Tesis sobre el tema "Experimental arthriti"
Crea una cita precisa en los estilos APA, MLA, Chicago, Harvard y otros
Consulte los 50 mejores tesis para su investigación sobre el tema "Experimental arthriti".
Junto a cada fuente en la lista de referencias hay un botón "Agregar a la bibliografía". Pulsa este botón, y generaremos automáticamente la referencia bibliográfica para la obra elegida en el estilo de cita que necesites: APA, MLA, Harvard, Vancouver, Chicago, etc.
También puede descargar el texto completo de la publicación académica en formato pdf y leer en línea su resumen siempre que esté disponible en los metadatos.
Explore tesis sobre una amplia variedad de disciplinas y organice su bibliografía correctamente.
Holm, Barbro. "Pathogenetic studies of adjuvant-induced arthritis /". Stockholm, 2002. http://diss.kib.ki.se/2002/91-7349-347-3/.
Texto completoLarsson, Esbjörn. "Tissue destruction in arthritis : experimental studies /". Stockholm, 2003. http://diss.kib.ki.se/2003/91-7349-708-8.
Texto completoRagno, Silvia. "Heat shock proteins and experimental arthritis". Thesis, Queen Mary, University of London, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.281712.
Texto completoRibbhammar, Ulrica. "Identification of genes that regulate arthritis and IgE production in rat and human /". Stockholm, 2005. http://diss.kib.ki.se/2005/91-7140-421-X/.
Texto completoLundberg, Karin. "Arthritogenic and immunogenic properties of modified autoantigens /". Stockholm, 2005. http://diss.kib.ki.se/2005/91-7140-303-5/.
Texto completoQuentin, Julie. "Immunomodulation de l'arthrite expérimentale par les cellules dendritiques tolérogènes". Thesis, Montpellier 1, 2011. http://www.theses.fr/2011MON1T018/document.
Texto completoTolerogenic dendritic cells for immumodulation in experimental arthritis.Dendritic cells (DCs) are the most potent antigen-presenting cells that play critical roles in the initiation and regulation of immune responses. Based on their tolerogenic properties, DCs offer potential as therapeutic tools to ameliorate or prevent graft rejection or graft-versus-host disease, or to treat autoimmune disorders.The objectives of my PhD consisted to:- reinforce the tolerogenic potential of DCs by in vitro handling.- assess the capacity of such tolerogenic DCs to induce a protective response in experimental autoimmune arthritis- identify cellular and molecular mechanisms implied in the tolerogenic DCs-induced protectionOur results suggest that, in contrast with conventional DCs, the rapamycin-conditioned iDCs maintain their tolerogenic potential upon injection in inflammatory settings and are able to dampen an already Th1-primed immune response, conferring a protection from arthritis. The protection of the mice was associated with an expansion of the IL-10-secreting CD49b+ Treg in the spleen and liver of the injected mice and a decrease of the Th1 immune response. These results underscore the therapeutic potential of tolerogenic DCs in an established autoimmune disease as well as the anti-inflammatory potential of the CD49b+ Treg cell population induced following DC vaccination
de, Souza Patricia Regina Soares. "GPR40 expression and function in immune cells and experimental arthritis". Thesis, Queen Mary, University of London, 2017. http://qmro.qmul.ac.uk/xmlui/handle/123456789/25975.
Texto completoBoström, Müssener Åsa. "Cytokine regulation in rodents with experimental arthritis /". Stockholm, 1998. http://diss.kib.ki.se/1998/91-628-2862-2.
Texto completoAndreń, Maria. "The role of Fc gamma receptors in experimental arthritis /". Uppsala : Acta Universitatis Upsaliensis : Univ.-bibl. [distributör], 2004. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-4724.
Texto completoDang, Thi Ngoc Dzung. "Studies of novel immunosuppressive agents in experimental arthritis /". Stockholm, 2006. http://diss.kib.ki.se/2006/91-7357-009-5/.
Texto completoPalmblad, Karin. "Cytokines and cytokine-directed intervention in experimental arthritis /". Stockholm, 2001. http://diss.kib.ki.se/2001/91-628-4589-6/.
Texto completoChalise, Jaya Prakash. "Immune tolerance by interferon-alpha in experimental arthritis". Doctoral thesis, Linköpings universitet, Avdelningen för neuro- och inflammationsvetenskap, 2015. http://urn.kb.se/resolve?urn=urn:nbn:se:liu:diva-122463.
Texto completoBäckdahl, Liselotte. "Genetic dissection of experimental arthritis in the DA rat /". Stockholm, 2005. http://diss.kib.ki.se/2005/91-7140-227-6/.
Texto completoBao, Lei. "Immunomodulation and immunopathogenesis in the autoimmune disease with emphasis on autoimmune neuritis and arthritis /". Stockholm, 2003. http://diss.kib.ki.se/2003/91-7349-447-X/.
Texto completoAndrén, Maria. "The Role of Fc Gamma Receptors in Experimental Arthritis". Doctoral thesis, Uppsala University, Department of Genetics and Pathology, 2004. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-4724.
Texto completoInduction of collagen-induced arthritis (CIA), an animal model for human rheumatoid arthritis, is dependent on anti-collagen type II (CII) antibodies. The effector mechanism by which autoantibodies contribute to inflammatory reactions in autoimmune diseases is not well understood. In this thesis I have studied the effector pathways used by IgG anti-CII antibodies to initiate arthritis, namely the IgG Fc receptors (FcγRs) and the complement system. We have found that FcγRIII is crucial for development of CIA, as CII-immunized mice lacking this receptor do not develop arthritis and IgG1 and IgG2b anti-CII antibodies require FcγRIII to trigger arthritis when transferred to naïve mice. The antibody-mediated arthritis was further enhanced in mice deficient in the inhibitory FcγRIIB, indicating that FcγRIIB regulates the activation of FcγRIII. Furthermore, we demonstrate that FcγRIII exist as three distinct haplotypes in mice, FcγRIII:H, FcγRIII:V and FcγRIII:T. Mice expressing the FcγRIII:H haplotype are more susceptible to CIA than mice expressing the FcγRIII:V haplotype, indicating that certain FcγRIII haplotype predisposes for CIA. We also show that the most likely FcγRIII-expressing effector cell in CIA is the macrophage, since FcγRIII-expressing macrophages exclusively can induce arthritis in FcγRIII-deficient mice challenged for CIA.
The complement system was also investigated in development of CIA. We found that this effector pathway is also necessary for onset of arthritis, as CIA was inhibited by treatment with anti-complement factor 5 (C5) antibodies. C5-deficient mice could neither develop CIA unless provided with C5-containing sera.
Taken together, the work presented in this thesis indicates that FcγRs and the complement system are crucial for the induction of experimental arthritis. These findings are important for understanding the mechanisms behind rheumatoid arthritis and blocking of these effector pathways may in the future be used as treatment of rheumatoid arthritis.
Kolodziej, Lukasz. "An investigation of the kynurenine pathway in experimental arthritis". Thesis, Imperial College London, 2011. http://hdl.handle.net/10044/1/9641.
Texto completoGillet, Pierre. "Etude d'un modele experimental de spondylarthropathie : l'arthrite au collagene de type ii chez le rat". Nancy 1, 1988. http://www.theses.fr/1988NAN11245.
Texto completoGarrett, Neil Edward. "Substance P and experimental joint inflammation". Thesis, Queen Mary, University of London, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.244679.
Texto completoKokkola, Riikka. "HMGB1 as a proinflammatory mediator in arthritis /". Stockholm, 2003. http://diss.kib.ki.se/2003/91-7349-506-9.
Texto completoWeiss, Rüdiger J. "Joint destruction in rheumatoid arthritis : experimental, clinical and epidemiological studies /". Stockholm, 2007. http://diss.kib.ki.se/2007/978-91-7357-354-2/.
Texto completoFoong, W. C. "Treatment of an experimental allergic arthritis with liposome-entrapped cytotoxics". Thesis, University of Portsmouth, 1985. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.370171.
Texto completoKuhn, Kristine Ann. "Antibodies to citrulline-modified proteins in collagen-induced arthritis /". Connect to full text at ProQuest Digital Dissertations. IP filtered, 2005.
Buscar texto completoTypescript. Includes bibliographical references (leaves 91-100). Free to UCDHSC affiliates. Online version available via ProQuest Digital Dissertations;
Svelander, Lena. "Studies on immunological mechanisms of induced arthritis in the rat /". Stockholm, 2002. http://diss.kib.ki.se/2002/91-7349-349-X/.
Texto completoPalm, Anna-Karin E. "Function and Regulation of B-cell Subsets in Experimental Autoimmune Arthritis". Doctoral thesis, Uppsala universitet, Kemisk biologi, 2015. http://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-265024.
Texto completoBlaho, Victoria Alison. "Lipid mediators in the development and resolution of experimental lyme arthritis". Diss., Columbia, Mo. : University of Missouri-Columbia, 2007. http://hdl.handle.net/10355/4819.
Texto completoThe entire dissertation/thesis text is included in the research.pdf file; the official abstract appears in the short.pdf file (which also appears in the research.pdf); a non-technical general description, or public abstract, appears in the public.pdf file. "May 2007" Includes bibliographical references.
Guo, Yongzhi. "Plasmin : a potent pro-inflammatory factor". Doctoral thesis, Umeå : Umeå University, 2008. http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-1607.
Texto completoTeixeira, Vivian de Oliveira Nunes. "O envolvimento do proteossomo na perda muscular de modelo de artrite induzida por colágeno e o efeito do tratamento com inibidor do fator de necrose tumoral". reponame:Biblioteca Digital de Teses e Dissertações da UFRGS, 2015. http://hdl.handle.net/10183/139772.
Texto completoBackground: Rheumatoid arthritis is an autoimmune inflammatory disease associated with systemic complications like fatigue and muscle wasting. Muscle wasting could be related to the activation of the ubiquitin-proteasome system. The aim of this study was to evaluate muscle loss and involvement of the proteasome in collagen-induced arthritis (CIA), with or without treatment with methotrexate or a TNF inhibitor (etanercept). Methods: Male DBA1/J mice were divided into 4 groups (n=8 each): CIA (saline); ETN (etanercept, 5.5 /) and MTX (methotrexate, 35 /), treated twice a week for 6 weeks, and a healthy control group (CO). Treatments started one week after booster injection. Clinical score, hind paw oedema, and body weight were analysed during the experimental period. Gastrocnemius muscles (GA) were weighted after death and used to quantify proteasome activity, protein levels and mRNA expression of its subunits by Western blot and rtPCR, respectively. Results: Treatments slowed disease development, observed through smaller clinical score and hindpaw edema in ETN and MTX groups. ETN presented higher body weight compared to MTX group at weeks 5 and 7. GA weight was heavier in ETN than CIA and MTX, a result also observed in the normalized muscle weight. The catalytic properties of 26S proteasome showed an increase of caspase-like activity in CIA and MTX groups. Muscles tissues of MTX treated animals showed higher protein levels for proteasomal subunits PSMB8 and PSMB9 and higher gene expression for Psmb5, Psmb8 and Psmb9. In contrast, expression of Psmb6 was decreased and of Psmb9 was enhanced in CIA. Conclusions: Although both drugs improved the disease score, ETN presented a stronger anti-arthritic effect and was the only treatment able to partially prevent muscle wasting. In contrast to ETN, CIA and MTX treatment did not prevent muscles loss due to increased proteasome expression and activity.
Julià, Cano Antonio. "Genomic approaches for the identi cation of risk loci for Rheumatoid Arthritis". Doctoral thesis, Universitat Autònoma de Barcelona, 2010. http://hdl.handle.net/10803/48650.
Texto completoLove, W. G. "The stability and distribution of radiolabelled liposomes in an experimental model of arthritis". Thesis, Cardiff University, 1988. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.233762.
Texto completoWu, Qinyang. "Galanin and leu-enkephalin in the rat with special reference to adjuvant arthritis /". Stockholm, 2004. http://diss.kib.ki.se/2004/91-7349-977-3/.
Texto completoDonaldson, Lucy F. "The primary afferent nociceptor and neuropeptide gene expression : importance in experimental arthritis". Thesis, University of Edinburgh, 1994. http://hdl.handle.net/1842/20937.
Texto completoConigliaro, Paola. "Dissecting the contribution of B cells in an experimental model of rheumatoid arthritis". Thesis, University of Glasgow, 2014. http://theses.gla.ac.uk/6209/.
Texto completoPaim, Luciana BrandÃo. "AÃÃo antiinflamatÃria da lectina de semente de dioclea violacea na artrite induzida por zymosan". Universidade Federal do CearÃ, 2006. http://www.teses.ufc.br/tde_busca/arquivo.php?codArquivo=744.
Texto completoLectinas de origem vegetal inibem quimiotaxia neutrofÃlica, provavelmente por aÃÃo competitiva com selectinas endÃgenas por um sÃtio glicosÃdico na membrana de cÃlulas endoteliais, leucÃcitos ou em componentes da matrix extracelular. Exploramos os efeitos de lectina isolada de sementes de Dioclea violacea (Dviol) na artrite induzida por zymosan (Azy). Ratos Wistar (180 a 220g) receberam injeÃÃo intra-articular (i.a.) de zymosan (Zy) (1mg) no joelho direito. A hiperalgesia foi avaliada pelo teste de incapacitaÃÃo articular, medido pelo tempo de suspensÃo da pata (TSP) em s/min. O influxo celular (IC) foi medido no lavado articular, obtido 6 h apÃs a injeÃÃo do Zy, por lavagem e aspiraÃÃo da articulaÃÃo. Grupos foram prÃ-tratados (30 min) antes do Zy com Dviol (1 - 30 Âg; i.a. ou 1 - 10mg/kg; e.v.), sendo comparados ao grupo nÃo-tratado (NT), que recebeu apenas Zy e o veÃculo. Outros grupos receberam apenas Dviol (0,3- 30 Âg) i.a. e o grupo Naive, apenas salina i.a. A administraÃÃo de Dviol (6mg/kg; e.v.), reduziu significantemente (p<0,01) a hiperalgesia (TSP= 14,08  1,4) quando comparado ao NT (TSP= 36,06  3,3). A injeÃÃo endovenosa de Dviol inibiu o IC (18.266,7  1.890,1; 14.633,3  3.207,2; 2.790  503,3 e 120  37,4 cÃlulas/mm3 para 1, 3, 6 e 10mg de Dviol, respectivamente) quando comparados ao NT (37.583,3  6.007,2 cÃlulas/mm3). A administraÃÃo i.a. de apenas Dviol (30 Âg) aumentou significativamente o TSP (15,5  0,9), em relaÃÃo ao NV. Dviol i.a. isolada (0,3 a 30; Âg), aumentou significantemente o IC (3.600  676; 4.958,3  1037,2 e 8.350  1.511,5 cÃlulas/mm3 para lectina 0,3; 3 e 30, respectivamente), comparado ao NV (858,3  389,5 cÃlulas/mm3). Dviol (10 Âg; i.a.), 30 min antes da injeÃÃo do Zy, inibiu significantemente a hiperalgesia (TSP = 20,15  2,2) (p<0,01), em relaÃÃo ao NT (TSP= 35,9  2,7). Dviol i.a. (1, 10 e 30μg) reduziu significantemente o IC (18.266,7  1.890,1; 11.366,7  2.883,7 e 19.866,7  1.783,4 cÃlulas/mm3, respectivamente), comparado ao NT. A administraÃÃo e.v. de Dviol (6 mg/kg) + manose (0,1M), reverteu a inibiÃÃo da Dviol na hiperalgesia (TSP= 38,4  4,4) (P<0,01) e no IC (15200  1829,7 cÃlulas/mm3) da AZy, em relaÃÃo a Dviol (6mg/kg;e.v.) (TSP= 14,08  1,4 e IC= 2.790  503,3 cÃlulas/mm3). Os resultados demonstram, de maneira inÃdita, que a lectina de semente de Dviol tem aÃÃo antiinflamatÃria em artrite experimental. Esse efeito parece ser prioritariamente associado à ligaÃÃo da Dviol a sÃtios de polissacarÃdeos intra-articulares, embora nÃo possamos descartar que a ligaÃÃo a domÃnios protÃicos possa estar envolvida nessa aÃÃo
Plant-derived lectins inhibit neutrophil chemotaxis, probably through a competitive mechanism with endogenous selectins for a glycosidic residue in the membrane of endothelial cells, leukocytes or in components of the extracellular matrix. We investigated the effects of a lectin isolated from Dioclea violacea (Dviol) seeds in the zymosan-induced arthritis (Azy). Wistar rats (180 a 220g) received an intraarticular (i.a.) injection of 1 mg zymosan (Zy) into the right knee. The hyperalgesia was evaluated with the test for articular incapacitation, measured as the paw elevation time (PET) in s/1min. Cell influx (IC) was assessed in the joint exudate, obtained 6 h after injection of the Zy, through washing and aspiration of the joint. Groups were pretreated 30min before the Zy with Dviol (1 - 30 Âg; i.a. ou 1 - 10mg/kg; e.v.), and were compared to non-treated groups (NT), that received the Zy and the vehicle. Others groups received only Dviol (0,3 - 30Âg; i.a. and the naÃve animals (NV) received just saline i.a. The i.v. administration of Dviol (6mg/kg) significantly reduced the hyperalgesia (p<0.01) (PET= 14,08 Â 1,4) as compared to NT (PET= 36,06 Â 3,3). The i.v. injection of Dviol inhibited IC (18.266,7 Â 1.890,1; 14.633,3 Â 3.207,2; 2.790 Â 503,3 e 120 Â 37,4 cells/mm3 for the 1, 3, 6, and 10mg doses of Dviol, respectively). Dviol given i.a. isolated (30Âg) increased PET (15,5 Â 0,9) significantly, as compared to NV. Dviol i.a. isolated (0,3 - 30 Âg) significantly increased IC (3.600 Â 676; 4.958,3 Â 1037,2 e 8.350 Â 1.511,5 cells/mm3 for 0,3, 3 e 30 Âg, respectively), as compared to NV (858,3 Â 389,5 cells/mm3). Dviol (10 Âg i.a.) given 30min before the Zy significantly inhibited the hyperalgesia (PET = 20,15 Â 2,2) (p<0.01), as compared to NT (TSP= 9,9 Â1,2). Dviol i.a. (1, 10, and 30μg) significantly reduced IC (18.266,7 Â 1.890,1; 11.366,7 Â 2.883,7 e 19.866,7 Â 1.783,4 cells/mm3, respectively), as compared to NT. The i.v. administration of Dviol (6 mg/kg) + manose reversed the inhibitory action of Dviol in the hyperalgesia (PET= 38,4 Â 4,4) (P<0.01) and in the IC (15200 Â 1829,7 cells/mm3) of the AZy, as compared to Dviol (6mg/kg; i.v.) (TEP= 14,08 Â 1,4 and IC= 2.790 Â 503,3 cells/mm3). The results demonstrate, for the first time, that the lectin isolated from Dviol has anti-inflammatory effect in an experimental arthritis model. This effect appears to be prominently due to the coupling of Dviol to intrarticular polysaccharide residues. However, we can not exclude that coupling to protein residues may be also involved in this mechanism
Howat, D. W. "Metabolic and cellular changes in rheumatoid arthritis, natural and experimental : A quantitative cytochemical study". Thesis, Brunel University, 1986. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.371782.
Texto completoChenna, Narendra Sudeep. "Systemic and local regulation of experimental arthritis by IFN-α, dendritic cells and uridine". Doctoral thesis, Linköpings universitet, Avdelningen för neuro- och inflammationsvetenskap, 2017. http://urn.kb.se/resolve?urn=urn:nbn:se:liu:diva-136238.
Texto completoSchweinhardt, Petra. "Neural correlates of clinical pain processing in neuropathic and inflammatory pain patients and comparison with experimental pain". Thesis, University of Oxford, 2006. http://ora.ox.ac.uk/objects/uuid:12e71d31-24f8-47e8-ba83-129575007644.
Texto completoMANOURY, SCHNARTZ BENEDICTE. "Appretement du collagene de type ii antigene fibrillaire inducteur d'une arthrite auto-immune". Paris 5, 1996. http://www.theses.fr/1996PA05N060.
Texto completoAlabarse, Paulo Vinicius Gil. "Biomarcadores de caquexia reumatoide : uma abordagem metabolômica em modelo experimental de artrite". reponame:Biblioteca Digital de Teses e Dissertações da UFRGS, 2016. http://hdl.handle.net/10183/148071.
Texto completoBackground: Rheumatoid Arthritis (RA) is an autoimmune disease that affects the joints and has a symmetric development and it is erosive. Besides joint damage, it can develop muscle loss progress into cachexia syndrome. Currently, there is no marker that can predict it development in rheumatoid patients. Metabolomics in RA have shown to be complex to find out a biomarker for this syndrome. Also, there is no experimental model of cachexia described in literature yet; however the collageninduced arthritis (CIA) animal model seems to be a feasible model for rheumatoid cachexia. With this model, the research for a biomarker of rheumatoid cachexia can be done by metabolomics. Objectives: It will be evaluated if the CIA animal model can be also an animal model of rheumatoid cachexia. Afterwards, it will be evaluated a metabolic profile from urine of this animal model and correlate with clinical signs of rheumatoid cachexia to find out plausible biomarkers of it. Methods: Male DBA/1J mice were submitted to CIA (n=13), immunization occurred at day zero and a booster was performed 18 days after, and a healthy group with no induction (CO; n=11). At the 0,18, 25, 35, 45, 55 and 65 days after the first injection, it was done: urine collection; physical performance test; free exploratory locomotion test; strength test; hindpaw edema volume measurement; follow up disease development; weighted; and food intake. After the 65 days, animals were euthanized and muscle (gastrocnemious – GA; and tibial anterior – TA) were dissected, and weighted for sarcoplasmic ratio. Data were analyzed by two-way ANOVA followed by Bonferroni post hoc, and t-test of Pearson, and statistical critical limit was set for p<0.05. The collected urine was used for nuclear magnetic resonance (1D and 2D J-res). Metabolites were identified by Chenomx (1D) and by the Birmingham Metabolite Library (BML; 2D J-res). Statistical model were performed using PCA, PLSDA and PLSR to create a ranking list of the metabolites (statistical critical limit was set for p<0.05). It was analyzed the metabolic pathway by Metaboanalyst from the data of metabolite ranking list. Then, the metabolite list was filtered by the metabolic pathways that take place in muscle tissue, in order to identify plausible biomarkers of muscle loss. Results: CIA group has shown reduction in up to 24% of free locomotion fatigue, up to 66% of strength and up to 24% of endurance physical performance after 35 days of the induction, as well as a decrease in GA (24%) and TA (25%) weight, and sarcoplasmic ratio also reduced (22 and 23%, respectivamente) related to CO group. The PCA, PLSDA and PLSR statistical models, and the filter by metabolic pathways related to muscle provided a list of 28 metabolites related to disease development, as can be listed: 3-methylhistidine, 4-aminobutyrate, acetylcholine, arginine, aspartate, carnosine, creatine, creatinine, glutamine, histamine, histidine, isoleucine, leucine, methionine, lysine, myo-inositol, dimethylglycine, acetylalanine, acetylmethionine, pantothenate, phenylalanine, phosphocholine, phosphocreatine, pyridoxine, sarcosine, succinylacetone, thiamine, and urocanate. Conclusions: Accordingly with the data with reduction of: muscle mass, spontaneous locomotion, strength and physical performance, added with absence of anorexia as well as weight change, CIA animal model is a feasible experimental model for rheumatoid cachexia. Concerning the metabolic profile from this model, it can be suggested 28 metabolites related to muscle loss in which can be tested for biomarker of rheumatoid cachexia, targeting prognosis, diagnosis, and syndrome follow up. From those metabolites, the main ones are engaged to metabolism of: histidine; arginine and proline; glycine, serine and threionine; phosphorcreatine, as well as other amino acids and vitamins from B complex.
Quadros, Andreza Urba de. "Novo método de avaliação da incapacidade articular na artrite experimental: investigação do papel das células da glia". Universidade de São Paulo, 2013. http://www.teses.usp.br/teses/disponiveis/17/17133/tde-25052018-155256/.
Texto completoA good experimental model must rely on effective methods of evaluation of its parameters. This is an important observation when it is necessary to evaluate the articular nociception and disability in experimental animals. Establishing new criteria to test animals is essential for inflammatory joint can continue being studied, understood and resolved. Seeking help in this sense, this work constitutes a test dynamic weight bearing (DWB) standardization for assessment of articular incapacitation in experimental models of arthritis. The results show that the DWB is sensitive in assessing the impairment models articular antigen-induced arthritis (AIA) or zimosana. Furthermore is predictive for studying the pharmacological effects of drugs that interfere with articular incapacitation as antiinflammatory or analgesic. Since the early 90s, when participation of glial cells in pain was described, several studies have emerged showing its role in different animal models. The involvement of glial cells in the spinal pain and disability in experimental models of arthritis and rheumatoid arthritis have been reported, but no description of this contribution versus time of induction of joint inflammation. Through molecular and pharmacological tools, this work shows that the glial cells, both as the spinal dorsal root ganglio are participating in the genesis and maintenance of inflammatory joint incapacitation in AIA model. The participation of these cells occurs through the release of IL-1? and TNF? in the spinal cord and the first time it is shown that astrocytic activation appears to precede the microglial activation in this model.
Gauldie, Stephan D. "The role of some putative mediators of peripheral nociceptor activation in adjuvant-induced experimental arthritis". Thesis, University of Edinburgh, 2002. http://hdl.handle.net/1842/23013.
Texto completoBergh, Anna. "Defocused CO₂ laser irradiation in the rehabilitation of horses : an experimental and clinical study /". Uppsala : Dept. of Anatomy and Physiology, Swedish University of Agricultural Sciences, 2006. http://epsilon.slu.se/200654.pdf.
Texto completoBessis, Natacha. "Therapie genique cellulaire par des cytokines anti-inflammatoires dans des modeles experimentaux de la polyarthrite rhumatoide". Paris 5, 1997. http://www.theses.fr/1997PA05N069.
Texto completoIshikawa, Larissa Lumi Watanabe. "Estratégias tolerogênicas antígeno-específicas visando profilaxia e terapia na artrite autoimune experimental /". Botucatu, 2014. http://hdl.handle.net/11449/124050.
Texto completoBanca: Liana Maria Cardoso Verinaud
Banca: Vânia Luiza Deperon Bonato
Banca: Angela Maria Victoriano de Campos Soares
Banca: Paula Schmidt Azevedo Gaiolla
Resumo: A artrite reumatoide (AR) é uma doença autoimune que compromete as articulações. A maioria das terapias utilizadas para o seu tratamento é baseada na inibição global da resposta imune, podendo aumentar a susceptibilidade a agentes infecciosos. O objetivo geral deste projeto foi definir estratégias tolerogênicas específicas para profilaxia ou terapia da AR. Para isso, em uma primeira etapa, estabelecemos um modelo de artrite induzida por proteoglicano (PG) bovino. Camundongos BALB/c fêmeas retired breeders imunizados com PG bovino associado ao adjuvante brometo de dimetil dioctadecil amônio apresentaram os sinais clínicos característicos da artrite, como eritema e edema decorrentes da inflamação articular de uma ou mais patas. A análise histopatológica mostrou a presença de hiperplasia sinovial, infiltrado inflamatório (formação de pannus), destruição da cartilagem e erosão óssea. A incidência da doença foi de 100% e os animais artríticos produziram níveis significativos de citocinas pró e anti-inflamatórias e anticorpos IgG1 e IgG2a anti-PG. Em uma segunda etapa, testamos o potencial profilático do PG. A inoculação de três doses de 50 μg de PG determinou um efeito profilático caracterizado pela diminuição significativa da incidência da artrite e do escore clínico dos animais. A diminuição da produção de IFN-g e IL-17, bem como o aumento da produção de IL-4 e IL-10 por células esplênicas estimuladas com PG, podem estar contribuindo para o efeito profilático observado neste grupo. Em uma terceira etapa, avaliamos o potencial terapêutico da associação da vitamina D ativa (VitD3) com o PG. A associação VitD3+PG determinou um efeito terapêutico na artrite experimental caracterizado por diminuição significativa do escore clínico. Este feito foi confirmado pela análise histopatológica que revelou que a maioria das patas do grupo tratado apresentou estrutura articular bem preservada, ...
Abstract: Rheumatoid arthritis (RA) is an autoimmune disease that affects the joints. Most of the therapies used for RA treatment are based on general suppression of immune response, which may increase the susceptibility to infectious agents. The main objective of this work was to establish specific tolerogenic strategies for prophylaxis or therapy of RA. For this purpose, we first established a model of arthritis induced by bovine proteoglycan (PG). Female BALB/c retired breeder mice immunized with bovine PG associated with dimethyl-dioctadecyl ammonium bromide adjuvant developed a typical arthritis characterized by erythema and edema resulting from joint inflammation of one or more paws. Histopathological analysis showed the presence of synovial membrane hyperplasia, inflammatory infiltrates (pannus formation), cartilage destruction and bone erosion. Disease incidence was 100% and the arthritic mice produced significant levels of pro and anti-inflammatory cytokines and IgG1 and IgG2a anti-PG antibodies. Further, we tested the prophylactic potential of PG. Three doses of 50 μg of PG determined a prophylactic effect characterized by a significant decrease in both, arthritis incidence and clinical scores. The decrease in IFN-g and IL-17, as well as the increase in IL-5 and IL-10 production by spleen cells stimulated with PG may be contributing to the prophylactic effect observed in this group. Lastly, we evaluated the therapeutic potential of the combination of active vitamin D (VitD3) with PG. The VitD3+PG association determined a therapeutic effect in experimental arthritis. There was a significant decrease in the clinical scores after VitD3+PG treatment that was confirmed by the histopathological analysis. Most mice paws from the treated group presented well preserved joint structures that were similar to the ones present in healthy animals. Both pro and anti-inflammatory cytokines were decreased after this treatment. No differences were ...
Doutor
Blake, Simon M. "Metabolic and histological changes associated with the experimentally induced arthritis in the rabbit". Thesis, Brunel University, 1992. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.332069.
Texto completoCatchpole, Brian. "Antigen presentation to autoreactive T cells in experimentally-induced arthritis in the rat". Thesis, Royal Veterinary College (University of London), 1999. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.314347.
Texto completoCorvo, Maria Luisa Teixeira de Azevedo Rodrigues. "Liposomes as delivery system for superoxide dismutase in experimental arthritis = Liposomen als dragersystemen voor superoxide dismutase in experimental artritis : Lipossomas come sistema terapêutico para superóxido dismutase na artrite experimental /". [S.l. : s.n.], 1998. http://www.gbv.de/dms/bs/toc/300314604.pdf.
Texto completoIshikawa, Larissa Lumi Watanabe [UNESP]. "Estratégias tolerogênicas antígeno-específicas visando profilaxia e terapia na artrite autoimune experimental". Universidade Estadual Paulista (UNESP), 2014. http://hdl.handle.net/11449/124050.
Texto completoFundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)
A artrite reumatoide (AR) é uma doença autoimune que compromete as articulações. A maioria das terapias utilizadas para o seu tratamento é baseada na inibição global da resposta imune, podendo aumentar a susceptibilidade a agentes infecciosos. O objetivo geral deste projeto foi definir estratégias tolerogênicas específicas para profilaxia ou terapia da AR. Para isso, em uma primeira etapa, estabelecemos um modelo de artrite induzida por proteoglicano (PG) bovino. Camundongos BALB/c fêmeas retired breeders imunizados com PG bovino associado ao adjuvante brometo de dimetil dioctadecil amônio apresentaram os sinais clínicos característicos da artrite, como eritema e edema decorrentes da inflamação articular de uma ou mais patas. A análise histopatológica mostrou a presença de hiperplasia sinovial, infiltrado inflamatório (formação de pannus), destruição da cartilagem e erosão óssea. A incidência da doença foi de 100% e os animais artríticos produziram níveis significativos de citocinas pró e anti-inflamatórias e anticorpos IgG1 e IgG2a anti-PG. Em uma segunda etapa, testamos o potencial profilático do PG. A inoculação de três doses de 50 μg de PG determinou um efeito profilático caracterizado pela diminuição significativa da incidência da artrite e do escore clínico dos animais. A diminuição da produção de IFN-g e IL-17, bem como o aumento da produção de IL-4 e IL-10 por células esplênicas estimuladas com PG, podem estar contribuindo para o efeito profilático observado neste grupo. Em uma terceira etapa, avaliamos o potencial terapêutico da associação da vitamina D ativa (VitD3) com o PG. A associação VitD3+PG determinou um efeito terapêutico na artrite experimental caracterizado por diminuição significativa do escore clínico. Este feito foi confirmado pela análise histopatológica que revelou que a maioria das patas do grupo tratado apresentou estrutura articular bem preservada, ...
Rheumatoid arthritis (RA) is an autoimmune disease that affects the joints. Most of the therapies used for RA treatment are based on general suppression of immune response, which may increase the susceptibility to infectious agents. The main objective of this work was to establish specific tolerogenic strategies for prophylaxis or therapy of RA. For this purpose, we first established a model of arthritis induced by bovine proteoglycan (PG). Female BALB/c retired breeder mice immunized with bovine PG associated with dimethyl-dioctadecyl ammonium bromide adjuvant developed a typical arthritis characterized by erythema and edema resulting from joint inflammation of one or more paws. Histopathological analysis showed the presence of synovial membrane hyperplasia, inflammatory infiltrates (pannus formation), cartilage destruction and bone erosion. Disease incidence was 100% and the arthritic mice produced significant levels of pro and anti-inflammatory cytokines and IgG1 and IgG2a anti-PG antibodies. Further, we tested the prophylactic potential of PG. Three doses of 50 μg of PG determined a prophylactic effect characterized by a significant decrease in both, arthritis incidence and clinical scores. The decrease in IFN-g and IL-17, as well as the increase in IL-5 and IL-10 production by spleen cells stimulated with PG may be contributing to the prophylactic effect observed in this group. Lastly, we evaluated the therapeutic potential of the combination of active vitamin D (VitD3) with PG. The VitD3+PG association determined a therapeutic effect in experimental arthritis. There was a significant decrease in the clinical scores after VitD3+PG treatment that was confirmed by the histopathological analysis. Most mice paws from the treated group presented well preserved joint structures that were similar to the ones present in healthy animals. Both pro and anti-inflammatory cytokines were decreased after this treatment. No differences were ...
Teixeira, Vivian de Oliveira Nunes. "Envolvimento muscular em modelo experimental de artrite". reponame:Biblioteca Digital de Teses e Dissertações da UFRGS, 2011. http://hdl.handle.net/10183/37042.
Texto completoObjective: Although causing great functional impact, the mechanisms of muscle wasting in RA have been poorly studied. The objective of this study is to describe the muscular involvement in an experimental model of arthritis and its pathways and compare with disuse atrophy. Methods: Female Wistar rats were separated in three groups: control (CO), collageninduced arthritis (CIA) and immobilized (IM). Spontaneous locomotion and weight were evaluated weekly. Gastrocnemius muscle was evaluated by histology and immunoblotting to measure LC3, MuRF-1 and myogenin expression. Significance was considered at p<0.05 level. Results: Histological analysis of the joint confirmed the severity of the arthropathy. There was significant difference in spontaneous locomotion (distance, velocity, number of times standing and number of times resting) in CIA group. Animal body weight, gastrocnemius muscle weight and relative muscle weight decreased 20%, 30% and 20% in CIA rats. Inflammatory infiltration, swelling and type 2 fiber atrophy was present in CIA gastrocnemius muscles, with reduced cross-sectional area by 30%, and 60% in IM. Imunoblotting analysis demonstrated increased expression of myogenin and MuRF-1 in CIA muscles by about 70%, while in IM remained similar to control. Conclusions: This study demonstrated that the development of experimental arthritis is associated to decreased mobility, weight loss, muscle atrophy, increased expression of markers of muscle proteolysis and regeneration. For the first time it is demonstrated that muscle atrophy in arthritis is associated with the disease itself, and not simply due to decreased mobility, since immobilized group presented no activation of the same atrophy pathways.
Cordano, Pablo. "Evolution of caprine arthritis encephalitis virus in goats experimentally infected with molecularly cloned virus /". [S.l.] : [s.n.], 1999. http://www.stub.unibe.ch/html/haupt/datenbanken/diss/bestell.html.
Texto completoSchütte, Anja. "Depletion of CD8+ T-cells in goats experimentally infected with caprine arthritis encephalitis virus /". [S.l.] : [s.n.], 1999. http://www.ub.unibe.ch/content/bibliotheken_sammlungen/sondersammlungen/dissen_bestellformular/index_ger.html.
Texto completo