Global ETD Search

61	Extrathymic T cell receptor gene rearrangement in human alimentary tract Bas, Anna January 2003 (has links) <p>T lymphocytes regulate the initiation, duration, and magnitude of adaptive immune responses and function as effector cells in cell mediated immunity. To become immunologically competent they must generate functional antigen receptors. This process takes place in the thymus and requires somatic recombination of T cell receptor (TCR) genes. It is mediated by the endonucleases recombination activating gene-1 (RAG1) and RAG2. Although the thymus regresses at puberty, T cells are present throughout life implying that other tissues must provide the proper milieu for T cell development. This thesis describes extrathymic T cell maturation in man. RAG1, RAG2, and the preTα-chain (pTα), which is exclusively utilized in developing T cells, were used as markers for TCR gene rearrangement. Two new exons (1A and 1B) encoding sequences in the 5’ untranslated region (5’UTR) of mRNA were discovered in the human RAG1 gene. The previously described 5’UTR exon (renamed 1C) was located between the new exons and exon 2, the latter containing the entire coding sequence. We found that small intestinal lymphocytes of the T cell lineage expressed the new exons in three different splice forms. RAG1 mRNA containing the 1C exon was not expressed in small intestinal lymphocytes. In contrast, splice forms containing the 1A exon were not expressed in thymocytes. RAG1 and pTα mRNA expressing lymphocytes were seen both within the epithelium and in lamina propria. Thymocyte-like CD2<sup>+</sup>CD7<sup>+</sup>CD3<sup>-</sup>, CD4<sup>+</sup>CD8<sup>+</sup>, CD1a<sup>+</sup>, and IL7-R+ lymphocytes were identified in the small intestinal mucosa. CD2<sup>+</sup>CD7<sup>+</sup>CD3<sup>-</sup> cells had the highest expression levels of mRNA for RAG1 and pTα, suggesting that the small intestinal mucosa is indeed a site for T cell maturation. Small intestinal T lymphocytes were also shown to kill via the Fas/FasL pathway in a TCR/CD3 independent manner and via the perforin/granzyme pathway in a TCR/CD3 dependent manner. The Fas/FasL-mediated cytotoxicity may reflect an ongoing selection process of extrathymically maturated T cells. </p><p>The nasopharyngeal tonsil is the major inductive site for immune reactions against inhaled antigens. Previous demonstration of RAG1 expression in tonsillar B cells was interpreted as antigen driven receptor revision. The present study confirms the expression of RAG1 in B cells. We also found that RAG1, RAG2, and pTa mRNAs were expressed in lymphocytes of the T cell lineage. A small population of cells with the immature phenotype CD2+CD7+CD3- was demonstrated. This population had the highest expression levels of mRNA for RAG1, RAG2, pTα and terminal deoxynucleotidyl transferase. All four splice-forms of RAG1 mRNA were expressed. RAG1 and pTα mRNA expressing cells were mainly located in the proximity of the surface epithelium and in the outer rim of the follicles. These results suggest that the nasopharyngeal tonsil is a site where extrathymic T cell development and antigen driven TCR revision are occurring in parallel. </p><p>Celiac disease (CD) is a small intestinal enteropathy characterized by permanent intolerance to gluten. Gluten reactive intestinal T cells are central in the pathogenesis and CD can be regarded as a failure to maintain tolerance to this food antigen. Expression of the RAG1 1A/2 splice form was significantly decreased in small intestinal T cell subsets of CD patients suggesting that impaired TCR gene rearrangement could contribute to failure of maintain tolerance in CD. </p><p>Together, these findings show that both small intestinal and nasopharyngeal tonsillar lymphocytes of T cell lineage have the molecular machinery for antigen receptor rearrangement and that thymocyte-like lymphocytes are present in both tissues. Thus these organs are likely sites of T lymphocyte ontogeny as well as for secondary T cell receptor rearrangement in man. </p> Immunology T cell maturation recombination activating gene preTα human intestinal mucosa intraepithelial lymphocytes lamina propria lymphocytes nasopharyngeal tonsil Immunologi Immunology Immunologi
62	Extrathymic T cell receptor gene rearrangement in human alimentary tract Bas, Anna January 2003 (has links) T lymphocytes regulate the initiation, duration, and magnitude of adaptive immune responses and function as effector cells in cell mediated immunity. To become immunologically competent they must generate functional antigen receptors. This process takes place in the thymus and requires somatic recombination of T cell receptor (TCR) genes. It is mediated by the endonucleases recombination activating gene-1 (RAG1) and RAG2. Although the thymus regresses at puberty, T cells are present throughout life implying that other tissues must provide the proper milieu for T cell development. This thesis describes extrathymic T cell maturation in man. RAG1, RAG2, and the preTα-chain (pTα), which is exclusively utilized in developing T cells, were used as markers for TCR gene rearrangement. Two new exons (1A and 1B) encoding sequences in the 5’ untranslated region (5’UTR) of mRNA were discovered in the human RAG1 gene. The previously described 5’UTR exon (renamed 1C) was located between the new exons and exon 2, the latter containing the entire coding sequence. We found that small intestinal lymphocytes of the T cell lineage expressed the new exons in three different splice forms. RAG1 mRNA containing the 1C exon was not expressed in small intestinal lymphocytes. In contrast, splice forms containing the 1A exon were not expressed in thymocytes. RAG1 and pTα mRNA expressing lymphocytes were seen both within the epithelium and in lamina propria. Thymocyte-like CD2+CD7+CD3-, CD4+CD8+, CD1a+, and IL7-R+ lymphocytes were identified in the small intestinal mucosa. CD2+CD7+CD3- cells had the highest expression levels of mRNA for RAG1 and pTα, suggesting that the small intestinal mucosa is indeed a site for T cell maturation. Small intestinal T lymphocytes were also shown to kill via the Fas/FasL pathway in a TCR/CD3 independent manner and via the perforin/granzyme pathway in a TCR/CD3 dependent manner. The Fas/FasL-mediated cytotoxicity may reflect an ongoing selection process of extrathymically maturated T cells. The nasopharyngeal tonsil is the major inductive site for immune reactions against inhaled antigens. Previous demonstration of RAG1 expression in tonsillar B cells was interpreted as antigen driven receptor revision. The present study confirms the expression of RAG1 in B cells. We also found that RAG1, RAG2, and pTa mRNAs were expressed in lymphocytes of the T cell lineage. A small population of cells with the immature phenotype CD2+CD7+CD3- was demonstrated. This population had the highest expression levels of mRNA for RAG1, RAG2, pTα and terminal deoxynucleotidyl transferase. All four splice-forms of RAG1 mRNA were expressed. RAG1 and pTα mRNA expressing cells were mainly located in the proximity of the surface epithelium and in the outer rim of the follicles. These results suggest that the nasopharyngeal tonsil is a site where extrathymic T cell development and antigen driven TCR revision are occurring in parallel. Celiac disease (CD) is a small intestinal enteropathy characterized by permanent intolerance to gluten. Gluten reactive intestinal T cells are central in the pathogenesis and CD can be regarded as a failure to maintain tolerance to this food antigen. Expression of the RAG1 1A/2 splice form was significantly decreased in small intestinal T cell subsets of CD patients suggesting that impaired TCR gene rearrangement could contribute to failure of maintain tolerance in CD. Together, these findings show that both small intestinal and nasopharyngeal tonsillar lymphocytes of T cell lineage have the molecular machinery for antigen receptor rearrangement and that thymocyte-like lymphocytes are present in both tissues. Thus these organs are likely sites of T lymphocyte ontogeny as well as for secondary T cell receptor rearrangement in man. Immunology T cell maturation recombination activating gene preTα human intestinal mucosa intraepithelial lymphocytes lamina propria lymphocytes nasopharyngeal tonsil Immunologi Immunology Immunologi
63	Malignant transformation of the colorectal mucosa in inflammatory bowel disease / Sjöqvist, Urban, January 2003 (has links) Diss. (sammanfattning) Stockholm : Karol. inst., 2003. / Härtill 5 uppsatser.
64	Toxicidade do tabagismo passivo: efeito mitigador de alimentos funcionais nos parâmetros histomorfométricos e histopatológicos duodenais em ratos / Passive Smoking Toxicity: Functional Food Mitigating Effect on Duodenal Histomorphometric and Histopathological Parameters of Mice TAKABATAKE, Thiago Tomio 13 June 2017 (has links) Submitted by Adriana Martinez (amartinez@unoeste.br) on 2017-08-15T18:51:27Z No. of bitstreams: 1 Thiago Tomio Takabatake.pdf: 507776 bytes, checksum: 49290d180286e792c57d528837031b6e (MD5) / Made available in DSpace on 2017-08-15T18:51:27Z (GMT). No. of bitstreams: 1 Thiago Tomio Takabatake.pdf: 507776 bytes, checksum: 49290d180286e792c57d528837031b6e (MD5) Previous issue date: 2017-06-13 / Passive smoking has become a major problem stemming from damage to the body from people involuntarily exposed to cigarette smoke. Concern with this group of people has led the scientific community to research alternatives that might be used to prevent the harm caused by secondhand smoke. Thus, the objective of the present study was to evaluate the deleterious effects of chronic passive smoking on the histomorphometry and histopathology of the duodenum of growing rats supplemented or not with functional prebiotic, probiotic and symbiotic foods. A total of 96 rats were distributed in a completely randomized design in a 2 x 4 factorial scheme. Animals were supplemented with functional foods and passively or not exposed to cigarette smoke for 180 days for one hour daily five days a week. At the end of the experimental period, samples of the initial duodenum were collected for histomorphometric evaluation and histopathological analysis. Animals exposed to secondhand smoke showed less development of duodenal villi and crypts, increased inflammatory profiles and degenerative changes. It was observed that supplementation with functional foods provided a mitigating effect of the toxic effects of exposure to passive smoking in all analyzed parameters. It is concluded that the use of prebiotic, probiotic and symbiotic in the diet of rats exposed to passive smoking may be a possible way to attenuate the toxic effects induced by secondhand smoke on the duodenal mucosa, and may serve as prevention of mucosal damage and development of Diseases caused by passive exposure to cigarette smoke. / O tabagismo passivo tornou-se um grande problema decorrente de danos causados ao organismo de pessoas expostas involuntariamente a fumaça de cigarro. A preocupação com esse grupo de pessoas levou a comunidade científica a pesquisar alternativas que possam vir a ser utilizadas para prevenir os danos causados pelo fumo passivo. Dessa forma, o objetivo do presente trabalho foi avaliar os efeitos deletérios do tabagismo passivo crônico sobre a histomorfometria e histopatologia do duodeno de ratos em crescimento suplementados ou não com os alimentos funcionais prebiótico, probiótico e simbiótico. Foram utilizados 96 ratos distribuídos em um delineamento inteiramente casualizado em esquema fatorial 2 x 4. Os animais foram suplementados com os alimentos funcionais e expostos passivamente ou não a fumaça de cigarro durante 180 dias por uma hora diária cinco dias por semana. Ao final do período experimental, foram colhidas amostras da porção inicial do duodeno para avaliação histomorfométrica e análise histopatológica. Os animais expostos ao fumo passivo apresentaram menor desenvolvimento das vilosidades e criptas duodenais, aumento nos perfis inflamatórios e alterações degenerativas. Foi observado que a suplementação com os alimentos funcionais proporcionou um efeito mitigador dos efeitos tóxicos da exposição ao tabagismo passivo em todos os parâmetros analisados. Conclui-se que a utilização de prebiótico, probiótico e simbiótico na dieta de ratos expostos ao tabagismo passivo pode ser uma possível forma de atenuar os efeitos tóxicos induzidos pelo fumo passivo sobre a mucosa duodenal, podendo servir como prevenção de danos a mucosa e desenvolvimento de doenças futuras ocasionadas pela exposição passiva a fumaça de cigarro. CIENCIAS AGRARIAS::MEDICINA VETERINARIA
65	Repercussões morfológicas da lesão térmica corporal nos componentes do plexo mioentérico do jejuno de ratos adultos. / Morphological repercutions of burn injury components of the myenteric plexus in the jejunum of adults rats. Seyfert, Carlos Eduardo 02 September 2009 (has links) As lesões térmicas corporais (LTC) são um sério problema de saúde, atingindo principalmente crianças. A extensão e a profundidade da lesão são fatores que alteram várias estruturas. Alterações gastrintestinais também são relatadas, sendo a principal delas, a atrofia das mucosas, provocando ulcerações e a perda da barreira seletiva. Na presente pesquisa avaliou-se através de técnicas histoquímicas, imunohitoquimicas e de microscopia de luz, as alterações ocorridas nos componentes do plexo mioentérico e na espessura da mucosa do jejuno em três porções: oral (O), média (M) e aboral (A), de ratos adultos com 30% da superfície corpórea exposta ao escaldamento, 4 dias (q4) e 10 dias (q10) após a LTC. Verificou-se em q10 o não restabelecimento da massa corpórea, a diminuição da área do jejuno, bem como espessura de sua mucosa. No plexo mioentérico, a área média do perfil celular dos neurônios NADPH não variou, tendo estes uma menor densidade em q10, sendo estes corpos altamente reativos em q4 e q10. Varicosidades grandes destacaram-se em q4 e q10, quando pela SP e VIP. / Burn is a determinant factor to alter body structures as the striated muscle. It also determines gastrintestinal mucosal atrophy what produce loss of selective barrier. With histochemical, immunohistochemical and light microscopy methods the myenteric plexus (MP) of the jejunum was evaluated in rats submitted to burn injury. The scalding was performed in 30% of the body surface. The MP and the mucosa of the oral (O), middle (M) and aboral (A) parts of the jejunum were analyzed four (q4) and ten (q10) days post-lesion. The loss of weight due the burn is not recovered in q10 where the jejunal surface area and the thickness of the mucosa decreased. The neuronal profile of nitregic neurons was similar in q4, q10. The density of nitregic neurons was lower in q10 showing that the time post injury is an important factor able to alter this parameter. The q4 and q10 groups exhibited neuronal bodies highly reactive to NADPH. The immunoreactivity to SP and VIP in q4 and q10 was expressed mainly in large varicosities. Anatomia Anatomy Animal morphogenesis Burn injury Intestinal mucosa Intestino delgado Jejuno de animal Jejunum animal Lesão térmica corporal Lesions in animals Lesões em animais Morfogênese animal Mucosa intestinal Myenteric plexus Plexo mioentérico Small intestine Thermal body lesion
66	Barrier function of the Follicle-Associated Epithelium in Stress and Crohn's disease Keita, Åsa January 2007 (has links) Crohns sjukdom är en kronisk inflammatorisk tarmsjukdom av okänd orsak. Det tidigaste tecknet på Crohns sjukdom är mikroskopiska sår i det s.k. follikelassocierade epitelet (FAE) som täcker ansamlingar av immunceller i tarmen. FAE är specialiserat för att fånga innehåll från tarmen och transportera det till underliggande immunvävnad. Denna funktion är viktig för att inducera skyddande immunsvar, men den utgör också en ingångsväg för sjukdomsalstrande bakterier. Crohns sjukdom är associerat med ett kraftigt ökat immunsvar mot bakterier, och sjukdomsförloppet kan ändras av stress. Det övergripande syftet med avhandlingen var att studera effekterna av stress på FAE samt att undersöka rollen av FAE vid utvecklingen av tarminflammation, särskilt vid Crohns sjukdom. Inledningsvis studerades effekterna av psykologisk stress på FAE. Stressade råttor uppvisade ökad genomsläpplighet av bakterier efter stress, och passagen var högre i FAE än i vanligt epitel. Efterföljande experiment visade att stressförändringarna i slemhinnan regleras via kortikotropinfrisättande hormon och mastceller. Vidare visade det sig att vasoaktiv intestinal peptid kunde efterlikna stressens effekter på genomsläppligheten, och att detta kunde förhindras genom att blockera mastcellerna. Studier av tunntarmsslemhinna från patienter med icke-inflammatorisk tarmsjukdom och friska kontroller visade en högre passage av bakterier i FAE än i vanligt epitel. Hos patienter med Crohns sjukdom var bakteriepassagen genom FAE betydligt ökad jämfört med kontroller. Resultaten från detta avhandlingsarbete visar att stress kan förändra upptaget av bakterier från tarmen via FAE, med mekanismer som innefattar kortikotropinfrisättande hormon och mastceller. Detta har gett nya kunskaper kring regleringen av slemhinnebarriären. Vidare presenterar denna avhandling nya insikter i sjukdomsuppkomsten vid Crohns sjukdom genom att påvisa en tidigare okänd defekt i barriärfunktionen i FAE. / The earliest observable signs of Crohn’s disease are microscopic erosions in the follicle-associated epithelium (FAE) covering the Peyer’s patches. The FAE, which contains M cells, is specialised in sampling of luminal content and delivery to underlying immune cells. This sampling is crucial for induction of protective immune responses, but it also provides a route of entry for microorganisms into the mucosa. Crohn’s disease is associated with an increased immune response to bacteria, and the disease course can be altered by stress. The overall aim of this thesis was to study the effects of stress on the FAE and elucidate the role of FAE in the development of intestinal inflammation, specifically Crohn’s disease. Initially, rats were submitted to acute and chronic water avoidance stress to study the effects of psychological stress on the FAE. Stressed rats showed enhanced antigen and bacterial passage, and the passage was higher in FAE than in regular villus epithelium (VE). Further, stress gave rise to ultrastructural changes. Subsequent experiments revealed the stress-induced increase in permeability to be regulated by corticotropin-releasing hormone and mast cells. Furthermore, vasoactive intestinal peptide (VIP) mimicked the stress effects on permeability, and the VIP effects were inhibited by a mast cell stabiliser. Human studies of ileal mucosa from patients with non-inflammatory disease and healthy controls showed a higher antigen and bacterial passage in FAE than in VE. In patients with Crohn’s disease, the bacterial passage across the FAE was significantly increased compared to non-inflammatory and inflammatory controls (ulcerative colitis). Furthermore, there was an enhanced uptake of bacteria into dendritic cells, and augmented TNF-α release in Crohn’s disease mucosa. Taken together this thesis shows that stress can modulate the uptake of luminal antigens and bacteria via the FAE, through mechanisms involving CRH and mast cells. It further shows that human ileal FAE is functionally distinct from VE, and that Crohn’s disease patients exhibit enhanced FAE permeability compared to inflammatory and non-inflammatory controls. This thesis presents novel insights into regulation of the FAE barrier, as well as into the pathophysiology of Crohn’s disease by demonstrating a previously unrecognised defect of the FAE barrier function in ileal Crohn’s disease. Corticotropin-releasing hormone Crohn’s disease 51Cr- EDTA Escherichia coli follicle-associated epithelium horseradish peroxidase human ileum inflammatory bowel disease intestinal mucosa mast cell M cell permeability Peyer’s patches rat Ussing chamber vasoactive intestinal peptide villus epithelium Surgery Kirurgi
67	Repercussões morfológicas da lesão térmica corporal nos componentes do plexo mioentérico do jejuno de ratos adultos. / Morphological repercutions of burn injury components of the myenteric plexus in the jejunum of adults rats. Carlos Eduardo Seyfert 02 September 2009 (has links) As lesões térmicas corporais (LTC) são um sério problema de saúde, atingindo principalmente crianças. A extensão e a profundidade da lesão são fatores que alteram várias estruturas. Alterações gastrintestinais também são relatadas, sendo a principal delas, a atrofia das mucosas, provocando ulcerações e a perda da barreira seletiva. Na presente pesquisa avaliou-se através de técnicas histoquímicas, imunohitoquimicas e de microscopia de luz, as alterações ocorridas nos componentes do plexo mioentérico e na espessura da mucosa do jejuno em três porções: oral (O), média (M) e aboral (A), de ratos adultos com 30% da superfície corpórea exposta ao escaldamento, 4 dias (q4) e 10 dias (q10) após a LTC. Verificou-se em q10 o não restabelecimento da massa corpórea, a diminuição da área do jejuno, bem como espessura de sua mucosa. No plexo mioentérico, a área média do perfil celular dos neurônios NADPH não variou, tendo estes uma menor densidade em q10, sendo estes corpos altamente reativos em q4 e q10. Varicosidades grandes destacaram-se em q4 e q10, quando pela SP e VIP. / Burn is a determinant factor to alter body structures as the striated muscle. It also determines gastrintestinal mucosal atrophy what produce loss of selective barrier. With histochemical, immunohistochemical and light microscopy methods the myenteric plexus (MP) of the jejunum was evaluated in rats submitted to burn injury. The scalding was performed in 30% of the body surface. The MP and the mucosa of the oral (O), middle (M) and aboral (A) parts of the jejunum were analyzed four (q4) and ten (q10) days post-lesion. The loss of weight due the burn is not recovered in q10 where the jejunal surface area and the thickness of the mucosa decreased. The neuronal profile of nitregic neurons was similar in q4, q10. The density of nitregic neurons was lower in q10 showing that the time post injury is an important factor able to alter this parameter. The q4 and q10 groups exhibited neuronal bodies highly reactive to NADPH. The immunoreactivity to SP and VIP in q4 and q10 was expressed mainly in large varicosities. Anatomia Intestino delgado Jejuno de animal Lesão térmica corporal Lesões em animais Morfogênese animal Mucosa intestinal Plexo mioentérico Anatomy Animal morphogenesis Burn injury Intestinal mucosa Jejunum animal Lesions in animals Myenteric plexus Small intestine Thermal body lesion
68	Impact des trichothécènes sur l'immunité des muqueuses et utilisation de Lactobacillus sobrius comme moyen de lutte microbiologique contre ces mycotoxines / Trichothenes' impacts on immunity of mucosa and the using of Lactobacillus sobrius bacteria to counteract the effect of these mycotoxins Seeboth, Julie 25 October 2013 (has links) Les mycotoxines sont des métabolites secondaires des moisissures qui peuvent naturellement contaminer de nombreux supports (céréales, fruits, papiers peints, compost). Dans ces travaux de thèse, nous avons focalisé notre intérêt sur deux mycotoxines produites principalement par les champignons du genre Fusarium, appartenant toutes deux au même groupe des trichothécènes, le déoxynivalénol (DON) et la toxine T-2 (T-2). Les objectifs de cette thèse ont été de déterminer les effets de ces deux toxines sur la mise en place des réponses immunitaires au sein de la muqueuse respiratoire et intestinale. L’ensemble de ces études a été réalisé chez le porc, espèce cible de ces contaminants et animal modèle pour l’Homme. Les résultats de ces travaux ont montré que ces deux toxines affectent la réponse immunitaire. Au niveau du tractus respiratoire, une faible dose de toxine T-2 altère l’activation des macrophages alvéolaires lorsqu’ils sont stimulés par les agonistes des TLRs -4, -2/6 (lipopolysaccharides et acides lipoteichoïques, respectivement) en diminuant la synthèse du composé antimicrobien NO et des cytokines pro-inflammatoires IL-1β et TNF-α. Cette immunosuppression pourrait alors conduire à une susceptibilité plus accrue des porcs à des infections opportunistes. Au niveau du tractus intestinal, à l’état basal, nous avons mis en évidence que le DON comme la toxine T-2 induit une forte réponse inflammatoire innée associée à la stimulation de la voie IL-17 en inhibant le développement des cellules T régulatrices. Des études mécanistiques ont permis de déterminer que les cytokines associées à la voie IL-17 suite à une exposition aux trichothécènes, sont produites par une des sous-populations de cellules T innées, les cellules Tγδ productrices d’IL-17. La troisième partie de ce travail a porté sur l’utilisation de la souche Lactobacillus sobrius DSM 16698T dans le but de lutter contre les effets immunomodulateurs générés lors d’une exposition aux trichothécènes. Les résultats de ce travail ont montré que cette souche bactérienne est capable de réduire les effets inflammatoires IL-17 et de rétablir les paramètres impliqués dans les fonctions de la barrière intestinale, suite à une exposition ex vivo et in vivo au DON. En revanche, cette souche a peu d’effet contre la toxine T-2. L’ensemble de ce travail de thèse suggère donc qu’une exposition à de faibles doses de trichothécènes pourrait accroître la susceptibilité des animaux aux perturbations de nature infectieuse ou inflammatoire. / Mycotoxins are fungi secondary metabolites that can contaminate a lot of environments worldwild such as cereals, fruits, wallpapers, and compost heaps. Throughout this phD work, we focused on two mycotoxins mainly produced by Fusarium species, both belonging to the trichothecenes group: the deoxynivalenol (DON) and the T-2 toxin (T-2). The aims of this study were to determine the effects of these two toxins on the immune response implementation in respiratory and intestinal mucosa. Studies were performed on swine being a target species of these contaminants and a model species for Humans. The results of these works proved that these two mycotoxins can affect the immune response. In the respiratory tract, a low dose of T-2 toxin alters the activation of the alveolar macrophages when they are stimulated by the agonists of TLRs -4 and -2/6 (lipopolysaccharides and lipoteichoic acids, respectively). This alteration is due to the decrease of the synthesis of the anti-microbial compound NO and the pro-inflammatory cytokines such as IL-1β and TNF-α. This immunosuppression can induce the emergence of opportunist infections in pig. In the intestinal tract, in background level, we demonstrated that DON as well as T-2 toxin induces a strong inflammatory immune response associated with stimulation of IL-17 pathway by inhibiting of the development of regulatory T cells. Mechanistic studies were used to determine the production origin of the cytokin associated to the IL-17 pathway. This cytokine is produced by one of the subpopulations of Tregs, the Tγδ cells IL-17 producing when exposed to trichothecenes. The third part of this work was about the use of Lactobacillus sobrius DSM 16698T strain to counteract the immunomodulatory effects induced after trichothecen exposure. The results of this study showed that this bacterial strain is able to reduce IL-17 inflammatory effect and is also able to re-etablish the parameters involved in the intestinal barrier functions in ex vivo and in vivo response to DON. Nevertheless, this strain is less effective against the T-2 toxin. Taken together, results of this phD suggest that an exposure to low doses of trichothecens could be intensify the susceptibility of animal to infectious or inflammatory disease. Déoxynivalénol Toxine T-2 Muqueuses respiratoire et intestinale Réponses immunitaires Homéostasie Balance IL-17/Tregs Bactérie commensale Porc Maladies inflammatoires intestinales Deoxynivalenol T-2 toxin Respiratory and intestinal mucosa Immune responses Homeostasis IL-17/Tregs balance Commensal bacteria Pig Intestinal bowel disease
69	Identification et caractérisation moléculaire et fonctionnelle des cellules tissulaires de l’immunité innée chez les patients atteints de maladies inflammatoires intestinales Chapuy, Laurence 01 1900 (has links) Les maladies inflammatoires intestinales (MII), maladie de Crohn (MC) et colite ulcéreuse (CU), représentent un problème de santé publique majeur en raison de leur prévalence, de leur chronicité et de l’absence de traitement curatif disponible. La physiopathologie de ces maladies implique des facteurs de prédisposition génétique, des facteurs environnementaux et une réponse anormale du système immunitaire. De par leur position à l’interface entre les facteurs environnementaux, les cellules épithéliales et les cellules de l’immunité adaptative, les cellules de l’immunité innée (phagocytes monocucléés (MNPs) et granulocytes) sont des acteurs importants dans l’initiation et le maintien de l’inflammation intestinale. Largement étudiés chez la souris, leur investigation chez l’humain restait parcellaire, souvent contradictoire dans le colon et rarement étudiée dans le ganglion mésentérique (MLN). Nous avons caractérisé par des méthodes de cytométrie de flux multi-couleurs, de cytométrie de masse (CyTOF) et de séquencage de l’ARN (total et à l’échelon de la cellule unique), les MNPs de la muqueuse colique et des ganglions mésentériques chez les patients atteints de MC et de CU. Nous avons également évalué la fonction des MNPs et des basophiles sur les réponses mémoires T CD4+ autologues tissulaires. Notre travail a mis en évidence des similitudes et des différences entre la MC et la CU, dans la distribution des MNPs et le profil de la réponse mémoire T CD4+ dans le colon et le ganglion. La sous-population de MNPs HLADR+SIRPα+CD14+CD64+CD163- qualifiée de monocytes inflammatoires, et non les macrophages HLADR+SIRPα+CD14+CD64+CD163+, s’accumule dans la muqueuse inflammatoire des patients atteints de MC et de CU, et promeut les réponses mémoires de type Th17 et Th17/Th1 d’une manière dépendante de l’IL-1β. La fréquence de cette population corrèle avec le score de sévérité endoscopique en MC. Cependant, la distribution des MNPs ganglionnaires diffère entre la MC et la CU. Nous montrons que, dans les ganglions des patients atteints de CU, les MNPs HLADR+SIRPα+CD14+CD64+ sont enrichis en cellules CD163+, qui incluent principalement des cellules ‘monocyte-like’ HLA-DRdim en plus de macrophages HLA-DRhi. Parmi les cellules dendritiques (DCs) HLADR+SIRPα+CD14-CD64-, les DCs plasmocytoides prédominent dans les deux MII, avec une fréquence supérieure en MC qu’en CU. Par ailleurs, l’IL-1β dans la MC et l’IL-12 dans la CU favorisent un profil pathogénique dans les lymphocytes T CD4+ (IFN-γ, TNF-α, GM-CSF, IL-6) de la muqueuse colique. Par sérendipité, nous avons aussi mis en évidence que l’IL-12 et les monocytes inflammatoires tissulaires induisent la production d’IL-8 par les lymphocytes T CD4+ mémoires de la muqueuse intestinale et des MLNs dans la CU mais pas dans la MC. Au cours de cette étude, nous avons également observé l’accumulation de basophiles, mais pas de mastocytes, dans la muqueuse colique et le MLN en MC et en CU, et montré qu’ils favorisaient également les réponses Th17 et Th17/Th1 et non Th1 dans les lymphocytes T CD4+ mémoires exprimant CCR7. En conclusion, la caractérisation des MNPs de la muqueuse intestinale et des MLNs dans les maladies inflammatoires intestinales (MII) permet de mieux appréhender la physiopathologie de la maladie, dans l’espoir d’optimiser la stratification des MII et de permettre ainsi une prise en charge thérapeutique personnalisée. / Crohn's disease (CD) and ulcerative colitis (UC), two common forms of inflammatory bowel disease (IBD), represent a major public health problem because of their prevalence, chronicity and lack of available curative treatment. The pathophysiology of these diseases involves predisposing genetic factors, environmental triggers, and a dysfunctional immune response. Innate immune cells, including mononuclear phagocytes (MNPs) and granulocytes, are important players in the initiation and maintenance of intestinal inflammation due to their position at the interface between the external environment, epithelium and adaptive immune cells. Although widely studied in mice, their investigation in humans remains fragmentary, often with contradictory findings reported in the colon, and they are rarely studied in the mesenteric lymph nodes (MLNs). MNPs from the colon and MLNs of patients with CD and UC were characterized by multi-color flow cytometry, mass cytometry (CyTOF) and RNA sequencing (bulk and single cell). The function of MNPs and basophils on autologous memory CD4+ T cell responses was also assessed. The results presented here highlight similarities and differences in the distribution of MNPs between CD and UC, and the profile of memory CD4+ T cell response in colon and MLNs. HLADR+SIRPα+CD14+CD64+CD163- MNPs, defined as inflammatory monocytes, but not HLADR+SIRPα+CD14+CD64+CD163+ macrophages, accumulated in the inflammatory mucosa of CD and UC patients, and promoted Th17 and Th17/Th1 memory responses in an IL-1β dependent manner. The frequency of this subpopulation correlated with endoscopic severity in CD. In contrast, the distribution of these two MNP populations in the MLNs differs between CD and UC. HLADR+SIRPα+CD14+CD64+ MNPs were enriched in CD163+ cells that predominantly included HLA-DRdim monocytes-like cells over HLA-DRhi macrophages in UC patients only. Among HLADR+SIRPα+CD14-CD64- dendritic cells (DCs), plasmocytoid DCs predominated in both UC and CD, with higher frequency in CD versus UC. IL-1β in CD and IL-12 in UC favor a pathogenic CD4+ T cell profile (IFN-γ, TNF-α, GM-CSF, IL-6 expression/production) in the colonic mucosa. It was also demonstrated that IL-12 and inflammatory tissue monocytes induced IL-8 production by memory CD4+ T cells in intestinal mucosa and MLNs of UC but not CD. In this study, it was also observed that basophils and not mast cells accumulated, in the colonic mucosa and MLNs of CD and UC patients, and favored Th17 and Th17/Th1, but not Th1, responses in CCR7+ memory CD4+ T cells. In conclusion, characterization of MNPs in the intestinal mucosa and MLNs of IBD patients contributes to a better understanding of IBD pathophysiology and opens avenues to optimize patient stratification, and thus, personalized treatment of IBD patients. Maladies inflammatoires intestinales Immunité innée maladie de Crohn Colite ulcéreuse Inflammatory bowel diseases Ulcerative colitis Crohn's disease Innate immunity

Search results