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Master's Dissertation
DOI
https://doi.org/10.11606/D.9.2013.tde-27032014-161621
Document
Author
Full name
Grasielle Pereira Jannuzzi
E-mail
Institute/School/College
Knowledge Area
Date of Defense
Published
São Paulo, 2013
Supervisor
Committee
Ferreira, Karen Spadari (President)
Batista, Wagner Luiz
Taborda, Carlos Pelleschi
Title in Portuguese
Caracterização fenotípica de células dendríticas transfectadas com scFv obtido a partir de anticorpo monoclonal anti-idiotípico Ab2-β, que mimetiza o antígeno gp43 de Paracoccidioides brasiliensis
Keywords in Portuguese
Células dendríticas
Paracoccidioidomicose
scFv
Abstract in Portuguese
A paracoccidioidomicose (PCM) é um a micose profunda de natureza granulomatosa, causada pelo fungo Paracoccidioides brasiliensis (P. brasiliensis) e que compromete preferencialmente o tecido pulmonar. O P. brasiliensis sintetiza várias substâncias, dentre estas, destaca-se a glicoproteína de 43 kDa (gp43), a qual é considerada o principal componente antigênico do fungo. Dada a importância da gp43, anticorpos monoclonais (Mabs) contra esta glicoproteína foram obtidos e posteriormente caracterizados. Baseado na hipótese da rede idiotípica, Jerne (1974) propôs que cada anticorpo, quando produzido em resposta a um antígeno, induz a formação de outros anticorpos dirigidos contra sua região variável, na qual é única. Anticorpos anti-idiotípicos, que reconhecem o paratopo, contendo a imagem interna do antígeno, são denominados de Ab2-β e seu potencial terapêutico tem sido explorado em diferentes sistemas. Apesar da molécula de anticorpo ser complexa estruturalmente, sabemos que a região Fab, é a responsável pelo mimetismo do antígeno. Então, nosso grupo de pesquisa construiu uma nova molécula de anticorpo à partir do Mab anti-idiotípico Ab2-β, que mimetiza o antígeno gp43 de P. brasiliensis, denominada de fragmento variável de cadeia única (scFv). A transfecção dessa molécula em células dendríticas (DCs) mostrou ser promissora na PCM experimental, visto que estes transfectomas foram eficientes em apresentar a proteína scFv às células dos linfonodos, induzindo linfoproliferação, além de diminuírem a carga fúngica pulmonar. Visto que a molécula de scFv que possui a região de reconhecimento e ativação de linfócitos T mostrou eficiência no modelo de terapia na PCM experimental, o principal objetivo deste trabalho foi analisar os mecanismos pelos quais os transfectomas de DCs ativam a resposta imune em camundongos infectados com o fungo, para que possamos entender melhor a capacidade destas células em modular a resposta imune na PCM experimental. Dessa maneira, avaliamos a capacidade das DCs trasfectadas com pMAC/PS-scFv em migrar para os linfonodos regionais e induzirem uma resposta protetora com produção de IgG, bem como, analisamos o fenótipo destas células e produção de citocinas. Nosso modelo de terapia com pMAC/PS-scFv mostrou-se eficiente, uma vez que observamos diminuição de células T regulatórias nos linfonodos regionais, bem como aumento da produção de citocinas como IFN-γ e IL-12. Ainda, observamos aumento do isotipo IgG2b, sugerindo a modulação de resposta imune para o tipo Th1, importante na proteção da PCM.
Title in English
Phenotypic characterization of dendritic cells transfected with scFv derived from monoclonal anti-β-idiotypic Ab2 which mimics the antigen gp43 of Paracoccidioides brasiliensis
Keywords in English
Dendritic cells
Paracoccidioidomycosis
scFv
Abstract in English
The paracoccidioidomycosis (PCM) is the nature of granulomatous mycosis caused by Paracoccidioides brasiliensis (P. brasiliensis) and preferentially compromises lung tissue. The P. brasiliensis synthesizes various substances, among these, there is a 43 kDa glycoprotein (gp43), which is considered a major antigenic component of the fungus. Given the importance of gp43 monoclonal antibodies (Mabs) against this glycoprotein were obtained and further characterized. Based on the idiotypic network hypothesis, Jerne (1974) proposed that each antibody, when produced in response to an antigen, induces the several of other antibodies production against its variable region, which is unique. Anti-idiotypic antibodies that recognize the paratope containing the internal image of the antigen are called Ab2 β and their therapeutic potential has been explored in different systems. Although the antibody molecule is structurally complex, we know that the Fab region, is responsible for antigen mimicking. Therefore, our research group has engineered a new molecule from the antibody Mab-anti-idiotypic Ab2 β that mimics the antigen gp43 of P. brasiliensis, known as single chain variable fragment (scFv). Transfection of this molecule on dendritic cells (DCs) has shown promise in experimental PCM, since these transfection were effective scFv protein present in the cells of the lymph nodes, inducing lymphoproliferation, in addition to reducing fungal burden in the lung. Since the scFv molecule that has the region recognition and activation of T lymphocytes showed efficiency in therapy model in experimental PCM, the main objective of this study was to analyze the mechanisms by which transfected DCs activate the immune response in infected mice with the fungus, so that we can better understand the ability of these cells to modulate the immune response in experimental PCM. Thus, the capacity of transfected DCs with pMAC / PS-scFv to migrate to regional lymph nodes and induce a protective response with IgG production, as well as analyze the phenotype of these cells and cytokine production. Our therapy model with pMAC / PS-scFv was efficient, since we observed decrease of regulatory T cells in regional lymph nodes, as well as increased production of cytokines such as IFN-γ and IL-12. Furthermore, we observed increased IgG2b isotype, suggesting modulation of the immune response to a Th1 response, the protect model of experimental PCM.
 
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Publishing Date
2014-04-15
 
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