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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.
1

Prediktivní a prognostické faktory nádoru žaludku / Predictive and prognostic factors of gastric cancer

Šmíd, David January 2016 (has links)
Predictive and prognostic factors in gastric cancer Šmíd D. Surgical clinic of University Hospital in Pilsen and Faculty of Medicine in Pilsen, Charles University in Prague. Introduction: Gastric cancer is one of malignant diseases which have the worst prognosis. Unfortunately, there are most patients with advanced-stage disease who have to be treated in a palliative way. Patients suffered from the same type of tumor, being at the same stage of disease and treated with the same chemotherapy have various rates of survival, which can be caused by diverse expression of selected genes impacting on the mechanism of cytostatic effects. The determination of these genes or microRNAs which regulate these genes could be used as a predictive factor for prediction of effects of administered chemotherapy. The determination of some microRNAs, or in the combination with suitable plasmatic factors, could be used as a prognostic factor for patients with gastric cancer. It is also possible to use this combination for early diagnosis of cancerogenesis Object: The aim is to verify the possibility to use expression of selected genes and some microRNAs in tumor tissue as a prognostic factor or a predictor for therapeutic effects of chemotherapy in patients with gastric cancer. Methodology: We retrospectively evaluated the group...
2

Prediktivní a prognostické faktory nádoru žaludku / Predictive and prognostic factors of gastric cancer

Šmíd, David January 2016 (has links)
Predictive and prognostic factors in gastric cancer Šmíd D. Surgical clinic of University Hospital in Pilsen and Faculty of Medicine in Pilsen, Charles University in Prague. Introduction: Gastric cancer is one of malignant diseases which have the worst prognosis. Unfortunately, there are most patients with advanced-stage disease who have to be treated in a palliative way. Patients suffered from the same type of tumor, being at the same stage of disease and treated with the same chemotherapy have various rates of survival, which can be caused by diverse expression of selected genes impacting on the mechanism of cytostatic effects. The determination of these genes or microRNAs which regulate these genes could be used as a predictive factor for prediction of effects of administered chemotherapy. The determination of some microRNAs, or in the combination with suitable plasmatic factors, could be used as a prognostic factor for patients with gastric cancer. It is also possible to use this combination for early diagnosis of cancerogenesis Object: The aim is to verify the possibility to use expression of selected genes and some microRNAs in tumor tissue as a prognostic factor or a predictor for therapeutic effects of chemotherapy in patients with gastric cancer. Methodology: We retrospectively evaluated the group...
3

Estudo do compartimento de linfócitos T CD4+ em pacientes com LLC-B: distribuição das subpopulações TH1, TH2, TH17 e TREG e avaliação da expressão de FAS e FASL. / Study of the CD4+ T lymphocytes in B-CLL patients: distribution of Th1, Th2, Th17 and Treg and expression of FAS and FASL.

Silva, Flávia Amoroso Matos e 17 October 2014 (has links)
LLC-B é uma neoplasia hematológica derivada de uma população de linfócitos B maduros CD5+ localizados na zona do manto dos folículos linfóides e é a mais comum das doenças linfoproliferativas. É uma doença clinicamente heterogênea na qual certos pacientes apresentam quadros indolentes que durante muitos anos podem ser controlados com pouco ou nenhum tratamento. Relatos da literatura sugerem que os linfócitos T na LLC-B podem ser incapazes de iniciar, manter e concluir uma resposta imune para a célula B maligna e outros antígenos, e podem estar diretamente envolvidos na manutenção do tumor. Os linfócitos são ativados, proliferam e polarizam sua resposta para padrões pro-inflamatórios ou antiinflamatórios, aumentando sua população e tornando-se capazes para realizar suas funções efetoras. Embora o processo de ativação dos linfócitos Th seja indispensável para a defesa do hospedeiro, é necessário que haja um equilíbrio homeostático, onde as células auto-reativas ou recorrentemente ativadas sejam eliminadas. A esse último mecanismo de manutenção do equilíbrio imunológico, dá-se o nome de Tolerância Periférica, sendo que o processo de morte celular induzida por ativação (AICD) constitui um dos principais mecanismos para sua manutenção. Assim, neste estudo também foram analisados membros do grupo de receptores de membrana da superfamília dos receptores de fatores de necrose tumoral (tumor necrosis factor receptor, TNFR). Esta família TNFR inclui diversos receptores, entre eles o FAS (CD95) e seu ligante FASL. O objetivo central deste trabalho é investigar alterações no compartimentos de linfócitos T como, Th1, Th2, Th17 e Treg, bem como membros da via extrínseca de morte, FAS e FASL nos linfócitos T CD4+. Os resultados mostraram que o número absoluto dos linfócitos T CD4+, CD8+ e Th1 é heterogêneo, sendo que alguns pacientes apresentaram aumento e outros diminuição destas células quando comparados com o grupo controle do estudo. Em relação a expressão de FAS e FASL os resultados também apresentaram heterogeneidade. Sendo assim foi analisado cada paciente e comparados com os fatores de prognósticos e dados clínicos em cada caso. Ainda há muito para ser investigado, mas este trabalho tem como perspectivas buscar melhor entendimento da participação dos linfócitos T CD4+ nas LLC-B, expandindo as possibilidade de tratamento e busca de novos alvos terapêuticos. / B-CLL is a hematologic malignancy derived from a mature population of CD5+ Blymphocytes located in the mantle zone of the lymphoid follicles and is the most common lymphoproliferative disorders. It is a clinically heterogeneous disorder in which patients have certain frames idle for many years that can be controlled with little or no treatment. Literature reports suggest that T lymphocytes in B-CLL may be unable to initiate, sustain and complete an immune response to the malignant B cell and other antigens, and may be directly involved in tumor maintenance. The lymphocytes are activated, proliferate and polarize their response patterns to pro-inflammatory or anti-inflammatory, increasing its population and becoming able to perform their effector functions. Although the process of Th lymphocyte activation is essential for host defense, there must be a homeostatic balance, where autoreactive cells are eliminated or recurrently activated. The latter mechanism of maintenance of immune balance, gives the name of Peripheral Tolerance, and the process of activation-induced cell death (AICD) is a major mechanism for its maintenance. In this study group members of the superfamily of membrane receptors of tumor necrosis factor (tumor necrosis factor receptor, TNFR) receptors were also analyzed. The TNFR family includes many receptors, including FAS (CD95) and its ligand FasL. The central objective of this study is to investigate changes in T lymphocyte compartments as Th1, Th2, Th17 and Treg as well as members of the extrinsic death pathway, FAS and FASL in CD4+ lymphocytes. The results showed that the absolute number of CD4+, CD8+ and Th1 lymphocytes is heterogeneous, with some patients showed an increase and others decrease of these cells when compared with the control group of the study. Regarding the expression of FAS and FASL results also showed heterogeneity. Thus each patient was analyzed and compared to the prognostic factors and to clinical data in each case. Much remains to be investigated, but this work has the prospects look better understanding of the role of the B-CLL CD4+ T lymphocytes, expanding the possibilities of treatment and the search for new therapeutic targets.
4

Estudo do compartimento de linfócitos T CD4+ em pacientes com LLC-B: distribuição das subpopulações TH1, TH2, TH17 e TREG e avaliação da expressão de FAS e FASL. / Study of the CD4+ T lymphocytes in B-CLL patients: distribution of Th1, Th2, Th17 and Treg and expression of FAS and FASL.

Flávia Amoroso Matos e Silva 17 October 2014 (has links)
LLC-B é uma neoplasia hematológica derivada de uma população de linfócitos B maduros CD5+ localizados na zona do manto dos folículos linfóides e é a mais comum das doenças linfoproliferativas. É uma doença clinicamente heterogênea na qual certos pacientes apresentam quadros indolentes que durante muitos anos podem ser controlados com pouco ou nenhum tratamento. Relatos da literatura sugerem que os linfócitos T na LLC-B podem ser incapazes de iniciar, manter e concluir uma resposta imune para a célula B maligna e outros antígenos, e podem estar diretamente envolvidos na manutenção do tumor. Os linfócitos são ativados, proliferam e polarizam sua resposta para padrões pro-inflamatórios ou antiinflamatórios, aumentando sua população e tornando-se capazes para realizar suas funções efetoras. Embora o processo de ativação dos linfócitos Th seja indispensável para a defesa do hospedeiro, é necessário que haja um equilíbrio homeostático, onde as células auto-reativas ou recorrentemente ativadas sejam eliminadas. A esse último mecanismo de manutenção do equilíbrio imunológico, dá-se o nome de Tolerância Periférica, sendo que o processo de morte celular induzida por ativação (AICD) constitui um dos principais mecanismos para sua manutenção. Assim, neste estudo também foram analisados membros do grupo de receptores de membrana da superfamília dos receptores de fatores de necrose tumoral (tumor necrosis factor receptor, TNFR). Esta família TNFR inclui diversos receptores, entre eles o FAS (CD95) e seu ligante FASL. O objetivo central deste trabalho é investigar alterações no compartimentos de linfócitos T como, Th1, Th2, Th17 e Treg, bem como membros da via extrínseca de morte, FAS e FASL nos linfócitos T CD4+. Os resultados mostraram que o número absoluto dos linfócitos T CD4+, CD8+ e Th1 é heterogêneo, sendo que alguns pacientes apresentaram aumento e outros diminuição destas células quando comparados com o grupo controle do estudo. Em relação a expressão de FAS e FASL os resultados também apresentaram heterogeneidade. Sendo assim foi analisado cada paciente e comparados com os fatores de prognósticos e dados clínicos em cada caso. Ainda há muito para ser investigado, mas este trabalho tem como perspectivas buscar melhor entendimento da participação dos linfócitos T CD4+ nas LLC-B, expandindo as possibilidade de tratamento e busca de novos alvos terapêuticos. / B-CLL is a hematologic malignancy derived from a mature population of CD5+ Blymphocytes located in the mantle zone of the lymphoid follicles and is the most common lymphoproliferative disorders. It is a clinically heterogeneous disorder in which patients have certain frames idle for many years that can be controlled with little or no treatment. Literature reports suggest that T lymphocytes in B-CLL may be unable to initiate, sustain and complete an immune response to the malignant B cell and other antigens, and may be directly involved in tumor maintenance. The lymphocytes are activated, proliferate and polarize their response patterns to pro-inflammatory or anti-inflammatory, increasing its population and becoming able to perform their effector functions. Although the process of Th lymphocyte activation is essential for host defense, there must be a homeostatic balance, where autoreactive cells are eliminated or recurrently activated. The latter mechanism of maintenance of immune balance, gives the name of Peripheral Tolerance, and the process of activation-induced cell death (AICD) is a major mechanism for its maintenance. In this study group members of the superfamily of membrane receptors of tumor necrosis factor (tumor necrosis factor receptor, TNFR) receptors were also analyzed. The TNFR family includes many receptors, including FAS (CD95) and its ligand FasL. The central objective of this study is to investigate changes in T lymphocyte compartments as Th1, Th2, Th17 and Treg as well as members of the extrinsic death pathway, FAS and FASL in CD4+ lymphocytes. The results showed that the absolute number of CD4+, CD8+ and Th1 lymphocytes is heterogeneous, with some patients showed an increase and others decrease of these cells when compared with the control group of the study. Regarding the expression of FAS and FASL results also showed heterogeneity. Thus each patient was analyzed and compared to the prognostic factors and to clinical data in each case. Much remains to be investigated, but this work has the prospects look better understanding of the role of the B-CLL CD4+ T lymphocytes, expanding the possibilities of treatment and the search for new therapeutic targets.

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