Tesis sobre el tema "Autoimmunity"
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Cucurella, Paula. "Autoimmunity in Antipoetry". Thesis, State University of New York at Buffalo, 2018. http://pqdtopen.proquest.com/#viewpdf?dispub=10639684.
Texto completoAntipoetry, a form of poetry developed by the Chilean poet Nicanor Parra, instances a privileged example of a self-regulatory trait of the poetic genre which responds to poetry’s need to destroy itself in order to renew itself. This need reveals a structural mechanism or a logic of autoimmunity, which informs the possibility of language and, moreover, of all living beings.
Antipoetry’s departure from the Nerudean poetic tradition justifies the use of a colloquial language that also preserves and continues Neruda’s interest in opening a space for the “popular” in poetry. Against Neruda, Antipoetry also consciously repels romantic and heroic aesthetic principles and ideas.
Parra’s aesthetic principles, however, do not result solely from avoidance. Parra is a realist poet heavily influenced by physics. His poetry needs to mirror reality. The principles of relativity and indetermination play major roles in his poetic experimentations, and will come to the aid of Antipoetry’s need to create in times of censorship. Parra’s experiments with language are in large measure interpretations of the laws of physics. In this regard, his scientific realism is related to Gertrude Stein’s work. The poetry and poetics of the latter provides a touchstone and a constant reference in Autoimmunity in Antipoetry.
Like all artistic expressions during the Chilean military dictatorship of Augusto Pinochet, Antipoetry was forced to negotiate what could be said with what the poet wanted to say. The necessary negotiation that Parra’s poetry needed to undergo gave rise to many experiments with language, including systematic ambiguity, contestation of the authority of the author, and of his own authorial control over his poetry. The use of masks, the multiplication of referents, and the systematic use of contradiction name some of Antipoetry’s tools for obstructing the univocal determination of meaning.
Antipoetry’s systematic explorations toward the creation of a poetry that attempts to fight all forms of dogmatism nevertheless reaches a limit in its figuration of gender. Antipoetry’s gender politics makes concessions to a type of gender dogmatism (sexism and homophobia) that contradicts the antipoetic program and reveals an inherent fear of gender contamination that jeopardizes Antipoetry’s most fortunate aspects.
Grant, Michael David. "Alloimmunity, autoimmunity, and AIDS". Thesis, University of British Columbia, 1989. http://hdl.handle.net/2429/27465.
Texto completoScience, Faculty of
Microbiology and Immunology, Department of
Graduate
Ye, Ping. "Autoimmunity in chronic periodontitis". Thesis, The University of Sydney, 2003. http://hdl.handle.net/2123/4256.
Texto completoYe, Ping. "Autoimmunity in chronic periodontitis". University of Sydney, 2003. http://hdl.handle.net/2123/4256.
Texto completoProfound perturbation of epithelial structure is a characteristic feature of the immunopatholoical response to bacterial antigens considered to be central in the pathogenesis of the destructive lesion of periodontitis. The pathological basis for the disturbance of epithelial structure is not understood. It was demonstrated that the structural integrity and functional differentiation of the lining epithelium is compromised in relation to inflammatory changes associated with destructive periodontitis. In the pathological lining epithelium of the periodontal pocket there was a marked reduction of epithelial cadherin important in intercellular adhesion, of involucrin, a marker of terminal differentiation, and of the gap junction connexions that form intercellular communication channels. These changes were associated with alterations of filamentous actin expression, collectively indicating profound perturbation of epithelial structure. The data reported support the concept that the ability of the pathological lining epithelium to function as an effective barrier against the ingress of microbial products into the tissues is severely compromised (Ye et al., 2000). In addition, a recent study (Ye et al., 2003) by Western analysis of serum IgG from all 22 patients with chronic periodontitis tested indicated recognition of multiple epithelial components in individual patterns. In contrast, subjects with a healthy periodontium displayed only trace recognition of epithelial antigens. Levels of epithelial-reactive antibodies were significantly correlated with attachment loss as an indication of disease activity. To investigate a possible relationship between the bacterial flora adjacent to the diseased sites and the presence of epithelial-reactive antibodies, subgingival plague samples were taken from deep periodontal pockets and cultured anaerobically. Gram positive bacteria containing antigens potentially cross-reactive with epithelial cells were reproducibly isolated by probing membrane colony lifts with affinity-isolated (epitheial-specific) antibodies. The bacteria were identified as streptococci (S. mitis, S. constellatus and two S. intermedius strains) and Actinomyces (A. georgiae, and A. sp. oral clone) by 16S rDNA sequence homology. Recognition by affinity-isolated antibodies of antigens from the captured organisms was confirmed by Western analysis. Conversely, absorption of affinity-isolated antibodies with bacterial species specifically reduced subsequent recognition of epithelial antigens. To identify the auto-antigens, a human keratinocyte cDNA expression library in Lambda phage was probed using a pooled sera. Groups of responders were detected for CD24 (a recently described adhesion molecule also known as P-selectin ligand), antioxidant protein 2 (a newly recognised member of the thiol-dependment anti-oxidant proteins), lavtate dehydrogenase A, the transcription factor NFAT5, and for three genes encoding novel proteins. Six identified bacteria, especially S intermedius were demonstrated to absorb antibodies reaching with identified auto-antigens in patterns varying between individuals. This evidence indicated that during the course of periodontits, subjects develop increased levels of antibodies to common oral bacteria amongst which are included tissue cross-reactive antigens. Periodontitis could therefore present a risk for the subsequent initiation or exacerbation of a broad spectrum of disease processes including autoimmune, inflammatory, proliferative and degenerative disorders.
Ye, Ping. "Autoimmunity In Chronic Periodontitis". Thesis, The University of Sydney, 2003. http://hdl.handle.net/2123/4872.
Texto completoCrisi, Giovanna M. "Autoimmunity and effect of ageing". [Maastricht : Maastricht : Universiteit Maastricht] ; University Library, Maastricht University [Host], 1999. http://arno.unimaas.nl/show.cgi?fid=8571.
Texto completoWodzig, Karel Willem Henricus. "Cyclosporine A-induced experimental autoimmunity". Maastricht : Maastricht : Rijksuniversiteit Limburg ; University Library, Maastricht University [Host], 1993. http://arno.unimaas.nl/show.cgi?fid=9486.
Texto completoJohnstone, Thomas W. "Neutrophil serine proteinases and autoimmunity". Thesis, Queen's University Belfast, 1994. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.241372.
Texto completoBari, Abu-saleh Mahfuzul. "Autoimmunity in canine joint disease". Thesis, University of Liverpool, 1989. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.257145.
Texto completoD'Cruz, David Pascal. "Autoimmunity, endothelium and vascular disease". Thesis, King's College London (University of London), 1998. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.298705.
Texto completoYoung, Joyce L. "The control of erythrocyte autoimmunity". Thesis, University of Bristol, 1989. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.292470.
Texto completoPalacios, Cuervo Fernando, Rivera Andrea Calderón, Reyes Fátima Espinal y Aybar Carlos Canelo. "Autoimmunity in dengue: Literature review". Elsevier B.V, 2015. http://hdl.handle.net/10757/595420.
Texto completoPalacios, Cuervo Fernando, Rivera Andrea Calderón, Reyes Fátima Espinal y Aybar Carlos Canelo. "Autoimmunity in dengue: Literature review". Elsevier B.V, 2016. http://hdl.handle.net/10757/609496.
Texto completoSelli, Mehmet Emrah. "Autoimmunity in obesity and myocarditis". Thesis, University of Bristol, 2016. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.702465.
Texto completoHansson, Monika. "Mercury-induced autoimmunity : Genetics and immunoregulation". Doctoral thesis, Stockholm University, Wenner-Gren Institute for Experimental Biology, 2004. http://urn.kb.se/resolve?urn=urn:nbn:se:su:diva-47.
Texto completoThe existence of immune self-tolerance allows the immune system to mount responses against infectious agents, but not against self-molecular constitutes. Although self-tolerance is a robust phenomenon, in some individuals as well as in experimental models, the self-tolerance breaks down and as a result, a self-destructive autoimmune disease emerges. The underlying mechanisms for the development of autoimmune diseases are not known, but genetic, environmental and immunological factors are suggested to be involved. In this thesis, we used murine mercury-induced autoimmunity to test this suggestion.
In susceptible mice mercuric chloride induces a systemic autoimmune disease characterized by increased serum levels of IgG1 and IgE, production of anti-nucleolar autoantibodies (ANolA) and formation of renal IgG deposits. In contrast, in resistant DBA/2 (H-2d) mice, none of these characteristics develop after exposure to mercury. By crossing and backcrossing mercury-resistant DBA/2 mice to mercury susceptible strains, we found that the resistance was inherited as a dominant trait in F1 hybrids and that one gene or a cluster of genes located in the H-2 loci determined the resistance to ANolA production, whereas resistance to the other characteristics was found to be controlled by two or three non-H-2 genes.
We further put forward the “cryptic peptide hypothesis” to investigate whether mercury and another xenobiotic metal use similar pathway(s) to induce the H-2 linked production of ANolA. We found that while mercury stimulated ANolA synthesis in all H-2 susceptible (H-2s, H-2q and H-2f) mouse strains, silver induced only ANolA responses in H-2s and H-2q mice, but not in H-2f mice. Further studies showed that the resistance to silver-induced ANolA production in H-2f mice was inherited as a dominant trait.
We next tested the proposition that mercury induces more adverse immunological effects in mouse strains, which are genetically prone to develop autoimmune diseases, using tight-skin 1 mice, an animal model for human Scleroderma. It was found that in this strain, mercury induced a strong immune activation with autoimmune characteristics, but did not accelerate the development of dermal fibrosis, a characteristic in Tsk/1 mice.
Finally we addressed the Th1/Th2 cross-regulation paradigm by examining if a Th1-type of response could interact with a Th2-type of response if simultaneous induced in susceptible mice. Our findings demonstrated that mercury-induced autoimmunity (Th2-type) and collagen-induced arthritis (CIA) (Th1-type) can interact in a synergistic, antagonistic or additive fashion, depending on at which stage of CIA mercury is administered.
Kozhakhmetova, Aizhan. "Multiple autoimmunity in type 1 diabetes". Thesis, University of Bristol, 2017. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.715747.
Texto completoMcKall-Faienza, Kim J. "The role of TNFRp55 in autoimmunity". Thesis, National Library of Canada = Bibliothèque nationale du Canada, 1997. http://www.collectionscanada.ca/obj/s4/f2/dsk2/ftp04/mq28774.pdf.
Texto completoAstern, Joshua Michael Falk Ronald J. Preston Gloria A. "Myeloperoxidase in vascular disease and autoimmunity". Chapel Hill, N.C. : University of North Carolina at Chapel Hill, 2007. http://dc.lib.unc.edu/u?/etd,1209.
Texto completoTitle from electronic title page (viewed Mar. 26, 2008). "... in partial fulfillment of the requirements for the degree of Doctor of Philosophy in the Department of Pathology and Laboratory Medicine." Discipline: Pathology and Laboratory Medicine; Department/School: Medicine.
Buckley, Camilla. "Autoimmunity in thymoma-associated Myasthenia gravis". Thesis, University of Oxford, 2001. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.394014.
Texto completoLewis, Graham Matthew. "The genetic basis of systemic autoimmunity". Thesis, University of Oxford, 2005. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.424728.
Texto completoWalker, Jennifer Anne. "CD22, autoimmunity and the B cell". Thesis, University of Cambridge, 2008. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.612192.
Texto completoThompson, Clare. "The role of iodine in autoimmunity". Thesis, University of Cambridge, 2004. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.615656.
Texto completoDalin, Frida. "Model diseases for studies of autoimmunity". Doctoral thesis, Uppsala universitet, Institutionen för medicinska vetenskaper, 2015. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-265276.
Texto completoHornsby, E. "Development of IL-17A-associated autoimmunity". Thesis, University College London (University of London), 2010. http://discovery.ucl.ac.uk/20224/.
Texto completoPrahalad, Sampath. "Juvenile Rheumatoid Arthritis and Familial Autoimmunity". University of Cincinnati / OhioLINK, 2001. http://rave.ohiolink.edu/etdc/view?acc_num=ucin991251421.
Texto completoGerhardt, Teresa [Verfasser], Andreas [Akademischer Betreuer] Zirlik y Marco [Akademischer Betreuer] Idzko. "Loss of protective autoimmunity in atherosclerosis". Freiburg : Universität, 2021. http://d-nb.info/1238016073/34.
Texto completoJha, Vibha. "Cellular regulation of mercury-induced autoimmunity". Diss., Temple University Libraries, 2009. http://cdm16002.contentdm.oclc.org/cdm/ref/collection/p245801coll10/id/60597.
Texto completoPh.D.
Etiological agents causing autoimmune diseases largely remain unknown. However, several lines of evidence suggest that environmental factors such as heavy metals (arsenic, lead and mercury) play a crucial role in the development of autoimmune disorders. In our model of mercury-induced autoimmunity, administration of subtoxic doses of HgCl2 to genetically susceptible strains of mice result in an autoimmune disease characterized by the production of highly specific anti-nucleolar autoantibodies, hypergammaglobulinemia and nephritis. However, mice can be tolerized to the disease by a single low dose administration of HgCl2 (tolerogenic dose). Previous studies from our lab had demonstrated that CD4+ CD25+ Foxp3+ regulatory T cells (Tregs) control the induction and maintenance of tolerance to mercury. We investigated the therapeutic role of Tregs in our model by utilizing agents that are known to stimulate in vivo expansion of Tregs. We studied two such agents, CD3-specific non-Fc receptor-binding [(Fab’)2 fragment] monoclonal antibody (Anti-CD3) and immune complexes containing recombinant IL-2 and anti-IL-2 monoclonal antibody (IC). In our model, treatment of mice with Anti-CD3 had no effect on Treg population. Administration of Anti-CD3 with the tolerogenic dose prevented induction of tolerance and failed to improve the maintenance period of tolerance. Anti-CD3 in presence of mercury activated the immune-system causing splenomegaly and expansion of B cell population. Overall, in contrast to its protective role in other experimental autoimmune disease models, Anti-CD3 exacerbated mercury-induced autoimmune syndrome. Treatment of mice with IC resulted in selective expansion of Tregs with a modest decrease in IgE levels and autoantibody production. Administration of IC with the tolerogenic dose led to a reduction in autoantibody response, thus IC was able to extend the maintenance period of tolerance to mercury. Lymphocyte Activation Gene-3 (LAG-3) is an inhibitory molecule that maintains lymphocyte homeostatic balance by controlling effector T cell expansion and contributing to the suppressive functions of Tregs. Thus, with the goal to understand the impact of homeostatic balance on Hg-induced autoimmunity, we investigated the role of LAG-3 in our model. Administration of an anti-LAG-3 monoclonal antibody broke tolerance to Hg resulting in autoantibody production and an increase in levels of serum IgE. Additionally, LAG-3-deficient B6.SJL mice exhibited an increased susceptibility to mercury-induced autoimmunity whereas, wild type controls suffered only from a mild disease. Moreover, adoptive transfer of wild-type CD4+ T cells protected LAG-3-deficient mice from mercury-induced autoimmunity. Therefore, we conclude that LAG-3 exerts an important regulatory effect on autoimmunity elicited by a common environmental pollutant.
Temple University--Theses
Villard, Marine. "Rôle de la profération induite par la lymphopénie dans la rupture de la tolérance périphérique des lymphocytes T CD8+". Thesis, Montpellier 2, 2013. http://www.theses.fr/2013MON20172/document.
Texto completoThe immune system has evolved multiple mechanisms of peripheral tolerance to control CD8+ T cell responses and to prevent autoimmunity. However, they also represent a barrier for the development of cytotoxic responses against tumors. Lymphodepleting protocols are currently used as adjuvants for adoptive cytotoxic T cell immunotherapy because they enhance their potency. These protocols are thought to promote the breakdown of peripheral CD8+ T cell tolerance. Under acute lymphopenic conditions, naive T cells proliferate, in the apparent absence of antigenic stimulation at least in part due to a greater availability of the cytokine IL-7. Proliferating CD8+ T cells acquire a phenotype and functionality that is similar to memory cells and are termed memory-like cells. Since memory cells have a lower activation threshold than naïve cells, it has been proposed that differentiation of potentially autoreactive CD8+ T cells into memory-like cells under lymphopenic conditions could drive the breakdown of peripheral tolerance. Here we studied whether lymphopenia induced proliferation and differentiation are required for the breakdown of CD8+ T cell cross-tolerance in irradiated transgenic mice expressing a model antigen in the beta cells of the pancreas. Surprisingly, we found that blocking lymphopenia-induced proliferation and differentiation into memory-like cells did not prevent self-reactivity. CD8+ T cells that did not differentiate into memory-like cells still became effectors upon antigen cross-presentation and migrated to the site of antigen expression. Nonetheless, LIP did enhance CD8+ T cell mediated self-reactivity at low T cell frequencies. This effect could not be explained by a Treg imbalance but by a net increase in autoreactive CD8+ T cell numbers. Thus, although LIP enhances CD8+ T cell anti-self responses, differentiation into memory-like cells is not essential for the breakdown of cross-tolerance under the lymphopenic conditions provided by irradiation
Beijleveld, Leonardus Johannes Josephus. "Thymus dependent autoimmunity thymic selection versus peripheral tolerance in the model of experimental Cyclosporin-A induced autoimmunity /". [Maastricht : Maastricht : Rijksuniversiteit Limburg] ; University Library, Maastricht University [Host], 1996. http://arno.unimaas.nl/show.cgi?fid=6692.
Texto completoRodríguez, Fernández Silvia. "Phosphatidylserine-rich liposomes to tackle autoimmunity. En route to translationality". Doctoral thesis, Universitat Autònoma de Barcelona, 2019. http://hdl.handle.net/10803/667944.
Texto completoAutoimmune diseases are caused by defective immunological tolerance, and reportedly affect up to 10% of the global population. In the last years, current medical interventions have transformed these disorders into chronic and manageable, but they still entail high rates of morbidity and mortality. Hence, there is an urgent need to develop therapies capable of restoring the breach of tolerance selectively, which halt the autoimmune aggression and allow the regeneration of the targeted tissue. In physiological conditions, the phagocytosis of apoptotic cells performed by phagocytes such as dendritic cells (DCs) —a process termed efferocytosis— prompts the acquisition of tolerogenic features and the ability to restore tolerance. Indeed, a cell immunotherapy consisting of DCs rendered tolerogenic (tolDCs) by apoptotic β-cell efferocytosis arrested the autoimmune attack against β-cells in an experimental model of type 1 diabetes (T1D). However, in light of the hurdles in obtaining and standardising human autologous apoptotic β-cells for its implementation in the clinics, a nanotherapeutic strategy based on liposomes mimicking apoptotic cells was designed. The fundamental characteristics of these synthetic vesicles are: a high percentage of phosphatidylserine (PS) —phospholipid unique to the apoptotic cell membrane—, diameter superior to 500 nm, negative charge and efficient encapsulation of insulin peptides. Importantly, this strategy was equally effective in inducing tolDCs and blunting β-cell autoimmunity as the immunotherapy based on apoptotic cells. The hypothesis of this work is that autoantigen-loaded PS-liposomes can re-establish tolerance in several antigen-specific autoimmune diseases through the induction of tolDCs and the expansion of regulatory T lymphocytes, and that they have translational potential to tackle human autoimmune disorders. The main aim of the present work has been to characterise the tolerogenic potential of PS-liposomes globally. To this end, different autoantigenic peptides relevant in autoimmune diseases have been efficiently encapsulated into PS-liposomes, without difficulties in preserving their appropriate diameter and charge, thus demonstrating the versatility of the therapy to different autoimmune pathologies. In the experimental model of T1D, the administration of PS-liposomes causes the expansion of clonal CD4+ regulatory T cells and CD8+ T cells, which contribute to the long-term re-establishment of tolerance. Moreover, in the same model, the biocompatibility and safety of the final product have been confirmed given its optimal tolerability. Furthermore, PS-liposomes have been adapted to the experimental multiple sclerosis model by merely replacing the encapsulated autoantigen. In this model, PS-liposomes elicit the generation of tolDCs and decrease the incidence and severity of the disease correlating with an increase in the frequency of regulatory T cells, a fact that validates the potential of PS-liposomes to serve as a platform for tolerance re-establishment in different autoimmune diseases. Finally, considering its future clinical implementation, the effect of the PS-liposomes therapy has been determined in human DCs obtained from patients with T1D. In DCs from adult patients, PS-liposomes are efficiently phagocyted by DCs with rapid kinetics dependent on the presence of PS, and this induces a tolerogenic transcriptome, phenotype and functionality that are similar to those observed in experimental models. However, DCs from paediatric patients display defects in their phagocytic capacity correlating with the time of disease progression, albeit their phenotype and immunoregulatory gene expression after PS-liposomes phagocytosis point to an optimal tolerogenic ability. In conclusion, the liposomal immunotherapy herein described, which is based on efferocytosis as a powerful tolerance-inducing mechanism, achieves apoptotic mimicry in a simple, safe and efficient manner. Additionally, liposomes offer advantages in terms of production and standardisation. Therefore, PS-liposomes possess translational potential and constitute an encouraging strategy to restore immunological tolerance in antigen-specific autoimmune diseases.
Isaksson, Magnus. "Initiation of Autoimmunity in Experimental Autoimmune Encephalomyelitis". Doctoral thesis, Uppsala universitet, Molekylär medicin, 2012. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-173427.
Texto completoDe, Smet Joseph Marc Dominique. "Observations in clinical and experimental ocular autoimmunity". [S.l. : Amsterdam : s.n.] ; Universiteit van Amsterdam [Host], 2000. http://dare.uva.nl/document/83518.
Texto completoOmslagtitel: Observations on clinical and experimental ocular autoimmunity. - Auteursnaam op omslag: Marc D. de Smet. Met lit. opg. - Met samenvatting in het Nederlands.
Pratigya, Gautam. "Deciphering the link between PTPN22 and autoimmunity". Thesis, Cardiff University, 2011. http://orca.cf.ac.uk/54471/.
Texto completoPritchard, Nicholas Russell. "Regulation of inhibitory receptor expression and autoimmunity". Thesis, University of Cambridge, 2003. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.619621.
Texto completoBadami, Ester. "Mechanisms of activation and regulation in autoimmunity". Thesis, University of Southampton, 2007. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.443060.
Texto completoHendler, Assi. "The link between autoimmunity and periodontal disease". Thesis, Queen Mary, University of London, 2012. http://qmro.qmul.ac.uk/xmlui/handle/123456789/3344.
Texto completoKiely, Patrick David Wolfenden. "Cellular mechanisms in mercuric chloride-induced autoimmunity". Thesis, University of Cambridge, 1996. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.627575.
Texto completoCoutinho, Maria Ester Freitas Barbosa Pereira. "Central nervous system autoimmunity in neuropsychiatric disorders". Thesis, University of Oxford, 2016. https://ora.ox.ac.uk/objects/uuid:389fb830-4b4e-4201-9965-19acb2c63ff3.
Texto completoConnor, Ruth Redlich. "Autoimmunity to cardiac muscle in myasthenia gravis /". The Ohio State University, 1988. http://rave.ohiolink.edu/etdc/view?acc_num=osu148759165817591.
Texto completoHuizinga, Hendrika Geertruida. "Autoimmunity to neuronal antignes in multiple sclerosis". [S.l.] : Rotterdam : [The Author] ; Erasmus University [Host], 2008. http://hdl.handle.net/1765/13809.
Texto completoWeiss, Julia Miriam. "Characterization of thymic hyperplasia associated with autoimmune Myasthenia Gravis : role of the chemokines CXCL12 and CXCL13". Thesis, Paris 11, 2011. http://www.theses.fr/2011PA114831/document.
Texto completoAutoimmune myasthenia gravis (MG) is a muscular disease mediated by autoantibodies, mainly directed against the acetylcholine receptor (AChR). The pathogenic antibodies are especially produced in the thymus, which is often characterized by a hyperplasia with germinal centers. Recent studies demonstrated the overexpression of chemokines and the abnormal development of high endothelial venules (HEV) in the MG thymus. The aim of my thesis was to better understand the mechanisms that lead to thymic hyperplasia in MG by analyzing the role of chemokines in peripheral cell recruitment. We demonstrated that the number of HEVs correlated with the degree of hyperplasia suggesting a direct link between HEVs and peripheral cell recruitment. To define its mechanism of action, we examined which chemokines were expressed on thymic HEVs. We uniquely detected SDF-1 and observed that B cells, myeloid dendritic cells (mDCs), plasmacytoid DCs and monocytes/macrophages that expressed the SDF-1 receptor CXCR4 localized inside and around thymic HEV. In parallel we observed a decreased CXCR4 expression and a decreased number of mDCs and also monocytes in the periphery suggesting their recruitment to the MG thymus. As the MG thymus was recently characterized by the overexpression of CXCL13 in thymic epithelial cells (TECs), we investigated its contribution to thymic hyperplasia. We therefore generated a transgenic mouse model overexpressing in medullary TECs CXCL13 under the control of keratin 5. We demonstrated that transgenic K5-CXCL13 mice specifically overexpressed CXCL13 in the thymus, while no other tested chemokines were upregulated. Preliminary results showed that elevated levels of CXCL13 resulted in an increased number of B cells in the thymus of transgenic mice, which localized preferentially in loose aggregates in medullary areas. We are presently investigating if immunization with purified AChR induces experimental MG with thymic hyperplasia in these mice. Myasthenic mice with a hyperplastic thymus could present a new animal model for MG with a phenotype that is closer to the human disease than the current MG model. As the hyperplastic MG thymus displays the hallmarks of a viral signature, we investigated the effect of pathogen-associated molecules on thymic changes associated with MG. We demonstrated that dsRNA signaling induced by Poly(I:C) specifically triggers the overexpression of α-AChR in human TECs through the release of IFN-I. We also observed that IFN-I was able to upregulate CXCL13 and CCL21, similarly to what is observed in the MG thymus. In addition, Poly(I:C) injections in wildtype mice, but not in IFN-I receptor KO mice, specifically increase thymic expression of α-AChR and, in parallel, CXCL13 and CCL21 expression. In periphery, Poly(I:C) even induced an anti-AChR autoimmune response characterized by a significant production of serum anti-AChR antibodies and a specific proliferation of B cells. Overall the results obtained in the course of my PhD showed that the abnormal development of SDF-1-expressing HEVs and the CXCL13 overexpression play a central role in the recruitment of peripheral cells to the MG thymus. Once these cells have arrived in the inflammatory environment, which is characteristic for MG, they could develop an autoimmune reaction against AChR. New therapeutic molecules that control chemokine expression and angiogenic processes could diminish the development of thymic hyperplasia and avoid thymectomy or the use of corticoids
Wallström, Erik. "Genetic regulation of, and autoimmunity in, myelin oligodendrocyte glycoprotein-induced experimental autoimmune encephalomyelitis and multiple sclerosis /". Stockholm, 2000. http://diss.kib.ki.se/2000/91-628-4067-3/.
Texto completoLundberg, Cecilia. "Autoimmune and innate inflammation in the nervous system : neurotrophin production and impact on neuronal survival /". Stockholm, 2000. http://diss.kib.ki.se/2000/91-628-4421-0/.
Texto completoMiyelani, Maringa Ignecious. "Implementation of an Aseptic Service for Radiolabelling of Autologous Blood Cells at the Department of Nuclear Medicine, Dr George Mukhari Hospital". Thesis, University of Limpopo (Medunsa Campus), 2013. http://hdl.handle.net/10386/1075.
Texto completoIntroduction: The Department of Nuclear Medicine at Dr George Mukhari Hospital (DGMH) received a biological safety cabinet (Laminar airflow hood - LAF) as a donation from the International Atomic Energy Agency (IAEA) in 2007, for the specific purpose of preparing radiolabelled blood cells. The laminar airflow hood was installed but has never been commissioned for use. Radiolabelled white blood cells are used in a range of Nuclear Medicine applications related to infection and pyrexia of unknown origin. Correct handling of the blood is essential for both patient and operator safety. A laminar airflow procedure is required for the radiolabelling of autologous blood. Therefore, there was a need to further investigate the guidelines for radiolabelling autologous blood cells with a view to commissioning the LAF and implementing a service for radiolabelling of autologous blood elements. Objectives: 1. Identify the equipment 2. Identify and development of the SOPs 3. Implement aseptic services to radiolabelling blood cells. Method: The study was conducted at the Department of Nuclear Medicine, Dr George Mukhari Hospital. The design of the study was prospective, descriptive and interventional. Data were collected through independent (objective) observation, questionnaires (subjective). In order to involve staff in the implementation of aseptic services in the respective department a focus group discussion (FGD) followed. The International Atomic Energy Agency (IAEA); Operational Guidance on Hospital Radiopharmacy and United Kingdom Radiopharmacy Group (UKRG) Guidelines were consulted to identify equipment and operational standards required. Permission to conduct the study was obtained from the Head of Department of Nuclear Medicine and Chief Executive Officer (CEO) of the Hospital. The proposal was approved by the Medunsa Campus Research and Ethics Committee (MCREC). xii Results: Premises: The room in which the LAF is situated is not in use as a clean room; hence few of the IAEA infrastructure and LAF requirements were met. Only, three aspects (18.75%) were compliant (type of LAF, lighting and dedicated equipment availability) and thirteen (81.25%) were not. For the hot lab only two (16.67%) of the fourteen items regarding structure and facilities were compliant, twelve (83.33%) were not (e.g. access, layout, cleanliness levels). The short term plan devised is to partition the area in which LAF is currently situated into a clean room and change room, seal the ceiling and windows, paint and ensure that walls, floors and surfaces are smooth and impervious in both the clean room and hot lab. The cost of alterations is (+/-) R50 000. The long term plan is to obtain funds (approximately R960 000) for the full development of the aseptic suite which will comply with local and international standards for radiolabelling of autologous blood cells recommended by ISORBE. Environment and Personnel: None of the four survey items on environment was compliant for the clean room (e.g. air not filtered, no temperature or humidity monitoring or control). Only in the hot lab was the temperature monitored. The LAF/clean room is not currently in use. In the hot lab, gowns and overshoes are not available. The plan is to have thermometers installed in both the clean room and hot lab and have log books for recording temperature. Microbial Contamination: In the Department, monitoring of microbial contamination is not performed. The IAEA recommends that surfaces, environment and equipment should be monitored for microbial contamination in an area where sterile products are handled. Staff Training & Improvement of Aseptic Services: Two staff had been trained in aseptic admixing. All eight respondents agreed that training on aseptic handling of radiopharmaceuticals is necessary. Hygiene and SOPs: Six respondents rated hygiene as satisfactory and two as not satisfactory. Despite these views, all felt that hygiene should be improved in the hot lab and that standard operating procedures (SOPs) should be developed. A group xiii was set up to develop SOPs. Four SOPs were developed - cleaning the clean room and LAF, hand washing, gowning/degowning and leukocyte radiolabelling. Radiolabelling of Autologous Blood Cells: Doctors in the Department want this service to help with the diagnosis of pyrexia of unknown origin (PUO) and infections. Therefore, they were supportive to the researcher in the project set-up the processes and facilities for radiolabelling cells. The short term plan is to train staff in radiolabelling of autologous blood cells. The long term plan is to have the facility to set-up correctly to facilitate service provision and research. Equipment: Staff mentioned that a centrifuge dedicated to the radiolabelling of blood cells should be obtained to ensure that all the procedures for labelling blood cells are followed. The short term plan is to commission the LAF (Cost: approximately R15 000 including VAT) and obtain a cooled centrifuge with sealable buckets (Cost: approximately R40 000 including VAT) for the purpose of commencing with the radiolabelling of blood cells service in the Department. Finance: Staff indicated that some of the problems in the department can be solved if they can obtain funding for infrastructure development. The short term plan is to have the budget for the upgrade of the facility included in the Departmental budget. And the long term plan is to obtain funds from the Gauteng Government for the full development of the facility Conclusion: Required standards and guidelines for radiolabelling of autologous blood cells in a radiopharmacy unit have been identified. Therefore, the upgrading process of the facility should commence and SOPs developed should be implemented. Recommendations: Necessary structural changes on the facility should be made to meet the local and international standards for radiolabelling blood products. Therefore, funds should be obtained for upgrading the facility and obtain the necessary minimum equipment for radiolabelling of autologous blood cells. It is recommended that a post for a radiopharmacist be created to increase capacity and help improve standards with regards to pharmaceutical services in the Department.
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