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The interactions of interleukin-3 and granulocyte-macrophage colony-stimulating factor with human monocytes / Michael J.H. Elliott.Elliott, Michael J. H. January 1989 (has links)
Typescript (Photocopy) / Bibliography: leaves 170-198. / xx, 198 leaves, 1 leaf of col. plates : ill. ; 30 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Thesis (Ph.D.)--University of Adelaide, Dept. of Medicine, 1991
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Der Einfluss von Interleukin-3 auf die Läsionslast der experimentellen autoimmunen Enzephalomyelitis / The influence of interleukin-3 on the lesion load of EAESaß, Benjamin 07 June 2018 (has links)
No description available.
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Effets des immunoglobulines intraveineuses sur les cellules de l'immunité innée / Effects of intravenous immunoglobulin on innate immune cellsGaleotti, Caroline 12 March 2018 (has links)
Les IgIV, une préparation thérapeutique d'IgG normales, sont utilisées dans le traitement de diverses maladies auto-immunes et inflammatoires. Les mécanismes par lesquels les IgIV exercent une activité anti-inflammatoire ne sont pas complètement compris. Elles interagissent avec de nombreux composants du système immunitaire et modulent leurs fonctions. Des études récentes ont rapporté que l'hème oxygénase-1 (HO-1) joue un rôle important dans la régulation de la réponse inflammatoire dans un certain nombre de pathologies. Plusieurs agents thérapeutiques exercent des effets anti-inflammatoires grâce à l'induction de l'HO-1. Etant donné le rôle commun anti-inflammatoire de l'HO-1 et des IgIV, j'ai étudié l'implication de l'HO-1 dans les mécanismes d'action des IgIV. J'ai montré que les effets des IgIV ne sont pas associés à l'induction de l'HO-1, que ce soit dans des cellules de l'immunité innée comme les monocytes, cellules dendritiques ou macrophages, ou dans les reins et foie de souris avec une encéphalomyélite auto-immune expérimentale traitées par les IgIV. Des données récentes dans des modèles expérimentaux suggèrent que les IgIV induisent la sécrétion d’IL-4 des basophiles en augmentant l’IL-33 des cellules innées SIGN-R1+. J’ai rapporté que les IgIV induisent directement l’activation de basophiles pré-stimulés avec l’IL-3 alors que contrairement au modèle murin, l’IL-33 n’est pas indispensable. L’activation des basophiles par les IgIV est associée à l’expression augmentée de CD69 et la sécrétion d’IL-4, d’IL-6 et d’IL-8. Ces fonctions sont médiées par les fragments F(ab’)2 qui se lient à des IgE membranaires et activent la voie Syk. / Intravenous immunoglobulin (IVIG), a therapeutic normal immunoglobulin G preparation, is used in the therapy of various autoimmune and inflammatory conditions. The mechanisms by which IVIG exerts anti-inflammatory effects are not completely understood. It interacts with numerous components of the immune system including dendritic cells, macrophages, T and B cells and modulates their functions. Recent studies have reported that heme oxygenase-1 (HO-1) pathway plays an important role in the regulation of inflammatory response in several pathologies. Several therapeutic agents exert anti-inflammatory effects via induction of HO-1. Therefore, in view of common anti-inflammatory role exerted by both HO-1 and IVIG, I investigated if mechanisms of IVIG implicate HO-1. I show that anti-inflammatory effects of IVIG were not associated with an induction of HO-1 either in innate cells such as monocytes, dendritic cells and macrophages or in the kidneys or liver of experimental autoimmune encephalomyelitis. Recent data in experimental models suggest that IVIG induces IL-4 in basophils by enhancing IL-33 in SIGN-R1+ innate cells. I reported that IVIG directly induces activation of IL-3-primed basophils while unlike mice IL-33 was dispensable. The activation of basophils by IVIG was associated with enhanced expression of CD69 and secretion of IL-4, IL-6 and IL-8. These functions of IVIG are mediated via F(ab’)2 fragments that bind to basophil surface IgE and activate Syk pathway.
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The role of βc subunit phosphorylation in the functioning of the GM-CSF/IL-3/IL-5 receptors.Winnall, Wendy January 2008 (has links)
The cytokines GM-CSF, IL-3 and IL-5 are central regulators of haemopoietic cell functions and are pivotal in the regulation of haemopoiesis and inflammatory responses of myeloid cells. In particular, these cytokines have been shown to perform essential functions in host defence against foreign pathogens through their ability to regulate innate immune responses in myeloid cells. As key regulators of such important processes, these cytokines play an important role in human inflammatory pathologies such as rheumatoid arthritis, asthma, multiple sclerosis and psoriasis as well as a number of leukemias such as JML and CMML. GM-CSF, IL-3 and IL-5 signal through receptors containing α subunits specific to each cytokine and a common β subunit (βc). Cytokine stimulation leads to tyrosine phosphorylation of the βc and promotes specific responses such as proliferation, survival and activation of haemopoietic cells. Mouse knockout studies identified a key function of these cytokines in the activation of effector functions of myeloid cells, including production of reactive oxygen species (ROS) and phagocytosis. These earlier studies provide a link between cytokine signalling and inflammation, but the molecular mechanisms by which βc activation regulates effector cell functions, and the receptor motifs involved, are unknown. The aim of this thesis was to address two broad questions with regard to βc signalling: (1) Does βc regulate specific cellular responses by phosphotyrosine-independent mechanisms? (2) What are the molecular mechanisms by which βc initiates signalling to promote specific biological responses such as activation of effector cell functions? To address the first question, we have focussed on Serine 585, a potential 14-3-3 binding site which lies in the cytoplasmic potion of huβc. Out results show that the mutation huβc S585G disrupted the interaction of 14-3-3ζ with βc, whilst not affecting receptor tyrosine phosphorylation. Both mouse and human βc were shown to interact with 14-3-3 proteins, indicating that this interaction is conserved between these species. Significantly, a huβc S585G mutant was unable to promote haemopoietic cell survival in response to IL-3. These results identify a new mechanism by which cytokine receptors are able to couple to downstream signalling pathways that regulate cell survival. An approach was developed and optimised to analyse specific GM-CSF-mediated responses in monocytes/macrophages expressing wildtype or mutant huβc, (including huβc S585G that was defective in regulating survival). Bone marrow-derived muβc -/-;muβIL-3 -/- monocytes/macrophages were retrovirally transduced with constructs expressing wildtype or mutant huβc, along with huGMRα, then purified by FACS. Two assays were established to measure effector functions in the transduced monocyte/macrophages; (1) a flow cytometry assay for ROS production, and (2) an assay for phagocytosis. The capacity for GM-CSF to prime (i.e. enhance effector functions) ROS production and phagocytosis was investigated in huGMRα-transduced monocytes/macrophages. Our results have identified two key residues in the cytoplasmic domain of βc subunit: Tyrosine 577 (required for huβc interaction with the adaptor protein Shc) and serine 585 (required for 14-3-3 association), that are essential for the ability of GM-CSF to regulate key effector functions in monocytes/macrophages. These novel findings are significant in that they establish a molecular link between the GM-CSF/IL-3/IL-5 receptor and the regulation of both haemopoietic cell survival and inflammatory responses, and therefore have important implications in our understanding of inflammatory diseases such as rheumatoid arthritis and asthma. / http://proxy.library.adelaide.edu.au/login?url= http://library.adelaide.edu.au/cgi-bin/Pwebrecon.cgi?BBID=1317007 / Thesis (Ph.D.) -- University of Adelaide, School of Medicine, 2008
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Efeito do tratamento com IL-3, IL-7 OU IL-9 em camundongos experimentalmente infectados com Trypanosoma cruziAlves, Rosiane Nascimento 17 September 2015 (has links)
Fundação de Amparo a Pesquisa do Estado de Minas Gerais / Chagas disease, caused by the protozoan Trypanosoma cruzi, is ranked as the most serious parasitic disease in Latin America and has become a worldwide problem. A bulk of studies substantiates that Th1-associated cytokines are essential elements in early resistance against the parasite and are associated with the development of the chronic cardiac form. Although cytokines have a key role in the immune response against T. cruzi, little is known about IL-3, IL-7 and IL-9 in this context. Then the aim of this study was to analyze the role of IL-3, IL-7 and IL-9 in the acute phase of T. cruzi experimental infection. For this purpose, parameters indicative of improvement in clinical status of the animals both infected and treated as just treated were studied, such as: morbidity, mortality and histopathology. The amount of cardiac mast cells and the serum cytokines profile were also evaluated. Our data revealed that the treatment with IL-3, IL-7 or IL-9 did not alter the clinical parameters analyzed or the amount of cardiac mast cells in mice infected with T. cruzi. However the treatment with IL-3 decreased the cardiac T. cruzi-induced inflammation and the treatment with IL-7 increased serum levels of IL-5 in infected animals. In addition, the treatment with IL-9 increased the serum levels of Th1 cytokine profile (IL-2, IFN-y and TNF-α) and decreased cardiac fibrosis in infected animals, suggesting a possible protective role of this cytokine in this context. Taken together, our results underline the importance of these cytokines in modulation of T. cruzi infection. Since studies involving IL-3, IL-7 and IL-9 activity during Chagas disease are critical in
understanding the parasite control process and the protective and/or harmful action of these cytokines in the host. In addition, understanding of the immunological mechanisms mediated by these cytokines that are involved in disease development may contribute to the establishment of new therapeutic interventions to prevent Chagas disease and treat their symptomatic forms. / A Doença de Chagas, causada pelo protozoário Trypanosoma cruzi, é classificada como a doença parasitária mais grave da América Latina e tornou-se um problema mundial. A maior parte dos estudos confirma que as citocinas de perfil Th1 são elementos essenciais na resistência precoce contra o parasita e estão associadas ao desenvolvimento da forma cardíaca crônica. Embora as citocinas tenham um papel chave na resposta imune contra T. cruzi, pouco se sabe a respeito da função de IL-3, IL-7 e IL-9 neste contexto. Assim, o objetivo deste estudo foi analisar o papel destas citocinas na fase aguda da infecção experimental com T. cruzi. Para isto, parâmetros indicativos de melhora clínica dos animais tanto infectados e tratados como apenas tratados foram estudados, tais como: morbidade, mortalidade e histopatologia. A quantidade de mastócitos cardíacos e o perfil de citocinas séricas também foram avaliados. Os dados revelaram que o tratamento com IL-3, IL-7 ou IL-9 não alterou os parâmetros clínicos analisados nem a quantidade de mastócitos cardíacos nos camundongos infectados com T. cruzi. No entanto, o tratamento com IL-3 diminuiu a inflamação cardíaca T. cruzi-induzida e o tratamento com IL-7 aumentou os níveis séricos de IL-5 nos animais infectados. Além disso, o tratamento com IL-9 aumentou os níveis séricos das citocinas de perfil Th1 (IL-2, IFN-y e TNF-α) e diminuiu a fibrose cardíaca nos animais infectados, sugerindo um possível papel protetor desta citocina neste contexto. Em suma, os nossos resultados demonstram a importância destas citocinas na modulação da infecção
por T. cruzi. Já que estudos envolvendo a atividade de IL-3, IL-7 e IL-9 durante a doença de Chagas são fundamentais na compreensão sobre o processo de controle parasitário e da ação protetora e/ou prejudicial dessas citocinas no hospedeiro. Além disso, o entendimento dos mecanismos imunológicos mediados por estas citocinas que estão envolvidos no desenvolvimento da doença pode contribuir para o estabelecimento de novas intervenções terapêuticas a fim de prevenir a doença de Chagas e tratar suas formas sintomáticas / Doutor em Imunologia e Parasitologia Aplicadas
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Papel da atividade física regular realizada durante vários anos na função imune do idoso / Role of regular practice of physical activity over several years on immune function in the elderlyArai, Milton Hideaki 12 November 2004 (has links)
A proposta principal deste estudo foi de avaliar o efeito da prática regular de atividade física por longos anos na imunossenescência, isto é, nas alterações que o sistema imune sofre com o envelhecimento. Para tal, comparou-se os resultados dos exames imunológicos de 20 idosos praticantes de corrida (idade média = 67 anos) aos de 20 idosos sedentários (idade média = 66 anos) e 10 jovens sedentários (idade média = 26 anos). Os idosos corredores eram praticantes da modalidade em média nos últimos 23 anos e vinham percorrendo uma distância semanal média de 39 quilômetros. O consumo máximo de oxigênio (VO2 max) deles foi 52% maior do que o dos idosos sedentários, atingindo valores similares aos dos jovens. Os parâmetros imunológicos analisados foram: contagem de linfócitos e seus subtipos, resposta proliferativa dos linfócitos T a mitógenos, atividade citotóxica das células natural killer e produção de citocinas (interleucinas 2, 3, 4, 6, 10 e 12). A dosagem das mesmas citocinas no soro também foi realizada, porém somente nos dois grupos de idosos. Os idosos corredores apresentaram resposta proliferativa dos linfócitos T a OKT-3 e produção de interleucina-2 significativamente maiores do que as dos idosos sedentários. Eles apresentaram também uma produção de interleucina-3 significativamente menor do que a dos seus pares sedentários. Por outro lado, não apresentaram diferença significativa destes parâmetros em relação aos jovens. Os níveis séricos das interleucinas 3, 6 e 12 dos idosos corredores foram significativamente menores do que os dos idosos sedentários. A influência da prática de atividade física regular sobre os níveis séricos do hormônio de crescimento, da testosterona e da dehidroepiandrosterona sulfato (DHEAS), que sofrem redução com o envelhecimento (\"endocrinossenescência\"), também foi estudada. Não houve diferença significativa entre os níveis séricos destes hormônios anabólicos dos idosos corredores e dos idosos sedentários. O efeito da atividade física regular sobre a beta-endorfina também foi avaliado. Os idosos corredores não apresentaram diferença significativa nos níveis séricos deste neuropeptídeo em relação aos idosos sedentários. Em virtude do possível envolvimento do sistema endócrino na imunossenescência, avaliou-se a correlação entre os hormônios anabólicos e as citocinas. Não se constatou correlação relevante entre eles, especialmente entre a DHEAS e a interleucina-6. Os resultados indicam que a prática regular de atividade física por longos anos tem o potencial de desacelerar a imunossenescência / The main objective of this study was to assess the effect of regular practice of physical activity on immunosenescence, that is, the changes that occur when the immune system is affected by aging. The results of immune tests conducted on 20 elderly runners (mean age = 67 years) were compared to those of 20 elderly sedentary individuals (mean age = 66 years) and to those of 10 young sedentary individuals (mean age = 26 years). On average, the elderly runners had practiced this activity for the last 23 years, running a mean weekly distance of 39 kilometers. Their maximum oxygen consumption (VO2 max) was 52% higher than that of sedentary elderly group, and similar to that of the group of younger individuals. The immune parameters studied were: lymphocyte and lymphocyte subtype counts, the proliferative response of T-lymphocytes to mitogens, cytotoxic activity of natural killer cells and production of cytokines (interleukins 2, 3, 4, 6, 10 and 12). The same cytokines were measured in serum, but only in the two groups of elderly people. Elderly runners presented a significantly higher proliferative response of T-lymphocytes to OKT-3 as well as interleukin-2 production than the sedentary group. The production of interleukin-3 was also significantly lower in the group of runners. On the other hand, the results of these parameters did not differ significantly from those of young subjects. Serum levels of interleukins 3, 6, and 12 were significantly lower in elderly runners than in sedentary individuals. The impact of regular physical activity on serum levels of growth hormone, testosterone, and dehydroepiandrosterone sulfate (DHEAS), which are affected by aging (\"endocrinosenescence\"), was also studied. The serum levels of these anabolic hormones did not differ significantly between the groups of elderly runners and the elderly sedentary individuals. When the impact of regular physical activity on beta-endorphin was studied, again no significant difference in the serum levels of this neuropeptide was found between the two elderly groups. Owing to the possible involvement of the endocrine system in immunosenescence, the correlation between anabolic hormones and cytokines was assessed. No relevant correlation was found, especially between DHEAS and interleukin-6. The results indicate that the regular practice of physical activity for several years may delay immunosenescence
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Papel da atividade física regular realizada durante vários anos na função imune do idoso / Role of regular practice of physical activity over several years on immune function in the elderlyMilton Hideaki Arai 12 November 2004 (has links)
A proposta principal deste estudo foi de avaliar o efeito da prática regular de atividade física por longos anos na imunossenescência, isto é, nas alterações que o sistema imune sofre com o envelhecimento. Para tal, comparou-se os resultados dos exames imunológicos de 20 idosos praticantes de corrida (idade média = 67 anos) aos de 20 idosos sedentários (idade média = 66 anos) e 10 jovens sedentários (idade média = 26 anos). Os idosos corredores eram praticantes da modalidade em média nos últimos 23 anos e vinham percorrendo uma distância semanal média de 39 quilômetros. O consumo máximo de oxigênio (VO2 max) deles foi 52% maior do que o dos idosos sedentários, atingindo valores similares aos dos jovens. Os parâmetros imunológicos analisados foram: contagem de linfócitos e seus subtipos, resposta proliferativa dos linfócitos T a mitógenos, atividade citotóxica das células natural killer e produção de citocinas (interleucinas 2, 3, 4, 6, 10 e 12). A dosagem das mesmas citocinas no soro também foi realizada, porém somente nos dois grupos de idosos. Os idosos corredores apresentaram resposta proliferativa dos linfócitos T a OKT-3 e produção de interleucina-2 significativamente maiores do que as dos idosos sedentários. Eles apresentaram também uma produção de interleucina-3 significativamente menor do que a dos seus pares sedentários. Por outro lado, não apresentaram diferença significativa destes parâmetros em relação aos jovens. Os níveis séricos das interleucinas 3, 6 e 12 dos idosos corredores foram significativamente menores do que os dos idosos sedentários. A influência da prática de atividade física regular sobre os níveis séricos do hormônio de crescimento, da testosterona e da dehidroepiandrosterona sulfato (DHEAS), que sofrem redução com o envelhecimento (\"endocrinossenescência\"), também foi estudada. Não houve diferença significativa entre os níveis séricos destes hormônios anabólicos dos idosos corredores e dos idosos sedentários. O efeito da atividade física regular sobre a beta-endorfina também foi avaliado. Os idosos corredores não apresentaram diferença significativa nos níveis séricos deste neuropeptídeo em relação aos idosos sedentários. Em virtude do possível envolvimento do sistema endócrino na imunossenescência, avaliou-se a correlação entre os hormônios anabólicos e as citocinas. Não se constatou correlação relevante entre eles, especialmente entre a DHEAS e a interleucina-6. Os resultados indicam que a prática regular de atividade física por longos anos tem o potencial de desacelerar a imunossenescência / The main objective of this study was to assess the effect of regular practice of physical activity on immunosenescence, that is, the changes that occur when the immune system is affected by aging. The results of immune tests conducted on 20 elderly runners (mean age = 67 years) were compared to those of 20 elderly sedentary individuals (mean age = 66 years) and to those of 10 young sedentary individuals (mean age = 26 years). On average, the elderly runners had practiced this activity for the last 23 years, running a mean weekly distance of 39 kilometers. Their maximum oxygen consumption (VO2 max) was 52% higher than that of sedentary elderly group, and similar to that of the group of younger individuals. The immune parameters studied were: lymphocyte and lymphocyte subtype counts, the proliferative response of T-lymphocytes to mitogens, cytotoxic activity of natural killer cells and production of cytokines (interleukins 2, 3, 4, 6, 10 and 12). The same cytokines were measured in serum, but only in the two groups of elderly people. Elderly runners presented a significantly higher proliferative response of T-lymphocytes to OKT-3 as well as interleukin-2 production than the sedentary group. The production of interleukin-3 was also significantly lower in the group of runners. On the other hand, the results of these parameters did not differ significantly from those of young subjects. Serum levels of interleukins 3, 6, and 12 were significantly lower in elderly runners than in sedentary individuals. The impact of regular physical activity on serum levels of growth hormone, testosterone, and dehydroepiandrosterone sulfate (DHEAS), which are affected by aging (\"endocrinosenescence\"), was also studied. The serum levels of these anabolic hormones did not differ significantly between the groups of elderly runners and the elderly sedentary individuals. When the impact of regular physical activity on beta-endorphin was studied, again no significant difference in the serum levels of this neuropeptide was found between the two elderly groups. Owing to the possible involvement of the endocrine system in immunosenescence, the correlation between anabolic hormones and cytokines was assessed. No relevant correlation was found, especially between DHEAS and interleukin-6. The results indicate that the regular practice of physical activity for several years may delay immunosenescence
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