Global ETD Search

261	Avaliação da qualidade de vida de sobreviventes de câncer na infância: uma proposta alternativa de coleta de dados / Evaluation of quality of life of survivors of childhood cancer: an alternative proposal for data collection Souza, Clelia Marta Casellato de 10 October 2014 (has links) O acometimento do câncer na infância é relativamente raro, com taxas relevantes de incidência de alguns tumores, como a leucemia linfoblástica aguda (LLA) e o tumor de Wilms (TW). Embora o câncer seja uma das dez primeiras causas de óbito de crianças e adolescentes e a primeira por doença a partir dos cinco anos, nas últimas décadas o progresso da terapêutica tem possibilitado um declínio nas taxas de mortalidade e expansão dos prazos de sobrevida. Desta forma, o acompanhamento efetivo no enfrentamento da doença passou a buscar análises mais amplas dos efeitos orgânicos tardios da doença e da terapêutica, incluindo as condições psicossociais do sobrevivente, como nas avaliações da qualidade de vida relacionada à saúde (QVRS). No sentido de ampliar o conhecimento e alternativas para o acompanhamento ambulatorial e periódico da condição de sobrevivência, este estudo buscou comparar o impacto na QVRS do sobrevivente adulto, dada a diferença na terapêutica de escolha para a remissão da LLA (quimioterapia) e do TW (cirurgia e quimioterapia), utilizando uma avaliação a distância da QVRS (SF-36, via telefone).Objetivos: Analisar e comparar a QVRS de sobreviventes adultos de LLA e TW, entre si e em relação a participantes sadios, acompanhados no Ambulatório Fora de Terapia do ITACI-HC-FMUSP, através da aplicação alternativa (via telefone) do SF-36.Casuística e Método: 90 participantes, acima de 18 anos. Grupo controle(CTRL) (30 sujeitos, fisicamente saudáveis, com ausência de diagnóstico prévio de câncer, recém-ingressos em curso superior) e Grupos experimentais (60 sobreviventes - Ambulatório Fora de Terapia - ITACI - HCFMUSP): grupo LLA (GLLA) - 30 sobreviventes LLA e grupo TW (GTW) 30 sobreviventes TW. A avaliação foi realizada através da aplicação, via telefone, do SF- 36. Após compilação dos domínios do SF-36, os resultados foram analisados através do teste de qui-quadrado, teste t-independente e teste de ANOVA. Resultados: Os participantes não apresentaram diferença significativa quanto a idade, a maioria eram solteiros, sem filhos e provenientes de São Paulo. O nível mais elevado de escolaridade do CTRL decorreu do critério de inclusão, mas com relevante proporção de sobreviventes no nível superior. Nos sobreviventes não houve diferença significativa de idade de diagnóstico e tempo de fora de terapia. Quanto a QVRS, houve melhores resultados dos sobreviventes masculinos em relação às sobreviventes e participantes CTRL. Especificamente, GLLA e GTW para Vitalidade e GLLA para Aspectos sociais, Saúde mental e Aspectos emocionais, no último aspecto detectada diferença também para as sobreviventes GTW. Nos sobreviventes com diagnóstico tardio (acima 53 meses) o GLLA apresentou melhores resultados na Capacidade funcional. Na percepção da própria saúde, houve diferença para todos os domínios, exceto nos Aspectos sociais e emocionais, estando as diferenças circunscritas a percepções positivas (boa, muito boa e excelente) da própria saúde pelos sobreviventes e controles. Conclusão: Particularmente no período do estudo, para a amostra selecionada e os aspectos analisados pelo SF-36 pode-se inferir que, apesar de algumas diferenças encontradas, os sobreviventes não apresentaram evidências de comprometimento de QVRS. O SF-36 (via telefone) pode ser um recurso de acesso e avaliação de QVRS de sobreviventes sob acompanhamento ambulatorial / The involvement of childhood cancer is relatively rare, with relevant incidence rates of some cancers such as Acute Lymphoblastic Leukemia (ALL) and Wilms Tumor (WT). Although cancer is one of the top ten causes of death in children and adolescents and the first disease from the age of five, in recent decades the therapeutic progress has made possible a decline in mortality rates and expansion of the survival periods. In this way, the effective monitoring in the confrontation of the disease passed to seek broader analyses of later organic effects from disease and therapy, including the psychosocial conditions of survivor, as in evaluations of healthrelated quality of life (HRQoL). In order to increase knowledge and alternatives for monitoring outpatient and periodic survival condition, this study sought to compare the impact on HRQoL of adult survivor, given the difference in the choice therapy for the remission of ALL (chemotherapy) and WT (surgery) using a remote assessment of HRQoL (SF -36 via telephone call). Objectives: Analyze and compare the HRQoL of adult survivors of ALL and WT between themselves and in relation to healthy participants, followed at the Ambulatory outside ITACI - HC - USP therapy , by alternative application ( by phone calls) of the SF - 36 . Methods: 90 participants , above 18 years. Control group (CTRL): (30 subjects, physically healthy, no history of oncological diagnosis, newly joined in higher education) and experimental groups (60 survivors - Outpatient Therapy - ITACI - HCFMUSP ): ALL group ( GALL ) - 30 ALL survivors and WT group ( GWT ) 30 WT survivors. The evaluation was performed by applying SF-36, via telephone calls. After compilation of the SF -36 domains, the results were analyzed through chi - square test, independent t test and ANOVA test. Results: Participants showed no significant difference regarding age, most were single, childless and from Sao Paulo. CTRL highest level of schooling resulted from inclusion criterion but with relevant proportion of survivors at the top level. In survivors there was no significant difference in age of diagnosis and time outside therapy. As for HRQoL there have been better results of male survivors in relation to female survivors and CTRL participants. Specifically GALL and GWT for vitality domain and GALL for social aspects, mental health and emotional aspects. In the last domain, it was detected also difference female survivors GWT. In survivors with late diagnosis (above 53 months) the GALL presented better results in functional capacity. In the perception of their own health, there were differences for all domains except in social and emotional aspects, with differences confined to positive perceptions (good, very good and excellent ) of own health by survivors and controls. Conclusion: Particularly during the study period, for the selected sample and the analyzed aspects by SF -36 can be inferred that, despite some differences, survivors did not show evidence of impairment of HRQoL . The SF -36 (via telephone calls) can be a resource of access HRQoL evaluation of survivors under ambulatory followup Adult Adulto Child Criança Qualidade de vida Quality of life Questionários Questionnaires Sobreviventes Survivors Tumor de Wilms Wilms tumor
262	Role of vascular plasticity in muscle remodeling in the child / Rôle de la plasticité vasculaire dans le remodelage musculaire chez l’enfant Gitiaux, Cyril 27 March 2015 (has links) Le muscle strié squelettique est un tissu richement vascularisé. Au delà de l'apport en oxygène et en nutriments, de nouvelles fonctions des vaisseaux ont été récemment identifiées, par le biais des interactions établies entre les cellules du vaisseau (cellules endothéliales) et les cellules du muscle, en particulier les cellules souches musculaires (cellules satellites). Celles-ci interagissent étroitement avec les cellules endothéliales pour leur expansion et leur différenciation, puis avec les cellules péri-endothéliales pour leur auto-renouvellement et leur retour à la quiescence. Les vaisseaux participent ainsi au contrôle de l’homéostasie du muscle squelettique. Grâce à ces interactions, les cellules vasculaires jouent donc un rôle central dans le remodelage tissulaire après un phénomène destructif, survenant par exemple au cours d’un trauma ou d’une myopathie. Pour étudier, les mécanismes de la plasticité vasculaire au cours du remodelage tissulaire, deux situations paradigmatiques de muscle en régénération chez l’enfant : la dermatomyosite juvénile (DMJ) et la dystrophie musculaire de Duchenne (DMD) ont été étudiées. Il existe, dans ces deux pathologies une souffrance musculaire associée à des cycles de nécrose/régénération. Elles se différencient par leur plasticité vasculaire et par leur évolution. En effet, la DMJ, la myopathie inflammatoire la plus fréquente de l’enfant est caractérisée par une vasculopathie avec perte en capillaires. L’évolution peut être favorable avec restitution ad integrum du muscle. La DMD est une myopathie génétique conduisant à une dégradation progressive de la force musculaire associée à une néovascularisation compensatrice. Le volet clinique/histologique incluant une analyse multiparamétrique des critères évolutifs cliniques et de réponse thérapeutique couplée à une réévaluation des données histologiques de la DMJ (analyse morphométrique des muscles DMJ) a permis de montrer qu’il existait des sous groupes phénotypiques homogènes de sévérité différente dans la DMJ. Le degré de sévérité clinique est relié à la gravité de la vasculopathie musculaire Par ailleurs, des marqueurs cliniques et histologiques simples permettant de repérer au diagnostic les patients nécessitant une escalade thérapeutique rapide (CMAS>34, atteinte gastrointestinale, fibrose endomysiale musculaire au diagnostic) ont été identifiés. Le volet cellulaire a permis l’identification in vitro des interactions cellulaires spécifiques et différentielles des myoblastes issues de patients DMD et DMJ sur les cellules endothéliales normales par l’analyse de leur rôle sur la prolifération, migration et différenciation des cellules vasculaires. Dans la DMD, les myoblastes entrainent une réponse angiogénique importante mais non efficace (néovascularisation anarchique). Dans la DMJ, les myoblastes participent efficacement à la reconstruction vasculaire notamment via la sécrétion de facteurs proangiogéniques. Ces résultats ont été renforcés par analyse transcriptomique effectuée à partir de cellules endothéliales et satellites isolées de muscles de patients confirmant le rôle central de la vasculopathie associée à un contexte inflammatoire spécifique lié à l’interféron dans la physiopathologie de la DMJ et montrant dans la DMD une dérégulation de l’homéostasie normale des interactions vaisseau-muscle avec mise en jeu d’un remodelage tissulaire non efficace. Ces données permettent d'identifier de nouvelles fonctions des cellules vasculaires dans le remodelage du muscle strié squelettique au cours des pathologies musculaires de l'enfant, et devraient ouvrir la voie à de nouvelles approches thérapeutiques. / Skeletal muscle is highly vascularised. Beyond oxygen and nutriment supply, new functions for vessels have been recently identified, through the interactions that vessel cells (endothelial cells) establish with muscle cells, particularly with muscle stem cells (satellite cells). These latter closely interact with endothelial cells for their expansion and their differentiation, then with periendothelial cells for their self-renewal and return to quiescence. During skeletal muscle regeneration endothelial cells reciprocally interact with myogenic cells by direct contact or by releasing soluble factors to promote both myogenesis and angiogenesis processes. Skeletal muscle regeneration typically occurs as a result of a trauma or disease, such as congenital or myopathies. To better understand the role of vessel plasticity in tissue remodeling, we took advantage of two muscular disorders that could be considered as paradigmatic situations of regenerating skeletal muscle in the child: Juvenile Dermatomyositis (JDM), the most frequent inflammatory myopathy and Duchenne Muscular Dystrophy (DMD), the most common type of muscular dystrophy. Although these two muscular disorders share, at the tissue level, similar mechanisms of necrosis-inflammation, they differ regarding the vessel domain. In JDM patients, microvascular changes consist in a destruction of endothelial cells assessed by focal capillary loss. This capillary bed destruction is transient. The tissue remodeling is efficient and muscle may progressively recover its function. By contrast, in DMD, despite an increase of vessels density in an attempt to improve the muscle perfusion, the muscle function progressively alters with age. We identified clinical and pathological markers of severity and predictive factors for poor clinical outcome in JDM by computing a comprehensive initial and follow-up clinical data set with deltoid muscle biopsy alterations controlled by age-based analysis of the deltoid muscle capillarization. We demonstrated that JDM can be divided into two distinctive clinical subgroups. The severe clinical presentation and outcome are linked to vasculopathy. Furthermore, a set of simple predictors (CMAS<34, gastrointestinal involvement, muscle endomysial fibrosis at disease onset) allow early recognition of patients needing rapid therapeutic escalation with more potent drugs. We studied in vitro the specific cell interactions between myogenic cells issued from JDM and DMD patients and normal endothelial cells to explore whether myogenic cells participate to the vessel remodeling observed in the two pathologies. We demonstrated that MPCs possessed angiogenic properties depending on the pathological environment. In DMD, MPCs promoted the development of establishment of an anarchic, although strong, EC stimulation, leading to the formation of weakly functional vessels. In JDM, MPCs enhanced the vessel reconstruction via the secretion of proangiogenic factors. This functional analysis was supported by the transcriptomic analysis consistent with a central vasculopathy in JDM including a strong and specific response to an inflammatory environment. On the contrary, DMD cells presented an unbalanced homeostasis with deregulation of several processes including muscle and vessel development with attempts to recover neuromuscular system by MPCs. To summarize, our data should allow the definition of new functions of vessel cells in skeletal muscle remodelling during muscle pathologies of the child that will open the way to explore new therapeutic options and to gain further insights in the pathogenesis of these diseases. Dermatomyosite juvénile Cellules endothéliales Juvenile dermatomyositis Duchenne muscular dystrophy Muscle biopsy Prognostic factors Endothelial cells Myogenic precursor cells Skeletal muscle regeneration 571.6
263	Mechanismen der Schädigung und der gestörten Regeneration im entzündeten zentralen Nervensystem Topphoff, Ulf Schulze 16 April 2009 (has links) Schädigungen im zentralen Nervensystem treten nicht nur bei der Multiplen Sklerose (MS), sondern auch bei einer Vielzahl weiterer entzündlicher Schadensparadigmen auf. Allgemeines Kennzeichen dieser primär wie auch sekundär entzündlichen neurodegenerativen Erkrankungen ist das Auftreten von oxidativem Stress in Verbindung mit einer eingeschränkten Regeneration von Nervenzellen und einem übermäßiges Auftreten von Astrozyten. Allerdings ist bislang nicht bekannt, welche Faktoren für eine frühe neuronale Schädigung verantwortlich sind, und welche Faktoren zu einem übermäßigen Auftreten von Astrozyten beitragen. Vorarbeiten belegten, dass Apoptose-regulierende Systeme, wie z.B. der TRAIL-Signalweg, sowohl an der Immunregulation als auch an Schädigungsprozessen im Gehirn beteiligt sein können. Im Rahmen dieser Arbeit wurde gezeigt, dass eine auf das ZNS beschränkte Blockade des TRAIL-Signalwegs in der EAE, dem Tiermodell der MS, zu einer signifikanten Verminderung des Erkrankungsgrades führte. Darüber hinaus wurde eine reduzierte Enzephalitogenität von TRAIL-defiziente Myelin-spezifischen Lymphozyten belegt. Die Ergebnisse deuten darauf hin, dass der TRAIL-vermittelte Schädigungsmechanismus die Pathogenese der Neuroinflammation entscheidend mitbestimmt und die immunregulatorische Wirkung eine eher untergeordnete Rolle spielt. Dagegen stellte sich im Tiermodell der bakteriellen Meningitis heraus, dass TRAIL hier eine anti-inflammatorische Rolle im ZNS spielt, die vor allem durch eine TRAIL-R-abhängige apoptotische Minderung der Entzündungsreaktion vermittelt wird. Eine Beeinflussung der Migration von Effektorzellen durch TRAIL konnte in diesem Modell ausgeschlossen werden. Anscheinend hängt die therapeutische Modulation des TRAIL-Systems entscheidend von der jeweils zu Grunde liegenden Ätiopathogenese ab und kann nicht allgemein auf entzündliche ZNS-Erkrankungen übertragen werden. Als mögliche Ursache für eine verminderte Regenerationsfähigkeit endogener Stammzellen konnte hier ein endogener Mechanismus aufgedeckt werden, der als Antwort auf oxidativen Stress zu einem quantitativen Überwiegen von Astrozyten führt. Dabei zeigte sich, dass nicht toxische oxidative Bedingungen das Proliferationsvermögen von neuralen Stammzellen deutlich hemmten und dazu führten, dass anstelle von Neuronen vornehmlich Astrozyten entstehen. Dieses veränderte Differenzierungsvermögen ließ sich sowohl in vitro als auch in vivo experimentell nachvollziehen und wies darauf hin, dass durch milde Entzündungsprozesse hervorgerufene basale metabolische Veränderungen die neuronale und astrogliale Entwicklung aus neuralen Stammzellen reziprok reguliert wird. In weiteren Untersuchungen stellte sich heraus, dass die Histondeacetylase Sirt1 in neuralen Stammzellen als Sensor für das Redox-Potenzial dient. Schon geringe metabolische Änderungen induzierten die Bindung an den bHLH-Transkriptionsfaktor Hes1, die zu einer direkten Modulation des pro-neuronalen Transkriptionsfaktors Mash1 führten und die Differenzierung von neuralen Stammzellen zugunsten der astroglialen Entwicklung beeinflussten. Die Aufklärung dieses Mechanismus könnte somit zukünftig helfen, intrinsische Regenerationsprozesse nach Schädigung des ZNS zu verstärken und damit neue therapeutische Perspektiven bei neurologischen Erkrankungen zu öffnen. / Damage processes of the central nervous system (CNS) are not only found in Multiple sclerosis (MS) even in a variety of inflammatory diseases. A common feature of these inflammatory neurodegenerative disorders is the existence of oxidative stress in combination with a failure of neuronal replenishment and the predominant occurrence of astrocytes (known as astrogliosis). So far, factors, which are responsible for early neuronal damage and overwhelming generation of astrocytes, are not known. Recent studies could show that the tumor necrosis factor related apoptosis-inducing ligand (TRAIL) might be involved in immunregulation as well as damage processes in the CNS. Here, it could be shown that blockade of TRAIL in the CNS of animals suffering from experimental autoimmune encephalomyelitis (EAE) significantly ameliorates the disease. Furthermore, transfer of myelin-specific TRAIL-deficient T cells into wild type recipients lead to a significantly attenuated disease score. These findings underline the contribution of TRAIL to irreversible CNS damage. In the adult mammalian brain, multipotent and self-renewing neural progenitor cells (NPCs) have the capacity to generate new neurons, astrocytes and oligodendrocytes. NPCs may thus serve as a regenerative tool by which brain damage could be compensated. However, repair processes in response to all forms of neuronal injury, be they inflammatory, ischemic, metabolic, traumatic or other, are characterized by the failure of neuronal replenishment and the predominant occurrence of astrocytes. The common molecular pathways underlying this phenomenon are only poorly understood. Here, it could be shown that subtle alterations of the redox state, found in different brain damage scenarios, substantially regulate the fate of murine NPCs via the histone deacetylase silent mating type information regulation 2 homolog 1 (Sirt1). Mild oxidative conditions suppress proliferation of NPCs and direct their differentiation towards the astroglial at the expense of the neuronal lineage (and vice versa). Under oxidative conditions, NPCs upregulate Sirt1 in vitro and in vivo, which then binds to the transcriptional repressor Hes1 and finally downregulates the pro-neuronal basic helix-loop-helix transcription factor Mash1. Furthermore, it could be shown that targeted modulation of Sirt1 activity mimics the effects of subtle redox alterations. The results provide evidence for an as yet unknown metabolic master switch, which determines the fate of NPCs. Targeting these mechanisms may minimize undesired aspects of reactive astrogliosis as well as improve the success of therapeutic neural stem cell implantation. oxidativer Stress EAE TRAIL Stammzellen Regeneration oxidative stress EAE TRAIL neuronal precursor cells regeneration 570 Biowissenschaften, Biologie 32 Biologie YG 4500 ddc:570
264	Aspectos epidemiológicos, biotipologia e evolução do tratamento da leucemia linfocítica aguda na infância e adolescência no Rio Grande do Sul / Epidemiological aspects, biotipologia and evolution of the treatment of acute lymphocytic leukemia in childhood and adolescence in Rio Grande do Sul Pereira, Waldir Veiga 31 August 2010 (has links) A Leucemia Linfocítica Aguda na infância e adolescência é uma neoplasia de precursores linfóides de natureza heterogênea. Foi a primeira neoplasia disseminada a tornar-se curável pela quimioterapia. No Brasil os estudos cooperativos para o seu tratamento foram iniciados em 1980 com a criação do primeiro protocolo para o tratamento desta leucemia, denominado Grupo Brasileiro para o Tratamento da Leucemia na Infância. Na seqüência destes estudos foram observadas Sobrevidas Livre de Eventos de 50%, 58% e 70% nos protocolos 80, 82 e 85 respectivamente. Durante as décadas de 1980 e 1990, com a divulgação dos excelentes resultados alcançados com os regimes dos protocolos do grupo Berlin Frankfurt Münster, uma série de instituições em nosso País passou a adotá-los. Apesar de termos conhecimento dos dados referentes a evolução dos pacientes protocolados no GBTLI e dos demais estudos divulgados pelas instituições de origem, não tínhamos, porém, uma avaliação epidemiológica nem o conhecimento dos índices de sobrevivência alcançados no estado do Rio Grande do Sul. Neste trabalho foram avaliados 1472 pacientes com LLA, 833 (56,59%) do sexo masculino, 639 (43,41%) do sexo feminino, com idades entre zero e 20 anos, média de 7,40 anos (desvio padrão 5,14) e mediana de 5,70 anos (amplitude 0,06 a 20,76), no período de 1980 a 2008 provenientes deste Estado. Os dados foram colhidos individualmente dos prontuários dos pacientes admitidos nas principais instituições hospitalares que mantém assistência a pacientes pediátricos com neoplasias hematológicas. No presente estudo 487 pacientes (39,40%) foram registrados oficialmente nos protocolos do GBTLI; 678 (54,85%) receberam tratamento baseados nos regimes do grupo BFM e 71 (5,75%) por outros regimes incluindo os tratados segundo o protocolo UKALL. Os casos não foram, no entanto, protocolados e, na grande maioria não foram observados a totalidade dos itens exigidos para os pacientes registrados oficialmente. A sobrevida livre de eventos dos pacientes protocolados foi significativamente superior comparada aos não protocolados, 62,41% ± 2,43% e 53,86% ± 2,04% respectivamente, em cinco anos. De acordo com a faixa etária os pacientes que apresentavam idade de 15 a 19 anos tiveram um índice de SLE de 37,98% ± 4,72% em cinco anos, inferior quando comparado aos de zero a 4 anos e 5 a 9 anos respectivamente: 62,78% ± 2,28% e 62,43% ± 2,84%. Foi observada, na população estudada, uma SG de 63,73% ± 1,49% e SLE de 57,27% ± 1,57%, o que sugere uma discussão para implementar projetos com a finalidade de elevar estes índices de sobrevida. Epidemiologicamente a incidência da LLA com progenitores B seguiu o padrão observado em países desenvolvidos com um pico de freqüência absoluta entre as idades de 2 a 4 anos. Houve diferença significativa entre a população proveniente da região urbana ou rural sendo a SLE em cinco anos de 61,76% ± 1,76% e 49,81% ± 4,28% respectivamente. A SLE e a SG em lactentes e portadores de Síndrome de Down foi inferior aos resultados obtidos em instituições dos países desenvolvidos o que torna aconselhável uma revisão das condições para a assistência destes pacientes. Este estudo teve como finalidade principal retratar a situação passada e a atual do tratamento da LLA na infância e adolescência no Rio Grande do Sul e acumular dados aqui não interpretados e que poderão ser analisados posteriormente / Acute lymphocytic leukemia in childhood and adolescence is a neoplastic disease of lymphoid precursor of heterogeneous nature, being the first disseminated neoplasia to become curable through Chemotherapy. In Brazil, cooperative studies for the treatment of ALL started in 1980 with the creation of the first protocol by the Grupo Brasileiro para o Tratamento da Leucemia na Infância. According to these studies, Event Free Survival of 50%, 58% and 70% in the protocols of 1980, 1982 e 1985 respectively was observed. During the 80s and 90s many Brazilian institutions adopted the protocols motivated by the excellent results achieved by the Berlin Frankfurt Münster group. In spite of the knowledge provided by data related to the evolution of patients protocoled by the GBTLI and other studies published by medical institutions, there was not an epidemiologic evaluation or knowledge of survival indexes achieved in the state of Rio Grande do Sul. In this work, 1472 patients with ALL from the state of Rio Grande do Sul were evaluated. Among the subjects, 833 (56,59%) were male, 639 (43,41%) female, with age range between 0- 20 y average age of 7,40 (standard deviation 5,14) and median 5,70 years old (amplitude 0,06 to 20,76). Data was collected from the medical registers of patients with hematologic neoplasia in medical institutions, which offered pediatric assistance for ALL comprising the period between 1980 until 2008. In the present study, 487 patients (39,40%) were officially registered in the protocols of GBTLI; 678 (54,85%) received treatment based on the regime of the BFM group and 71 (5,75%) were treated according to other regimens (including the UKALL protocol). The cases, however, were not protocoled and, in most cases, the totality of items required for the patients registered officially were not observed. The EFS of the patients protocoled were significantly superior to those who were not protocoled (62,41% ± 2,43% and 53,86% ± 2,04% respectively) in five years. In respect to the age range, the patients which were between 15-20 years had an EFS index of 37,98% ± 4,72% in five years, which is inferior to the index of patients 0-4 years and 5-9 years: 62,78% ± 2,28% e 62,543± 2,84% respectively. An overall survival (OS) of 63,73% ± 1,49% and EFS of 57,27% ± 1,57% was observed in the population studied. These results indicate that a discussion for the implementation of projects, which can increase the indexes of cure, should be carried out. Epidemiologically, the incidence of ALL in B progenitors followed the pattern observed in developed countries with an absolute frequency peak in the age range of 2-4 years. The outcome was superior for patients coming from urban area in comparison to those from rural area. EFS and OS in infant and Down syndrome patients were inferior to the results obtained in developed countries, showing how important it is to review the conditions of the assistance provided to these patients. The objective of this work is to present the development of ALL treatment in childhood and adolescence in the state of Rio Grande do Sul, Brazil, from its beginning until the current days providing data, which can be analyzed and interpreted posteriorly Análise de sobrevida Antineoplastic protocols Brasil Brazil Epidemiologia Epidemiology Incidence Incidência Protocolos antineoplásicos Survival analysis
265	Desenvolvimento de processo de produção de conjuntos eletrodo-membrana-eletrodo para células a combustível baseadas no uso de membrana polimérica condutora de prótons (PEMFC) por impressão a tela / Development of a membrane electrode assembly production process for proton exchange membrane fuel cell (PEMFC) by sieve printing Rafael Nogueira Bonifacio 30 March 2010 (has links) Energia é um recurso que historicamente apresenta tendência de crescimento de demanda. Projeções indicam que, para suprir as necessidades energéticas do futuro, será necessário um uso massivo do hidrogênio como combustível. O uso de sistemas de célula a combustível baseada no uso de membrana polimérica condutora de prótons (PEMFC) tem características que permitem sua aplicação para geração de energia elétrica em aplicações estacionárias, automotivas e portáteis. O uso de hidrogênio como combustível para PEMFC apresenta a vantagem de resultar em baixa emissão de poluentes quando comparado às dos combustíveis fósseis. Para que ocorram as reações em uma PEMFC é necessária a construção de conjuntos eletrodo-membrana-eletrodo (MEA), sendo o processo de produção de MEAs e os materiais utilizados, relevantes no custo final do kW instalado para geração de energia por sistemas de célula a combustível, o que é, atualmente, uma barreira tecnológica e financeira para a aplicação em grande escala desta tecnologia. Nesse trabalho foi desenvolvido um processo de produção de MEAs por impressão a tela que apresenta alta reprodutibilidade, rapidez e baixo custo. Foram desenvolvidos o processo de impressão a tela e a composição de uma tinta precursora da camada catalisadora (TPCC), que permitem o preparo de eletrodos para confecção de MEAs com a aplicação da massa exata de eletrocatalisador adequada para cátodos 0,6 miligramas de platina por centímetro quadrados (mgPt.cm-2) e ânodos 0,4 mgPt.cm-2 em apenas uma aplicação por eletrodo. A TPCC foi desenvolvida, produzida, aplicada e caracterizada, apresentando características semelhantes a de tintas de impressão a tela para outras aplicações. Os MEAs produzidos apresentaram desempenho de até 712 mA.cm-2 a 600 mV para MEAs de 25 cm2 e o custo para produção de MEAs de 247,86 cm2 capazes de gerar 1 kW de energia foi estimado em R$ 13.939,45, considerando custo de equipamentos, materiais e mão de obra. / Energy is a resource that presents historical trend of growth in demand. Projections indicate that future energy needs will require a massive use of hydrogen as fuel. The use of systems based on the use of proton exchange membrane fuel cell (PEMFC) has features that allow its application for stationary applications, automotive and portable power generation. The use of hydrogen as fuel for PEMFC has the advantage low pollutants emission, when compared to fossil fuels. For the reactions in a PEMFC is necessary to build membrane electrode assembly (MEA). And the production of MEAs and its materials are relevant to the final cost of kW of power generated by systems of fuel cell. This represent currently a technological and financial barriers to large-scale application of this technology. In this work a process of MEAs fabrication were developed that showed high reproducibility, rapidity and low cost by sieve printing. The process of sieve printing and the ink composition as a precursor to the catalyst layer were developed, which allow the preparation of electrodes for MEAs fabrication with the implementation of the exact catalyst loading, 0.6 milligrams of platinum per square centimeters (mgPt.cm-2) suitable for cathodes and 0.4 mgPt.cm-2 for anode in only one application step per electrode. The ink was developed, produced, characterized and used with similar characteristics to ink of sieve printing build for other applications. The MEAs produced had a performance of up to 712 mA.cm-2 by 600 mV to 25 cm2 MEA area. The MEA cost production for MEAs of 247.86 cm2, that can generate 1 kilowatt of energy was estimated to US$ 7,744.14 including cost of equipment, materials and labor. célula a combustível PEMFC electrode membrane assembly impressão a tela electrode membrane assembly fuel cell PEMFC sieve printing
266	Efeito da toxina distensora citoletal de Aggregatibacter actinomycetemcomitans na atividade osteoclástica. / Aggregatibacter actinomycetemcomitans cytolethal distending toxin effect in osteoclast activity. Kawamoto, Dione 22 May 2014 (has links) Aggregatibacter actinomycetemcomitans está associado à periodontite agressiva, caracterizada pela intensa reabsorção do osso alveolar. Esta espécie produz a toxina distensora citoletal (AaCDT) que possui atividade de DNAse, e promove o bloqueio das células alvo na fase G2 ou G1/ G2. Por outro lado, CDT ativa a cascata apoptótica pela atividade de PIP3, regulando a proliferação e sobrevivência de linfócitos, pelo bloqueio de Akt. Em monócitos, AaCDT induz aumento da produção de citocinas pró-inflamatórias e inibe a produção de óxido nítrico e fagocitose. Células precursoras de osteoclastos têm origem hematopoiética e sofrem diferenciação em osteoclastos, mediada pelo RANKL, mas outros fatores co-estimulatórios estão envolvidos. A AaCDT induz a produção de RANKL por fibroblastos. Assim, formulamos a hipótese se CDT influenciaria a homeostase óssea por afetar a diferenciação de células precursoras de osteoclastos. O estudo visou determinar o efeito de AaCDT sobre a sobrevivência, diferenciação e atividade em RAW264.7 e BMC. Os dados sugerem que a CDT interfere na homeostase óssea, favorecendo a indução da diferenciação de células precursoras de osteoclastos e alterando o perfil de citocinas produzidas. / Aggregatibacter actinomycetemcomitans is associated with aggressive periodontitis, characterized by severe alveolar bone resorption. This species produces a distending toxin cytolethal (AaCDT) which has DNase activity, and promotes the blocking of target cells in G2 or G1 / G2 phase. On the other hand, CDT activates the apoptotic cascade by PIP3 activity, regulating lymphocyte proliferation and survival by blocking Akt. In monocytes, AaCDT enhances the production of proinflammatory cytokines and inhibits nitric oxide production and phagocytosis. Osteoclast precursor cells are of hematopoietic origin and must undergo differentiation into osteoclasts mediated by RANKL although other co-stimulatory factors are involved. AaCDT induces the production of RANKL by fibroblasts. Thus, CDT is hypothesized to influence bone homeostasis by affecting the differentiation of precursor cells into osteoclasts. This study aimed to determine the effect of AaCDT on survival, differentiation and activity of osteoclasts precursor cells. The data suggested that CDT interfere in bone homeostasis, favoring the differentiation of osteoclasts precursors cells and by altering their cytokines profile. Aggregatibacter actinomycetemcomitans Aggregatibacter actinomycetemcomitans Células de medula óssea murínica Células RAW 264.7 Cytolethal distending toxin Murine bone marrow cells Osteoclast precursor cells Osteoclastos RAW 264.7 cells Toxina distensora citoletal
267	Capacidade proliferativa in vitro de precursores neuro-gliais, telencefálicos e expressão dos genes 1 e 2 do Complexo da Esclerose Tuberosa (TSC1 e TSC2) / Proliferation capability of telencephalic neuroglial progenitors and expression of the Tuberous Sclerosis Complex 1 and 2 genes (TSC1 and TSC2) Marín, Alexandra Belén Saona 10 December 2012 (has links) O complexo da esclerose tuberosa (TSC) é um transtorno clínico, com expressividade variável, caracterizado por hamartomas que podem ocorrer em diferentes órgãos. Tem herança autossômica dominante e é devido a mutações em um de dois genes supressores de tumor, TSC1 ou TSC2. Estes codificam para as proteínas hamartina e tuberina, respectivamente, que se associam formando um complexo macromolecular que regula funções como proliferação, diferenciação, crescimento e migração celular. As lesões cerebrais podem ser muito graves em pacientes com TSC e caracterizam-se por nódulos subependimários (SEN), astrocitomas subependimários de células gigantes (SEGA), tuberosidades corticais e heterotopias neuronais, podendo relacionar-se clinicamente à epilepsia refratária à terapia medicamentosa, deficiência intelectual, desordens do comportamento e hidrocefalia. O potencial de crescimento de SEGA até os 21 anos de idade dos pacientes exige acompanhamento periódico por exame de imagem e condutas clínicas ou cirúrgicas, conforme indicação médica. As lesões subependimárias têm sido explicadas por déficits de controle da proliferação, crescimento e diferenciação de precursores neuro-gliais na zona subventricular telencefálica. Embora a capacidade da tuberina em inibir a proliferação celular pela repressão do alvo da rapamicina em mamíferos (mTOR) esteja bem documentada, outros aspectos celulares do desenvolvimento de SEGA ainda não foram examinados. Assim, é importante estabelecer um sistema in vitro para o estudo de células da zona subventricular e testá-lo na análise das proteínas hamartina e tuberina. Neste sentido, o cultivo de neuroesferas em suspensão é muito apropriado. Neste estudo, buscamos relacionar a expressão e distribuição subcelular da hamartina e tuberina à capacidade proliferativa e de diferenciação das células de neuroesferas cultivadas in vitro a partir da dissociação da vesícula telencefálica de embriões de ratos normais. Analisamos a expressão e distribuição subcelular da hamartina e tuberina por imunofluorescência indireta em células entre a primeira e a quarta passagens das neuroesferas, sincronizadas nas fases G1 ou S do ciclo celular e após a reentrada no ciclo celular, através da incorporação de 5-bromo-2\'-desoxiuridina (BrdU) e imunofluorescência com anticorpo anti-BrdU. Em geral, células de neuroesferas apresentaram baixa colocalização entre hamartina e tuberina in vitro. A expressão da tuberina foi elevada em basicamente todas as células das esferas e fases do ciclo celular; ao contrário, a hamartina apresentou-se principalmente nas células da periferia das esferas. A colocalização entre hamartina e tuberina foi observada em células mais periféricas das esferas, sobretudo no citoplasma e, em G1, no núcleo celular. A proteína rheb, que conhecidamente interage diretamente com a tuberina, apresentou distribuição subcelular muito semelhante à desta. Ao carenciamento das células visando à parada do ciclo celular na transição G1/S, tuberina distribuiu-se ao núcleo celular em quase todas as células avaliadas e, de forma menos frequente, a hamartina também. À reentrada no ciclo celular pelo reacréscimo dos fatores de crescimento, avaliaram-se células com incorporação de BrdU ao seu núcleo celular, após 72 e 96 horas. Nestas, tuberina mostrou-se novamente no citoplasma de forma preponderante e hamartina manteve-se citoplasmática, em geral subjacente à membrana plasmática, em níveis mais baixos. Os grupos cujas células reciclaram por 72 ou 96 horas diferiram quanto ao aumento significativo da expressão da hamartina em células proliferativas no último. À diferenciação neuronal, aumentaram-se os níveis de expressão de hamartina observáveis à imunofluorescência indireta, tornando-se equivalentes àqueles da tuberina. Concluímos que as células de neuroesferas cultivadas em suspensão apresentam-se como um sistema apropriado ao estudo da distribuição das proteínas hamartina e tuberina e sua relação com o ciclo celular / The tuberous sclerosis complex (TSC) is a clinical disorder with variable expressivity, characterized by hamartomas that can occur in different organs. It has autosomal dominant inheritance and is due to mutations in one of two tumor suppressor genes, TSC1 or TSC2. These encode for the proteins hamartin and tuberin, respectively, which are associated in a macromolecular complex which functions as a regulator of cell proliferation, differentiation, growth and migration. TSC brain lesions may be severe and are characterized by subependymal nodules (SEN), subependymal giant cell astrocytomas (SEGA), neuronal heterotopias and cortical tubers, and may be clinically related to refractory epilepsy, intellectual disability, behavioral disorders and hydrocephaly. The growth potential of SEGA up to 21 years of age in TSC patients requires regular monitoring by imaging. Clinical and surgical interventions may be medically indicated. Subependymal lesions have been explained by deficient control of proliferation, growth and differentiation of neuro-glial progenitors from the telencephalic subventricular zone. While tuberin ability to inhibit cell proliferation by repressing the mammalian target of rapamycin (mTOR) has been well documented, other cell aspects of SEGA development have not been thoroughly examined. Therefore, it is important to establish conditions for an in vitro system to study the cells from the subventricular zone and to test its suitability for the study of the TSC proteins. In this regard, the neurosphere suspension culture is very appropriate. We evaluated the expression and subcellular distribution of hamartin and tuberin in relation to the proliferation and differentiation capability of neurosphere cells derived in vitro from the dissociation of the telencephalic vesicle of normal E14 rat embryos. These analyses were performed by indirect immunofluorescence in cells from first through fourth passages of neurospheres, synchronized in G1 or S phases of the cell cycle, and after reentry into the cell cycle by the addition of 5-brome-2\'-desoxyuridine (BrdU) and immunolabeling with anti-BrdU antibody. In general, neurosphere cells presented low colocalization between hamartin and tuberin in vitro. Tuberin expression was relatively high in basically all neurosphere cells and cell cycle phases, whereas hamartin distributed mainly to cells from the periphery of the spheres. In these cells, hamartin and tuberin colocalization was evident mostly in the cytoplasm and, in G1, also in the cell nucleus. Rheb, which is known to interact directly with tuberin, had subcellular distribution very similar to tuberin. Cell starvation indicating cell cycle arrest at G1/S redistributed tuberin to the cell nucleus in virtually all cells examined, what was accompanied by nuclear location of hamartin in a small subset of cells. When cells were allowed to reenter cell cycle by adding growth factors, we evaluated BrdU-labeled nuclei 72 and 96 hours later. In the two groups, tuberin was shown to move back to the cytoplasm as well as hamartin, which apparently maintained its lower expression levels distribution underneath the plasma membrane. Group of cells that recycled for 96 hours had significantly more expression of hamartin than those cells that cycled for only 72 hours. After neuronal differentiation, hamartin expression levels observed by immunofluorescence were similar to those of tuberin. We conclude that neurosphere cells cultured in suspension showed to be an appropriate cell system to study hamartin and tuberin distribution in respect to the cell cycle Cell proliferation Cerebral cortex Córtex cerebral Esclerose tuberosa Hamartin Hamartina Neuroglial progenitor Precursor neuro-glial Proliferação celular TSC1 TSC1 TSC2 TSC2 Tuberin Tuberina Tuberous sclerosis
268	Glicogênio sintase quinase3B e proteína precursora do amilóide em plaquetas de indivíduos com comprometimento cognitivo leve e doença de Alzheimer / Glycogen synthase kinase 3B and amyloid precursor protein in adults platelets with cognitive impairment and Alzheimers disease Torres, Carolina Akkari 10 February 2010 (has links) A doença de Alzheimer (DA) é uma doença neurodegenerativa caracterizada pelo declínio progressivo da memória e de outras funções cognitivas, acometendo, sobretudo, indivíduos idosos. A anormalidade do metabolismo da proteína precursora do amilóide (APP) e a hiperfosforilação da proteína TAU são processos celulares característicos desta doença. A enzima glicogênio sintase quinase 3B (GSK3B) é altamente expressa no sistema nervoso central e apresenta grande importância na regulação da plasticidade neuronal e também nos mecanismos de sobrevivência celular. Estudos têm associado a GSK3B aos mecanismos que levam à formação das placas senis e dos emaranhados neurofibrilares na DA. Diante da dificuldade para se estabelecer com precisão o diagnóstico clínico da DA, sobretudo nas fases iniciais da doença, a identificação de biomarcadores se torna particularmente importante, principalmente em tecidos periféricos. Este trabalho avaliou, por meio de dois preparos distintos, dois possíveis candidatos a marcadores bioquímicos para a DA. Em plaquetas de pacientes com DA, comprometimento cognitivo leve (CCL) e idosos saudáveis, determinamos: (1) a razão de APP (APPr), que consiste na proporção entre fragmentos de 130kDa e 110kDa da APP; e (2) a expressão das formas fosforilada (fosfo-GSK3B) e total (total-GSK3B) da enzima GSK3B, possibilitando o cálculo da razão de GSK3B (fosfo-GSK3B/total-GSK3B). Ambas as razões foram avaliadas por Western Blot utilizando anticorpos específicos. Não observamos diferença estatisticamente significante nos valores de APPr entre os três grupos estudados (p=0,847). Para o cálculo da razão de GSK3B, foram necessárias adaptações do protocolo de preparo e análise de plaquetas, prevenindo a ativação plaquetária durante o procedimento, bem como a degradação do substrato pela ação de proteases e fosfatases presentes nesta matriz biológica; deste modo foram encontradas diferenças estatisticamente significantes entre os grupos nas médias de GSK3B total e da razão de GSK3B (p=0,05 e p=0,06 respectivamente). Não foi encontrada correlação entre a razão de APP e a razão de GSK3B. Contudo, a razão de GSK3B mostrou correlação com o desempenho em testes de memória, segundo o escore na bateria cognitiva CAMCOG. Estes resultados sugerem que a razão de GSK3B em plaquetas sinaliza algumas alterações biológicas que ocorrem na progressão do CCL para a demência na DA / Alzheimer\'s disease (AD) is a neurodegenerative disease characterized by progressive decline of memory and other cognitive functions, affecting mainly elderly. The abnormal metabolism of amyloid precursor protein (APP) and protein TAU hyperphosphorylation are cellular hallmarks of this disease. Glycogen synthase kinase 3B (GSK3B) is an enzyme highly expressed in the central nervous system and of great importance in the regulation of neuronal plasticity and also the mechanisms of cell survival. Studies have associated GSK3B with the mechanisms that lead to the formation of senile plaques and neurofibrillary tangles in AD. Given the difficulty to establish the precise clinical diagnosis of AD, especially in the early stages of the disease, identification of biomarkers is particularly important, especially in peripheral tissues. This work evaluated two candidate biochemical markers for AD, using two different preparations. We investigated the ratio between 130kDa and 110kDa APP fragments (APPr) and between phosphorylated and total GSK3B (phospho-GSK3B / total-GSK3B) in platelets of patients with AD and mild cognitive impairment (MCI), comparing their results with those from healthy older adults (controls). The expression of APP fragments and GSK3B was assessed by Western blot using specific antibodies. No statistically significant differences in APPr were found between the study groups (p=0.847). We found statistically significant differences in mean total GSK3B and GSK3B ratio across disgnostic groups (p=0.05 and p=0.06, respectively). APPr and GSK3B ratio were not correlated, but the latter parameter did correlate with the performance on memory tests, as shown by the CAMCOG sub-score. The present data indicate that platelet GSK3B ratio may indicate biological changes that occur in the MCI-AD continuum Alzheimer disease Amyloid precursor protein Biological markers Biomarcadores Biomarkers Doença de Alzheimer Glicogênio sintase Glycogen synthase Marcadores biológicos Plaquetas Platelets Proteína precursora do amilóide
269	S?ntese, sinteriza??o e caracteriza??o de ferritas ? base de Ni-Zn Moura, Alysson Elson Galv?o de 24 September 2008 (has links) Made available in DSpace on 2014-12-17T15:41:43Z (GMT). No. of bitstreams: 1 AlyssonEGM.pdf: 4274696 bytes, checksum: 0f940193275b15ce59b4b1f45e3dc11c (MD5) Previous issue date: 2008-09-24 / Conselho Nacional de Desenvolvimento Cient?fico e Tecnol?gico / Were synthesized different ferrites NixZn1-xFe2O4 (0,4 ≤ x ≤ 0,6) compositions by using citrate precursor method. Initially, the precursors citrates of iron, nickel and zinc were mixed and homogenized. The stoichiometric compositions were calcined at 350?C without atmosphere control and the calcined powders were pressed in pellets and toroids. The pressed material was sintered from 1100? up to 1200?C in argon atmosphere. The calcined powders were characterized by XRD, TGA/DTG, FTIR, SEM and vibrating sample magnetometer (VSM). All sintered samples were characterized using XRD, SEM, VSM and measurements of magnetic permeability and loss factor were obtained. It was formed pure ferromagnetic phase at all used temperatures. The Rietveld analyses allowed to calculate the cations level occupation and the crystallite size. The analyses obtained nanometric crystals (12-20 nm) to the calcined powder. By SEM, the sintered samples shows grains sizes from 1 to 10 μm. Sintered densities (ρ) were measured by the Archimedes method and with increasing Zn content, the bulk density decrease. The better magnetization results (105-110 emu/g) were obtained for x=0,6 at all sintering temperatures. The hysteresis shows characteristics of soft magnetic material. Two magnetization processes were considered, superparamagnetism at low temperature and the magnetic domains formation at high temperatures. The sintered toroids presents relative magnetic permeability (μr) from 7 to 32 and loss factor (tanδ) of about 1. The frequency response of toroids range from 0,3 kHz to 0,2 GHz. The composition x=0,5 presents both greater μr and tanδ values and x=0,6 the most broad range of frequency response. Various microstructural factors show influence on the behavior of μr and tanδ, such as: grain size, porosity across grain boundary and inside the grain, grain boundary content and domain walls movement during the process of magnetization at high frequency studies (0,3kKz 0,2 GHz) / Foram sintetizadas diferentes composi??es da ferrita Ni1-xZnxFe2O4 com 0,4 ≤ x ≤ 0,6 pelo uso do m?todo dos citratos precursores. Para se obter a fase estequiom?trica do sistema Ni1-xZnxFe2O4 foram misturados e homogeneizados os citratos precursores de ferro, n?quel e zinco. As composi??es estequiom?tricas foram calcinadas em atmosfera ambiente na temperatura de 350?C e depois prensadas em pastilhas e tor?ides. As amostras prensadas foram sinterizadas nas temperaturas de 1100?, 1150? e 1200?C em atmosfera de arg?nio. Os p?s calcinados foram caracterizados por DRX, TGA/DTG, FTIR, MEV e magnetometria de amostra vibrante (MAV) e as amostras sinterizadas por DRX, MEV, MAV, massa espec?fica e medidas de permeabilidade e perdas magn?ticas. Observou-se a forma??o de fase pura ferrimagn?tica em todas as temperaturas aplicadas. A an?lise pelo m?todo de Rietveld calculou o n?vel de ocupa??o dos c?tions e o tamanho de cristalito. Foram obtidos tamanhos de cristais nanom?tricos, de 12 a 20 nm para os p?s calcinados. Por MEV, as amostras sinterizadas apresentam tamanhos de gr?os na faixa de 1 a 10 μm. A massa espec?fica (ρ) do material sinterizado apresenta uma tend?ncia de diminui??o com a adi??o de Zn. Os melhores resultados de magnetiza??o foram obtidos para x=0,6 nas tr?s temperaturas de sinteriza??o, variando de 105 a 110 emu/g. As histereses mostram um perfil de materiais magn?ticos moles. Dois processos de magnetiza??o foram considerados, o superparamagnetismo a baixa temperatura (350?C) e a forma??o de dom?nios magn?ticos em altas temperaturas. Os materiais sinterizados apresentam permeabilidade (μ) de algumas unidades, de 7 a 30, e perdas magn?ticas (tanδ) por volta de 1. A resposta em freq??ncia dos n?cleos toroidais est? na faixa de 0,3 kHz a 0,2 GHz. Os maiores valores de μ e tanδ s?o para x=0,5 e a maior faixa de resposta em freq??ncia ? para x=0,6. V?rios fatores da microestrutura contribuem para o comportamento das grandezas μ e tanδ, tais como: os tamanhos dos gr?os, porosidade inter e intragranular, quantidade de contornos de gr?os e os aspectos da din?mica das paredes de dom?nios quando excitadas magneticamente sob alta freq??ncia Ferrita Ferrita espin?lio Fase ferrimagn?tica Citratos precursores Ferrite Ferrites spinel Phase ferromagnetic Citrate precursor
270	Study of the evolution of symbiosis at the metabolic level using models from game theory and economics / L’étude de l’évolution de la symbiose au niveau métabolique en utilisant des modèles de la théorie des jeux et de l’économie Wannagat, Martin 04 July 2016 (has links) Le terme symbiose recouvre tous types d'interactions entre espèces et peut être défini comme une association étroite d'espèces différentes vivant ensemble. De telles interactions impliquant des micro-organismes présentent un intérêt particulier pour l'agriculture, la santé, et les questions environnementales. Tous les types d'interactions entre espèces tels que le mutualisme, le commensalisme, et la compétition, sont omniprésents dans la nature et impliquent souvent le métabolisme. La libération de métabolites par des organismes dans l'environnement permet à d'autres individus de la même espèce ou de différentes espèces de les récupérer pour leur usage propre. Dans cette thèse, nous étudions comment les interactions entre espèces façonnentl'environnement. Nous examinons les questions de (i) quels sont les besoins minimaux en éléments nutritifs pour établir la croissance, et (ii) quels métabolites peuvent être échangés entre un organisme et son environnement. L'énumération de tous les ensembles minimaux stoechiométriques de précurseurs et de tous les ensembles minimaux de métabolites échangés,en utilisant des modèles complets de réseaux métaboliques, fournit un meilleur aperçu des interactions entre les espèces. Dans un environnement spatialement homogène, les métabolites qui sont libérés dans un tel environnement sont partagés par tous les individus. Le problème qui se pose alors est de savoir comment les tricheurs, les individus qui profitent des métabolites libérés sans contribuer au bien public, peuvent être exclus de la population. Ceci et d'autres configurations ont déjà été modélisées avec des approches de la théorie des jeux et de l'économie. Nous examinons comment les concepts d'ensembles minimaux de précurseurs stoechiométriques et d'ensembles minimaux de composés échangés peuvent être introduits dans ces modèles / Symbiosis, a term that brings all types of species interaction under one banner, is defined as a close association of different species living together. Species interactions that comprise microorganisms are of particular interest for agriculture, health, and environmental issues. All kinds of species interactions such as mutualism, commensalism, and competition, are omnipresent in nature and occur often at the metabolic level. Organisms release metabolites to the environment which are then taken up by other individuals of the same or of different species. In this thesis, we study how species interactions shape the environment. We examine the questions of (i) what are the minimal nutrient requirements to sustain growth, and (ii) which metabolites can be exchanged between an organism and its environment. Enumerating all minimal stoichiometric precursor sets, and all minimal sets of exchanged metabolites, using metabolic network models, provide a better insight into species interactions. In a spatially homogeneous environment, the metabolites that are released to such an environment are shared by all individuals. The problem that then arises is how cheaters, individuals that profit from the released metabolites without contributing to the public good, can be prevented from the population. This and other configurations were already modeled with approaches from game theory and economics. We examine how the concepts of minimal stoichiometric precursor sets and minimal sets of exchanged compounds can be introduced into such models Symbiose Métabolisme Modélisation des réseaux métaboliques Énumération Ensembles minimaux de précurseurs Théorie des jeux Économie Symbiosis Metabolism Metabolic network modeling Enumeration Minimal stoichiometric precursor sets Game theory Economics 570.15

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