Estudo da imunomodulação induzida pela crotoxina do veneno de Crotalus durissus terrificus em modelo experimental de doença inflamatória no intestino. / Evaluation of immunomodulation induced by crotoxin from Crotalus durissus terrificus snake venom in experimental model of inflammatory bowel disease.

Caroline de Souza Almeida

16 June 2014

Neste trabalho foi estudado o potencial imunorregulador da crotoxina (CTX) obtida do veneno de C. d. terrificus, em modelo experimental de colite induzida pelo TNBS em camundongos. A CTX foi capaz de diminuir a perda de peso, o score clínico e histológico, síntese de MPO e citocinas pró-inflamatórias. Menor número de neutrófilos e macrófagos com fenótipos M1 e M2 na lâmina própria foi observado nos grupos TNBS/CTX em relação ao TNBS. A CTX induziu TGF-b e IL-10, PGE2 e LXA4. A neutralização in vivo dessas citocinas ou o bloqueio da síntese desses eicosanoides indica que estas moléculas exercem papel relevante na ação moduladora da CTX no quadro inflamatório. As análises das diferentes populações celulares da lâmina própria, linfonodos e Placas de Peyer mostraram que não houve diferença nos linfócitos CD4+Tbet+ entre os grupos TNBS e TNBS/CTX. No entanto, a CTX promoveu aumento de CD4+FoxP3+ e diminuição de CD4+RORg+. Estes resultados indicam que a CTX é capaz de modular a resposta inflamatória aguda intestinal melhorando o quadro clinico observado nos animais. / In this work it was analyzed the immunomodulatory effect of crotoxin (CTX) isolated from C.d. terrificus snake venom, on the experimental model of colitis induced by TNBS in mice. The CTX was able to inhibit the weight loss, clinical and histological score, MPO synthesis and pro-inflammatory cytokines. Lower number of neutrophils and macrophage (M1 and M2) in lamina propria was observed in TNBS/CTX mice compared with the TNBS group. In contrast, the CTX induced increased TGF-b, IL-10, PGE2 and LXA4. The in vivo neutralization of these cytokines or eicosanoids synthesis indicates that these molecules exert significant role in the modulatory effect of CTX. The analyzes of distinct cell populations from lamina propria, lymph nodes and Peyers pathes showed no difference in CD4+Tbet+ between TNBS or TNBS/CTX mice. However, CTX induced an increase of CD4+FoxP3+ and decreased CD4+RORgt+. Together, these results indicate that CTX is able to modulate intestinal acute inflammatory response induced by TNBS improving the clinical status of the mice.

Crotalus durissus terrificus

Células T reguladoras e Th17

Crotoxina

Imunomodulação

Inflamação intestinal

TNBS

Crotalus durissus terrificus

Crotoxin

Immunomodulation

Inflammatory bowel disease

T regulatory and Th17 cells

TNBS

Avaliação da atividade anti-inflamatória intestinal da dieta enriquecida com farinha de Coix lachryma-jobi L. no modelo de inflamação intestinal induzida por TNBS em ratos

Guimarães, Ariane Fernandes

January 2019

Orientador: Luiz Claudio Di Stasi / Resumo: A Doença Inflamatória Intestinal é uma doença considerada multifatorial com etiologia ainda pouco elucidada que compreende duas principais formas clinicas, denominadas como Retocolite Ulcerativa e a Doença de Crohn que induzem quadros crônicos de inflamação em diferentes regiões do trato gastrointestinal, com períodos de exacerbação e remissão dos sintomas. Os tratamentos farmacológicos disponíveis para a doença apresentam sérios efeitos colaterais e alto custo, o que faz com que o desenvolvimento de estratégias complementares de prevenção e tratamento seja uma importante meta na terapia da DII. A busca por estratégias complementares de prevenção e tratamento, como o uso de alimentos funcionais ricos em fibras e compostos bioativos, é uma perspectiva promissora, visto que as fibras têm sido associadas à promoção de efeitos prebióticos com consequente proteção ao processo inflamatório intestinal. Coix lacryma-jobi L., é uma planta cuja semente é rica em fibras e são amplamente utilizadas tanto na culinária quanto na medicina tradicional chinesa onde são indicadas para o tratamento de diversas doenças. Este trabalho tem como objetivo avaliar os efeitos da dieta enriquecida com farinha das sementes inteiras C. lachryma-jobi. no modelo de inflamação intestinal induzida por ácido trinitrobenzenosulfônico em ratos. Para tanto foram testadas três dietas com ração enriquecida de farinha de C. lachryma-jobi nas proporções de 5%, 10% e 20%, onde foram avaliados parâmetros clínicos (con... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Inflammatory Bowel Disease is a multifactorial disease with a not fully elucidated etiology that comprises two main clinical forms designate as Ulcerative Colitis and Crohn's Disease, which present chronic inflammation in different regions of the gastrointestinal tract, with periods of exacerbation and remission of the symptoms. The pharmacological treatments available for the disease have serious side effects and high cost, which makes the development of complementary prevention and treatment strategies an important goal in IBD therapy. The search for complementary treatment and prevention strategies, such as the use of functional foods rich in fiber and bioactive compounds, are a promising prospect, since the fibers have been associated with the promotion of prebiotic effects with consequent protection of the inflammatory bowel process. Coix lacryma-jobi L., is a plant containing seed rich in fiber and are widely used both in cooking and traditional Chinese medicine for the treatment of several diseases. This work aims to evaluate the effects of the diet enriched with flour of the whole seeds of C. lachryma-jobi in the experimental model of intestinal inflammation induced by trinitrobenzenesulfonic acid in rats. Three diets enriched with C. lachryma-jobi flour were tested in the proportions of 5%, 10% and 20% and were evaluated in the clinical parameters (daily food intake, body weight, diarrhea), macroscopic damage (score, lesion extension, weight/length ratio, adherence),... (Complete abstract click electronic access below) / Mestre

Doença Inflamatória Intestinal

TNBS

Adlay

lágrimas de Nossa Senhora

Doenças inflamatórias intestinais.

Job tears

Platelet-Derived Growth Factor-BB is the Dominant Mitogen for Intestinal Smooth Muscle Cells in the Trinitrobenzenesulfonic Acid Model of Rat Colitis

Stanzel, ROGER

28 September 2012

In normal adult physiology, intestinal smooth muscle cells (ISMC) are characterized as contractile and non-proliferative. Inflammation induces permanent changes to the intestine including hypertrophy of the smooth muscle layer largely due to smooth muscle cell (SMC) proliferation. While the consequences of this hyperplasia are largely unknown, increased muscularis mass may present permanent challenges to organ motility. Similar SMC hyperplasia is observed in other inflammatory pathologies including atherosclerosis and pulmonary arterial hypertension (PAH) where SMC de-differentiate into a ‘synthetic’ phenotype and the mitogens responsible for hyperplasia have been well studied. However, there are limited investigations of SMC mitogens in intestinal inflammation. The identification of these factors may be of critical importance in the case of intestinal strictures, whereby recurring inflammation can lead to bowel obstruction requiring surgical intervention. A novel, primary rat ISMC model was developed to identify the factors responsible for ISMC proliferation in vitro. Primary ISMC cultures are likely more representative of SMC in vivo than the commonly used late-passage cultures. As such, this primary ISMC model is valuable in the evaluation of mitogens involved in the onset of proliferation. This primary ISMC model was used to conduct a comprehensive evaluation of potential mitogens including basic fibroblast growth factor (bFGF), epidermal growth factor (EGF), insulin-like growth factor-1 (IGF-1) and platelet-derived growth factor-BB (PDGF-BB. This work identified IGF-1 and PDGF-BB as ISMC mitogens. However, multiple lines of evidence indicated that PDGF-BB was a more potent mitogen and the involvement of PDGF-BB was subsequently examined in vivo using the trinitrobenzenesulfonic acid (TNBS) model of rat intestinal inflammation. While control ISMC lacked expression of the PDGF-BB receptor (PDGF-Rβ), robust expression was observed within only 6 hr following the induction of TNBS inflammation. By Day 2, when ISMC proliferation in vivo is maximal, freshly isolated ISMC showed on-going PDGF-Rβ activation that was further increased by exogenous PDGF-BB. Taken together, the conclusions from this work in vitro identify PDGF-BB as a potent ISMC mitogen in vivo. Further, this work establishes PDGF-BB and its receptor as potential targets in the medical treatment of intestinal stricture formation. / Thesis (Ph.D, Biology) -- Queen's University, 2012-09-24 19:26:57.201

Intestinal Inflamation

Intestinal Smooth Muscle Cells

TNBS

Mitogen

IGF-1

PDGF-BB

Gial cell line-derived neutrotrophic factor expression in proliferating intestinal smooth muscle cells is important for enteric neuron survival

HAN, TIAN YU

28 September 2012

Normal intestinal functions are coordinated by enteric neurons within the enteric nervous system (ENS). In the embryonic and neonatal gut, enteric neuron survival is dependent on the expression of glial cell line-derived neurotrophic factor (GDNF) from its targets of innervation - the intestinal smooth muscle cells (ISMC). In the inflamed adult intestine, enteric neuron loss is immediately followed by ISMC proliferation, resulting in severe disruption of normal intestinal functions. Although GDNF can support the survival of postnatal enteric neurons, whether adult ISMC can secrete GDNF and support neuron survival is unclear. Results from qPCR analysis showed that freshly isolated adult ISMC have acquired the ability to express GDNF at the onset of proliferation, in vitro. Western blot analysis indicates that GDNF continues to be upregulated in ISMC at Passage 2 (P2), but its expression is decreased after long periods of proliferation at Passage 10 (P10). A neuron survival bioassay suggests that GDNF expression is correlated with enteric neuron survival. Results showed that P2 ISMC or conditioned media (CM) - but not P10 ISMC and CM, significantly increased enteric neuron survival. In subsequent experiments, the RET tyrosine kinase inhibitor vandetanib was used to block GDNF receptor-ligand interactions, and anti-GDNF neutralizing antibody was used to sequester soluble GDNF within the culture media. Both methods were successful at decreasing myenteric neuron survival. Furthermore, abolishing GDNF expression in P2 ISMC with GDNF siRNA also resulted in a decreased myenteric neuron survival. The above observations suggest that ISMC-derived GDNF is important in supporting myenteric neuron survival in vitro. / Thesis (Master, Neuroscience Studies) -- Queen's University, 2012-09-28 09:43:23.968

Enteric nervous system

ISMC proliferation

intestinal inflammation

TNBS-induced colitis

GDNF

myenteric plexus

Enteric neuron

Avaliação da atividade anti-inflamatória intestinal de Cnidoscolus aconitifolius (Mill.) I.M. Johnst no modelo de indução por TNBS em ratos

Moya Dalmau, Lesvi

January 2018

Orientador: Luiz Claudio Di Stasi / Resumo: A Doença Inflamatória Intestinal (DII) inclui duas principais doenças: a Doença de Crohn e a Retocolite Ulcerativa, ambas caracterizadas por períodos de exacerbação dos sintomas acompanhados por intervalos prolongados de remissão. Apesar da etiologia ser pouco elucidada, sabe-se da influência de fatores genéticos, imunológicos e ambientais. A terapia farmacológica atual não é eficaz para todos os pacientes, apresenta alto custo e desencadeia diversos efeitos colaterais, portanto é necessário o desenvolvimento de novas terapias sendo que as plantas medicinais e componentes presentes na dieta, devido as suas propriedades antioxidantes e/ou imunomoduladora, apresentam uma opção atrativa como terapia complementar. A espécie Cnidoscolus aconitifolius (Mill.) I.M. Johnst, popularmente conhecida como chaya, foi selecionada dada sua composição química, rica em fibra e compostos antioxidantes e suas atividades antioxidante e anti-inflamatória testadas em outras afecções. O objetivo deste trabalho foi avaliar a atividade anti-inflamatória intestinal das folhas escaldadas e desidratadas de chaya em duas formas: como extrato metanólico 70% (100, 200 e 300 mg/kg, via oral por gavage) e como farinha incorporada na dieta nas concentrações 5, 10 e 20%, no modelo de indução de inflamação intestinal pelo ácido trinitrobenzenosulfonico (TNBS) em ratos. Para tanto, foram avaliados os parâmetros clínicos gerais (ingestão diária de alimentos, peso corporal, diarréia), parâmetros macroscópicos da l... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Inflammatory Bowel Disease (IBD) comprise two major diseases, Crohn's disease and Ulcerative Colitis, both characterized by periods of exacerbation of symptoms accompanied by prolonged remission intervals. Although the etiology is not certain elucidated, the influence of genetic, immunological and environmental factors is well known. The current pharmacological therapy is not effective for all patients, due to a high cost and triggers several side effects. Therefore, it is necessary to develop new therapies and medicinal plants with their antioxidant and/or immunomodulatory properties are an attractive option as complementary therapy. Cnidoscolus aconitifolius (Mill.) I.M. Johnst, popularly known as chaya, was selected because of its chemical composition, rich in fiber and antioxidant compounds and its antioxidant and anti-inflammatory activity tested in other diseases. The aim of this study was to evaluate the intestinal anti-inflammatory activity of the blanched and dehydrated Chaya leaves in two preparations: as a 70% methanol extract (100, 200 and 300 mg/kg, oral route by gavage) and as flour incorporated in the diet at 5%, 10% and 20% concentrations in the experimental model of intestinal inflammation induced by trinitrobenzenesulfonic acid (TNBS) in rats. For that, clinical parameters (daily food intake, body weight, diarrhea), macroscopic damage (score, lesion extension, weight/length ratio and adherence), biochemical parameters (quantification of total glutathione con... (Complete abstract click electronic access below) / Doutor

Doença Inflamatória Intestinal

TNBS

Cnidoscolus aconitifolius

chaya

alimento funcional

functional food

Doenças inflamatórias intestinais.

Avaliação da dieta enriquecida com Persea americana Mill. na inflamação intestinal induzida por TNBS em ratos

Oliveira, Ellen Cristina Souza

January 2016

Orientador: Aline Witaicenis Fantinati / Resumo: A Doença Inflamatória Intestinal (DII) engloba duas principais doenças: a Doença de Crohn e a Retocolite Ulcerativa. Esta doença é multifatorial com etiologia complexa e não totalmente elucidada. Considerando-se que não existe cura e que os fármacos utilizados podem apresentar sérios efeitos colaterais, além de muitos pacientes não responderem aos tratamentos disponíveis; estudos voltados para o desenvolvimento de novas estratégias de tratamento são importantes. Estudos têm evidenciado que a associação entre fármacos e alimentos funcionais, pode resultar em uma relação de muito sucesso no tratamento de pacientes com doenças crônicas, sobretudo nas doenças que afetam o trato gastrointestinal. Assim, o uso de alimentos funcionais, especialmente, os ricos em fibras, compostos antioxidantes e lipídeos bioativos podem ser potenciais na prevenção ou tratamento da DII. Com base nisto, a espécie Persea americana Mill., conhecida popularmente como abacate ou avocado, foi selecionada para o presente estudo, pois além de possuir estes compostos, apresenta descrita atividade antioxidante, anti-cancerígena, anti-bacteriana, anti-inflamatória e cicatrizantes. Diante disso, o presente estudo teve como objetivo avaliar a atividade da dieta enriquecida com a polpa de Persea americana Mill. var. Hass no modelo experimental de inflamação intestinal induzida por TNBS em ratos. Para tanto, a polpa da espécie foi incorporada na dieta de ratos Wistar machos, nas concentrações de 5%, 10% ou 20%, por... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Inflammatory Bowel Disease (IBD) comprises two major diseases: Crohn Disease and Ulcerative Colitis. This disease is multifactorial with complex and not fully elucidated etiology. Considering that there is no cure and the drugs may cause serious side effects, and many patients do not respond to the available treatments; therefore researches focused on the development of new treatment strategies are important. Studies have evidenced that the association between drugs and functional foods can result in a very successful relationship forward treating patients with chronic diseases, mainly diseases that affect the gastrointestinal tract. Thus, the use of functional foods, especially ones rich in fibers, antioxidants and bioactive lipids could be potential candidates to the prevention or treatment of IBD. Based on this, Persea americana Mill., popularly known as avocado, was selected for this study, due to the presence of mentioned compounds and also for the antioxidant, anti-cancer, anti-bacterial, anti-inflammatory and cicatrizing activities. Therefore the present study aimed to evaluate the activity of enriched diet with Persea americana Mill. var. Hass pulp in the experimental model of intestinal inflammation induced by TNBS in rats. For this, the fruit pulp was incorporated in the diet of male Wistar rats, in concentrations of 5%, 10% or 20% for 21 days before and 7 days after of induction of intestinal inflammation by TNBS and the animals were killed on the 29º day. Addition... (Complete abstract click electronic access below) / Mestre

Doença Inflamatória Intestinal

TNBS

Alimentos funcionais.

Abacate.

Abacate.

Doenças inflamatórias intestinais.

Functional foods

Abacate.

Avocado

Etude des mécanismes cellulaires et moléculaires impliqués dans la fonction suppressive des lymphocytes T régulateurs/Study of molecular and cellular mechanisms involved in regulatory T cell suppressive activity

DENOEUD, Julie

18 June 2010

La réponse immune représente une réponse complexe à laquelle correspond une succession d’événements orchestrés finement. Parmi les mécanismes qui régulent la réponse immune, les lymphocytes T régulateurs (Tregs) assurent le maintien de la tolérance en périphérie et le contrôle des réponses immunes adaptatives. Ils représentent une population hétérogène et leurs mécanismes de suppression sont toujours l’objet d’intenses recherches. Suivant le contexte de suppression et leur nature, les lymphocytes Tregs réalisent une inhibition de l’activation des lymphocytes Th, soit directement, soit via la modulation de la fonction des cellules dendritiques (DC). Dans un modèle d’immunisation par des cellules dendritiques chargées de KLH, les lymphocytes Tregs naturels contrôlent sélectivement l’initiation des réponses de type Th1/CTL spécifiques de l’antigène. Le but de ce travail était de définir quels sont les acteurs potentiels du contrôle de cette réponse. A l’aide de l’anticorps PC61 dirigé contre le récepteur CD25 et éliminant les lymphocytes Tregs naturels, nous avons montré que le ligand de costimulation CD70 joue un rôle clé dans leur régulation de la réponse Th1/CTL (Article 1). Ainsi, dans des conditions normales, la cytokine IL-12 induit principalement l’initiation de la réponse Th1 in vivo, tandis qu’en l’absence de lymphocytes Tregs naturels, la voie CD70/CD27 est une voie alternative d’induction de l’IFN-γ. Cette voie d’activation pourrait être opérationnelle dans certains contextes infectieux lorsque les lymphocytes Tregs sont déstabilisés voire éliminés, par exemple lors d’infections par Toxoplasma gondii ou par les virus HTLV1, SIV ou HIV. Nous avons montré que les lymphocytes Tregs naturels diminuent l’expression du ligand CD70 sur les DC, de manière dépendante de son récepteur CD27. Ensuite, nous nous sommes intéressés à une deuxième population de lymphocytes T régulateurs, les lymphocytes Tregs ICOShigh induits in vivo par le traitement avec l’anticorps anti-CTLA-4. Dans le cadre d’une colite induite par l’agent alkylant TNBS et mettant en jeu une réponse Th1, cette population de lymphocytes Tregs amplifiée par le traitement à l’anticorps anti-CTLA-4 régule la réponse immune via la cytokine anti-inflammatoire IL-10 et l’enzyme immunosuppressive IDO (Article 2). Ainsi, les résultats obtenus nous ont permis de répondre à notre objectif et de définir certains mécanismes de suppression des lymphocytes Tregs naturels et des lymphocytes Tregs induits. Dans la dernière partie de ce travail, nous avons cherché à comparer les populations de lymphocytes Tregs naturels et ICOShigh présentes dans l’intestin d’une souris naïve. Une analyse transcriptomique a révélé que ces deux populations s’opposent sur les plans phénotypique et fonctionnel. Nous proposons un modèle dans lequel les deux populations de lymphocytes Tregs agiraient en synergie pour maintenir l’homéostasie intestinale. Les lymphocytes Tregs ICOShigh différenciés au niveau local et continuellement activés contrôleraient la réponse inflammatoire associée à la présence de la flore commensale. Les lymphocytes Tregs naturels, en quiescence dans les ganglions mésentériques, n’interviendraient qu’en cas d’infection par des pathogènes. L’étude des lymphocytes T régulateurs soulève un certain nombre de concepts clés de l’immunité : la spécificité des réponses, la distinction des microorganismes commensaux et pathogènes… Mieux connaître les lymphocytes Tregs dans un modèle murin permettra de mieux comprendre les réponses inflammatoires intestinales chroniques observées chez l'homme et d’envisager, à terme, de nouveaux traitements. / An immune response is complex and implies numerous sequential events. It is regulated by different mechanisms, among which regulatory T cells maintain peripheral tolerance and control adaptive immune responses. Regulatory T cells are very heterogeneous and suppress immune responses through different mechanisms, still under investigation. They can inhibit T cell activation directly or through the modulation of dendritic cell function, depending on their nature and the tissular context. In a dendritic cell-mediated immunization model, naturally occurring regulatory T cells selectively control the priming of antigen-specific Th1/CTL responses. Our goal was to define the potential actors of this control, targeted by natural regulatory T cells. Using the PC61 antibody which targets and depletes these cells, we showed that the costimulation ligand CD70 plays a key role in their control of Th1/CTL responses (first article). We showed that mainly IL-12 provokes Th1 development in normal conditions, wheras CD70 plays a major role in priming Th1 responses in the absence of natural Tregs. This pathway can be operational if regulatory T cells are destabilized or even depleted, for example during infection with Toxoplasma gondii or with HTLV1, SIV or HIV. We showed that natural Tregs downregulate CD70 expression on the surface of DCs. Next, we focused on another regulatory T cell population, induced in vivo by the anti-CTLA-4 mAb treatment. In a model of pro-Th1 colitis, induced by the alkylating agent TNBS, these ICOShigh regulatory T cells exert an IL-10 and IDO-dependant control over the immune response (second article). Thus, we succeeded in determining some control mechanisms of the immune response targeted by two populations of regulatory T cells. Finally, we compared two regulatory T cell populations: naturally occurring regulatory T cells and ICOShigh regulatory T cells from the intestines of naïve mice. A transcriptional analysis revealed two populations phenotypically and functionally distinct. We proposed a model in which these populations act synergistically and both maintain intestinal homeostasis. ICOShigh regulatory T cells might control commensal gut flora-specific inflammatory responses and quiescent natural regulatory T cells from mesenteric lymph nodes might control potential pathogen infections. As a conclusion, this study raises some immunological issues: specificity of immune responses, distinction between commensal and pathogenic microorganisms… A better knowledge of these regulatory populations will lead to a better understanding of human intestinal responses and in the medium term will lead to new therapeutic approaches and tools.

CD70

3-dioxygenase

indoleamin-2

Th1 responses

IL-10/ regulatory T cells

colite TNBS

IL-10

TNBS colitis

ICOS

anti-CTLA-4

ICOS

anti-CTLA-4

lymphocytes T régulateurs

réponse Th1

indoléamine-2

3-dioxygénase

CD70

Einflüsse von 17β-Östradiol, ER-subtypspezifischen Agonisten und Phytoöstrogenen auf inflammatorische Prozesse im Kolon

Seibel, Jan

28 August 2007

Die niedrige Inzidenz chronisch-entzündlicher Darmerkrankungen (CED) in ostasiatischen Ländern im Vergleich zu Westeuropa und den USA könnte auf unterschiedliche Lebensstile und Ernährungsgewohnheiten zurückzuführen sein. Asiaten nehmen mit der Nahrung viel höhere Mengen an Isoflavonen zu sich als Europäer und US-Amerikaner. Diese sind in der Lage, wie natürliche Östrogene an Östrogenrezeptoren (ER) zu binden. Für das Östrogen 17β-Östradiol (E2) sowie selektive Liganden des ERβ sind antiinflammatorische Wirkungen im Darm bereits nachgewiesen worden. Diese Arbeit untersuchte in Modellsystemen für CED die antiinflammatorischen Eigenschaften von Isoflavonen, speziell von Genistein, und stellte einen Vergleich mit synthetischen ER-selektiven Liganden sowie E2 her, um die Involvierung der beiden ER-Subtypen zu evaluieren. In tierexperimentellen Studien wurde der Einfluss der Testsubstanzen auf Ausprägung und Verlauf einer Kolitis in zwei Nagermodellen (HLA-B27 transgene Ratte und TNBS-induzierte Kolitis) analysiert. Ein Ernährungsexperiment, in dem eine Gruppe der Tiere bereits in utero sowie postnatal über Muttermilch und Futter hohen Phytoöstrogenspiegeln ausgesetzt war, zeigte wider Erwarten keine antiinflammatorischen Effekte auf die akute Ausprägung der induzierten Kolitis. Stattdessen waren die untersuchten Parameter bei dieser Ernährungsform gegenüber prä- und postnatal normal ernährten Tieren verstärkt. Dagegen bewirkte oral verabreichtes Genistein in der chronischen Phase der TNBS-induzierten Kolitis eine Unterdrückung der Entzündungsparameter im Darm. Die subkutane Verabreichung von Genistein, eines steroidalen ERβ-selektiven Agonisten, oder von E2 führte hingegen zu keiner signifikanten Einflussnahme auf die untersuchten Parameter in der akuten Phase der Inflammation. Zur Charakterisierung der molekularen Grundlagen einer antiinflammatorischen Wirkung von E2, synthetischen ER-selektiven Agonisten und Genistein wurden in vitro Studien mit Kolonkarzinomzelllinien (HT-29 und Caco-2) durchgeführt. Hierzu wurden die Zellen mit Interleukin-1β (IL-1β) stimuliert, was eine Induktion der inflammationsassoziierten Gene Cyclooxygenase-2 und Interleukin-6 auf mRNA Ebene bewirkte. Bis auf Genistein konnten für die getesteten Substanzen keine antiinflammatorischen Effekte auf die mRNA-Expression der induzierten Markergene beobachtet werden. Genistein bewirkte in Caco-2 Zellen eine Hemmung der untersuchten Gene. Weitere Analysen ergaben, dass die beiden Zelllinien ER nur schwach bzw. gar nicht exprimieren. Eine Transfektion von HT-29 Zellen mit ERα führte zu einer deutlichen Hemmung der Expression der Markergene durch E2, während eine Transfektion mit ERβ lediglich einen schwach hemmenden Effekt bewirkte. Die Ergebnisse der vorliegenden Arbeit legen nahe, dass die niedrigen CED-Inzidenzraten in Ostasien wohl nicht allein auf dem dortigen hohen Isoflavonkonsum beruhen, sondern auch anderen Komponenten des Lebensstils zuzuschreiben sind. Dennoch deutet sich an, dass das Genistein, bei oraler Administration, die Regeneration des geschädigten Darmgewebes im chronischen Erkrankungsverlauf unterstützen und damit auch zur Prävention von Kolonkarzinomen beitragen könnte. Bei antiinflammatorischen Effekten von ER-Liganden spielt die Transaktivierung von ER eine entscheidende Rolle. Die Wirkung von Genistein in untransfizierten Caco-2 Zellen legt jedoch auch die Teilnahme weiterer Mechanismen nahe, die noch zu untersuchen sind. Vor diesem Hintergrund erscheinen weiterführende Untersuchungen zum Einsatz von steroidalen ER-Agonisten und Genistein bei CED und den zugrunde liegenden Mechanismen als sinnvoll.

Entzündung

Kolitis

Östrogenrezeptor

Phytoöstrogene

Genistein

Darm

CED

TNBS

HLA-B27

HT-29

Caco-2

Kolon

ER-Agonisten

inflammation

Colitis

Estrogen receptor

phytoestrogens

genistein

intestinal tract

IBD

TNBS

HLA-B27

HT-29

Caco-2

colon

ER agonists

ddc:570

rvk:WD 5085

Sélection in vitro et in vivo de souches probiotiques ayant des propriétés bénéfiques contre l’inflammation, les infections et l’obésité / In vitro and in vivo screening of probiotics strains against inflammation, infections and obesity

Alard, Jeanne

19 September 2017

Des études récentes ont montré que le microbiote participe à l’homéostasie intestinale en contribuant au développement morphologique, à l’éducation du système immunitaire, aux mécanismes de défense de l’hôte et à la régulation du métabolisme. Une dysbiose de ce microbiote ainsi qu’une réduction de la diversité bactérienne a été observé dans diverses pathologies chroniques telles que les maladies inflammatoires chroniques (MICI) et l’obésité. Le microbiote constitue donc une cible thérapeutique de choix dans la prise en charge de ces maladies chroniques. Les probiotiques, microorganismes bénéfiques pour l’hôte représentent une alternative intéressante, mais dont les critères de sélection nécessitent d’être améliorés.Dans une première étude, nous avons pu mettre en évidence les propriétés bénéfiques d’un mélange de deux probiotiques comprenant un bifide et un lactobacille dans un modèle murin d’obésité résultant d’une alimentation riche en graisses (Alard et al, 2016). Ce mélange probiotique a réduit significativement la prise de poids, amélioré les paramètres inflammatoires et métaboliques dont l’insulino-résistance, et augmenté l’expression intestinale des récepteurs aux acides gras à chaine courte (AGCC). Il a également favorisé dans un système d’intestin artificiel la production de butyrate et propionate ; principaux AGCCs. Les effets protecteurs ont été associés à l’amélioration de la dysbiose du microbiote, notamment la restauration de l’abondance d’Akkermansia muciniphila.L’objectif principal de cette thèse a été ensuite de sélectionner au sein d’une collection de 23 souches bactériennes provenant de la société PiLèJe, une ou plusieurs souche(s) probiotique(s) possédant des propriétés protectrices contre les MICI et l’obésité. Les propriétés immuno-modulatrices des souches ainsi que leur capacité à renforcer la barrière intestinale ont été étudiées in vitro à l’aide cellules mononuclées sanguines humaines, puis dans un modèle in vitro de perméabilité membranaire, induite par la sensibilisation d’une monocouche de cellules Caco-2 par de l’eau oxygénée. Six souches ont été sélectionnées, cinq souches induisant de forts niveaux de la cytokine anti-inflammatoire IL-10 et capables de restaurer la barrière intestinale et une souche capable de renforcer fortement cette barrière. Ces souches ont été ensuite évaluées en modèles in vivo de colite chronique et aigüe induite par du TNBS (2,4,6 trinitrobenzene sulfonic acid). De façon intéressante les souches protégeant en colite aigüe ne protègent pas aussi efficacement en colite chronique et inversement.Nous avons poursuivi la sélection de souches ou mélanges de souches dans le contexte de l’obésité et des maladies métaboliques associées. Nous avons utilisé les mêmes critères que précédemment (capacités anti-inflammatoires et à restaurer la barrière intestinale) complétés par l’étude de la capacité des souches à limiter l’accumulation des lipides dans un modèle in vitro de différenciation adipocytaire basé sur l’utilisation de la lignée 3T3-L1 et à induire la sécrétion de peptides entéro-endocrines impliqués notamment dans la satiété par l’utilisation de la lignée murine de cellules entéro-endocrine STC-1. Trois mélanges de souches et une souche seule ont été sélectionnées et évaluées dans un modèle murin d’obésité induite par un régime hyperlipidique à 45% de gras. Nous avons pu mettre en évidence des capacités positives d’un mélange de deux souches et d’une souche seule à réduire la prise de poids, ainsi que l’inflammation dans le tissu adipeux.Ces résultats indiquent que des criblages in vitro basés sur l’étude des propriétés immunomodulatrices, des capacités à restaurer la barrière, à diminuer l’accumulation des lipides et à induire des peptides de satiété, permettent une pré-sélection de souches ou mélanges de souches ayant un effet protecteur et démontrent à nouveau que les capacités bénéfiques des probiotiques sont souche-dépendantes et spécifiques des modèles ciblés. / Recent studies have reported that the microbiota is involved in intestinal homeostasis by contributing to the morphological development, the education of the immune system, the mechanisms of defense, and to metabolic regulation. Dysbiosis of this microbiota as well as reduction in bacterial diversity has been observed in various chronic pathologies such as chronic inflammatory diseases (IBD) and obesity. The microbiota thus constitutes a therapeutic target of choice in the management of these chronic diseases. Probiotics, which are beneficial microorganisms for the host represent therefore an interesting alternative, however their selection criteria need to be improved.In a first study, we were able to highlight the beneficial properties of a mixture of two probiotics comprising a bifidobacteria and a lactobacilli, in a murine model of high fat diet (HFD)-induced obesity (Alard et al., 2016). This probiotic mixture significantly reduced weight gain, improved inflammatory and metabolic parameters including insulin resistance, and increased intestinal expression of receptors involved in short-chain fatty acid (AGCC) recognition. It also promoted in an artificial intestinal system the production of butyrate and propionate, the two main AGCCs. The protective effects were associated with the improvement of microbiota dysbiosis, in particular the restoration of the abundance of Akkermansia muciniphila.The main objective of this thesis was then to select within a collection of 23 bacterial strains provided by PiLèJe, one or more probiotic strain (s) possessing protective properties against IBD and obesity. Immunomodulatory properties of the strains and their ability to strengthen the intestinal barrier were studied in vitro using human mononuclear blood cells and an in vitro model of epithelial permeability induced by the sensitization of a Caco-2 cells monolayer with hydrogen peroxide. Six strains were selected, five strains inducing high levels of the anti-inflammatory cytokine IL-10 and capable of restoring the intestinal barrier and a strain capable of strongly reinforcing this barrier. These strains were then evaluated in in vivo models of TNBS (2,4,6 trinitrobenzene sulfonic acid)-induced chronic and acute colitis. Interestingly, strains able to rescue mice from acute colitis did not protect as efficiently in chronic colitis and vice versa.The selection of strains or mixtures was then pursued in the context of obesity and associated metabolic diseases. We used the same criteria as previously (anti-inflammatory capacities and to restore the intestinal barrier) in addition with the capacity of the strains to limit the accumulation of lipids in an in vitro model of adipocyte differentiation based on the use of the 3T3-L1 cell line and to induce the secretion of entero-endocrine peptides, notably involved in satiety, by the use of the murine STC-1 entero-endocrine cell line. Three mixtures and one single strain were selected and evaluated in a mouse model of obesity induced by 45% HFD diet. We demonstrated the positive capacities of a mixture composed of two strains and the single strain to reduce weight gain, as well as adipose tissue inflammation.These results indicate that in vitro screenings based on the immunomodulatory properties, the capacity to restore the gut barrier, to decrease lipid accumulation and to induce gut peptides allow pre-selection of strains or mixtures exhibiting protective effects and demonstrate that the beneficial capacities of probiotics are strain-dependent and specific to the targeted models.

Probiotiques

Obésité

MICI

Modèles animaux

Techniques in vitro

TNBS

In vivo

Colite

In vitro model

Obesity

Chronic inflammatory diseases

Probiotics

Evolução dos perfis elétricos e mecânicos da motilidade colônica em modelo animal de doença inflamatória intestinal

Calabresi, Marcos Felipe de Freitas.

January 2017

Orientador: José Ricardo de Arruda Miranda / Resumo: Inflammatory bowel disease (IBD) is an idiopathic gastrintestinal tract disease that affects a large part of the world population and has its symptoms related to changes in colon motility. However, the evolution of these changes is not completely understood, and may be related to symptoms that appear in stages when the disease is apparently controlled. The objective of this work was to perform a long-term evaluation of the mechanical and electrical aspects of colonic contractility during the model of inflammation induced by trinitrobenzene sulfonic acid (TNBS) in rats. This work applied an efficient and low invasive methodology associating mechanical, electrical, chemical and histological information. The contractility and inflammatory parameters were acquired in the same animal at six different times: before induction of TNBS (control) and at 2, 5, 8, 11 and 14 days thereafter. The mechanical activities were acquired by Alternating Current Biosusceptometry (ACB) and subdivided in Rhythmic Propagation Ripples (RPR) and Rhythmic Propulsive Motor Complex (RPMC). We recorded the electrical activity by electromyography (EMG) and evaluated the inflammation processes determining the myeloperoxidase activity (MPO) in the feces. Additionally, we compared the thickness of colon layers throughout the inflammation by histopathological analyzes. Our results showed transient changes in MPO activity levels and frequency of RPMC contraction, while RPR and electrical activity underwent perma... (Resumo completo, clicar acesso eletrônico abaixo) / Doutor

Motilidade colônica

Doença inflamatória intestinal

TNBS

Contratilidade colônica

Biosusceptometria de Corrente Alternada.

Colonic motility

Doenças inflamatórias intestinais.

Colonic contractility

Alternating current biosusceptometry