Global ETD Search

91	GH70 dextransucases : Insights on the molecular determinants of dextran molar mass control / Dextransucrases de la famille GH70 : investigations sur les déterminants moléculaires du contrôle de la masse molaire des dextranes produits Claverie, Marion 20 December 2017 (has links) Les glucane-saccharases (GS) de la famille GH70 sont des enzymes produites par certaines bactéries lactiques. A partir de saccharose, substrat renouvelable et peu coûteux, elles sont capables de catalyser la synthèse d’α-glucanes, homopolysaccharides dont les propriétés diffèrent suivant la spécificité de l’enzyme (taille, type de liaisons α-osidiques, degrés de branchement). Les glucanes contenant une très grande majorité de liaisons α-(1,6), appelés dextranes, présentent de nombreuses applications industrielles qui dépendent principalement de leur taille. Cependant, la synthèse directe de dextranes de taille contrôlée (de 1 à plusieurs millions de kg/mol) avec une faible polydispersité et en utilisant une seule enzyme n’est encore pas envisageable. En effet, les mécanismes moléculaires mis en jeu pour le contrôle de la taille des polymères produits n’ont encore été que peu explorés. Dans ce contexte, deux GSs ont été sélectionnées. La première, DSR-M synthétise uniquement des dextranes de faible masse molaire (MM) (28 kg/mol) exclusivement composés de liaisons α-(1,6). A contrario, le second modèle, DSR-OK produit le plus long dextrane décrit à ce jour (>109 g/mol). La caractérisation biochimique et structurale ainsi que la construction de mutants ont permis l’exploration du mode d’action de ces deux candidats. Plusieurs structures 3D de DSR-M2 (forme tronquée de DSR-M) - sans ou en complexe avec son substrat ou ses produits (isomaltotetraose) - ont été résolues. C’est la première fois que de tels complexes sont décrits et l’une de ces structures présente le domaine V le plus complet décrit à ce jour. L’analyse de ces structures couplée au suivi cinétique de la synthèse du polymère ont montré que la spécificité de DSR-M pour la synthèse de dextranes courts s’explique par un mode d’élongation distributif dû à la faible affinité de deux poches à sucre de son domaine V envers la chaîne en cours de synthèse. Des analyses RMN (15N1H – HSQC) – jamais réalisées auparavant sur une protéine si grosse – ont également étayé l’importance de la présence de résidus aromatiques dans le domaine catalytique pour la synthèse de dextranes supérieurs à 2 kg/mol. En comparaison, la synthèse de dextranes de haute MM par DSR-OK est principalement due au plus grand nombre de poches à sucre de son domaine V, permettant d’assurer une meilleure interaction avec la chaîne en cours d’élongation. L’implication de ces poches dans la détermination de la taille du dextrane a été montrée pour les deux candidats. Leur fonctionnalité est fortement liée à la présence d’un résidu aromatique de stacking, et leur répartition le long du domaine V a aussi une influence. L’ensemble de ces résultats démontre la coopération du domaine V avec le domaine catalytique pour l’élongation des dextranes, tout en offrant de nouvelles perspectives pour approfondir la compréhension de ce mécanisme. Ils offrent également des stratégies prometteuses pour l’ingénierie d’enzyme de la famille des GH70 pour la modulation de la taille des glucanes. / Glucansucrases (GS) from glycoside hydrolase family 70 (GH70) are -transglucosylases produced by lactic acid bacteria. From sucrose, an economical and abundant agro resource, they catalyze the polymerization of glucosyl residues. Depending on the enzyme specificity, α-glucans vary in terms of size, types of glucosidic bonds and degree of branching and have found multiple industrial applications mainly related to their molar mass (MM). However synthesizing polymers of controlled size with average MM ranging from 1 kg/mol to several millions g/mol and low polydispersity using one single enzyme remains challenging. Indeed, the molecular mechanisms underpinning the control of polymer size have been scarcely explored. To tackle this question, two GSs producing dextran (glucan composed of a majority of α-(1,6) linkages) were selected, and their mode of action explored via biochemical and structural analyses coupled to mutagenesis. The first enzyme selected, called DSR-M synthesizes only low molar mass (LMM) dextran (28 kg/mol) exclusively composed of -(1→6) linkages without any trace of HMM dextran (105 to 108 g/mol). In contrast, DSR-OK (second model), produces the highest MM dextran (>109 g/mol) described to date. Several 3D crystallographic structures of a truncated form of DSR-M (DSR-M2), either free or in complex with its substrate or product (isomaltotetraose) in the domain V or in the active site were solved. Such complexes were never obtained before. Noteworthy, one structure encompassed the most complete domain V reported to date. Analyses of these structures coupled to dextran synthesis monitoring, showed that the LMM dextran specificity of DSR-M2 is explained by a distributive elongation mode due to the weak affinity of its two sugar binding pockets in the domain V which interact with the growing dextran chains and allow the synthesis of dextran longer than 16 kg/mol. 15N1H NMR analyses (HSQC), for the first time performed with such a big protein, further revealed the crucial role of aromatic residues in the catalytic domain for the production of dextran from 2 to 16 kg/mol. In comparison, synthesis of HMM dextran by DSR-OK was shown to be mainly due to the sugar binding pockets of its domain V, ensuring much stronger interactions with growing dextran chains. The role of these pockets was evidenced for both enzymes, their functionality proposed to be linked to the presence of one aromatic stacking residue. Their positioning along domain V relatively to the active site is also important to promote efficient binding. All these findings highlight the cooperation between domain V and the catalytic domain for dextran elongation, offer new perspectives to acquire a deeper knowledge on this interplay and open promising strategies for GH70 enzyme engineering aiming at modulating glucan size. Glucane-saccharase Dextrane-saccharase GH70 Transglucosylase Dextrane Domaine de liaison au glucane Processivité Distributivité Glucansucrase Transglucosylase GH70 Dextransucrase Dextran Glucan binding domain Processivity Distributivity 572 630
92	Eferências do núcleo lateral superior da oliva no rato (rattus norvegicus). / Efferences of lateral superior olive nucleus in the rat ( rattus norvegicus) Souto, Suzana Souza 22 October 2007 (has links) Após a descrição da Urocortina 1, um neuropeptídeo encontrado principalmente no núcleo de Edinger-Westphal e no núcleo lateral superior da oliva (LSO), atentou-se para a ausência do conhecimento das projeções de ambos os núcleos. Nós pretendemos contribuir para o conhecimento das projeções ascendentes e descendentes do LSO, usando um traçador neuronal anterógrado. Nós utilizamos o Biotin-Dextran-Amine (BDA) injetado no LSO de ratos, 15 a 20 dias depois os ratos eram perfundidos, os encéfalos e medulas foram seccionados e tratados histoquimicamente. Nós encontramos que existem 4 vias eferentes do LSO, tanto ascendentes como descendentes no sistema nervoso central, como segue: duas vias ascendentes, uma ipsilateral à injeção, a mais proeminente e a via contralateral que é menos densa; duas vias descendentes, uma ipsilateral muito menos evidente, e a contralateral que é moderada. Seguindo a via ascendente ipsilateral, nós encontramos as seguintes estruturas bem marcadas com BDA: o próprio LSO, núcleo do corpo trapezóide, o lemnisco lateral e seus núcleos, colículos inferior e superior e os seguintes núcleos talâmicos: suprageniculado, geniculado medial, partes dorsal e medial e córtex somatosensorial primário. Seguindo a via descendente contralateral nós encontramos as seguintes estruturas: o LSO ipsi e contralateral, o núcleo do corpo trapezóide, núcleo coclear ventral, parte anterior, núcleo coclear dorsal, núcleo coclear ventral, parte posterior e VIII nervo. Os dados que nós encontramos neste trabalho sugerem que as vis do LSO podem se estender até o córtex somatosensorial no prosencéfalo e o complexo de núcleos cocleares no tronco, enviando colaterais para os principais núcleos relacionados a via auditiva, provavelmente contribuindo para a localização da fonte sonora, em acordo com a anatomia desta informação sensorial específica. / After the discovery of the Urocortin-1, a neuropeptide found mainly in the Edinger-Westphal nucleus and in the lateral superior olive nucleus (LSO), the attention was caught about the lack of known projections of both nuclei. We intended to contribute to the knowledge of both ascending and descending projections of the LSO, using a neuronal anterograde tracer. In order to do that we use the Biotin-Dextran-Amine (BDA) injected in the LSO of rats, fifteen to twenty days later the rats were perfused, the brains and spinal cords were cut and the sections treated histochemically. We have found that there are four pathways leaving the LSO either ascending or descending in the central nervous system, as following: two ascending pathways, one ipsilateral to the injection, the most proeminent one and the contralateral pathway that is less dense; two descending pathways, one ipsilateral, much less evident, and the contralateral that is very moderate. Tracking the ipsilateral ascending pathway we have found the following structures well labeled with BDA: the LSO itself, nucleus of the trapezoid body, the lateral lemniscus and its nuclei, inferior and superior colliculus, the following thalamic nuclei: suprageniculate, medial geniculate, dorsal and medial parts and the primary somatosensory cortex. Tracking the contralateral descending pathway we have found the following structures: the LSO ipsi and contralateral; the nucleus of the trapezoid body; ventral cochlear nucleus, anterior part; dorsal cochlear nucleus; ventral cochlear nucleus, posterior part and, the eight nerve. The data we have found in this work suggests that the pathways from the LSO could reach as far as the somatosensory cortex in the prosencephalon and the cochlear complex nuclei in the brainstem, sending collaterals to the main nuclei related to the auditory pathway, probably contributing to the localization of the sound source, due to the anatomy of this specific sensory information. Anterograde tracer Auditory pathway BDA Biotin-dextran Eferências Efferences Lateral superior olive nucleus Núcleo lateral superior da oliva Traçador anterógrado Urocortin 1 Urocortina I Via auditiva
93	Estudo das projeções hipotalâmicas para a região urocortinérgica do complexo oculomotor. / Study of the hypothalamic projections to the urocortinergic cells in the oculomotor complex. Silva, André Valerio da 17 August 2010 (has links) O neuropeptídeo urocortina 1 (UCN 1) tem entre os seus principais locais de expressão o núcleo de Edinger-Westphal (EW) e o núcleo lateral superior da oliva. Após sua descoberta, sugeriu-se que o EW e o núcleo paraventricular do hipotálamo (PVH) possuíssem papéis complementares e opostos na resposta ao estresse, porém, não existem trabalhos que relacionam anatomicamente núcleos hipotalâmicos e o EW. A fim de contribuir para esta área foi proposto o mapeamento das aferências hipotalâmicas do EW, através da injeção de Fluoro-Gold neste núcleo e posterior mapeamento de suas aferências. Os resultados encontrados foram: PVH, área hipotalâmica lateral (LHA) e o núcleo posterior do hipotálamo (PH) e outras regiões do sistema nervoso central. Para controle, o traçador anterógrado Amina Dextrana Biotinilada, foi injetado nos núcleos/áreas hipotalâmicas PVH, LHA e PH sendo encontradas fibras próximas as células urocortinérgicas do EW. Nossos dados mostram um possível envolvimento das células UCN 1 do EW com o controle de funções autonômicas e neuroendócrinas. / The neuropeptide urocortin 1 (UCN 1) has its main sites of expression at the Edinger-Westphal nucleus (EW) and the lateral superior olivary nucleus. After its discovery has suggested that EW and paraventricular nucleus of hypothalamus (PVH) have complementary and opposing roles in the stress response. However, there are no works relating anatomically the hypothalamic nuclei and EW. To contribute to this area we proposed mapping the hypothalamic afferents of the EW. We have used the Fluoro-Gold injected in the EW as a result of we have found retrogradely labeled cells in the following nuclei: PVH, lateral hypothalamic area (LHA), posterior hypothalamic nucleus (PH) and other regions of the central nervous system. For control, the anterograde tracer biotinylated dextran amine was injected into the nuclei/areas hypothalamic PVH, LHA, and PH we have found anterogradely labeled fibers in a very close apposition over urocortinergic cells at EW. Based on these data we are suggesting a involvement of cells with UCN 1 EW control of autonomic and neuroendocrine functions. Fluoro-gold Fluoro-gold Amina-Dextrana-Biotinilada Dextran-Amine-Biotin Edinger-Westphal nucleus Estereotaxia Hipotálamo (Estudo) Hypothalamus (Study) Núcleo de Edinger-Westphal Stereotaxic Urocortin-1 Urocortina-1
94	Participação do eixo hipotálamo-pituitária-adrenal na Doença Inflamatória Intestinal induzida experimentalmente / Participation of the hypothalamic-pituitary-adrenal axis in experimentally induced inflammatory bowel disease Souza, Patrícia Reis de 06 August 2015 (has links) As doenças inflamatórias intestinais (DII) são causadas por desequilíbrio entre as respostas imunes efetoras e reguladoras na mucosa intestinal e podem ser moduladas pelo eixo hipotálamo-hipófise-adrenal (HPA) por meio de interações neuroimunoendócrinas e secreção de cortisol. Embora os glicocorticóides (GC) sejam utilizados para tratar a DII, o cortisol produzido pelas glândulas supra-renais também está envolvido na resposta ao estresse, que pode levar a doenças inflamatórias descontroladas. Portanto, o objetivo deste trabalho é avaliar a participação do eixo HPA na modulação da resposta imune de mucosa intestinal. Para tal, camundongos C57BL/6 foram submetidos à remoção das glândulas adrenais seguida por indução de colite pela administração de água contendo 3% de dextran sulfato de sódio (DSS). Os resultados demonstraram que a ausência das adrenais levou à maior suscetibilidade à doença e mortalidade precoce, fenômeno que não foi prevenido pela reposição de GC. Os animais adrenalectomizados com colite apresentaram níveis significativamente menores de LPS, concomitantemente ao aumento de IL-6 no soro quando comparados aos camundongos não adrenalectomizados. Além disso, os animais adrenalectomizados apresentaram menor celularidade na lâmina própria (LP), menos áreas de erosão e menor escore histopatológico associado ao aumento de IFN-? e FasL, no intestino, sem produção local compensatória de corticosterona. Houve aumento na atividade das enzimas mieloperoxidase (MPO), N- acetilglicosaminidase (NAG) e eosinófilo-peroxidase (EPO) no intestino dos animais expostos ao DSS quando comparados ao grupo de camundongos controles saudáveis, independentemente da presença do eixo HPA intacto e o tratamento com GC nos animais adrenalectomizados levou à redução significativa da atividade de MPO. Também foi observado na LP dos camundongos adrenalectomizados aumento significativo na frequência de células dendríticas tolerogênicas CD11b+CD11c+CD103+, T auxiliares (CD3+CD4+), T citolíticas (CD3+CD8+) e NKT (CD3+CD49b+), além de redução significativa da população de células dendríticas pró-inflamatórias CD11b+CD11c+CD103-, leucócitos CD11b+ e linfócitos intra-epiteliais, de maneira dependente de GC. A ausência do eixo HPA intacto levou à diminuição de leucócitos totais no baço quando comparados ao grupo com colite, relacionada principalmente à redução significativa na frequência de células NKT (CD3+CD49b+), as quais foram restauradas nos camundongos tratados com GC exógenos. Durante a exposição ao DSS houve aumento de células Th2 e Th1 no baço dos camundongos não adrenalectomizados, enquanto que a remoção das adrenais levou a notável redução na população de células T CD4 produtoras de IL-4, IL-10, IFN-? ou IL-17, com aumento de células Th17 e diminuição significativa de células Th1 no baço dos camundongos adrenalectomizados e tratados com GC. De forma interessante, houve menor acúmulo de células T reguladoras juntamente à redução na intensidade média de fluorescência (MFI) de FOXP3 em células T CD4+CD25+ do baço dos camundongos adrenalectomizados expostos ao DSS, de maneira geral dependente de GC. Por fim, esta diminuição de mecanismos reguladores foi acompanhada de menor índice de proliferação e aumento de IL-10 no sobrenadante de cultura de esplenócitos de camundongos com o eixo HPA não ii funcional, indicando que a ausência de GC endógenos pode alterar significativamente a homeostase do sistema imunológico. Juntos, nossos resultados demonstram que o eixo HPA é importante na modulação da resposta imunológica durante a colite induzida experimentalmente / Inflammatory bowel diseases (IBD) are caused by imbalance between regulatory and effector immune responses in the intestinal mucosa and can be modulated by the hypothalamic-pituitary-adrenal (HPA) axis via neuroimmune endocrine interactions and secretion of cortisol. Although glucocorticoids (GC) are used to treat IBD, cortisol produced by the adrenals glands is also involved in the stress response, which can lead to uncontrolled inflammatory diseases. Therefore, the aim of this study was to evaluate the HPA axis in the modulation of the immune response of intestinal mucosa. C57BL/6 mice were subjected to removal of the adrenal glands followed by induction of colitis by administration of water containing 3% dextran sulfate sodium (DSS). The results showed that the absence of adrenals led to increased susceptibility to disease and early mortality, a phenomenon that was not prevented by GC replacement. Adrenalectomized animals exposed to DSS had significantly lower levels of LPS, concomitantly to increased IL-6 in the serum when compared to non-adrenalectomized mice. In addition, adrenalectomized animals had lower cellularity in the lamina propria (LP), less erosion areas and less histopathologic score associated with increased IFN-? and FasL in the intestine, without compensatory local production of corticosterone. There was an increase in the activity of the myeloperoxidase (MPO) enzyme, N- acetilglicosaminidase (NAG) and eosinophil-peroxidase (EPO) in the intestines of DSS-exposed animals when compared to the healthy control group of mice, regardless of the presence of intact HPA axis, while treatment with GC led to significantly reduced MPO activity. It was also observed in the LP of adrenalectomized mice significant increase in the frequency of tolerogenic dendritic cells CD11b+CD11c+CD103+, helper T (CD3+ CD4+), cytolytic T (CD3+ CD8+) and NKT (CD3+ CD49b+) besides significant reduction in the population of pro-inflammatory dendritic cells CD11c+ CD11b+ CD103-, leukocyte CD11b+ and intraepithelial lymphocytes, GC-dependent manner. The absence HPA intact carried decrease in total leukocytes in spleen when compared to the group with colitis, related mainly to significant reduction in the frequency of NKT cells (CD3+CD49b+), which were restored in the GC treated mice. During exposure to DSS there was increased Th2 and Th1 cells in the spleen of non-adrenalectomized mice, while the removal of the adrenals was associated to a marked reduction in the population of CD4 T cells producing IL-4, IL-10, IFN-? or IL-17 with increased Th17 cells and significant decrease in Th1 cells in the spleen of adrenalectomized mice treated with GC. Interestingly there was less accumulation of regulatory T cells together to a reduction in mean fluorescence intensity (MFI) of FOXP3 in CD4+CD25+ T cells in the spleen of mice exposed to DSS after adrenalectomy, most dependent on GC. Finally, the decline of regulatory mechanisms was accompanied by lower rates of proliferation and increased IL-10 in the supernatant culture of splenocytes of mice with disrupted HPA axis, indicating that the absence of endogenous GC altered significantly the homeostasis of the immune system. Together, our results demonstrate that the HPA axis is important in modulating the immune response during experimentally induced colitis Adrenalectomia Adrenalectomy Camundongos Colite Doença inflamatória intestinal Eixo hipotálamo-pituitária-adrenal Glicocorticoides Glucocorticoids Hypothalamic-pituitary-adrenal Inflammatory bowel disease
95	Uso terapêutico de ultrassom abdominal diminui severidade de colite aguda induzida por DSS através da via anti-inflamatória colinérgica Nunes, Natália Schneider January 2018 (has links) Introdução: Colite Ulcerativa (UC) é uma Doença Inflamatória Intestinal (DII) caracterizada por uma resposta imune exacerbada, com sintomas como diarreia, perda de peso e sangue nas fezes. Apesar dos medicamentos disponíveis, a remissão da doença nem sempre consegue ser alcançada e há a necessidade de terapias alternativas. A colite induzida por DSS (Dextran Sulfate Sodium) é um modelo animal utilizado na investigação de novas terapias por sua semelhança à UC humana. DSS provoca dano à barreira epitelial do cólon, induzindo uma resposta imune exacerbada; entretanto, o exato mecanismo não está totalmente esclarecido. O Ultrassom Terapêutico (TUS) foi utilizado para tratamento de injúria renal em modelo experimental, sua ação se dá através da estimulação do nervo vago (VN) e consequente ativação da via antiinflamatória colinérgica (CAIP). Uma vez que pacientes com DII podem exibir atividade disfuncional do VN, TUS pode ser investigado como terapia alternativa. Objetivos: Investigar temporalmente o perfil clínico, proteômico, histológico e imunológico da colite aguda induzida por DSS; e determinar os efeitos de TUS na colite induzida por DSS. Métodos: No primeiro estudo, a severidade da colite foi avaliada pela administração de DSS 1-3%, observando a resposta clínica e histológica. A análise temporal de DSS 3% incluiu uma avaliação proteômica e histológica do cólon, e a resposta imune celular no baço, linfonodo mesentérico (MLN) e cólon. No segundo estudo, utilizando o modelo de DSS 2%, TUS foi aplicado no abdômen dos animais e foram observados os sintomas clínicos, dano histológico, proteômica do cólon e respostas imunes celulares no baço, MLN e cólon. Animais esplenectomizados ou knockout para a7nAChR (marcador clássico para ativação de CAIP) foram utilizados. Resultados: No primeiro estudo, observou-se que a severidade da doença foi aumentada seguindo concentrações de 1-3% DSS. A análise temporal de DSS 3% demonstrou que os macrófagos (F4/80+) se apresentam como a primeira resposta celular, seguidos por células T CD25+, CD4+ e CD8+. A piora clínica da doença correspondeu ao aumento progressivo de fatores pró-inflamatórios e dano tecidual no cólon, exceto no dia 8. Foram observados menores níveis dos marcadores de células T CD25+, CD4+ e CD8+ no MLN e/ou baço, sugerindo a ocorrência de tropismo destas células para o intestino. No segundo estudo, a aplicação de TUS diminuiu a severidade da doença através da melhora de sintomas clínicos, danos teciduais e encurtamento do cólon. A proteômica do cólon demonstrou uma resposta anti-inflamatória durante a fase de injúria (D0-7), induzindo uma resolução acelerada da doença na fase de recuperação (D8-14). TUS diminuiu os níveis de células T CD8+ e normalizou os níveis de células T CD25+ no cólon. Animais esplenectomizados não demonstraram melhora clínica ou histológica, enquanto animais a7nAChR KO apresentaram piora da colite experimental. Além disso, TUS aumentou os níveis de células F4/80+a7nAChR+ no intestino de animais WT DSS 2%. Conclusão: Nossos resultados demonstram que a severidade da doença depende da concentração de DSS, relacionada com as respostas clínica, proteômica e imune no modelo animal de DSS 3%; e TUS diminuiu a severidade da colite induzida por DSS presumidamente pela da estimulação do VN e consequente ativação de CAIP através do baço. / Introduction: Ulcerative Colitis (UC) is an Inflammatory Bowel Disease (IBD) characterized by uncontrolled immune response, presenting with symptoms of diarrhea, weight loss and bloody stools. Despite available treatments, UC sustained remission is not achievable and there is still the need for alternative therapies. Dextran Sulfate Sodium (DSS)-induced colitis is a mouse model used to investigate novel therapies, since it closely mimics human UC. DSS damages the colonic epithelial barrier, leading to an exacerbated immune response. However, the exact mechanism is not totally understood. Previous studies showed the use of Therapeutic Ultrasound (TUS) to prevent kidney injury in mice through stimulation of the vagus nerve (VN) and activation of the cholinergic anti-inflammatory pathway (CAIP). Since IBD patients can present with dysfunctional VN activity, TUS could be studied as an alternative therapy. Objectives: To investigate the temporal clinical, proteomic, histological and cellular immune profiles of DSS-induced acute colitis; and to determine the effects of TUS directed toward the VN and spleen in the course of DSS-induced colitis. Methods: First, we analyzed DSS-induced colitis severity by administration of 1-3% DSS, observing the clinical course and histological damage. A time course analysis was performed at 3% DSS, including colon proteomics, colon histology and immune cell responses in the spleen, MLN (mesenteric lymph node) and colon. Next, utilizing 2% DSS in drinking water, we applied TUS over the mice abdomen and analyzed clinical symptoms, histological damage, colon proteomics and immune cell responses in the spleen, MLN and colon. Splenectomized and a7nAChR (key indicator of CAIP activation) KO animals were also used. Results: In the first study, we observed worsening of the disease when increasing DSS concentrations from 1 to 3%. Time course analysis of 3% DSS revealed macrophages to be the first responders, followed by CD25+, CD4+ and CD8+ T cells. Worsening of the disease corresponded to a progressive increase in pro-inflammatory colonic factors and histological damage, except at day 8. Lower levels of CD25+, CD4+ and CD8+ T cells in MLN and/or spleen suggest an immune cell tropism to the gut. In the second study, TUS attenuated DSS induced colitis through amelioration of clinical symptoms, histological damage and colon shortening. Proteomic colon analysis demonstrated an antiinflammatory profile during the injury phase (D0-7), whilst inducing an early resolution of the disease during the recovery phase (D8-14). TUS decreased CD8+ and normalized CD25+ T cell levels in the gut. Splenectomized animals demonstrated no improved clinical and pathological outcomes, and a7nAChR KO mice presented with worsening of the disease. Furthermore, there were increased levels of F4/80+a7nAChR+ cells in the colon of 2% DSS WT mice under TUS treatment. Conclusion: Our results demonstrate that the severity of colitis is dependent on DSS concentration, correlated with clinical, proteomic and cellular immune responses on 3% DSS; and TUS significantly improved DSS-induced acute colitis presumably through stimulation of the VN and consequent activation of CAIP through the spleen. Colite ulcerativa Ultrassom Nervo vago Ulcerative Colitis Alpha 7 Nicotinic Acetylcholine Receptor Vagus Nerve Cholinergic Anti-Inflammatory Pathway Inflammatory Bowel Diseases Therapeutic Ultrasound Proteomics Dextran sulfate sodium
96	INFLUÊNCIA DE DIFERENTES TEORES DE DEXTRANA E AMIDO EM AÇÚCAR CRISTAL NA FORMAÇÃO DE FLOCOS EM SOLUÇÕES ÁCIDAS CARBONATADAS E SOLUÇÕES ALCOÓLICAS Lemos, Lorena Ranucci 03 August 2012 (has links) Made available in DSpace on 2017-07-21T18:53:18Z (GMT). No. of bitstreams: 1 Lorena Lemos.pdf: 1400448 bytes, checksum: 208ef78ab99ed1032b0c3fc7832c38df (MD5) Previous issue date: 2012-08-03 / Several investigations have been performed to determine the influence of the sugarcane composition in the quality of its products, especially crystal sugar. There is interest in studies about dextran and starch to be causative agents of major problems during the processing of sugarcane and also to be related to the appearance of flakes or precipitated in alcoholic drinks and acidic carbonated beverage. The objective of the present work was to evaluate the influence of these polysaccharides in the formation of flakes in acidic carbonated and alcoholic solutions. Samples of crystal sugar (n = 21) produced in the central-southern Sao Paulo state were analyzed for quantification of dextran and starch and values between 15.39 ± 0.38 and 830.25 ± 2.58 mg/kg and between 49.11 and 299.92 ± 1.14 ± 1.05 mg/kg were found for dextran and starch, respectively. The test evaluated the formation of flake in alcoholic solution at 55 and 89 % v/v ethanol. The 55 % v/v ethanol was performed to read the absorbance of the samples and values between 0.018 ± 0.001 and 1.063 ± 0.010 NTU were found. For the 89 % v/v ethanol solution the formation of flakes in the first 15 hours of storage the test solution was observed. There was reduction of starch content in solution with the methodology used by alcoholic flake and the reduction varied between 13.78 and 34.15 %. The test evaluated the formation of acid flake following the standard methodology and modification of the method by using a 0.8 μm filter for removal of starch. The turbidity readings were lower when using the modified method. The results obtained for the solutions tested according to standard methodology ranged from 3.72 ± 0.17 to 33.46 ± 6.31 NTU and by using the modified method they were between 1.94 ± 0.08 and 10.97 ± 1.04 NTU. All tests showed that dextran and starch present in the samples of crystal sugar show a positive correlation with the results of acid flake and alcohol flake. The formation of these two types of flakes were also interdependent (has a relation). / Várias pesquisas estão sendo realizadas com o objetivo de determinar a influência da composição da cana-de-açúcar na qualidade final de seus produtos, em especial no açúcar cristal. Existe interesse em estudos sobre dextrana e amido por serem agentes causadores de sérios problemas durante o processamento da cana, estando relacionados ao aparecimento de flocos ou precipitados em bebidas ácidas carbonatadas e em bebidas alcoólicas destiladas. O objetivo desse trabalho foi avaliar a influência desses polissacarídeos na formação de flocos em soluções ácidas carbonatadas e em soluções alcoólicas. Amostras de açúcar cristal (n = 21) produzidas na região centro-sul do Estado de São Paulo foram analisadas para quantificação de dextrana e amido. Foram realizados testes para avaliação da formação de floco alcoólico em soluções hidroalcoólicas a 55 e a 89 % v/v etanol e teste para avaliação da formação de floco ácido seguindo método padrão e método com modificação através da utilização de filtro 0,8 μm para retirada do amido. Foram encontrados teores de dextrana entre 15,39 ± 0,38 e 830,25 ± 2,58 mg/kg e teores de amido entre 49,11 ± 1,14 e 299,92 ± 1,05 mg/kg nas amostras de açúcar cristal analisadas. A 55% v/v de etanol foi realizada a leitura de absorbância das amostras segundo teste de floco alcoólico, sendo encontrados valores de turbidez entre 0,018 ± 0,001 e 1,063 ± 0,010 NTU. A 89 % v/v de etanol, foi observada a formação de flocos nas primeiras 15 horas de estocagem da solução teste. Ocorreu redução do amido presente na solução com o método de floco alcoólico utilizado e as reduções variaram entre 13,78 e 34,15%. Foram verificadas reduções das leituras de turbidez com a utilização do método modificado de floco ácido. Os resultados obtidos para as soluções testadas, de acordo com o método padrão, variaram de 3,72 ± 0,17 a 33,46 ± 6,31 NTU e com a utilização do método modificado, ficaram entre 1,94 ± 0,08 e 10,97 ± 1,04 NTU. Todos os ensaios realizados demonstraram que o amido e a dextrana presentes nas amostras de açúcar cristal apresentam relação positiva com os resultados de floco ácido e floco alcoólico. A formação desses dois tipos de flocos se mostrou diretamente relacionada (apresenta relação positiva). cana-de-açúcar amido dextrana floco ácido floco alcoólico sugarcane starch dextran acid flake alcoholic flake
97	Estudo das projeções hipotalâmicas para a região urocortinérgica do complexo oculomotor. / Study of the hypothalamic projections to the urocortinergic cells in the oculomotor complex. André Valerio da Silva 17 August 2010 (has links) O neuropeptídeo urocortina 1 (UCN 1) tem entre os seus principais locais de expressão o núcleo de Edinger-Westphal (EW) e o núcleo lateral superior da oliva. Após sua descoberta, sugeriu-se que o EW e o núcleo paraventricular do hipotálamo (PVH) possuíssem papéis complementares e opostos na resposta ao estresse, porém, não existem trabalhos que relacionam anatomicamente núcleos hipotalâmicos e o EW. A fim de contribuir para esta área foi proposto o mapeamento das aferências hipotalâmicas do EW, através da injeção de Fluoro-Gold neste núcleo e posterior mapeamento de suas aferências. Os resultados encontrados foram: PVH, área hipotalâmica lateral (LHA) e o núcleo posterior do hipotálamo (PH) e outras regiões do sistema nervoso central. Para controle, o traçador anterógrado Amina Dextrana Biotinilada, foi injetado nos núcleos/áreas hipotalâmicas PVH, LHA e PH sendo encontradas fibras próximas as células urocortinérgicas do EW. Nossos dados mostram um possível envolvimento das células UCN 1 do EW com o controle de funções autonômicas e neuroendócrinas. / The neuropeptide urocortin 1 (UCN 1) has its main sites of expression at the Edinger-Westphal nucleus (EW) and the lateral superior olivary nucleus. After its discovery has suggested that EW and paraventricular nucleus of hypothalamus (PVH) have complementary and opposing roles in the stress response. However, there are no works relating anatomically the hypothalamic nuclei and EW. To contribute to this area we proposed mapping the hypothalamic afferents of the EW. We have used the Fluoro-Gold injected in the EW as a result of we have found retrogradely labeled cells in the following nuclei: PVH, lateral hypothalamic area (LHA), posterior hypothalamic nucleus (PH) and other regions of the central nervous system. For control, the anterograde tracer biotinylated dextran amine was injected into the nuclei/areas hypothalamic PVH, LHA, and PH we have found anterogradely labeled fibers in a very close apposition over urocortinergic cells at EW. Based on these data we are suggesting a involvement of cells with UCN 1 EW control of autonomic and neuroendocrine functions. Fluoro-gold Amina-Dextrana-Biotinilada Estereotaxia Hipotálamo (Estudo) Núcleo de Edinger-Westphal Urocortina-1 Fluoro-gold Dextran-Amine-Biotin Edinger-Westphal nucleus Hypothalamus (Study) Stereotaxic Urocortin-1
98	Polyelectrolyte adsorption on oppositely charged surfaces - Conformation and adsorption kinetics Enarsson, Lars-Erik January 2006 (has links) <p>Denna avhandling presenterar experimentella studier av polyelektrolytadsorption på motsatt laddade ytor, där substrat av både kiseloxid och blekt barrsulfatmassa har använts. Ett huvudsakligt syfte med denna forskning var att karaktärisera konformationen hos adsorberade skikt av katjonisk polyakrylamid (CPAM) i jämförelse med katjonisk dextran (Cdextran) och relatera denna information till inbindningskapaciteten av kolloidal kiselsyra. Ett andra syfte i denna avhandling var att studera kinetiken för sekventiell adsorption av polyamidamin epiklorhydrin (PAE) och karboxymetyl cellulosa (CMC) på massafibrer och att bestämma adsorptionsisotermer för deponering av polyelektrolyter skikt för skikt på massafibrer.</p><p>Adsorptionen av CPAM på kiseloxidytor studeras med stagnationspunkts-reflektometri och kvartskristalls-mikrogravimetri för att bestämma adsorptionskinetiken och mättnadsadsorptionens beroende av polyelektrolytens laddningstäthet, pH och NaCl koncentration. Konformationen hos adsorberade skikt av CPAM och Cdextran bestämdes både före och efter sekundär tillsats av kolloidal kiselsyra (CS) och adsorptionen av CS kvantifierades också som funktion av yttäckningen av polyelektrolyt.</p><p>Resultaten indikerar att laddningstätheten hos CPAM kontrollerar den adsorberade mängden på kiseloxidytor vid låga NaCl koncentrationer. Både adsorptionen av CPAM och Cdextran på kiseloxid visades vara effektiv i NaCl koncentrationer upp till 1 M, vilket indikerar ett signifikant bidrag av icke-jonisk interaktion mellan polyelektrolyterna och kiseloxid. Adsorptionen av CS var högre på föradsorberad CPAM än Cdextran. Konformationen hos de adsorberade skikten efter tillsats av CS sågs expandera signifikant för skikt baserade på CPAM medan skikt av Cdextran vid låga salthalter verkade återta sin konformation efter en temporär expansion.</p><p>I den andra delen av avhandlingen studerades sekventiell adsorption av PAE och CMC på massafibrer. Adsorptionsisotermer skikt för skikt på avkryllad massa visade att PAE adsorberade i större mängd än CMC, både i hänseende av massa och laddning. Adsorptionen av PAE var signifikant långsammare än CMC och adsorptionstiden till 90% av mättnadsadsorptionen bestämdes till 3 respektive 1 minut. Zetapotentialen för kryll bestämdes för adsorption av de två första polyelektrolytskikten och resultaten tydde på att kryllmaterialet omladdade inom en minut efter tillsatserna av polyelektrolyt. Reflektometriförsök inom sekventiell adsorption av PAE och CMC på kiseloxid antydde att den låga molekylviktsfraktionen av PAE störde uppbyggnaden av polyelektrolyt-multiskikten.</p> / <p>This thesis presents experimental studies of polyelectrolyte adsorption on oppositely charged surfaces, where substrates of both silica and bleached softwood kraft pulp were used. A major aim of this research was to characterise the conformation of adsorbed layers of cationic polyacrylamide (CPAM), in comparison to cationic dextran (Cdextran), and relate this information to the binding capacity of colloidal silica. A second aim in this thesis was to study the kinetics of the sequential adsorption of polyamide epichlorohydrine (PAE) and carboxymethyl cellulose (CMC) on pulp fibres, and to determine the adsorption isotherms for the layer-by-layer deposition of polyelectrolytes on pulp fibres.</p><p>The adsorption of CPAM on silica surfaces was studied using stagnation point adsorption reflectometry and quartz crystal microgravimetry to determine its adsorption kinetics as well as the dependencies of polyelectrolyte charge densities, pH, and NaCl concentration on saturation adsorption. The conformation of adsorbed layers of CPAM and Cdextran, analysed in terms of amount of water and layer thickness, was determined both before and after the secondary adsorption of colloidal silica (CS), and the adsorption of CS was also quantified as a function of the surface coverage of the polyelectrolyte.</p><p>Results indicate that the charge density of CPAM controlled the amount of the polyelectrolyte adsorbed on silica surfaces at low NaCl concentrations. The adsorption of both CPAM and Cdextran on silica was shown to be effective at up to 1 M NaCl concentrations, which indicates that non-ionic interactions between the polyelectrolytes and silica contribute significantly. CS adsorption was higher on pre-adsorbed CPAM than on Cdextran. The conformation of the adsorbed layer after CS addition was seen to expand significantly in CPAM-based layers, while the Cdextran layer appeared to restore its conformation after a temporary expansion at low salt concentrations.</p><p>In the second part of the thesis, the sequential adsorption of PAE and CMC on pulp fibres was determined using the polyelectrolyte titration technique. Layer-by-layer adsorption isotherms derived on fractionated pulp showed that PAE adsorbed in higher amounts than CMC did, both in terms of adsorbed mass and adsorbed charge. The adsorption of PAE was significantly slower compared to CMC, and the adsorption times required to reach 90% of the saturation adsorption were 3 and 1 min, respectively. The zeta potential of pulp fines was determined for the adsorption of the two first polyelectrolyte layers, and data indicated that the fines recharge within one minute after the polyelectrolyte additions. Reflectometry experiments regarding the sequential adsorption of PAE and CMC on silica indicated that the low-molecular-weight fraction of PAE disturbed the formation of polyelectrolyte multilayers.</p> Polyelectrolyte adsorption adsorption kinetics adsorption isotherms conformation bridging quartz crystal microgravimetry polyelectrolyte titration cationic polyacrylamide cationic dextran colloidal silica silica surfaces pulp Chemistry Kemi
99	Microdialysis Sampling of Macro Molecules : Fluid Characteristics, Extraction Efficiency and Enhanced Performance Chu, Jiangtao January 2015 (has links) In this thesis, fluid characteristics and sampling efficiency of high molecular weight cut-off microdialysis are presented, with the aim of improving the understanding of microdialysis sampling mechanisms and its performance regarding extraction efficiency of biological fluid and biomarkers. Microdialysis is a well-established clinical sampling tool for monitoring small biomarkers such as lactate and glucose. In recent years, interest has raised in using high molecular weight cut-off microdialysis to sample macro molecules such as neuropeptides, cytokines and proteins. However, with the increase of the membrane pore size, high molecular weight cut-off microdialysis exhibits drawbacks such like unstable catheter performance, imbalanced fluid recovery, low and unstable molecule extraction efficiency, etc. But still, the fluid characteristics of high molecular weight cut-off microdialysis is rarely studied, and the clinical or in vitro molecule sampling efficiency from recent studies vary from each other and are difficult to compare. Therefore, in this thesis three aspects of high molecular weight cut-off microdialysis have been explored. The first, the fluid characteristics of large pore microdialysis has been investigated, theoretically and experimentally. The results suggest that the experimental fluid recovery is in consistency with its theoretical formula. The second, the macromolecule transport behaviour has been visualized and semi-quantified, using an in vitro test system and fluorescence imaging. The third, two in vitro tests have been done to mimic in vivo cerebrospinal fluid sampling under pressurization, using native and differently surface modified catheters. As results, individual protein/peptide extraction efficiencies were achieved, using targeted mass spectrometry analysis. In summary, a theory system of the fluid characteristics of high molecular weight cut-off microdialysis has been built and testified; Macromolecular transport of microdialysis catheter has been visualized; In vivo biomolecules sampling has been simulated by well-defined in vitro studies; Individual biomolecular extraction efficiency has been shown; Different surface modifications of microdialysis catheter have been investigated. It was found that, improved sampling performance can be achieved, in terms of balanced fluid recovery and controlled protein extraction efficiency. microdialysis high molecular weight cut-off fluid characteristics fluid recovery extraction efficiency biomarker microporous membrane macromolecule transport transmembrane large pore surface modification pluronic dextran in vitro microdialysis catheter
100	Effet protecteur des polyphénols de la verveine odorante dans un modèle d'inflammation colique chez le rat Lenoir, Loïc 11 July 2011 (has links) (PDF) La consommation de polyphénols, micronutriments largement répandus dans lesaliments d'origine végétale, a été associée à la diminution du risque de développement denombreuses pathologies telles que maladies cardiovasculaires, maladies neurodégénérativesou cancers. Cet effet des polyphénols s'explique en partie par leurs propriétés antioxydanteset anti-inflammatoires. Du fait de leur faible absorption au niveau de l'intestin grêle, lespolyphénols sont présents en grande quantité dans le côlon où ils peuvent exercer cespropriétés. L'inflammation intestinale fait interagir le système immunitaire intestinal avecde nombreux facteurs environnementaux et est fréquemment associée à une augmentationdu stress oxydant via la production d'espèces réactives de l'oxygène par les cellulesimmunitaires. De nombreuses études ont montré, sur des modèles animaux d'inflammationintestinale, les effets protecteurs de certains polyphénols. La verveine odorante (Aloysiatriphylla (L'Hérit.) Britton) est une plante médicinale connue pour ses vertus thérapeutiquesdigestives et anti-spasmodiques et couramment consommée en infusion. L'infusé deverveine odorante contient de grandes quantités de polyphénols (acides phénoliquescomplexes et dérivés de flavones) et ses propriétés antioxydantes ont été mises en évidenceaussi bien in vitro qu'in vivo.L'objectif de cette thèse a donc été d'évaluer l'effet d'une consommation préventived'un infusé de verveine odorante à dose nutritionnelle (40 g/l et 4 g/l) sur le développementd'une inflammation intestinale modérée chez le rat. Des rats Wistar ont consommé commeboisson l'infusé de verveine seul pendant deux semaines puis associé à un agentinflammatoire, le sulfate de dextran sodique (DSS), à 4% pendant 7 ou 9 jours. L'effet de laverveine a été évalué sur différents paramètres cliniques (diarrhée, saignements rectaux,poids corporel), marqueurs de l'inflammation (longueur du côlon, score histologique,activité myéloperoxydase, cytokines) et du stress oxydant (peroxydation lipidique,glutathion, défenses antioxydantes enzymatiques). Les cellules immunitaires ont étéidentifiées dans le sang ainsi que dans les structures lymphoïdes secondaires par cytométrieen flux. Enfin l'étude du métabolisme des polyphénols en situation inflammatoire ou non aété initiée par l'analyse de l'excrétion urinaire des dérivés polyphénoliques.Lors d'une inflammation de 7 jours, la consommation préventive d'infusé deverveine à 40 g/l et 4 g/l retarde l'apparition de diarrhée et de saignements rectaux, limite larétraction du côlon et la diminution de la prise de poids des rats. Malgré l'absence d'effetsur l'activité myéloperoxydase, l'infusé à 40 g/l atténue les altérations histologiques de lamuqueuse colique induites par l'inflammation. L'infusé à 4 g/l stimule l'activité de lasuperoxyde dismutase et réduit la peroxydation lipidique. Les deux infusés modulent lespopulations de cellules immunitaires dans les structures lymphoïdes secondaires (ganglionsmésentériques et plaques de Peyer), en particulier les lymphocytes B et les lymphocytes Tcytotoxiques. L'excrétion urinaire des polyphénols de la verveine est faible et n'est pasaffectée par l'inflammation. Lors d'une inflammation de 9 jours, les deux infusés limitentl'augmentation d'activité de la myéloperoxydase. Seul l'infusé à 40 g/l limite la rétractiondu côlon, stimule l'activité de la glutathion réductase et diminue les taux d'IL-6 et deTNF-α. Ainsi, nous avons montré qu'une consommation préventive d'un infusé de verveineodorante offre des effets protecteurs lors de l'inflammation intestinale en agissant àdifférents niveaux. L'exploration des voies de signalisation impliquées pourrait permettre demieux comprendre les effets protecteurs de cette boisson de consommation courante. Verveine odorante (Aloysia triphylla) Polyphénols Inflammation intestinale Stress oxydant Immunité Sulfate de dextran sodique Rats

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