possível efeito sinérgico entre BDNF e diferentes combinações de tratamento para câncer de ovário, as células foram expostas a cisplatina, etoposideo, doxorrubicina e paclitaxel concomitantemente com BDNF durante 48 horas. Administração sequencial de BDNF e quimioterapia foi realizada para avaliar o potencial de BDNF em modificar a resposta ao tratamento quimioterápico dependendo de qual agente é aplicado em primeiro lugar. Resultados: Houve uma redução da viabilidade de células OVCAR-3 quando expostas a cisplatina, doxorubicina e etoposideo concomitantemente com BDNF em 61,18% (SE±1.12, p=0.002), 38,96% (SE±1.08, p=0.001) e 49,63% (SE±1.17, p<0.001), respectivamente. BDNF também reduziu significativamente o efeito do paclitaxel e doxorrubicina quando usado antes da quimioterapia com uma redução de efeito de 53,46% (SE±3.48, p=0.001) e 48,25% (SE±1.25, p=0.018), respectivamente. Além disso, o BDNF utilizado sequencialmente à doxorrubicina foi capaz de reverter a quimiotoxicidade deste agente em 37,77% (SE±1.25, p=0.018). Conclusão: Utilizando a linhagem celular de câncer de ovário (OVCAR-3), BDNF exibiu um efeito sinérgico quando administrado concomitantemente com os agentes citotóxicos doxorrubicina, etoposideo e cisplatina. Observamos também um efeito protetor de BDNF quando aplicado 24 horas antes de doxorrubicina e paclitaxel. Notavelmente, quando BDNF foi administrado após a exposição a agentes antineoplásicos, uma reversão da citotoxicidade foi observada apenas para a doxorrubicina e não para os outros agentes. / Background: Ovarian cancer is the most prevalent and lethal of gynecological malignancies. Chemotherapy is an important component of the systemic treatment with a combination of a platinum complex and a taxane one of the classic treatments. Invariably, advanced ovarian cancer becomes resistant to chemotherapy. Objective: Based on recent data demonstrating a possible role of neurotrophins regulating chemosensitivity, we decided to study the impact of brain-derived neurotrophic factor (BDNF) on the antitumor activity of different classes of antineoplastic agents. Methods: Primarily, to evaluate a possible synergistic effect of BDNF and different ovarian cancer treatments combination, cells were exposed to cisplatin, etoposide, doxorubicin and paclitaxel concomitantly with BDNF for 48 hours. Sequential administration of BDNF and any of the agents was carried out to evaluate if BDNF has the potential of enhancing or protecting cells from the effects of treatment depending of each agent is applied first. Results: There were a reduction in viability of OVCAR-3 cells exposed to cisplatin, doxorubicin and etoposide when used concomitantly with BDNF in 61.18% (SE 1.12, p=0.002), 38.96% (SE 1.08, p=0.001) and 49.63% (SE 1.17, p<0.001) respectively. We also found that BDNF reduced significantly the effect of paclitaxel and doxorubicin when used before chemotherapy with a reduction of effect of 53.46% (SE±3.48, p=0.001) and 48.25% (SE±1.25, p=0.018), respectively. Furthermore, BDNF used sequentially to doxorubicin was able to reverse the chemotoxicity of this agent in 37.77% (SE 1.25, p=0.018). Conclusion: In conclusion, using the human ovarian carcinoma cell line OVCAR-3, BDNF exhibited a synergistic effect when administered concomitantly to the cytotoxic agents doxorubicin, etoposide and cisplatin. We have also observed a protective effect of BDNF when applied 24 hours before doxorubicin and paclitaxel. Notably, when BDNF was administered after the exposure to the antineoplastic agents, a reversal of cytotoxicity was observed only for doxorubicin and not for the other agents.

Neoplasias ovarianas

Ovarian cancer

OVCAR-3

Paclitaxel

Doxorubicin

Etoposide

Cisplatin

BDNF

Correlação entre os níveis de BNDF e melatonina na endometriose

Costa, Gislene Dalferth

January 2012

O fator neurotrófico derivado do cérebro (BDNF) e o turnover da melatonina estão associados à dor pélvica crônica (DPC) associada à endometriose. Nós realizamos este estudo para entender se a secreção de melatonina, avaliada pela 6-sulfatoximelatonina urinária (aMT6-s), está correlacionada com o controle do BDNF a outros fatores como fator de necrose tumoral (TNF), interleucina 6 (IL-6), interleucina 10 (IL-10), cortisol ou nível de dor. Foram analisadas vinte mulheres com idade entre 18 e 45 anos com dor pélvica crônica e diagnóstico de endometriose por videolaparoscopia. Diferenças nos padrões temporais de aMT6-s e cortisol salivar de acordo com os intervalos de tempo no dia sugerem que ambos apresentaram padrões fisiológicos de flutuação. A dispersão da média da aMT6-s obtida a cada 6 h foi plotada em uma curva de regressão polinomial correspondendo por 43% da variância no perfil de excreção. Aumentos de 1 ng/mL no BDNF sérico levaram a uma modificação média da aMT6-s de -14,32 [intervalo de confiança (IC) 95% (-24,09 a -4,59)] ou vice-versa, enquanto aumentos de 1 ng/mL no TNF sérico levaram a um aumento da excreção média de aMT6-s em 1,32 (IC 95% 0,65 a 1,98). aMT6-s não estava associada com IL-6, IL-10 ou nível de dor. Portanto, nós encontramos que o BDNF sérico está inversamente correlacionado com a aMT6-s, enquanto os níveis de TNF sérico estão positivamente correlacionados com aMT6-s. Estes achados demonstraram que a interação e as relações entre BDNF e secreção de melatonina na endometriose são complexas e que estudos longitudinais subsequentes são necessários para elucidar como estes sistemas interagem a longo prazo. / The brain-derived neurotrophic factor (BDNF) and melatonin turnover has been involved in the endometriosis-associated chronic pelvic pain (EACPP). We run this study to understand whether melatonin secretion, indexed by urinary 6-sulfatoxymelatonin (aMT6-s), is correlated with BDNF controlling to other factors such as tumor necrosis factor (TNF), interleukin 6 (IL-6), interleukin 10 (IL-10), cortisol or pain index. Twenty females, aged 18 to 45, with chronic pelvic pain and endometriosis diagnoses by videolaparoscopy, were analyzed. Differences in the temporal patterns of aMT6-s and salivary cortisol according to time-of-day intervals suggest that both presented physiological patterns of flotation. The dispersion of mean aMT6-s obtained every 6 h fitted a quadratic curve of polynomial regression accounting for 43% of the variance in the excretion profile. Increases of 1 ng/mL in serum BDNF led to a mean change in aMT6-s of -14.34 [confidence interval (CI) 95% (-24.09 to -4.59)] or vice versa, while increases of 1 ng/mL in serum TNF led to an increment of the mean aMT6-s excretion by 1.32 (CI 95%, 0.65 to 1.98). aMT6-s was not associated with interleukin (IL-6), interleukin (IL-10) or pain index. Therefore, we found that serum BDNF is inversely correlated with aMT6-s, while levels of serum TNF are positively correlated with aMT6-s. These findings demonstrated that the interaction and relations of BDNF and melatonin secretion in endometriosis are complex and that further longitudinal studies are needed to elucidate how these systems interact over a longer term.

Melatonina

Endometriose

Melatonin

6-sulfatoximelatonin

BDNF

TNF

Endometriosis

Efeitos comportamentais e neuroquímicos da harmina em modelos animais de depressão

Fortunato, Jucélia Jeremias

January 2009

Harmina é uma β-carbolina que atua sobre o SNC, inibindo a enzima monoaminooxidase tipo A-MAO. Esse alcalóide liga-se com relativa afinidade a receptores cerebrais de serotonina como a 5-hidroxitriptamina, subtipos 5-HT2C e 5-HT2A e receptores imidazólicos (I2). O objetivo deste estudo foi investigar os efeitos comportamentais e fisiológicos da administração aguda e crônica de harmina (5, 10 e 15 mg/kg) e imipramina (10, 20 e 30 mg/kg), utilizando o teste do nado forçado (TNF) e o protocolo de estresse crônico moderado (ECM) em modelo animal. Os resultados mostraram que os ratos tratados aguda e cronicamente com harmina e imipramina diminuíram o tempo de imobilidade no TNF, aumentaram o tempo de climbigns e de nado quando comparados com o grupo controle, sem, no entanto, afetar a atividade locomotora avaliada pelo teste de exploração ao campo aberto. Os níveis do fator neurotrófico derivado do cérebro (BDNF) no hipocampo dos ratos também foram aumentados pelos tratamentos agudo e crônico com harmina. Os animais submetidos ao protocolo de ECM apresentaram comportamento anedônico, aumento do peso médio da glândula adrenal e aumento nos níveis de ACTH e BDNF. O tratamento crônico com harmina durante 7 dias consecutivos, reverteu a anedonia e a hipertrofia da glândula adrenal, além de normalizar os níveis de ACTH e BDNF. O conjunto desses resultados auxiliam a compreensão do mecanismo de ação neuroprotetor da harmina e sugerem que este alcalóide possa representar um novo alvo farmacológico para o tratamento da depressão. / Harmine is a β-carboline that acts on the CNS, by inhibiting the enzyme monoamine oxidase type A-MAO. This alkaloid binds with affinity to receptors on serotonin as 5- hydroxytryptamine, 5-HT2C subtypes and 5-HT2A receptors and imidazole (I2). The objective of this study was to investigate the physiological and behavioral effects of acute and chronic administration of harmine (5, 10 and 15 mg / kg) and imipramine (10, 20 and 30 mg / kg) using the forced swimming test (TNF) and the protocol of chronic mild stress (ECM) in an animal model. The results showed that rats treated acutely and chronically with harmine and imipramine reduced the immobility time in the TNF, and increased both climbigns and swimming time of rats compared to saline group, without affecting locomotor activity in the open field test. Both acute and chronic administration of harmine increased factor brain-derived neurotrophic (BDNF) protein levels in the rat hippocampus. Our findings demonstrated that chronic stressful situations induced anhedonia, hypertrophy of adrenal gland weight, increase ACTH circulating levels in rats and increase BDNF protein levels. Interestingly, treatment with harmine for 7 consecutive days, reversed anhedonia, the increase of adrenal gland weight, normalized ACTH circulating levels and BDNF protein levels. Finally, these findings further support the hypothesis that harmine could be a new pharmacological tool for the treatment of depression.

Harmina

Depressão

Sistema nervoso central

Harmine

Depression

BDNF

Avaliação de modelo de menopausa em ratas : parâmetros fisiológicos, comportamentais, bioquímicos e novas estratégias terapêuticas

Moreira, Sônia Fátima da Silva

January 2014

Introdução: Os sintomas psíquicos e vasomotores são altamente prevalentes na transição menopáusica e na pós-menopausa, e estão relacionados ao hipoestrogenismo decorrente da falência ovariana que ocorre na mulher na meiaidade. Sua exata fisiopatogenia é desconhecida, porém alterações de neurotransmissores, como a serotonina e a noradrenalina, parecem estar relacionados ao aparecimento dessa sintomatologia. A terapia estrogênica geralmente é efetiva em aliviar esses sintomas, no entanto muitas mulheres não podem ou não desejam este tipo de tratamento, por isso, diversas alternativas têm sido estudadas. Objetivos: esta tese teve como objetivo avaliar, em um modelo experimental de climatério em ratas, parâmetros fisiológicos, comportamentais e bioquímicos, visando testar duas novas terapias: a cetamina, um antagonista não competitivo do receptor N-metil-D-aspartato (NMDA) e a eletroestimulação transcraniana de corrente contínua (ETCC) respectivamente, para o comportamento do tipo depressivo e a disfunção termorregulatória. Métodos: Ratos Wistar fêmeas adultas (200 a 250 g) foram randomizadas pelo peso e submetidas a modelo de menopausa por meio de ovariectomia bilateral ou a procedimento sham (falsa cirurgia). No primeiro experimento, os animais foram submetidos ao teste do nado forçado para avaliar comportamento do tipo depressivo e posteriormente receberam uma dose de cetamina 10mg/kg de peso intraperitoneal. No segundo experimento, os animais foram avaliados quanto à disfunção termorregulatória e tratados com ETCC catódica. Resultados: No primeiro experimento, as ratas em estado hipoestrogênico apresentaram comportamento do tipo depressivo que foi revertido pela cetamina. As ratas sham apresentaram um quadro de menopausa precoce indexado por citologia vaginal, provavelmente decorrente da manipulação de anexos. Além disso, as ratas ovariectomizadas apresentaram comportamento tipo ansioso. No entanto, não houve alteração da atividade locomotora e exploratória entre os grupos. No segundo experimento, as ratas ovariectomizadas apresentaram aumento da temperatura retal que foi parcialmente revertido pela eletroestimulação transcraniana de corrente contínua; as ratas ovariectomizadas apresentaram níveis elevados de interleucina 8 no soro, em relação às não ovariectomizadas, sem diferença nos níveis hipotalâmicos; houve aumento dos níveis séricos e diminuição dos níveis hipotalâmicos de BDNF nas ratas ovariectomizadas e interação do modelo com a ETCC em relação aos níveis corticais de BDNF. Nos testes nociceptivos, as ratas ovariectomizadas apresentaram diminuição do tempo de latência de resposta no teste da placa quente e alodinia mecânica no teste Von Frey, parcialmente revertida pela ETCC, no entanto, não houve diferença entre os grupos no teste tail flick. Conclusão: Nossos estudos demonstram que o modelo de ovariectomia utilizado foi eficaz em reproduzir os sintomas apresentados no período perimenopausa tendo, portanto, potencial translacional. Adicionalmente, sugerem que, além dos sistemas serotoninérgico e noradrenérgico, outros sistemas parecem estar associados ao aparecimento de sintomas na transição menopáusica como, por exemplo, o sistema glutamatérgico. Demonstram ainda que a cetamina e a ETCC podem ser eficazes como adjuvantes no tratamento dos sintomas do climatério, respectivamente, farmacológico (nos sintomas depressivos) e não farmacológico (nos “fogachos”). / Introduction: Psychological and vasomotor symptoms have a high prevalence in women during menopause transition and post menopausal years. Though these symptoms are associated to decline of estrogen levels due to ovarian failure, their exact pathophysiology is unknown. Variations on neurotransmitters such as serotonin and norepinephrine seem to be responsible by great amount of these symptoms. Estrogen therapy is usually effective in relieving these symptoms. However, many women have contraindications or do not wish to use this kind of treatment, thus several therapeutic alternatives have been studied. Objectives: This thesis was designed to evaluate, in an experimental model of menopause in rats, physiological, behavioral and biochemical parameters, aiming to test two new therapies: ketamine, a noncompetitive antagonist of the N-methyl-D-aspartate (NMDA) receptor and transcranial direct current stimulation (tDCS) respectively for the depressive-like behavior and thermoregulatory dysfunction. Methods: Female adult Wistar rats (200- 250g) were randomized by weight and subjected to a menopause model through bilateral ovariectomy or sham (false surgery) procedure. In the first experiment, the animals were subjected to the forced swimming test to assess depressive-like behavior and subsequently received a dose of 10mg/kg of weight of intraperitoneal ketamine. In the second experiment, the animals were evaluated for thermoregulatory dysfunction and treated with cathodal tDCS. Results: In the first experiment, the rats in hypoestrogenic state showed depressive-like behavior that was reversed by ketamine. The sham rats presented a precocious menopause indexed by vaginal cytology, probably due to the surgical handling of the tubes and ovaries. Moreover, the ovariectomized rats showed anxiety-like behavior. However, there was no change in locomotor activity between groups. In the second experiment, the ovariectomized rats showed an increase in rectal temperature that was partially reversed by tDCS. Moreover, the ovariectomized rats showed elevated serum levels of interleukin-8, compared to non-ovariectomized rats, with no difference in hypothalamic levels; there was an increase in serum levels and decreased hypothalamic BDNF levels in ovariectomized rats, and there was interaction of ovariectomy and ETCC in relation to cortical BDNF levels. In the nociceptive tests, the ovariectomized rats presented decreased response latency in the hot plate test and mechanical alodinia in the von Frey test; however, there was no difference between groups in the tail flick test. Conclusion: Our studies demonstrate that the ovariectomy model used was effective in reproducing the symptoms that women present during perimenopause and therefore has translational potential. Additionally, these data suggest that, beyond the serotonergic and noradrenergic systems, other systems seem to be associated with the onset of symptoms in menopausal transition such as the glutamatergic system. Our data also demonstrate that ketamine and ETCC can be effective adjuvant therapeutic tools to the relief of climacteric symptoms, respectively, pharmacological (on depressive symptoms) and non pharmacological (on "hot flashes").

Menopausa

Ketamina

Fogachos

Depressão

Menopause

tDCS

Ketamine

Estradiol

BDNF

Cytokines

Hot flushes

Avaliação de interleucinas, fator neurotrófico derivado do cérebro e marcadores de estresse oxidativo em pacientes com fibromialgia

Ranzolin, Aline

January 2014

Base teórica: Pacientes com alguns distúrbios psiquiátricos, como transtorno bipolar e depressão maior apresentam alteração de biomarcadores ligados à inflamação, estresse oxidativo e neurotrofinas. A relação entre estas susbstâncias tornou possível a criação de um Índice de Toxicidade Sistêmica (ITS) aplicável a algumas desordens psiquiátricas. Transtornos do humor são comuns em pacientes com fibromialgia (FM), despertando o interesse no estudo destes biomarcadores e do ITS nesta síndrome. Objetivos: Determinar os níveis de citocinas (IL-6, IL-10, IL-8 e TNF-α), de Brain-derived Neurotrophic Factor (BDNF) e de marcadores de estresse oxidativo (carbonil e TBARS - Thiobarbituric Acid Reactive Substances) em pacientes femininas com FM, relacionando com dados clínicos, níveis de depressão/qualidade de vida e comparando a mulheres saudáveis. Métodos: Foram avaliados os níveis de IL-6, IL-10, IL-8, TNF-α, BDNF, carbonil e TBARS em um estudo transversal incluindo 69 pacientes femininas com FM e 61 mulheres saudáveis. Os níveis de interleucinas foram medidos por citometria de fluxo, as concentrações de BDNF foram avaliadas pelo método de ELISA, e os marcadores de estresse oxidativo foram estudados por espectrofotometria (TBARS) e determinação de grupos carbonil. Além disso, o grupo com FM foi avaliado pelo Questionário de Impacto da Fibromialgia – Fibromyalgia Impact Questionnaire (FIQ) e pelas escalas de depressão de Hamilton e de Beck. Resultados: Os grupos tinham a mesma faixa etária (44,5 ± 6,4 anos no grupo FM e 44,0 ± 6,7 no grupo saudável; p = 0,613). As pacientes com FM tinham, caracteristicamente, longa duração de doença (8,5 ± 6,5 anos), importante impacto na qualidade de vida (FIQ 70,2 ± 17,8) e a maior parte apresentou depressão em algum grau (82,6% pelo BDI e 87,0% pelo HDRS). Os níveis séricos de IL-10 foram significativamente maiores no grupo com FM (p = 0,006), enquanto as demais citocinas, BDNF e marcadores de estresse oxidativo não diferiram entre os grupos. Não houve correlação significativa entre os diversos biomarcadores, tornando impossível o cálculo do ITS para pacientes com FM. Conclusão: Este estudo foi o primeiro a testar um índice conjunto de biomarcadores, já avaliados isoladamente em estudos prévios, em pacientes com FM. No entanto, a ausência de correlação estatística entre os níveis séricos destas substâncias não permitiu o cálculo do ITS e sua aplicação em FM, tal como em distúrbios do humor. No entanto, observamos níveis significativamente maiores de IL-10 em pacientes fibromiálgicas, resultado que merece avaliação específica em pesquisas futuras. / Background: Patients with certain psychiatric diseases, such as bipolar disorder and major depression present alteration of biomarkers related to inflammation, oxidative stress and neurotrophins. The relationship between these substances made possible the creation of a Systemic Toxicity Index (STI) applicable to some psychiatric disorders. Mood disorders are common in patients with fibromyalgia (FM), arousing the interest in the study of these biomarkers and STI in this syndrome. Objectives: Determine the levels of cytokines (IL-6, IL-10, IL-8 and TNF-α), Brain-derived Neurotrophic Factor (BDNF) and markers of oxidative stress (carbonyl and TBARS - Thiobarbituric Acid Reactive Substances) in female patients with FM, correlating with clinical data, levels of depression/quality of life and comparing to healthy women. Methods: We evaluated the levels of IL-6, IL-10, IL-8, TNF-α, BDNF, TBARS and carbonyl in a cross-sectional study including 69 female FM patients and 61 healthy women. Interleukins levels were measured by flow cytometry, BDNF concentrations were tested by ELISA method, and oxidative stress markers were studied spectrophotometrically (TBARS) and by the determination of carbonyl groups. In addition, the FM patients were evaluated by the Fibromyalgia Impact Questionnaire (FIQ) and Hamilton and Beck`s depression scales. Results: The groups had the same age range (44.5 ± 6.4 years in the FM group and 44.0 ± 6.7 in the healthy group; p = 0.613). The FM patients have characteristically long disease duration (8.5 ± 6.5 years), relevant impact on quality of life (FIQ 70.2 ± 17.8) and most presented depression in some level (82.6% by BDI and 87.0% by HDRS). Serum levels of IL-10 were significantly higher in the FM women (p = 0.006), while the other cytokines, BDNF and oxidative stress biomarkers did not differ between the groups. There was no significant correlation between the various biomarkers, making it impossible to calculate STI for patients with FM. Conclusion: This study was the first to test an index of a biomarkers set, already evaluated in isolation in previous studies, in patients with FM. However, the absence of statistical correlation between serum levels of these substances did not allow the calculation of STI and its application in FM, such as in mood disorders. However, we observed significantly higher levels of IL-10 in FM patients, a result that deserves in-depth evaluation in future surveys.

Fibromialgia

Interleucinas

Estresse oxidativo

Biomarcadores

Fibromyalgia

Interleukins

BDNF

Oxidative stress

Depression

Post-lesion plasticity of the Olivocerebellar pathway : molecular mechanism underlying the climbing fibre re-innervation of Purkinje cells / Plasticité post-lésionnelle de la voie olivocérébelleuse : mécanisme moléculaire sous-jacent à la réinnervation des cellules de Purkinje par les fibres grimpantes

Jara, Juan Sebastián

02 December 2016

La voie olivocérébelleuse (OCP) comprend les fibres grimpantes (CFs), terminaisons axonales des neurones de l'olive inferieure (ION), et leurs cibles, les cellules de Purkinje (PCs). La OCP suit une topographie hautement organisée. A la suite d'une lesion unilatérale de la OCP mature, l'application locale du facteur trophique ‘BDNF’ dans le hemicervelet dénervé induit la reinnervation fonctionnelle des PCs par les CFs. L'objectif de ce travail a était de comprendre les mécanismes activés par le BDNF permettant la plasticité post-lésionnelle dans le OCP mature. Avec un modèle ex vivo chez la souris, nous avons montré que l’injection de BDNF dans le cervelet dénervé augmente la croissance des branchements transverses des CFs intactes. Cette réponse est médiée par l'augmentation de l’expression de Pax3 dans l'ION intact. La surexpression du Pax3 dans l’ION augmente le niveau de PSA-NCAM dans le hemicervelet dénervé, probablement sur les CFs. Cette expression de PSA-NCAM est nécessaire et suffisante pour la réinnervation CF-PC. Nous proposons que la plasticité activée par le BDNF dans l'OCP mature implique le Pax3 et le PSA-NCAM dans l’ION, qui sous-tendent la genèse des branchements des CFs et la reconnaissance correcte des PC dénervés. Pendant le développement de la OCP, la plasticité post-lésionnelle spontanée est plus importante, permettant la compensation anatomique et fonctionnelle. Dans notre modèle ex vivo au stade immature, nous avons montré que cette plasticité spontanée implique l'expression de Pax3 et de PSA-NCAM. Ces résultats suggèrent que la reinnervation post-lésionnelle dans la OCP mature active certains mécanismes de la plasticité développementale. / In the olivocerebellar pathway (OCP) the afferent climbing fibres (CFs), which are the terminal axon projections of the inferior olivary nucleus (ION), innervate cerebellar Purkinje cells (PCs). Following unilateral transection of mature OCP, the addition of the neurotrophic factor BDNF into the denervated cerebellum induces functional CF reinnervation of PCs. What mechanism underlies the BDNF-activated plastic window in the mature OCP and whether recapitulates developmental plasticity remains unknown. Using an optimized ex vivo model of the mouse OCP, we have found that the addition of BDNF into the de-afferented hemicerebellum induces both the outgrowth and elongation of transverse branches from intact CFs. This BDNF-induced plastic response is mediated by the up-regulation of the expression of transcription factor Pax3 in the intact ION. Increased pax3 gene in the ION up-regulates polysialic acid-neural cell adhesion molecule (PSA-NCAM), most likely in the olivocerebellar axons, which was found to be necessary and sufficient for CF reinnervation to PCs. We propose that the BDNF-activated plastic mechanism in the mature OCP involves the afferent Pax3 and PSA-NCAM, which underlies the sprouting of CFs and their appropriate recognition of denervated PCs. Early postnatal OCP shows a spontaneous plasticity following lesion that compensates anatomically and functionally for PC denervation. Using our ex vivo model of the OCP, we found that developmental post-lesion plasticity intrinsically activates and depends on the expression of Pax3 and PSA-NCAM. These results suggest that BDNF treatment in mature OCP reactivates some steps of developmental plasticity mechanisms.

Plasticité post-Lésionnelle

Réinnervation

Voie olivocérébelleuse

Fibres grimpantes

Bdnf

Pax3

Reinnervation

Olivocerebellar pathway

Collateral sprouting

612.8

Role of Tyrosine-Related Kinase B Inhibition in the Mesocorticolimbic Stress and Reward Circuitries of the Adolescent and Adult Brain Following a Heterotypic Stress Regimen

Azogu, Idu

January 2017

The mesocorticolimbic system is involved in fundamental processes that drive motivational behaviors essential for survival (feeding, reproduction and sexual behavior, etc.), as well as neurochemical activity involved in mood regulation. Stressful life events are an important cause of dysregulated psychological functioning, which in some leads to a pathophysiology of mood disorders. A source of such disorder could be, among other underlying factors, an impairment of synaptic plasticity induced by alterations in the levels of neurotrophins and/or aberrant glucocorticoid responses. The role of the brain derived neurotrophic factor (BDNF) and its high affinity receptor tyrosine-related kinase B (TrkB) in the mesocorticolimbic reward circuitry has been largely studied in adulthood, yet a possible role of this system in mediating memory and emotional responses induced by stress during the juvenile, adolescence period has not been elucidated. The proposed set of thesis studies are designed to investigate the roles of BDNF and TrkB signaling, via the selective and non-competitive TrkB antagonist, ANA-12 (N-[2-[[(Hexahydro-2-oxo-1H-azepin-3-yl)amino]carbonyl]phenyl] benzo[b]thiophene-2-carboxamide), in the expression of stress-induced changes in the brain stress circuitry (including the medial prefrontal cortex (mPFC), hypothalamic-pituitary-adrenal (HPA) axis, and hippocampus) and reward signaling systems of the brain (including the nucleus accumbens (NAc) and ventral tegmental area (VTA)). In addition, experiments aim to determine behavioral changes following stress exposure in male and female Wistar rats. Finally, the possible interplay between BDNF, dopamine, glutamate and orexins in response to repeated stress is examined. Articles 1 and 2, aimed to assess the biochemical and behavioral effects of direct ANA-12 infusion (0.25 µg/ 0.5µl) into the nucleus accumbens shell during exposure to a 10-day heterotypic stress paradigm in male rats. Specifically, Article 1 demonstrated a key role for BDNF/TrkB signaling to regulate stress-induced effects. Notably, the impact of ANA-12 to attenuate anxiety-like behavior in repeatedly stressed rats while increasing anxiety behavior in non-stress rats suggest an interesting behavioral and neurochemical state-dependent process induced by TrkB receptor signaling. Article 2 supports the key role for BDNF secretion in basal and stress-induced behaviors in rats suggesting an influence of TrkB in sociability, motivation and passive avoidance. Furthermore, this role of TrkB extended to increased expression of orexin A in the Perifornical area (PfA) and a decrease in the ventral CA1 of the hippocampus, and in stress-induced elevations in orexinergic projections to the VTA, of which reductions were observed in non-stress groups treated with ANA-12. Article 3 demonstrated gender-specific behavioral and biochemical responses in different developmental periods and the impact of TrkB activation, dependent on stress exposure, to affect the regulation of TrkB receptor isoforms (full length and truncated TrkB, TrkB.FL and TrkB.T1, respectively) in adulthood. Results revealed increased CORT responses in adolescent females relative to males and attenuated CORT secretions in both genders by TrkB inhibition. Elevated activity levels in young adult females and increased passive coping behavior in the forced swim in stress-naïve females were also noted, in addition to novel observations on brain region and sex differences in TrkB receptor isoforms. Taken together, thesis findings derived from applications of ANA-12, shall foster knowledge on the contribution of BDNF in regulation of mood upon stress exposure at times when the brain is undergoing important maturation and remodelling, as well as on the relationship of stress exposure during adolescence and lasting brain and behavioral disorders in adulthood.

BDNF

TrkB

ANA-12

Heterotypic stress

Adolescence

Rats

HPA axis

Sex-specific differences

Corticosterone

Adulthood

BDNF-Related Gene Expression of Laser Capture Microdissected Glutamate Neurons from the Anterior Cingulate Cortex in Mouse Models of Autism Spectrum Disorder

Owens, Misty

01 August 2020

Autism spectrum disorder (ASD) is a neurodevelopmental disorder affecting social behaviors. ASD affects 1 in 59 children with males affected more frequently. ASD is postulated to result from excitatory and inhibitory neurotransmission imbalances. Brain-derived neurotrophic factor (BDNF) signaling affects ASD by influencing synaptogenesis, plasticity, and survival. Studying early in-utero neuropathological changes within ASD requires the use of animal models. Expression of BDNF-associated genes were analyzed within laser capture microdissected pyramidal neurons from the anterior cingulate cortex of male and female BTBR and valproic acid mouse models. No expression differences were found in any gene comparing the three groups. Gender comparisons did identify differences in NTRK2 and EFNB2. Significant correlations of gene expression were identified for male NTRK2 with EFNB2 and GRIN1 and EFNB2 with GRIN1 and female BDNF with GRIN1 expressions (p

Autism Spectrum Disorder

BDNF

Laser Capture Microdissection

Glutamatergic Neurons

Biology

Neurology

Neurosciences

Effects of physical and cognitive exercise on levels of peripheral BDNF in elderly : with cardiorespiratory fitness as a potential confounding factor

Tarassova, Olga

January 2019

<p>Kursen Projektarbete.</p>

BDNF

cardiorespiratory fitness

elderly

physical exercise

cognitive exercise

Sport and Fitness Sciences

Idrottsvetenskap

Trafic neuronal de l’activateur tissulaire du plasminogène (tPA) / Neuronal trafficking of tissue-type plasminogen activator (tPA)

Lenoir, Sophie

29 June 2018

L’activateur tissulaire du plasminogène est une sérine protéase initialement découverte dans le compartiment vasculaire et qui joue un rôle prépondérant dans le processus de fibrinolyse. De manière intéressante, le tPA est également présent dans le parenchyme cérébral, où il est notamment exprimé par les neurones. Le tPA est impliqué dans de nombreuses fonctions cérébrales dont la plasticité synaptique, les processus de mémoire et d’apprentissage ainsi que dans la survie et la mort neuronales. Le tPA est capable d’augmenter la signalisation calcique induite par une activation des récepteurs N-Méthyl-D-Aspartate (NMDAR) : un mécanisme à la base de la plasticité synaptique mais également de la mort neuronale excitotoxique. Cependant, il peut également activer les récepteurs du facteur de croissance épidermique (EGFR) pour induire un effet anti-apoptotique sur les neurones. Afin de mieux comprendre les différentes fonctions du tPA sur les neurones, nous nous sommes intéressés à la distribution et au trafic intracellulaire du tPA. Pour cela, nous avons créé un nouvel outil afin d’imager le tPA dans les neurones en temps réel: un plasmide codant pour une protéine fusion, le tPA-HaloTag®.Premièrement, nos résultats montrent que le tPA est présent dans les axones et les dendrites des neurones corticaux matures en culture et qu’il est majoritairement présent dans le compartiment post-synaptique. Cette étude a également permis de voir que le tPA est stocké et libéré par des vésicules d’exocytose VAMP2, qu’il peut être endocyté par des vésicules Rab5, recyclé par des vésicules Rab11 et dégradé par des vésicules Rab7. Deuxièmement, nous avons montré que le tPA est présent dans les mêmes vésicules synaptiques que le facteur neurotrophique issu du cerveau (BDNF) : une neurotrophine importante pour le bon fonctionnement cérébral et dont la maturation dépend de l’activité protéolytique du tPA. Ce travail fournit une meilleure compréhension du rôle et de la distribution du tPA dans les neurones et ouvre de nouvelles voies de recherche dans l’implication de du tPA et du BDNF dans la survie neuronale. / Tissue-type Plasminogen Activator (tPA) is a serine protease, firstly discovered for its fibrinolytic role in the vascular compartment. Interestingly, tPA is also present in the brain parenchyma, being notably expressed by neurons. tPA displays important roles in synaptic plasticity(Danny Baranes et al., 1998; Melchor and Strickland, 2006), learning, memory processes(R Madani et al., 1999; R Pawlak et al., 2002), neuronal survival and death. tPA is able to promote N-Methyl-D-Aspartate Receptors (NMDAR)-induced calcium influx, promoting synaptic plasticity or excitotoxic neuronal death. tPA is also able to activate Epidermal Growth Factor Receptors (EGFR), a mechanism mediating its anti-apoptotic effect. To better understand the different functions of tPA on neurons, we studied the pattern of distribution and trafficking of neuronal tPA. For that, we designed a new tool to image tPA in living neurons: a plasmid encoding for a tPA-HaloTag® fusion protein. We first found that tPA is present in both axons and dendrites of mature cultured cortical neurons and preferentially at the post-synaptic part. Our results also showed that tPA is stored and released by VAMP2 exocytotic vesicles, and can be endocytosed by Rab5 vesicles, recycled by Rab11 vesicles and degraded by Rab7 vesicles. Furthermore, tPA is localized and sorted in the same vesicles than Brain-Derived Neurotrophic Factor (BDNF), one of the most important neurotrophins, Interestingly, BDNF maturation is dependent of tPA proteolytic activity. This work provides a better understanding of the role and distribution of tPA in living neurons and opens new avenues into the involvement of tPA and BDNF in neuronal survival.

TPA

BDNF

Trafic

Tissue-type Plasminogen Activator

Brain-Derived Neurotrophic Factor

Neurons

Vesicles

Trafficking