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21	Monitoring of azathioprine therapy in pediatric population : relationship between pharmacokinetics pharmacodynamics in inflammatory bowel disease (IBD) and autoimmune hepatitis (AIH) / Optimisation thérapeutique de l’azathioprine dans la population pédiatrique : relation pharmacocinétique pharmacodynamie dans la maladie inflammatoire de l’intestin et dans l’hépatite autoimmune Nguyen, Thi Van Anh 03 July 2013 (has links) La présente étude a pour objectif de mettre en évidence l‘intérêt du suivi thérapeutique pharmacologique (STP) des métabolites thiopuriques en vue de l‘optimisation du traitement par l‘azathioprine chez les enfants atteints de maladie inflammatoire de l‘intestin et d‘hépatite autoimmune. Les travaux réalisés nous ont permis de montrer, en utilisant une analyse multi-niveaux, une corrélation significative entre la dose d‘azathioprine et les concentrations en 6-TGN et Me6-MPN ainsi qu‘avec le ratio Me6-MPN/6-TGN confortant l‘utilisation des métabolites pour ajuster la posologie d‘azathioprine chez les enfants présentant une maladie inflammatoire de l‘intestin. Différents facteurs pouvant modifier les concentrations de métabolites thiopuriques ont été identifiés. La co-administration d‘infliximab a conduit à une augmentation significative des concentrations de 6-TGN. Des concentrations plus faibles de 6-TGN ont été observées chez les jeunes enfants suggérant l‘influence de l‘âge sur le métabolisme ou sur l‘absorption de l‘azathioprine. Nous avons également montré qu‘une concentration de 6-TGN supérieure à 405 pmol/8.108RBCs chez des patients ayant une activité TPMT normale et pour lesquels la rémission clinique n‘a pas pu être obtenue en l‘absence de stéroïdes, était prédictive d‘une résistance à l‘azathioprine. Un seuil de 250 pmol/8.108RBCs en 6-TGN est significativement associé à une meilleure réponse thérapeutique. D‘autre part, une corrélation a été observée entre les métabolites thiopuriques et la leucopénie. Chez les enfants atteints d‘hépatite autoimmune, une corrélation positive entre la dose d‘azathioprine et les concentrations de métabolites a été retrouvée. L‘importante variabilité inter-individuelle dans les concentrations en métabolites thiopuriques et dans la réponse thérapeutique a été confirmée démontrant l‘intérêt d‘une individualisation de la thérapeutique. L‘instauration d‘un STP des métabolites thiopuriques associé au suivi hématologique, à la détermination de la TPMT et au suivi clinique paraît justifié afin d‘optimiser la thérapeutique par l‘azathioprine dans la population pédiatrique / The present study aimed to investigate the usefulness of thiopurine metabolite monitoring in pediatric inflammatory bowel disease (IBD) and Autoimmune Hepatitis (AIH) for optimizing azathioprine therapy. Using multilevel analysis, we demonstrated for the first time the significant positive correlations between the weight-based azathioprine dosage and the 6-thioguanine nucleotide (6-TGN) and 6-methyl-mercaptopurine (6-MeMPN) levels as well as 6-MeMPN/6-TGN ratio, supporting the use of metabolites to adjust dosing in IBD children. Other factors affecting metabolite levels were also identified. Co-administration of infliximab resulted in a significant increase in 6-TGN levels. Younger children exhibited lower metabolite levels, suggesting the influence of age on metabolism/absorption of azathioprine. We also reported that a 6-TGN level above 405 pmol/8.108RBCs in IBD children with normal TPMT activity who did not achieve steroid-free clinical remission was predictive of azathioprine refractoriness. A cut-off of 250 pmol/8.108RBCs for 6-TGN was found to be significantly associated with higher therapeutic response. Moreover, both 6-TGN and 6-MeMPN levels were correlated with leucopenia. In AIH children, a positive correlation between azathioprine dosage and metabolite levels was also observed. The wide variability in thiopurine metabolites and therapeutic response in both IBD and AIH children was confirmed, pointing to the important role of treatment individualization. Monitoring of thiopurine metabolites combined with hematological tests, TPMT activity and clinical evaluation may be of interest for optimizing thiopurine therapy and minimizing toxicity in IBD and AIH children Azathioprine Métabolites thiopuriques Pédiatrie Maladie inflammatoire de l‘intestin Hépatite autoimmune Azathioprine Thiopurine metabolites Pediatric Inflammatory bowel disease Autoimmune hepatitis 615
22	Inter-relações entre o Antígeno Leucocitário Humano-G, o pseudorreceptor inibidor de proteína morfogênica de osso e ativina ligado à membrana, e os processos inflamatórios/fibrogênicos hepáticos na hepatite autoimune / Interrelations between G-Human Leukocyte Antigen, pseudoreceptor morphogenic bone protein inhibitor and membrane-linked activin, and hepatic inflammatory / fibrogenic processes in autoimmune hepatitis Sergio Souza Figueiredo 22 September 2017 (has links) A Hepatite Autoimune (HAI) é uma doença inflamatória crônica oriunda de autoimunidade, ocasionando fibrose hepática. O objetivo desse estudo foi verificar possíveis inter-relações entre HLA-G, BAMBI e processos inflamatórios/fibrogênicos hepáticos na Hepatite Autoimune, tanto em biópsias de pacientes pré quanto póstratamento com imunossupressores. Foram selecionadas noventa e cinco biópsias de pacientes do Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto diagnosticados com HAI, associados ou não a depósitos de ferro no fígado. As biópsias foram submetidas à imuno-histoquímica para marcação das proteínas HLAG e BAMBI. As estatísticas foram determinadas pelos testes Mann-Whitney e correlação de Spearman. A expressão de HLA-G e de BAMBI se apresentou aumentados conforme o agravamento da inflamação e fibrose em pacientes pré- tratamento com boa ou má resposta ao tratamento. No entanto, a expressão de HLAG e de BAMBI foi reduzida nas biópsias pós-tratamento apenas nos pacientes bom respondedores (diminuição da fibrose). Não houve quaisquer relações entre as quantificações de HLA-G e BAMBI com o número de plasmócitos ou com depósitos de ferro no fígado tanto em pacientes pré quanto pós-tratamento. Os resultados sugerem que tanto HLA-G quanto BAMBI são imunorreguladores sensíveis à intensidade do processo inflamatório no fígado, tendo suas expressões aumentadas ou diminuídas de acordo com a demanda por substâncias que regulem compostos e células imunológicas na HAI. Sugerem também que o infiltrado plasmocitário não é regulado diretamente pelo HLA-G ou BAMBI, e que os depósitos de ferro no fígado não são capazes de influenciar nem o grau inflamatório, nem as expressões de HLAG e BAMBI. / Autoimmune Hepatitis (HAI) is a chronic inflammatory disease originating from autoimmunity, causing liver fibrosis. The objective of this study was to verify possible interrelations between HLA-G, BAMBI and inflammatory / fibrogenic hepatic processes in Autoimmune Hepatitis, both in pre and post-treatment immunosuppressive biopsies. Ninety-five biopsies of patients from the Clinical Hospital of the Medical School of Ribeirão Preto diagnosed with HAI, associated or not with iron deposits in the liver, were selected. Biopsies were submitted to immunohistochemistry for the labeling of HLA-G and BAMBI proteins. The statistics were determined by the Mann-Whitney tests and Spearman\'s correlation. The expression of HLA-G and BAMBI was increased as worsening of inflammation and fibrosis in pre-treatment patients with good or poor response to treatment. However, the expression of HLA-G and BAMBI was reduced in post-treatment biopsies only in patients with good responders (decreased fibrosis). There were no relationships between the quantifications of HLA-G and BAMBI with the number of plasma cells or with liver iron deposits in both pre and post-treatment patients. The results suggest that both HLA-G and BAMBI are immunoregulators sensitive to the intensity of the inflammatory process in the liver, their expressions being increased or decreased according to the demand for substances that regulate immune cells and compounds in HAI. They also suggest that plasmacytic infiltrate is not directly regulated by HLA-G or BAMBI, and that the liver iron deposits are not capable of influencing either the inflammatory grade or the expressions of HLA-G and BAMBI. BAMBI Fibrose Hepática Hemossiderose Hepatite Autoimune (HAI) HLAG Autoimmune hepatitis (HAI) BAMBI Hemosiderosis Hepatic fibrosis HLA-G
23	Inter-relações entre o Antígeno Leucocitário Humano-G, o pseudorreceptor inibidor de proteína morfogênica de osso e ativina ligado à membrana, e os processos inflamatórios/fibrogênicos hepáticos na hepatite autoimune / Interrelations between G-Human Leukocyte Antigen, pseudoreceptor morphogenic bone protein inhibitor and membrane-linked activin, and hepatic inflammatory / fibrogenic processes in autoimmune hepatitis Figueiredo, Sergio Souza 22 September 2017 (has links) A Hepatite Autoimune (HAI) é uma doença inflamatória crônica oriunda de autoimunidade, ocasionando fibrose hepática. O objetivo desse estudo foi verificar possíveis inter-relações entre HLA-G, BAMBI e processos inflamatórios/fibrogênicos hepáticos na Hepatite Autoimune, tanto em biópsias de pacientes pré quanto póstratamento com imunossupressores. Foram selecionadas noventa e cinco biópsias de pacientes do Hospital das Clínicas da Faculdade de Medicina de Ribeirão Preto diagnosticados com HAI, associados ou não a depósitos de ferro no fígado. As biópsias foram submetidas à imuno-histoquímica para marcação das proteínas HLAG e BAMBI. As estatísticas foram determinadas pelos testes Mann-Whitney e correlação de Spearman. A expressão de HLA-G e de BAMBI se apresentou aumentados conforme o agravamento da inflamação e fibrose em pacientes pré- tratamento com boa ou má resposta ao tratamento. No entanto, a expressão de HLAG e de BAMBI foi reduzida nas biópsias pós-tratamento apenas nos pacientes bom respondedores (diminuição da fibrose). Não houve quaisquer relações entre as quantificações de HLA-G e BAMBI com o número de plasmócitos ou com depósitos de ferro no fígado tanto em pacientes pré quanto pós-tratamento. Os resultados sugerem que tanto HLA-G quanto BAMBI são imunorreguladores sensíveis à intensidade do processo inflamatório no fígado, tendo suas expressões aumentadas ou diminuídas de acordo com a demanda por substâncias que regulem compostos e células imunológicas na HAI. Sugerem também que o infiltrado plasmocitário não é regulado diretamente pelo HLA-G ou BAMBI, e que os depósitos de ferro no fígado não são capazes de influenciar nem o grau inflamatório, nem as expressões de HLAG e BAMBI. / Autoimmune Hepatitis (HAI) is a chronic inflammatory disease originating from autoimmunity, causing liver fibrosis. The objective of this study was to verify possible interrelations between HLA-G, BAMBI and inflammatory / fibrogenic hepatic processes in Autoimmune Hepatitis, both in pre and post-treatment immunosuppressive biopsies. Ninety-five biopsies of patients from the Clinical Hospital of the Medical School of Ribeirão Preto diagnosed with HAI, associated or not with iron deposits in the liver, were selected. Biopsies were submitted to immunohistochemistry for the labeling of HLA-G and BAMBI proteins. The statistics were determined by the Mann-Whitney tests and Spearman\'s correlation. The expression of HLA-G and BAMBI was increased as worsening of inflammation and fibrosis in pre-treatment patients with good or poor response to treatment. However, the expression of HLA-G and BAMBI was reduced in post-treatment biopsies only in patients with good responders (decreased fibrosis). There were no relationships between the quantifications of HLA-G and BAMBI with the number of plasma cells or with liver iron deposits in both pre and post-treatment patients. The results suggest that both HLA-G and BAMBI are immunoregulators sensitive to the intensity of the inflammatory process in the liver, their expressions being increased or decreased according to the demand for substances that regulate immune cells and compounds in HAI. They also suggest that plasmacytic infiltrate is not directly regulated by HLA-G or BAMBI, and that the liver iron deposits are not capable of influencing either the inflammatory grade or the expressions of HLA-G and BAMBI. Autoimmune hepatitis (HAI) BAMBI BAMBI Fibrose Hepática Hemosiderosis Hemossiderose Hepatic fibrosis Hepatite Autoimune (HAI) HLA-G HLAG
24	Étude de l'autoimmunité contre le foie induite par mimétisme moléculaire Piché, Chantal January 2008 (has links) Mémoire numérisé par la Division de la gestion de documents et des archives de l'Université de Montréal Hépatite autoimmune (HAI) Tolérance hépatique Adénovirus recombinant Mimétisme moléculaire Autoimmune hepatitis (AIH) Hepatic tolerance Recombinant adenovirus CYP2D6 FTCD Molecular mimicry
25	Étude de protection conférée par vaccination ADN dans un modèle murin d’hépatite auto-immune Habel, Catherine 08 1900 (has links) La vaccination ADN à l’aide de plasmides codant pour des autoantigènes s’est avérée efficace dans la protection contre plusieurs maladies auto-immunes. Le but de ce mémoire était dans un premier temps d’établir si un protocole de vaccination ADN composé de 3 injections de pCMV-CTLA-4-NP et de pVR-IL-12 à deux semaines d’intervalle avait un effet protecteur contre le développement d’une hépatite auto-immune chez la souris TTR-NP, un modèle murin transgénique de la maladie et précédemment développé au laboratoire. Dans un deuxième temps, le but était d’élucider, le cas échéant, les mécanismes sous-tendant la protection conférée par la vaccination ADN. Les hypothèses initiales étaient qu’une protection allait effectivement être conférée par la vaccination ADN et que celle-ci pouvait être attribuable à une déviation de la réponse typiquement Th1 de la maladie vers une réponse Th2, à un épuisement des cellules immunitaires et/ou à l’activation et à l’induction de prolifération de cellules régulatrices. Les résultats montrent que la vaccination ADN induit une protection transitoire contre le développement d’infiltrations lymphocytaires au foie. Cette protection se ferait via un épuisement des cellules CD4+, CD8+ et CD19+ se retrouvant à la rate et exprimant PD 1 dans une plus forte proportion à 3 mois, et ne serait médiée ni par les lymphocytes T régulateurs CD4+CD25+FoxP3+, ni par les cellules CD8+FoxP3+. Une déviation de la réponse Th1 vers une réponse Th2 demeure une explication supplémentaire plausible à la protection conférée mais nécessiterait une caractérisation en situation plus physiologique avant de pouvoir inférer sur son implication réelle. La vaccination ADN n’influe ni sur la présence d’autoanticorps, ni sur les niveaux d’alanine aminotransférase, deux marqueurs de la maladie. / DNA immunizations were proven effective in a range of autoimmune diseases. The first goal of this master’s thesis was thus to evaluate if a protocol of 3 intramuscular plasmidic injections of pCMV-CTLA4-NP and pVR-IL-12, at 2 weeks apart, would protect TTR-NP mice, a transgenic murine model previously developed in the laboratory, against the development of an autoimmune hepatitis. The second goal was, if the protection was indeed conferred by DNA vaccination, to elucidate the mechanisms underlying this effect. The initial hypotheses were that DNA vaccination would indeed elicit a protection against autoimmune hepatitis, and that this could be attributed to a skew from the typical Th1 response to a more tolerogenic Th2 response, to the exhaustion of the immune cells and/or to the activation and the proliferation of regulatory T cells. Results show that DNA vaccination induces a transient protection against lymphocytic infiltrates in the liver. This protection is thought to be caused by the exhaustion of the CD4+, CD8+ and CD19+ cells found in the spleen and expressing PD-1 in greater proportion at 3 months, and not to be mediated by CD4+CD25+FoxP3+ or CD8+FoxP3+ regulatory T cells. An immunomodulation from a Th1 to a Th2 response could still be a plausible explanation by the protection conferred by the DNA vaccination, but additional experimentations in a more physiological setting would be necessary to infer on its real implication. DNA vaccination had no effect on autoantibodies or on alanine aminotransferase levels, which are two biological markers of the disease. hépatite autoimmune vaccination ADN auto-immunité bris de tolérance foie autoimmune hepatitis DNA vaccination autoimmunity tolerance break liver
26	Clinical and experimental studies of organ-specific autoimmune diseases : With special reference to Addison's disease and autoimmune hepatitis : by Gennet Gebre-Medhin Gebre-Medhin, Gennet January 2001 (has links) <p>Organ-specific autoimmunity constitutes a large health problem, where both the clinical management and our understanding of the pathogenetic mechanisms need to improve. Women with Addison's disease have abnormally low levels of dehydroepiandrosterone (DHEA), its sulphate ester (DHEA-S) and androgens relative to age, and many patients complain of physical and mental fatigue and low stress tolerance. To define a suitable dose, the effect of oral DHEA replacement was evaluated in women with Addison's disease. </p><p> DHEA was administered for three months to nine women with Addison's disease in either of two doses, 50 mg (n=5) or 200 mg (n=4). A dose of 50 mg restored the DHEA(S) and androgen levels to normal without altering the insulin sensitivity, body composition or serum lipid profile.</p><p> Autoimmune polyendocrine syndrome type I (APS I) is a rare but useful model disorder of autoimmunity, characterised by multiple organ-specific autoimmune manifestations and high-titre autoantibodies and with adrenocortical insufficiency, Addison's disease, as one of its cardinal manifestations. Approximately 10-20% of APS I patients suffer from autoimmune hepatitis, which carries a high mortality, if untreated. The presence of putative antigenic targets in the liver was investigated.</p><p> Cytochrome P4501A2 (CYP1A2) and aromatic L-amino acid decarboxylase (AADC) were identified as hepatic autoantigens with the use of APS I sera for immunofluorescent staining of normal human liver, Western blot of microsomal and cytosol fractions of human liver homogenate, and immunoprecipitation of <i>in vitro</i> transcribed and translated radioactively labelled proteins. The presence of CYP1A2- and AADC-antibodies was significantly correlated to AIH, and CYP1A2 antibodies inhibited enzyme activity <i>in vitro</i>.</p><p><i> In conclusion</i>, a daily replacement dose of 50 mg of DHEA sufficiently restores levels of DHEA, DHEA(S) and androgens in women with Addison's disease, without severe side-effects. We have further identified CYP1A2 and AADC as hepatic autoantigens associated with autoimmune hepatitis in APS I.</p> Medical sciences Addison's Disease replacement therapy DHEA autoimmune hepatitis APS I autoantigen cytochrome P4501A2 aromatic L-amino acid decarboxylase MEDICIN OCH VÅRD MEDICINE MEDICIN
27	Clinical and experimental studies of organ-specific autoimmune diseases : With special reference to Addison's disease and autoimmune hepatitis : by Gennet Gebre-Medhin Gebre-Medhin, Gennet January 2001 (has links) Organ-specific autoimmunity constitutes a large health problem, where both the clinical management and our understanding of the pathogenetic mechanisms need to improve. Women with Addison's disease have abnormally low levels of dehydroepiandrosterone (DHEA), its sulphate ester (DHEA-S) and androgens relative to age, and many patients complain of physical and mental fatigue and low stress tolerance. To define a suitable dose, the effect of oral DHEA replacement was evaluated in women with Addison's disease. DHEA was administered for three months to nine women with Addison's disease in either of two doses, 50 mg (n=5) or 200 mg (n=4). A dose of 50 mg restored the DHEA(S) and androgen levels to normal without altering the insulin sensitivity, body composition or serum lipid profile. Autoimmune polyendocrine syndrome type I (APS I) is a rare but useful model disorder of autoimmunity, characterised by multiple organ-specific autoimmune manifestations and high-titre autoantibodies and with adrenocortical insufficiency, Addison's disease, as one of its cardinal manifestations. Approximately 10-20% of APS I patients suffer from autoimmune hepatitis, which carries a high mortality, if untreated. The presence of putative antigenic targets in the liver was investigated. Cytochrome P4501A2 (CYP1A2) and aromatic L-amino acid decarboxylase (AADC) were identified as hepatic autoantigens with the use of APS I sera for immunofluorescent staining of normal human liver, Western blot of microsomal and cytosol fractions of human liver homogenate, and immunoprecipitation of in vitro transcribed and translated radioactively labelled proteins. The presence of CYP1A2- and AADC-antibodies was significantly correlated to AIH, and CYP1A2 antibodies inhibited enzyme activity in vitro. In conclusion, a daily replacement dose of 50 mg of DHEA sufficiently restores levels of DHEA, DHEA(S) and androgens in women with Addison's disease, without severe side-effects. We have further identified CYP1A2 and AADC as hepatic autoantigens associated with autoimmune hepatitis in APS I. Medical sciences Addison's Disease replacement therapy DHEA autoimmune hepatitis APS I autoantigen cytochrome P4501A2 aromatic L-amino acid decarboxylase MEDICIN OCH VÅRD MEDICINE MEDICIN
28	Étude de protection conférée par vaccination ADN dans un modèle murin d’hépatite auto-immune Habel, Catherine 08 1900 (has links) La vaccination ADN à l’aide de plasmides codant pour des autoantigènes s’est avérée efficace dans la protection contre plusieurs maladies auto-immunes. Le but de ce mémoire était dans un premier temps d’établir si un protocole de vaccination ADN composé de 3 injections de pCMV-CTLA-4-NP et de pVR-IL-12 à deux semaines d’intervalle avait un effet protecteur contre le développement d’une hépatite auto-immune chez la souris TTR-NP, un modèle murin transgénique de la maladie et précédemment développé au laboratoire. Dans un deuxième temps, le but était d’élucider, le cas échéant, les mécanismes sous-tendant la protection conférée par la vaccination ADN. Les hypothèses initiales étaient qu’une protection allait effectivement être conférée par la vaccination ADN et que celle-ci pouvait être attribuable à une déviation de la réponse typiquement Th1 de la maladie vers une réponse Th2, à un épuisement des cellules immunitaires et/ou à l’activation et à l’induction de prolifération de cellules régulatrices. Les résultats montrent que la vaccination ADN induit une protection transitoire contre le développement d’infiltrations lymphocytaires au foie. Cette protection se ferait via un épuisement des cellules CD4+, CD8+ et CD19+ se retrouvant à la rate et exprimant PD 1 dans une plus forte proportion à 3 mois, et ne serait médiée ni par les lymphocytes T régulateurs CD4+CD25+FoxP3+, ni par les cellules CD8+FoxP3+. Une déviation de la réponse Th1 vers une réponse Th2 demeure une explication supplémentaire plausible à la protection conférée mais nécessiterait une caractérisation en situation plus physiologique avant de pouvoir inférer sur son implication réelle. La vaccination ADN n’influe ni sur la présence d’autoanticorps, ni sur les niveaux d’alanine aminotransférase, deux marqueurs de la maladie. / DNA immunizations were proven effective in a range of autoimmune diseases. The first goal of this master’s thesis was thus to evaluate if a protocol of 3 intramuscular plasmidic injections of pCMV-CTLA4-NP and pVR-IL-12, at 2 weeks apart, would protect TTR-NP mice, a transgenic murine model previously developed in the laboratory, against the development of an autoimmune hepatitis. The second goal was, if the protection was indeed conferred by DNA vaccination, to elucidate the mechanisms underlying this effect. The initial hypotheses were that DNA vaccination would indeed elicit a protection against autoimmune hepatitis, and that this could be attributed to a skew from the typical Th1 response to a more tolerogenic Th2 response, to the exhaustion of the immune cells and/or to the activation and the proliferation of regulatory T cells. Results show that DNA vaccination induces a transient protection against lymphocytic infiltrates in the liver. This protection is thought to be caused by the exhaustion of the CD4+, CD8+ and CD19+ cells found in the spleen and expressing PD-1 in greater proportion at 3 months, and not to be mediated by CD4+CD25+FoxP3+ or CD8+FoxP3+ regulatory T cells. An immunomodulation from a Th1 to a Th2 response could still be a plausible explanation by the protection conferred by the DNA vaccination, but additional experimentations in a more physiological setting would be necessary to infer on its real implication. DNA vaccination had no effect on autoantibodies or on alanine aminotransferase levels, which are two biological markers of the disease. hépatite autoimmune vaccination ADN auto-immunité bris de tolérance foie autoimmune hepatitis DNA vaccination autoimmunity tolerance break liver
29	Étude de l’impact de la grossesse sur l’hépatite auto-immune dans un modèle expérimental murin Bourbonnais, Sara 09 1900 (has links) L’hépatite auto-immune (HAI) est une maladie chronique caractérisée par une destruction progressive du parenchyme hépatique par le système immunitaire. La majorité des patients atteints d’HAI sont des femmes (75% à 90% des cas). L’amélioration des traitements au cours des dernières années a permis à un grand nombre de ces femmes de devenir enceintes. Pendant la grossesse, une rémission spontanée de la maladie a pu être observée chez les femmes atteintes d’HAI. Cette rémission est temporaire et elle est généralement suivie d’une rechute suite à l’accouchement (post-partum). Les causes exactes de cette rémission associée à la grossesse et de la rechute post-partum ne sont pas connues à ce jour. Nous avons donc tenté de reproduire ces phénomènes dans un modèle murin d’HAI développé dans notre laboratoire, afin de déterminer les mécanismes possiblement impliqués. Notre modèle d’HAI consiste en une xéno-immunisation de souris C57BL/6 avec les auto-antigènes impliqués dans l’HAI de type 2 chez l’humain. Nous avons ainsi accouplées des souris préalablement xéno-immunisées, puis nous les avons sacrifiées au début de la 3e semaine de gestation ou 2 à 3 semaines post-partum, afin d’évaluer les dommages hépatiques et afin d’étudier la réponse immunitaire. Comme chez les femmes atteintes d’HAI, les souris présentent une rémission de la maladie pendant la grossesse. Nous en sommes venus à cette conclusion par l’observation d’une diminution de l’inflammation hépatique, des niveaux de transaminases sériques et des titres d’auto-anticorps circulants. À l’inverse des humains, les souris xéno-immunisées ne présentent pas de rechute post-partum. Une analyse des cellules régulatrices (cellules T régulatrices et cellules B productrices d'IL-10) suggère une implication des Tregs hépatiques dans la rémission, car ceux-ci sont augmentés pendant la gestation. Ces Tregs hépatiques sont majoritairement d’origine thymique et ne semblent pas particulièrement attirés au foie en réponse à l’inflammation. La polarisation TH2 est un phénomène connu pendant la grossesse, par contre elle ne semble pas influencer la réponse auto-immune dans nos souris. Une meilleure compréhension des mécanismes d’immunosuppression observés lors de la grossesse pourrait mener au développement d’une thérapie mieux ciblée. / Autoimmune hepatitis (AIH) is a disease of unknown aetiology, characterized by a progressive destruction of the hepatic parenchyma by the immune system. Women are predominantly affected by AIH, with a prevalence of 75% in type 1 AIH and 90% in type 2. Improvement of treatments to control liver inflammation has contributed to increase the number of pregnant patients. During pregnancy, a spontaneous, but temporary, remission of the disease has been observed in women with AIH, often followed by post-partum relapse. Currently, this phenomenon is not fully understood. Thus, we aim to study the mechanisms responsible for the pregnancy-related remission and post-partum relapses in a murine model of AIH developed in our laboratory. Xenoimmunization of C57BL/6 mice with the antigens recognized by autoreactive cells of type 2 AIH patients results in a loss of tolerance, with clinical and biochemical features of AIH similar to those observed in patients. For this study, xenoimmunized mice were mated and sacrificed at the beginning of the 3rd week of gestation or 2-3 weeks post-partum, and liver disease was evaluated at that time as well as the immune response. As it occurs in women with AIH, pregnancy induces a remission of the disease in our murin model. Pregnant mice show a decrease of liver inflammation, ALT levels and circulating autoantibodies. The mice did not show any sign of relapse during the post-partum period. Our analysis of cellular populations with regulatory properties (regulatory T cells and IL-10 secreting B cells) revealed an increase of hepatic Tregs during pregnancy, which suggests an implication of those cells in the remission. Those Tregs infiltrating the liver are mainly originated from the thymus and do not seem to be recruited to the liver in response to inflammation. Although a switch towards a TH2 response is known to occur during pregnancy, this phenomenon does not seem to be implicated in the remission of AIH in our murine model. A better understanding of the natural immunosuppression occurring during pregnancy could bring important knowledge to design new and improved therapy for AIH. Auto-immunité Tolérance immunitaire Hépatite auto-immune Foie Grossesse Gestation Post-partum Fœtus Hormones Lymphocytes T régulateurs Autoimmunity Immune tolerance Autoimmune hepatitis Liver Pregnancy Fetus Regulatory T cells
30	Développement d’immunothérapies spécifiques pour le traitement de l’hépatite autoimmune de type 2 chez un modèle murin Yang, Roland 12 1900 (has links) L’hépatite autoimmune (HAI) est une maladie grave affectant le foie et présentant un haut taux de mortalité lorsque non traitée. Les traitements disponibles sont efficaces, mais de graves effets secondaires leur sont associés. Ces effets secondaires sont généralement le résultat d'une forte immunosuppression et d’autres sont spécifiques à chaque médicament. Aucune immunothérapie spécifique n’est présentement disponible pour le traitement de l’HAI. Récemment, un modèle murin d’HAI a été développé dans notre laboratoire par xénoimmunisation des souris C57BL/6 avec les antigènes humains de l'HAI de type 2. Ce modèle présente la plupart des caractéristiques biochimiques et cliniques retrouvées chez les patients atteints d'HAI de type 2. Dans cette étude, nous avons évaluée l’efficacité de deux types de traitement pour l’HAI de type 2 à l’aide de notre modèle murin. Dans un premier temps, l’anticorps anti-CD3ε a été étudié en prophylaxie et en traitement. Nous avons montré qu’une posologie de 5µg d’anti-CD3 i.v. par jour pendant 5 jours consécutifs induit une rémission chez les souris avec HAI de type 2 établie (traitement). Cette rémission est caractérisée par une normalisation des niveaux d’alanine aminotransférase et une diminution significative de l’inflammation hépatique. Cette rémission semble être associée à une déplétion partielle et transitoire des lymphocytes T CD3+ dans la périphérie et une augmentation des lymphocytes T régulateurs CD4+, CD25+ et Foxp3+ dans le foie. La même posologie lorsqu’elle est appliquée en prophylaxie n’a pas réussi à prévenir l’apparition de l’HAI de type 2. La deuxième voie de traitement consiste en l’administration par voie intranasale d’un forte dose de formiminotransférase cyclodésaminase murin (mFTCD), un autoantigène reconnu dans l’HAI de type 2. Une administration en prophylaxie par voie intranasale de 100µg de mFTCD par jour durant 3 jours consécutifs arrive à prévenir l’HAI de type 2 en diminuant l’inflammation hépatique au bout de deux semaines post-traitement. / Autoimmune hepatitis (AIH) is a severe liver disease with high mortality rates if left untreated. Current treatments, while effective, are associated with deleterious side-effects. These side effects are specific to each drug and the result of broad immunosuppression. Recently, a murine model of type 2 AIH has been created in our laboratory in wild-type naïve mice. In this model, DNA immunization with type 2 AIH human autoantigens breaks immune tolerance and induces an autoimmune response against the liver. Lately, new therapeutic strategies based on depletion of specific immune cell populations have been proposed for the treatment of several diseases, including autoimmune diseases. Currently, no immunotherapies using biological agents are available for the treatment of autoimmune liver diseases. Therefore, the goal of this project is to study the efficacy of new immunotherapeutic agents for the treatment of type 2 AIH in an experimental model. We evaluated the effectiveness of two approaches for treating type 2 AIH. First, we tested the anti-CD3ε antibody in prophylaxis and in treatment of type 2 AIH. We showed that a dosage of 5µg i.v. of anti-CD3ε antibody per day for 5 consecutive days induced remission in mice with established type 2 AIH. This remission was defined as a normalization of serum alanine aminostransferase levels and a significant decrease of liver inflammation in treated mice. This remission seems to be associated with a transitory depletion of CD3+ T lymphocytes in peripheral blood mononuclear cells and increased CD4+CD25+Foxp3+ regulatory T lymphocytes in the liver. But when this dosage was applied in prophylaxis, it could not prevent the induction of type 2 AIH. The second approach was to induce tolerance by nasal administration of murin formiminotransferase cyclodeaminase (mFTCD), an autoantigen of type 2 AIH. We showed that nasal administration of 100µg of mFTCD for 3 consecutive days prevented development of type 2 AIH in prophylaxis by reducing liver inflammation. Hépatite autoimmune de type 2 Anti-CD3 Tolérance intranasale Lymphocyte T régulateur Forminotransférase cyclodésaminase Type 2 autoimmune hepatitis Nasal tolerance Regulatory T lymphocyte Forminotransferase cyclodeaminase Anti-CD3 antibody

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