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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.

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1

CD279 (PD-1) e seus ligantes CD273 (PD-L1) e CD274 (PD-L2) regulam a linfoproliferação, a produção de il-10 e do óxido nítrico na leishmaniose visceral canina /

Silva, Kathlenn Liezbeth de Oliveira January 2016 (has links)
Orientador: Valéria Marçal Felix de Lima / Resumo: PD-1 ligado a PD-L1 ou PD-L2, desencadeia sinais incapacitantes às células T, podendo estar envolvidos na supressão das respostas imunes na LVC. Investigamos a expressão de PD-1 e seus ligantes no baço na LVC, e sua correlação com a carga parasitária. Para confirmar o seu papel regulador na leishmaniose, estes receptores foram avaliados após infecção in vitro por L. infantum. Em cães infectados, foi avaliado o bloqueio destes receptores na produção de citocinas e seus efeitos no sobrenadante da cultura, de linfoproliferação com antígeno solúvel (AtgS) de L. infantum. Foram selecionados 23 cães saudáveis e 54 com LV. PD-1 e seus ligantes foram determinados por imunohistoquímica em tecidos esplênicos. A carga parasitária de cães infectados foi avaliada por PCR em tempo real. As citocinas nos sobrenadantes de cultura foram determinados por ELISA de captura e o NO por Griess. A Linfoproliferação das células do linfonodo e expressão de PD-1 e seus ligantes após infecção in vitro por L. infantum foram avaliadas por citometria de fluxo. Observou-se que a infecção por L. infantum, aumenta a expressão de PD1 e seus ligantes. Uma correlação positiva foi observada entre a expressão de PD-1 e PD-L1 em linfócitos B e o aumento da carga parasitária. O bloqueio destes receptores restaura a proliferação de linfócitos, aumenta a produção de NO e diminui a IL-4 e IL-10. L. infantum modula a expressão de PD-1 e seus ligantes na LVC, suprimi a linfoproliferação, alterando a produção de citocinas... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: PD-1 when bound to PD-L1 or PD-L2, triggers signals disabling T cells, and they may be involved in the suppression of cellular immune responses in CVL. We investigated the expression of PD-1 and its ligands in spleen in CVL, and its correlation with parasite burden in this tissue, to confirm its regulatory role in leishmaniasis. These receptors were evaluated after in vitro infection by L. infantum. In infected dogs, we evaluated the blocking of these receptors in the production of cytokines in the effects of supernatant of cultured cells, and antigen specific lymphoproliferation. We selected 23 healthy dogs and 54 with VL. PD-1 and its ligands were determined by immunohistochemistry in splenic tissues. Parasitic load of infected dogs was evaluated by RT-PCR. Cytokines in culture supernatants were determined by capture ELISA and NO by Griess. Lymphoproliferation lymph nodes and expression of PD-1 and its ligand after in vitro infection by L. infantum was evaluated by flow cytometry. We observed that L. infantum infection increases expression of PD-1 and its ligands. A positive correlation was observed between the expression of PD-1 and PD-L1 B lymphocytes and an increase in parasite load. Blockade these receptors restores lymphocyte proliferation, increases the production of NO and decreases IL-4 and IL-10. In conclusion, L. infantum modulates expression of PD-1 and its ligands in CVL, suppressing lymphoproliferative response and altering cytokine production, which in turn ca... (Complete abstract click electronic access below) / Doutor
Leishmaniose.
Leishmaniose visceral.
Costimulatory molecules
Cães.
Moléculas coestimulatórias
2

Costimulatory molecules as genetic markers for relapse of Graves¡¦ disease

Chen, I-ya 23 March 2009 (has links)
Graves¡¦ disease (GD), an organ specific autoimmune disease, requires two signals to activate the T cells. In addition to the specific binding of T cell receptor to the antigenic peptide-MHC complex, an antigen-independent costimulatory pathway reportedly require generate subsequent cytokines and cell surface molecules. This regulation of T-cell response is a highly-organized multiple step program. T cell costimulatory signals is found to regulate the magnitude and duration of various type of autoimmune diseases. This study is to test whether genetic polymorphism of these costimulatory genes is related with the disease susceptibility or progression. We anticipated that the candidate genetic makers are beneficial for importing GD management. We recruited 262 GD patients from the Outpatient Department of Endocrine and 200 healthy controls from the Health Screening Center of Chang Gung Memorial Hospital in Kaohsiung.The GD patients were divided into three groups: recurred within 9 months (n=91), between 10-36 months (n=65), and more than 36 months (n=106). Clinical and laboratory attributes included: the genotypes of CTLA-4, CD28, ICOS, PD-1 and CD40; serum levels of T4, T3 and TSH; goiter size and TSH-receptor antibodies at the beginning and end of treatment. Genomic DNA was extracted from peripheral blood leucocytes by kit. The single nuclotide polymorphisms of the candidate genes were genotyped by polymerase chain reaction- restriction fragment length polymorphism and TaqMan® SNP Genotyping Assays with specific primers. Linkage disequilibuium between pairs of polymorphism was estimated by Haploview software. Haplotype analyses were performed using the Hap-Clustering program. Variance and correlation of data was statistically analyzed by Chi-square, general liner model, multiple logistic regression analysis and Kaplan-Meier plot. A p value <0.01 was considered significant. The results showed:(1) Genetic polymorphism within the costimulatory molecules affected the susceptibility and progression of GD; (2) GD patients carried more risk alleles than the controls; (3) Within the GD group, patients harboring more risk alleles wound relapse earlier after drug withdrawal; (4) Number of risk alleles, goiter size and TBII levels at end of treatment were independent predictors of disease relapse; (5) A risk score calculation based on odds ratio of risk alleles correlated with patients¡¦ relapse time after drug withdrawal. We concluded that patients¡¦ genetic makers of costimulatory molecules may be helpful in choosing appropriate treatment for GD.
CD40
PDCD-1
ICOS
CTLA-4
CD28
costimulatory factor
Graves' disease
haplotype
single nucleotide polymorphism
3

Follicular Dendritic Cells, Resting CD4+ T Cells and Human Immunodeficiency Virus Expression

Wang, Changna 04 September 2011 (has links) (PDF)
Many events associated with Human Immunodeficiency Virus (HIV) infection/replication occur in and around the germinal centers (GCs) of secondary lymphoid tissues where follicular dendritic cells (FDCs) reside, suggesting that this microenvironment may contribute unique signaling that is important to viral progression. My research focused on characterizing signaling, both positive and negative, contributed by FDCs that affects HIV infection and replication. Specifically, I determined if FDC signals could induce the expression of latent HIV in T cells and if so, to characterize the signaling pathways involved. Moreover, I also examined the ability of FDCs to produce inhibitory signals that might block active virus expression. I approached these problems using FDCs from tonsils and coculturing these with primary CD4+ T cells or latently-infected Jurket cells with a GFP reporter. Results indicated that FDCs dramatically augmented HIV production of these cells. FDC signaling was costimulatory in nature and was mediated by soluble TNFα. However, when ex vivo latently infected T cells were treated with PMA/ionomycin or IL2/IL7, little virus expression was observed until FDCs were added, which greatly increased virus production. The transcription factor NFAT is important for the reactivation of latent HIV. Inhibition studies as well as ELISA suggested that JAK/STAT signaling pathway was involved in virus reactivation. Because FDCs produce prostaglandins (PGs) E2 and I2, I determined the effect of PGE2 and PGI2 analogs on HIV infected T cells. Results indicated that both the PGE2 and PGI2 analogs inhibited proliferation and activation-induced cell death of HIV infected T cells in a dose- and time-dependent manner. Additionally, it was shown that indomethacin and CAY10404, cyclooxygenase and cyclooxygenase-2 inhibitors, partially restored HIV production in the presence of FDCs, suggesting that FDC-produced PGE2 and PGI2 may inhibit virus replication. Thus, FDCs produce PGs that can block virus gene expression in T cells, which may be ideal for viral persistence. Therefore, FDC signaling appears to both promote and inhibit HIV production. A better understanding of FDC signaling and regulation in GCs may suggest new treatment strategies that would be beneficial to infected subjects.
Follicular dendritic cell
HIV
resting CD4+ T cell
prostaglandin
costimulatory
Biochemistry
Chemistry
4

Two-signal requirement for the development of T lymphocytes

Zheng, Xincheng 02 March 2005 (has links)
No description available.
Health Sciences, Immunology
T lymphocyte development
NKT
costimulatory molecules
peripheral antigen expressing cells
immune tolerance
aire
5

Análise das células T regulatórias e expressão de moléculas coestimulatórias em células mononucleares de pacientes com Hanseníase com a produção de pacientes com Hanseníase e sua correlação com a produção de citocinas / T regulatory cells and expression of costimulatory molecules in peripheral blood mononuclear cells from patients with leprosy and their correlation with the cytokine secretion

Neves, Maria de Lourdes Palermo Fernandes 13 May 2013 (has links)
Introdução: Hanseníase, doença crônica, incapacitante, causada pelo M.leprae, que afeta a pele e os nervos periféricos. Manifesta-se como doença espectral, que exibe dois polos imunologicamente distintos, denominados hanseníase virchowiana (lepromatous - LL), caracterizada por uma resposta celular ineficiente; e hanseníase tuberculoide (Tuberculoid - TT), com resposta imune celular efetiva. A ativação de células T requer a sinalização através de moléculas coestimulatórias expressas em células apresentadoras de antígeno e seus ligantes nas células T. As células T regulatórias (Treg) exercem importante papel no mecanismo de falha do controle da disseminação antigênica nas formas graves das doenças crônicas granulomatosas, mas seu real papel na hanseníase ainda não foi elucidado. Métodos: Estudamos a expressão das moléculas coestimulatórias e células Treg na resposta imune de pacientes nos diferentes espectros da doença. A expressão de células Treg foi quantificada por citometria de fluxo (CD4+CD25+FoxP3+) nas células mononucleares do sangue periférico de pacientes e controles (16 eram virchowianos, 12 tuberculoides e 6 controles) estimulados in vitro com o antígeno do M. leprae e com o mitógeno phytohemaglutinina, bem como nas lesões de pele por imunohistoquímica. A expressão de moléculas coestimulatorias (CD80, CD86, CD28, CTLA-4, PD-1, ICOS) foi avaliada por citometria de fluxo in vitro, a partir do estimulo de células mononucleares provenientes de 14 pacientes virchowianos, 14 tuberculoides e 10 indivíduos saudáveis expostos ao bacilo. A resposta linfoproliferativa, a produção de citocinas (IL10 e IFN-?) in vitro e a expressão in situ de IL-10, TGF? e CTLA-4 também foram determinadas. Resultados: Nós demonstramos que pacientes virchowianos apresentam deficiência na expressão da molécula CD86 na superfície de monócitos, e isso contribui para uma apresentação antigênica ineficiente, favorecendo o estado de anergia observado nesse grupo de pacientes. Observamos ainda, que o bloqueio da expressão dessa molécula, mas não do CD80 inibe a resposta linfoproliferativa ao M.leprae. Ainda no polo virchowiano anérgico, observamos redução da expressão de moléculas coestimulatórias de sinalização positiva (CD28, CD86) na superfície dos linfócitos. Em contraste, nos pacientes tuberculoides notamos um aumento da expressão de moléculas de sinalização negativa (CTLA-4 e PD-1), que pode representar uma provável modulação da resposta imune exacerbada, regulando dessa forma os efeitos deletérios da hiperreatividade celular. Notavelmente, os contatos também expressão em menor intensidade CD86 e CD28, mas não se observou expressão exacerbada de CTLA-4 ou PD-1, sugerindo que eles provavelmente desenvolvem resposta imune balanceada sem que haja necessidade de sinalização imunossupressora. Observamos ainda, que o antígeno do M.leprae induz uma significativa redução da resposta linfoproliferativa, mas um aumento significativo de células Treg no sangue e na pele dos pacientes virchowianos, quando comparado ao grupo tuberculoide. Em paralelo, notamos o aumento da expressão de moléculas anti-inflamatórias (IL-10 e CTLA-4) nas lesões cutâneas desses pacientes virchowianos. Conclusão: Nossos resultados sugerem que células Treg e moléculas coestimulatórias desempenham papel importante na patogênese da hanseníase, especialmente no polo virchowiano, em que favoreceria a anergia e a multiplicação bacilar / Introduction: Leprosy, caused by the bacillus Mycobacterium leprae, is a chronic, incapacitating disease that affects the peripheral nerves and skin. Leprosy manifests as a spectral disease, exhibiting two polar sides, namely, lepromatous leprosy (LL) characterised by impaired T-cell responses and tuberculoid leprosy in which T-cell responses are strong. Proper T-cell activation requires signalling through costimulatory molecules expressed by antigen presenting cells and their ligands on T-cells. T regulatory cells (Tregs) play an important role in the mechanism of host\'s failure to control pathogen dissemination in severe forms of different chronic granulomatous diseases, but their role in leprosy has not yet been elucidated. The objective of this study was to investigate the influence of costimulatory molecules and Tregs cels on the immune responses of subjects along the leprosy spectrum. Patients and Methods: Tregs were quantified by flow cytometry (CD4+ CD25+ Foxp3+) in peripheral blood mononuclear cells (PBMC) of patients (16 lepromatous, 12 tuberculoids and controls (n = 6) stimulated in vitro with a M. leprae antigenic preparation and phytohemagglutinin as well as in skin lesions by immunohistochemistry. The expression of the costimulatory molecules (CD80, CD86, CD28, CTLA-4, PD-1, ICOS) was evaluated in in vitro-stimulated peripheral blood mononuclear cells isolated from 14 lepromatous and 14 tuberculoid patients, and 10 healthy individuals exposed to the bacillus. The lymphoproliferative (LPR), interleukin-10 (IL-10), and interferon-g (IFN-g) responses of the in vitro-stimulated peripheral blood mononuclear cells and the in situ expression of IL-10, transforming growth factor-b (TGF-b), and cytotoxic T-lymphocyte antigen 4 (CTLA-4) were also determined. Results: We show that lepromatous patients have defective monocytes\' CD86 expression, likely contributing to the impairment of the antigen presentation process and to their anergy. Accordingly, anti-CD86 blocking monoclonal antibody, but not anti-CD80 antibody, inhibited the lymphoproliferative response to Mycobacterium leprae. Consistent with the lepromatous pole anergy, there was reduced T-cells\' expression of the positive signaling costimulatory molecules CD28 and CD86 in these patients. Tuberculoid patients, on the other hand, had increased expression of the negative signaling CTLA-4 and PD-1 molecules, probably representing a means of modulating exacerbated immune response and avoiding immunopathology. Interestingly, contacts exhibited proper CD86 and CD28 expression, but not exacerbated CD152 and PD-1 expression, suggesting that they tend to develop a balanced immunity without requiring immunosuppressive costimulatory signaling. We also observed that M. leprae antigens induced significantly lower lymphoproliferation but significantly higher Treg numbers in lepromatous than tuberculoid patients and contacts. Mitogen-induced lymphoproliferation and Treg frequencies were not significantly different between the three groups. Tregs were also more frequent in situ in multibacillary patients, and this was paralleled by increased expression of the anti-inflammatory molecules IL-10 and CTLA-4, but not TGF. Conclusion: Our results suggest that Tregs and costimuatory molecules play a major role in the pathogenesis of leprosy, especially the lepromatous pole, in which they would act to favor the anergy and the unrestricted multiplication of the bacilli
Costimulatory molecules B7.1
Costimulatory molecules B7.2
Hanseníase
Interferon gama
Interferon-gamma
Interleucina-10
Interleukin-10
Leprosy
Linfócitos T reguladores
Molécula coestimuladora B7-1
Molécula coestimuladora B7-2
Mycobacterium leprae
Mycobacterium leprae
Regulatory T-Lymphocytes
6

Análise das células T regulatórias e expressão de moléculas coestimulatórias em células mononucleares de pacientes com Hanseníase com a produção de pacientes com Hanseníase e sua correlação com a produção de citocinas / T regulatory cells and expression of costimulatory molecules in peripheral blood mononuclear cells from patients with leprosy and their correlation with the cytokine secretion

Maria de Lourdes Palermo Fernandes Neves 13 May 2013 (has links)
Introdução: Hanseníase, doença crônica, incapacitante, causada pelo M.leprae, que afeta a pele e os nervos periféricos. Manifesta-se como doença espectral, que exibe dois polos imunologicamente distintos, denominados hanseníase virchowiana (lepromatous - LL), caracterizada por uma resposta celular ineficiente; e hanseníase tuberculoide (Tuberculoid - TT), com resposta imune celular efetiva. A ativação de células T requer a sinalização através de moléculas coestimulatórias expressas em células apresentadoras de antígeno e seus ligantes nas células T. As células T regulatórias (Treg) exercem importante papel no mecanismo de falha do controle da disseminação antigênica nas formas graves das doenças crônicas granulomatosas, mas seu real papel na hanseníase ainda não foi elucidado. Métodos: Estudamos a expressão das moléculas coestimulatórias e células Treg na resposta imune de pacientes nos diferentes espectros da doença. A expressão de células Treg foi quantificada por citometria de fluxo (CD4+CD25+FoxP3+) nas células mononucleares do sangue periférico de pacientes e controles (16 eram virchowianos, 12 tuberculoides e 6 controles) estimulados in vitro com o antígeno do M. leprae e com o mitógeno phytohemaglutinina, bem como nas lesões de pele por imunohistoquímica. A expressão de moléculas coestimulatorias (CD80, CD86, CD28, CTLA-4, PD-1, ICOS) foi avaliada por citometria de fluxo in vitro, a partir do estimulo de células mononucleares provenientes de 14 pacientes virchowianos, 14 tuberculoides e 10 indivíduos saudáveis expostos ao bacilo. A resposta linfoproliferativa, a produção de citocinas (IL10 e IFN-?) in vitro e a expressão in situ de IL-10, TGF? e CTLA-4 também foram determinadas. Resultados: Nós demonstramos que pacientes virchowianos apresentam deficiência na expressão da molécula CD86 na superfície de monócitos, e isso contribui para uma apresentação antigênica ineficiente, favorecendo o estado de anergia observado nesse grupo de pacientes. Observamos ainda, que o bloqueio da expressão dessa molécula, mas não do CD80 inibe a resposta linfoproliferativa ao M.leprae. Ainda no polo virchowiano anérgico, observamos redução da expressão de moléculas coestimulatórias de sinalização positiva (CD28, CD86) na superfície dos linfócitos. Em contraste, nos pacientes tuberculoides notamos um aumento da expressão de moléculas de sinalização negativa (CTLA-4 e PD-1), que pode representar uma provável modulação da resposta imune exacerbada, regulando dessa forma os efeitos deletérios da hiperreatividade celular. Notavelmente, os contatos também expressão em menor intensidade CD86 e CD28, mas não se observou expressão exacerbada de CTLA-4 ou PD-1, sugerindo que eles provavelmente desenvolvem resposta imune balanceada sem que haja necessidade de sinalização imunossupressora. Observamos ainda, que o antígeno do M.leprae induz uma significativa redução da resposta linfoproliferativa, mas um aumento significativo de células Treg no sangue e na pele dos pacientes virchowianos, quando comparado ao grupo tuberculoide. Em paralelo, notamos o aumento da expressão de moléculas anti-inflamatórias (IL-10 e CTLA-4) nas lesões cutâneas desses pacientes virchowianos. Conclusão: Nossos resultados sugerem que células Treg e moléculas coestimulatórias desempenham papel importante na patogênese da hanseníase, especialmente no polo virchowiano, em que favoreceria a anergia e a multiplicação bacilar / Introduction: Leprosy, caused by the bacillus Mycobacterium leprae, is a chronic, incapacitating disease that affects the peripheral nerves and skin. Leprosy manifests as a spectral disease, exhibiting two polar sides, namely, lepromatous leprosy (LL) characterised by impaired T-cell responses and tuberculoid leprosy in which T-cell responses are strong. Proper T-cell activation requires signalling through costimulatory molecules expressed by antigen presenting cells and their ligands on T-cells. T regulatory cells (Tregs) play an important role in the mechanism of host\'s failure to control pathogen dissemination in severe forms of different chronic granulomatous diseases, but their role in leprosy has not yet been elucidated. The objective of this study was to investigate the influence of costimulatory molecules and Tregs cels on the immune responses of subjects along the leprosy spectrum. Patients and Methods: Tregs were quantified by flow cytometry (CD4+ CD25+ Foxp3+) in peripheral blood mononuclear cells (PBMC) of patients (16 lepromatous, 12 tuberculoids and controls (n = 6) stimulated in vitro with a M. leprae antigenic preparation and phytohemagglutinin as well as in skin lesions by immunohistochemistry. The expression of the costimulatory molecules (CD80, CD86, CD28, CTLA-4, PD-1, ICOS) was evaluated in in vitro-stimulated peripheral blood mononuclear cells isolated from 14 lepromatous and 14 tuberculoid patients, and 10 healthy individuals exposed to the bacillus. The lymphoproliferative (LPR), interleukin-10 (IL-10), and interferon-g (IFN-g) responses of the in vitro-stimulated peripheral blood mononuclear cells and the in situ expression of IL-10, transforming growth factor-b (TGF-b), and cytotoxic T-lymphocyte antigen 4 (CTLA-4) were also determined. Results: We show that lepromatous patients have defective monocytes\' CD86 expression, likely contributing to the impairment of the antigen presentation process and to their anergy. Accordingly, anti-CD86 blocking monoclonal antibody, but not anti-CD80 antibody, inhibited the lymphoproliferative response to Mycobacterium leprae. Consistent with the lepromatous pole anergy, there was reduced T-cells\' expression of the positive signaling costimulatory molecules CD28 and CD86 in these patients. Tuberculoid patients, on the other hand, had increased expression of the negative signaling CTLA-4 and PD-1 molecules, probably representing a means of modulating exacerbated immune response and avoiding immunopathology. Interestingly, contacts exhibited proper CD86 and CD28 expression, but not exacerbated CD152 and PD-1 expression, suggesting that they tend to develop a balanced immunity without requiring immunosuppressive costimulatory signaling. We also observed that M. leprae antigens induced significantly lower lymphoproliferation but significantly higher Treg numbers in lepromatous than tuberculoid patients and contacts. Mitogen-induced lymphoproliferation and Treg frequencies were not significantly different between the three groups. Tregs were also more frequent in situ in multibacillary patients, and this was paralleled by increased expression of the anti-inflammatory molecules IL-10 and CTLA-4, but not TGF. Conclusion: Our results suggest that Tregs and costimuatory molecules play a major role in the pathogenesis of leprosy, especially the lepromatous pole, in which they would act to favor the anergy and the unrestricted multiplication of the bacilli
Hanseníase
Interferon gama
Interleucina-10
Linfócitos T reguladores
Molécula coestimuladora B7-1
Molécula coestimuladora B7-2
Mycobacterium leprae
Costimulatory molecules B7.1
Costimulatory molecules B7.2
Interferon-gamma
Interleukin-10
Leprosy
Mycobacterium leprae
Regulatory T-Lymphocytes
7

Avaliação da eficiência do antagonista seletivo de CD28, mPEG PV1-Fab´, no tratamento da uveíte autoimune experimental. / Efficacy of murine selective CD28 antagonist for the treatment of experimental autoimmune uveitis.

Rosa, Pedro Henrique Papotto 08 December 2014 (has links)
A uveíte autoimune é uma doença inflamatória crônica, caracterizada pela resposta imune a antígenos oculares. É mediada por linfócitos T CD4+ com perfil TH1, e responsável por uma parcela significativa de casos de deficiências visuais e cegueira. Embora efetivos, os tratamentos disponíveis estão associados a efeitos adversos importantes. Logo, a busca de novos alvos terapêuticos mais específicos tem sido o objetivo principal no campo da imunoterapia. Nesse trabalho foi avaliada a eficiência do antagonista seletivo de CD28, mPEG PV1-Fab´(PV1), no tratamento da uveíte autoimune experimental (EAU). Camundongos tratados com PV1 exibiram menores graus de doença quando comparados a controles não tratados. Tal achado foi acompanhado de uma diminuição da ativação de linfócitos T, tanto nos olhos quanto nos órgãos linfoides periféricos desses animais. Mais ainda, o tratamento com PV1 levou a uma diminuição da população de linfócitos T reguladores e de células do tipo TH1. Portanto, concluiu-se que PV1 é eficaz no tratamento da EAU por agir em linfócitos T efetores. / Autoimmune uveitis is a T-cell mediated disease that targets mainly the posterior eye pole. Similar to human uveitis, experimental autoimmune uveitis (EAU) is mostly dependent on T cells with a TH1 phenotype. Although many treatment strategies are available, most of them focus on general immunossuppression, resulting in undesirable side effects. Thus, the development of more specific therapies is the major aim in the field of immunotherapy. Here we evaluated the efficacy of mPEG PV-1-Fab´ (PV1), a specific CD28 antagonist, in the treatment of EAU. Our results indicate that PV1 blocks T cell activation by decreasing expression of different costimulatory molecules. Furthermore, PV1 treatment led to a decrease of Treg cell population in peripheral lymphoid organs. Also, IFN-g production by CD4+ cells and TH1 lymphocytes population were decreased. Altogether, our results raise this CD28 blockade strategy as a potential tool for the treatment of autoimmune disorders in the eye, and indicate that mPEG PV1-Fab acts mainly on IFN-g production and TH1 polarization.
Bloqueio co-­estimulatório
CD28
CD28
Costimulatory blockade
EAU
EAU
IFN-­gamma
IFN-­gamma
Th1
Th1
Uveíte
Uveitis
8

O microquimerismo e a importância das células da medula óssea do doador semi-alogênico na sobrevivência do enxerto. / Microchimerism and the importance of semi-allogeneic donor-derived bone marrow cells in graft survival.

Moraes, Luciana de Deus Vieira de 17 April 2003 (has links)
A indução de tolerância ao enxerto através da administração de células do doador, em períodos que antecedem o transplante, tem se demonstrado eficiente, mesmo em receptores não imunosuprimidos. Os dados da literatura científica são conflitantes quanto ao vínculo entre o microquimerismo e a tolerância aos aloantígenos. No presente estudo, observou-se que a infusão da mistura de células do baço com as da medula óssea, provenientes do doador (BALB/c x C57BI/6)F1, vinte e um dias antes do transplante, resultou em aumento do tempo de sobrevivência dos enxertos de pele e cardíaco, em parentais BALB/c, principalmente quando comparado ao grupo de animais que receberam somente as células do baço do mesmo doador. Assim, procurou-se investigar o estabelecimento do microquimerismo, sua relação com o aumento do tempo de sobrevivência do enxerto e possíveis mecanismos envolvidos. Observou-se um aumento de IL-10 no sobrenadante de cultura das células esplênicas provenientes de animais inoculados com a suspensão mista de células. Em contrapartida, os camundongos que receberam apenas as células do baço apresentaram um aumento da população de linfócitos B. Verificou-se, ainda, que o desenvolvimento de microquimerismo estável não se correlacionou com a tolerância ao enxerto cardíaco, apesar do tempo de sobrevivência do órgão. Esses resultados sugerem que a IL-10 participa no aumento da sobrevida do mesmo quando células do baço com as da medula óssea do doador são administradas antes do transplante. / Tolerance induction to allografts by the administration of donor cells before transplantation has been shown to be efficient, even in non immunosuppressed hosts. There are conflicting reports in the literature regarding the role of microchimerism and tolerance to alloantigens. In the present work, augmentation of skin and cardiac survival time was observed after the infusion of a mixture of donor (BALB/c x C57BI/6)F1 spleen and bone marrow cells twenty-one days before transplantation, specially when compared to donor spleen cell receptors. The establishment of microchimerism, correlation with graft survival time and possible mechanisms involved in this strategy were investigated. An overproduction of IL-10 in the supernatants from spleen cell cultures of mice inoculated with semi-allogeneic cells was observed. Mice that received donor spleen cells only showed increased number of B lymphocytes. Moreover, the establishment of microchimerism did not correlate to tolerance to cardiac allografts despite the augmentation of graft survival time. These results suggest that the development of microchimerism does not prevent graft rejection and that there is a role for IL-10 in graft survival when donor spleen and bone marrow cells are infused before transplantation.
Baço
Bone marrow
Costimulatory molecules
IL-10
IL-10
Medula óssea
Microchimerism
Microquimerismo
Moléculas co-estimuladoras
Rejection
Rejeição
Spleen
9

Le rôle biologique de l’interaction du CD40L avec l’intégrine α5β1 des lymphocytes T.

Naddaf, Nadim 02 1900 (has links)
Le CD40 ligand (CD40L) est un régulateur important de la réponse immunitaire et un contributeur clé dans les maladies auto-immunes. Nous avons rapporté précédemment que le CD40L se liait à l’intégrine α5β1, toutefois, les conséquences fonctionnelles de cette interaction demeurent inconnues. Les lymphocytes T sont au centre de la pathogénèse des maladies auto-immunes. Ils expriment, lors de celles-ci, des quantités aberrantes d’intégrines β1 faisant en sorte que la liaison CD40L/α5β1 pourrait être d’une haute importance dans les réponses inflammatoires. Dans cette étude, nous avons démontré que la forme soluble du CD40L (sCD40L) se liait aux lymphocytes T primaires ainsi qu’aux cellules Jurkat E6.1 et ce, dépendamment de l’intégrine α5β1. L’interaction du CD40L avec l’α5β1 lymphocytaire a induit l’activation des voies anti-apoptotiques dont les MAPKs (les protéines kinases mitogène activée) et les PI3 kinases (PI3K). La liaison du sCD40L à l’α5β1 n’a pas induit son changement structural ni son adhésion à la FN (fibronectine). Ceci pourrait avoir des conséquences directes sur la survie des cellules T lors de la progression des maladies inflammatoires. Ces résultats soulignent l’impact de l’interaction CD40L/α5β1 sur la fonction biologique des lymphocytes T et ils pourraient expliquer leur survie et leur persistance au niveau des sites d’inflammations durant les maladies auto- immunes. / CD40 ligand (CD40L) is a critical regulator of the immune response and a key contributor to autoimmune diseases. We have previously reported that CD40L binds to α5β1, albeit the functional consequences of this interaction remain elusive. T cells are central to the pathogenesis of autoimmune diseases and express high levels of β1 integrins in disease conditions, making the CD40L/α5β1 interaction a potential axis of significant importance in inflammatory complications. Here, we show that soluble CD40L (sCD40L) binds to freshly isolated primary T cells and to Jurkat E6.1 T cells in a α5β1-dependant manner. This leads to the activation of key survival proteins, including the mitogen-activated protein kinases (MAPKs) and the Akt PI3 kinase (PI3K). Binding of sCD40L to α5β1 does not induce its conformational change nor allow adherence to fibronectin. These results highlight the impact of the CD40L/α5β1 interaction in T-cell function and may explain the link between sCD40L and T-cell survival and persistence in inflammatory diseases.
Inflammation
Intégrines
Survie cellulaire
Molécules costimulatrices
inflammation
Integrins
Cell survival
costimulatory molecules
10

Le rôle biologique de l’interaction du CD40L avec l’intégrine α5β1 des lymphocytes T

Naddaf, Nadim 02 1900 (has links)
No description available.
Inflammation
Intégrines
Survie cellulaire
Molécules costimulatrices
inflammation
Integrins
Cell survival
costimulatory molecules

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