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231	Smart drug delivery systems designed to improve Inflammatory Bowel Disease therapy Hernández Teruel, Adrián 21 October 2019 (has links) Tesis por compendio / [ES] La presente tesis doctoral titulada "Sistemas de liberacio'n controlada de fa'rmacos diseñados para mejorar el tratamiento de Enfermedad Inflamatoria Intestinal" se centra en el diseño, preparación, caracterización y evaluación in vivo de distintos sistemas de liberación controlada de fármacos en colon (CDDS, por sus siglas en inglés) utilizando como soporte micropartículas de silice mesoporosa, funcionalizadas con puertas moleculares. En conclusión, los estudios realizados demuestran que los materiales de silice mesoporosa, en combinación con puertas moleculares sensibles a estímulos específicos, tienen un gran potencial para el desarrollo de nuevos sistemas de liberación controlada de fármacos en el colon, dirigidos a mejorar el arsenal terapéutico disponible para el tratamiento de EII. La posibilidad de adaptar o personalizar la carga y las puertas moleculares hace que estos soportes de sílice mesoporosa sean una opción interesante para el desarrollo de nuevos sistemas de liberación controlada de fármacos en diferentes aplicaciones biomédicas. Finalmente, esperamos que los resultados obtenidos en esta tesis doctoral sirvan de inspiración para el desarrollo de sistemas de liberación controlada de fármacos innovadores y cada vez más inteligentes, para su aplicación tanto en medicina como en otras áreas. / [CA] La present tesi doctoral titulada "Sistemes d'alliberament controlat de farmacs dissenyats per a millorar el tractament de Malaltia Inflamatoria Intestinal" se centra en el disseny, preparacio, caracteritzacio i avaluacio in vivo de diferents sistemes d'alliberament controlat de farmacs en colon (*CDDS, per les seues sigles en angles) utilitzant com a suport microparticules de si'lice mesoporosa, funcionalitzades amb portes moleculars. En conclusio, els estudis realitzats demostren que els materials de si'lice mesoporosa, en combinacio amb portes moleculars sensibles a estimuls especifics, tenen un gran potencial per al desenvolupament de nous sistemes d'alliberament controlat de farmacs en el colon, dirigits a millorar l'arsenal terapeutic disponible per al tractament de MII. La possibilitat d'adaptar o personalitzar la carrega i les portes moleculars, fa que aquests suports de silice mesoporosa siguen una opcio interessant per al desenvolupament de nous sistemes d'alliberacio controlada de farmacs en diferents aplicacions biomediques. Finalment, esperem que els resultats obtinguts en aquesta tesi doctoral servisquen d'inspiracio per al desenvolupament de sistemes d'alliberament controlat de farmacs innovadors i cada vegada mes intel·ligents, per a la seua aplicacio tant en medicina com en altres arees. / [EN] This PhD thesis entitled "Smart drug delivery systems designed to improve Inflammatory Bowel Disease therapy" is focused on the design, synthesis, characterization and in vivo evaluation of several Colon Drug Delivery Systems (CDDS) using hybrid mesoporous silica microparticles as scaffolds containing molecular gates. In conclusion, the studies shown in this Thesis demonstrate that mesoporous silica materials in combination with responsive molecular gates have great potential in the design and preparation of new CDDS to improve the therapeutic options available for IBD. The possibility to adapt the cargo and the molecular gate makes mesoporous silica support especially appealing for similar controlled drug delivery applications in the biomedical field. We hope that the obtained results could inspire the development of new innovative smart drug delivery systems in this or other fields. / We thank the Spanish Government (projects MAT2015-64139-C4-1-R and AGL2015-70235-C2-2-R (MINECO/FEDER)) and the Generalitat Valenciana (project PROMETEOII/2014/047) for support. AHT thanks to the Spanish MEC for his FPU grant. We thank the Generalitat Valenciana (Project PROMETEO2018/024) / Hernández Teruel, A. (2019). Smart drug delivery systems designed to improve Inflammatory Bowel Disease therapy [Tesis doctoral]. Universitat Politècnica de València. https://doi.org/10.4995/Thesis/10251/129863 / TESIS / Compendio Colon drug delivery systems Colon targeting Inflammatory bowel disease Ulcerative colitis Crohn's disease Mesoporous silica microparticles Gated materials Molecular gates Smart drug delivery. QUIMICA INORGANICA
232	Artificial intelligence-based clinical classification of diseases: Utilizing gut microbiota as a feature for supervised learning and diagnostic screening of inflammatory bowel diseases Manandhar, Ishan January 2021 (has links) No description available. Biomedical Research Bioinformatics
233	Transcriptome-Guided Drug Repositioning Arakelyan, Arsen, Nersisyan, Lilit, Nikoghosyan, Maria, Hakobyan, Siras, Simonyan, Arman, Hopp, Lydia, Loeffler-Wirth, Henry, Binder, Hans 11 April 2023 (has links) Drug repositioning can save considerable time and resources and significantly speed up the drug development process. The increasing availability of drug action and disease-associated transcriptome data makes it an attractive source for repositioning studies. Here, we have developed a transcriptome-guided approach for drug/biologics repositioning based on multi-layer self-organizing maps (ml-SOM). It allows for analyzing multiple transcriptome datasets by segmenting them into layers of drug action- and disease-associated transcriptome data. A comparison of expression changes in clusters of functionally related genes across the layers identifies “drug target” spots in disease layers and evaluates the repositioning possibility of a drug. The repositioning potential for two approved biologics drugs (infliximab and brodalumab) confirmed the drugs’ action for approved diseases (ulcerative colitis and Crohn’s disease for infliximab and psoriasis for brodalumab). We showed the potential efficacy of infliximab for the treatment of sarcoidosis, but not chronic obstructive pulmonary disease (COPD). Brodalumab failed to affect dysregulated functional gene clusters in Crohn’s disease (CD) and systemic juvenile idiopathic arthritis (SJIA), clearly indicating that it may not be effective in the treatment of these diseases. In conclusion, ml-SOM offers a novel approach for transcriptome-guided drug repositioning that could be particularly useful for biologics drugs. info:eu-repo/classification/ddc/610 ddc:610
234	Livet med inflammatorisk tarmsjukdom : En litteraturöversikt / Life with inflammatory bowel disease : A literature review Rahmani, Armin, Sundström, Maximilian January 2024 (has links) Bakgrund: Inflammatorisk tarmsjukdom innefattar både ulcerös kolit och Crohns sjukdom, vilka är kroniska inflammatoriska tarmsjukdomar. De båda sjukdomarna löper i skov med plötsliga försämringsperioder och långa perioder utan besvär. Det är viktigt att sjuksköterskan vidtar specifika omvårdnadsåtgärder samt förhåller sig personcentrerat där värden som värdighet bevaras för att stödja personen. Syfte: Att beskriva personers erfarenheter av att leva med inflammatorisk tarmsjukdom. Metod: Till metod valdes en litteraturöversikt och de databaser som användes var PubMed samt Cinahl Complete. Inklusionskriterier var vetenskapliga originalartiklar, genomgått peer-review, engelskt språk samt publicerade från år 2014 till 2024. Genom ett systematiskt urval arbetades tio artiklar fram, varav nio med kvalitativ design och en med mixad metod. Resultat: I litteraturöversiktens resultat framkom det att personer med inflammatorisk tarmsjukdom hade erfarenheten av att sjukdomen påverkade deras dagliga liv, både i det sociala livet och yrkeskarriären. Personer med inflammatorisk tarmsjukdom hade även erfarenheter att sjukdomen påverkade det emotionella välbefinnandet. Det lyftes även fram hur personer hanterade sjukdomen, vilka strategier som användes och stödets betydelse beskrevs. Slutsats: Litteraturöversikten visade att personer med inflammatorisk tarmsjukdom möter utmaningar inom många områden i livet. På grund av de anpassningar som individen måste genomgå är det viktigt att sjuksköterskan bidrar med stöd för att möjliggöra effektiv sjukdomshantering. Roys adaptionsteori kan ge sjuksköterskan en bättre förståelse för personernas anpassningsförmåga och kompensera med stöd för att hälsa och livskvalité ska upprätthållas. / Background: Inflammatory bowel disease encompasses both ulcerative colitis and Crohn's Disease, which are chronic inflammatory bowel diseases. Both diseases are characterized by periods of flare-ups with sudden exacerbations and long periods of remission. It is important for nurses to implement specific nursing interventions and to maintain a person-centered approach where values like dignity are preserved to support the person. Aim: To describe people's experiences of living with inflammatory bowel disease. Method: The chosen method was a literature review, with PubMed and CINAHL Complete as the selected databases. Inclusion criteria were scientific original articles that had undergone peer review, were in English, and were published from 2014 onwards. Through a systematic selection process, ten articles were identified, of which nine had a qualitative design and one used mixed methods. Results: In the results of the literature review, it was found that individuals with inflammatory bowel disease experienced the impact of the disease on their daily lives, including their social life and professional careers. They also reported that the disease affected their emotional well-being. Additionally, the review highlighted how individuals managed the disease, the strategies they used, and the significance of support. Conclusion: The literature review showed that individuals with inflammatory bowel disease face challenges in many areas of life. Due to the adaptations that the individual must undergo, it is important for nurses to provide support to enable effective disease management. Roy`s adaption theory can provide the nurse with a better understanding of individual`s adaptability and compensate with support to maintain health and quality of life. Inflammatory bowel disease Crohn's disease Ulcerative colitis Living with Lived experience Inflammatorisk tarmsjukdom Crohns sjukdom Ulcerös kolit leva med Levd erfarenhet Nursing Omvårdnad
235	Aberrant response of human myeloid dendritic cells to microbial stimuli in patients with inflammatory bowel disease Thomas, Saskia 06 July 2011 (has links) In zahlreichen Studien konnte an Mausmodellen gezeigt werden, dass dendritische Zellen eine wichtige Rolle im Rahmen der mukosalen Immunabwehr spielen. Eine unkontrollierte Aktivierung immunologischer Effektorzellen durch antigenpräsentierende Zellen ist die Folge, welche die Antigene der luminalen Flora folglich falsch erkennen und damit zu einer Schädigung des Gewebes führen. In der Arbeit wurden humane CD1c+CD11c+CD14-CD19- myeloide dendritische Zellen (mDCs) aus dem peripheren Blut und der intestinalen Mukosa von CED Patienten sowie von gesunden Probanden phänotypisch und funktionell näher charakterisiert. mDCs von Patienten reagieren auf LPS im Gegensatz zu DCs von Gesunden mit der Ausbildung eines aktivierten Phänotyps und der Sekretion pro-inflammatorischer Zytokine. Die Daten lassen vermuten, dass ihre tolerogene Rolle gestört ist und die Zellen so möglicherweise aktiv zum Entzündungsgeschehen durch eine Fehlreaktion auf die kommensale Flora beitragen. Es konnte gezeigt werden, dass zirkulierende mDCs von Erkrankten mehr LPS aufnehmen. Des Weiteren ist die Häufigkeit von mukosalen und aktivierten mDCs bei CED Patienten signifikant erhöht. Die vermehrte Häufigkeit von aktivierten mDCs in der entzündeten Mukosa ist ein Hinweis auf intestinales „homing“, also ein Wiedereinwandern der gereiften Lymphozyten in die Darmwand. Es ist bekannt, dass die Hefe Saccharomyces boulardii (Sb) eine Wirksamkeit bei entzündlichen sowie infektiösen Erkrankungen des Gastrointestinaltraktes hat. Kulturexperimente von mDCs mit Zellkulturüberständen von Sb (SbS) und LPS zeigten eine deutliche Reduzierung in der Expression von CD40 und CD80 sowie des Reifemarkers CD197. SbS reduzierte die Sekretion von TNF- und IL-6. Während es die Sekretion von IL-10 bei gesunden Probanden erhöhte, konnte bei CED Patienten eine leichte Abnahme verzeichnet werden. SbS vermindert die Proliferation von naïven T-Zellen in einer gemischten Lymphozytenreaktion mit gesunden mDCs signifikant. / Various animal studies have provided insights that mucosal dendritic cells play a key role in this process. However, the specific function of certain dendritic cells in IBD is still unknown. Primary CD1c+CD11c+CD14-CD19- myeloid blood (mDCs) and mucosal DCs from IBD patients and healthy controls were compared. More mDCs from IBD patients exhibited an activated phenotype shown by expression of co-stimulatory molecules. mDCs from patients secrete higher levels of pro- and anti-inflammatory cytokines. Circulating mDCs from IBD patients take up more LPS and the frequency of mucosal mDCs and the number of activated, i.e. CD40 and CD80 expressing mucosal mDCs, is significantly greater in CED. The increased frequency of activated mDCs in the inflamed mucosa suggests intestinal homing of mDCs in acute stages of IBD. Further, the data suggests an aberrant LPS response of mDCs in patients suffering from IBD which results in an inflammatory phenotype. The most widely accepted hypothesis for the cause of IBD is a disturbed interaction of the host immune system with commensal microflora and other luminal antigens. The well controlled balance of the intestinal immune system is disturbed and luminal antigens like LPS gain access to the underlying mucosal tissue via the leaky barrier. It was investigated whether the yeast preparation Saccharomyces boulardii (Sb) modulates dendritic cell function which has shown efficacy in inflammatory and infectious disorders of the gastrointestinal tract. Culture experiments of mDCs in the presence of Sb culture supernatant (SbS) significantly reduced the expression of CD40 and CD80 as well as the DC maturation marker CD197 (CCR7) induced by the prototypical microbial antigen LPS. SbS reduced secretion of TNF- and IL-6, while the secretion of anti-inflammatory IL-10 increased. IBD patients showed also a reduction in their secretion level of IL-10. SbS inhibited proliferation of naïve T cells in a mixed lymphocyte reaction with healthy mDCs. dendritic cells antigen-presenting cell inflammation Inflammatory Bowel Disease Crohn''s Disease Ulcerative colitis Saccharomyces boulardii T cells dendritic cells inflammation T cells antigen-presenting cell Inflammatory Bowel Disease Crohn''s Disease Ulcerative colitis Saccharomyces boulardii 570 Biowissenschaften, Biologie 32 Biologie YC 5387 ddc:570
236	Étude génétique et fonctionnelle de variantes de la région chromosomique 3p21 associée aux maladies inflammatoires de l'intestin Lévesque, Marie-Pierre 04 1900 (has links) Des études de liaison et d’association génétiques ont permis d’identifier certains des facteurs de risque génétiques aux maladies inflammatoires de l’intestin (MII) dans la région chromosomique 3p21. Dans cette région, le polymorphisme nucléotidique simple (SNP) codant non-synonyme du gène MST1, rs3197999, encodant pour la mutation R689C, a été associé et répliqué à la fois à la colite ulcéreuse (CU) et à la maladie de Crohn (MC). Un autre SNP, corrélé à des SNP codants non-synonymes du gène MST1R, a également été associé à la MC. Afin de déterminer si d’autres variantes des gènes MST1 et MST1R sont associés à la CU, nous avons testé pour association des SNP de ces gènes. Seul un proxy de R689C a montré un signal d’association significatif aux MII, ce qui suggère que R689C est la variante causale aux MII dans le gène MST1. En cherchant à déterminer si la région 3p21 contenait plusieurs signaux d’association mutuellement indépendants, trois SNP ont été identifiés comme possible facteurs de risque indépendants, et ont été génotypés dans des cas de CU et de MC et des témoins, puis nos résultats d’association ont été combinés à ceux provenant de trois autres cohortes indépendantes. Les trois SNP, R689C (MST1), rs6802890 et rs7629936 (CDHR4), sont associés aux MII, mais une étude d’association conditionnelle suggère qu’il existe en fait deux signaux d’association mutuellement indépendants dans la région 3p21. Le signal principal provient de R689C, une mutation de la protéine MSP. Cette protéine a un rôle dans l’inflammation chez les macrophages murins, et la migration, la cicatrisation et la survie chez les cellules épithéliales. Dans cette étude, le rôle de la MSP a été investigué dans des modèles de macrophages humains et de cellules épithéliales de côlon, et seule la phosphorylation d’AKT, un acteur dans la voie de signalisation de la survie cellulaire, a été modulée par la MSP dans nos modèles. Ce projet a donc permis d’apporter des connaissances sur les facteurs de risques génétiques aux MII dans la région 3p21, en identifiant 2 signaux d’association indépendants, et en nous informant sur le rôle de MST1, duquel provient le signal d’association principal, chez les cellules humaines. / Linkage studies and association studies allowed the discovery of some of the genetic risk factors of inflammatory bowel disease (IBD) in the chromosomal region 3p21. In this region, the non-synonymous coding single nucleotide polymorphism (SNP) rs3197999, situated in the gène MST1 and encoding for the mutation R689C, has been associated to UC and CD multiple times, and an other SNP, correlated to non-synonymous coding SNPs in the gene MST1R, has also been associated to CD. In order to verify if other variants of MST1 and MST1R are associatied to UC, we tested the association of some of their SNPs. Apart from R689C, only its proxy showed a significative association signal to IBD. It suggests that R689C might be the causal variant of IBD in the region 3p21. In the aim to determine if the region 3p21 has multiple independant association signals, 3 SNPs have been identified, from the results of a published meta-analysis of UC genome-wide association studies, as being possibly independant risk factors for UC based on their correlation. Their association to IBD and their independance have been tested by genotyping them in a cohort composed of controls, and UC and CD cases. The results of the association tests have been combined, in a meta-analysis, to the results of 3 other independent association studies. The 3 SNPs, R689C (MST1), rs6802890 and rs7629936 (CDHR4) are associated to IBD, but the results of the subsequent conditional association tests suggest that there is only 2 independant association signals in the region 3p21. The main signal is raising from R689C, a mutation of the protein MSP. According to published studies, this protein has a function in the inflammation in murine macrophages, and also in the scattering, wound healing and survival of epithelial cells. In this thesis, we investigated the role of MSP in human macrophage models and in human côlon epithelial cells, and it has been show that MSP modulates the phosphorylation of AKT, an actor in the pathway of cellular survival. This project brought some knowledges about the IBD genetic risk factors in the region 3p21. We identified 2 independent association signals to IBD in this region, and the main signal is coming from a SNP in MST1, a gene which has a role, based on our results, in the survival in human colon epithelial cells. 3p21 3p21 MST1 MST1 MST1R MST1R association association méta-analyse meta-analysis maladies inflammatoires de l'intestin inflammatory bowel diseases colite ulcéreuse ulcerative colitis maladie de Crohn Crohn’s disease phosphorylation de AKT phosphorylation of AKT
237	Vitamine D et prévention du cancer colorectal associé à la colite ulcéreuse : modèles murins Elimrani, Ihsan 03 1900 (has links) Les patients atteints de maladies inflammatoires de l'intestin (MII) ont un risque accru de développer un cancer colorectal dû aux lésions épithéliales secondaires à l’inflammation chronique. La vitamine D (vD) régule NOD2, gène impliqué dans la réponse inflammatoire et dans la susceptibilité aux MII, et induit son expression dans les monocytes et dans l’épithélium intestinal. Dans ce projet, nous avons d’abord induit le cancer colorectal associé à la colite ulcéreuse (CAC) en administrant un traitement combiné d’azoxyméthane (AOM) et de dextran de sulfate de sodium (DSS) aux souris C57BL/6J. Par la suite, nous avons étudié l'effet d’une carence en vD3 sur le développement du CAC et évalué la capacité préventive d’une supplémentation en vD3 sur la tumorigenèse, et vérifié si cet effet est médié par NOD2, en utilisant les souris Nod2-/-. Les C57BL/6J et les Nod2-/-, ayant reçu une diète déficiente en vD3, étaient moins résistantes au CAC par rapport aux souris supplémentées. Le pourcentage de perte de poids, l’indice d’activation de la maladie (DAI), le taux de mortalité et le poids relatif du côlon (mg/cm) chez les souris déficientes en vD3 étaient plus élevés en comparaison avec celles supplémentées en vD3. Une augmentation du score d'inflammation et de la multiplicité tumorale corrélait avec une expression accentuée de l’Il6 dans les colonocytes des souris déficientes en vD3. La vD3 régulait l’expression génétique de Cyp24, Vdr et de gènes pro-inflammatoires chez les C57BL/6, comme chez les Nod2-/-. En conclusion, la supplémentation en vD3 peut prévenir le développement du CAC indépendamment de NOD2. / Patients with inflammatory bowel disease (IBD) have an increased risk of developing colorectal cancer due to continuing epithelial cell injury from the chronic inflammatory process. Vitamin D (vD) regulates NOD2, a gene involved in the inflammatory response and in IBD susceptibility, and induces its expression in monocytes and intestinal epithelial cells. In this project, we first established an azoxymethane (AOM)/dextran sodium sulfate (DSS) murine model of colitis-associated colorectal cancer (CAC) using C57Bl/6J. We then investigated the effect of vD3 deficiency on CAC development, and evaluated the ability of vD3 supplementation to prevent tumorigenesis. Lastly, we assessed whether the preventive benefits of vD3 on colon carcinogenesis are mediated via NOD2 using Nod2 knockout mice (Nod2-/-). vD3 deficient C57Bl/6J and Nod2-/- mice displayed increased severity of AOM/DSS-induced CAC compared to mice given vD3 supplemented diets. In vD3 deficient mice, body weight loss, Disease Activity Index (DAI), mortality rate and the colon weight/length ratio were higher compared to vD3-supplemented mice. An increased inflammation score was observed in the mucosa of vD3 deficient mice along with augmentation in the expression level of IL-6. Higher tumour multiplicity was also observed in vD3 deficient groups compared to vD3-supplemented groups. In both C57Bl/6J and Nod2-/- mice, vD3 regulated Cyp24, Vdr and pro-inflammatory genes. In conclusion, vD3 supplementation can prevent CAC independently of NOD2. Vitamine D 25-hydroxyvitamine D3 maladies inflammatoires de l’intestin colite ulcéreuse cancer colorectal NOD2 murin AOM/DSS 25-hydroxyvitamin D3 Vitamin D inflammatory bowel disease ulcerative colitis colorectal cancer NOD2 murine AOM/DSS
238	Hipomotilidade da vesícula biliar em pacientes colectomizados por retocolite ulcerativa inespecífica / Hipomotilidade da vesícula biliar em pacientes colectomizados por retocolite ulcerativa inespecífica Damião, Aderson Omar Mourão Cintra 10 November 1995 (has links) Pacientes com retocolite ulcerativa inespecífica,quando submetidos à colectomia, apresentam aumento na freqüência de cálculos vesiculares de colesterol. A hipomotilidade da vesícula biliar tem sido apontada como um importante fator na formação dos cálculos vesiculares de colesterol, ao lado da supersaturação biliar de colesterol e da nucleação dos cristais de colesterol (fatores nucleantes e antinucleantes). A estase vesicular aumenta o tempo de reabsorção de água pela mucosa da vesícula biliar com conseqüente superconcentração dos solutos, além de gerar o tempo necessário para a nucleação do colesterol, retenção e fusão dos cristais e,finalmente,formação dos cálculos. Embora a composição biliar já tenha sido estudada em pacientes colectornizados, não há informações sobre o comportamento da motilidade da vesícula biliar em pacientes com retocolite ulcerativa inespecífica com e sem colectomia. No presente trabalho,o esvaziamento vesicular foi estudado através do método ultra-sonográfico e após ingestão de dieta líqüida gordurosa em indivíduos controles (n=40), pacientes com retocolite ulcerativa inespecífica sem (n=30) e com colectomia (n =20). Como o esvaziamento gástrico pode interferir no vesicular, o tempo de esvaziamento gástrico, medido por método ultra-sonográfico, foi calculado nos três grupos. O esvaziamento vesicular foi significantemente diminuído nos pacientes com retocolite ulcerativa inespecífica com colectomia e após estímulo alimentar: esta alteração não foi conseqüência de esvaziamento gástrico retardado pois o tempo de esvaziamento gástrico foi semelhante nos três grupos. Ademais, a redução da motilidade vesicular nos pacientes colectomizados relacionou-se com a colectomia propriamente dita, uma vez que indivíduos controles e pacientes com retocolite ulcerativa inespecífica sem colectomia apresentaram esvaziamentos vesiculares semelhantes. Além disso,os resultados desta investigação reforçam a relevância do papel da motilidade vesicular na colelitíase e sua participação, juntamente com a diminuição do \"pool\" de ácidos biliares,na patogênese da calculo se vesicular de colesterol em pacientes com retocolite ulcerativa inespecífica submetidos à colectomia. / Patients with ulcerative colitis, who have their colon removed, are at increased risk of developing cholesterol gallstones. Gallbladder hypomotility has been quoted as being an important factor for cholesterol gallstone formation, together with biliary supersaturation of cholesterol and nucleation of cholesterol crystals (nucleating and antinucleating factors). Gallbladder stasis increases the time for water reabsorption by the gallbladder mucosa with ensuing solute superconcentration; moreover, gallbladder stasis renders enough time for cholesterol nucleation. crystal retention and fusion, and finally, stone formation. Although bile composition, in these patients, has already been studied, there is no information concerning the nature of gallbladder motility in patients with ulcerative colitis with or without colectomy. ln the present work, gallbladder emptying was studied by means of ultrasound examination, and after ingestion of a standard liquid fatty meal in controls (n=40), ulcerative colitis patients without colectomy (n=30) and with colectomy (n=20). Also, in order to rule out the influence of gastric emptying on gallbladder motility, the gastric emptying time was calculated, in the three groups, using the ultrasound method. Gallbladder emptying was significantly impaired in patients with ulcerative colitis with colectomy after a fatty-meal stimulus. and this abnormality was not a consequence of delayed gastric ernptying. since gastric emptying time was similar in the three groups. Furthermore. impaired gallbladder motility in ulcerative colitis patients with colectomy was related to the colectorny itself, since controls and ulcerative colitis Cholelithiasis/physiopathology Colectomia/efeitos adversos Colectomy/adverse effects Colelitíase/fisiopatologia Colite ulcerativa/diagnóstico Gallbladder/physiopathology Gallbladder/ultrasonography Gastrointestinal motility/physiology Motilidade gastrointestinal/fisiologia Retocolite ulcerativa Ulcerative colitis/diagnosis Ultrasonografia/métodos Ultrasonography/methods Vesícula biliar/fisiopatologia Vesícula biliar/ultrasonografia
239	Antigenpräsentation in der intestinalen Mukosa Baumgart, Daniel C. 26 May 2005 (has links) Die Ätiologie chronisch entzündlicher Darmerkrankungen ist bis heute ungeklärt. Sie beinhaltet eine unkontrollierte Aktivierung von immunologischen Effektorzellen durch antigenpräsentierende Zellen, wie zum Beispiel dendritische Zellen und intestinale Epithelzellen, die Antigene der luminalen Flora fehlerkennen und/oder falsch verarbeiten und den daraus resultierenden Gewebsschädigungsmechanismen. Am Interleukin-2 defizienten Mausmodell der Colitis ulcerosa konnten wir zeigen, daß T-Zellen eine zentrale Rolle beim mukosalen Entzündungsprozeß bei chronisch entzündlichen Darmerkrankungen und insbesondere bei Colitis ulcerosa spielen. So kann zum Beispiel im Tiermodell eine Colitis ulcerosa durch Injektion von T-Zellen aus kranken Tieren auf gesunde Kontrolltiere übertragen werden. T-Zellen gehören zu den wichtigsten Produzenten pro-inflammatorischer Zytokine. Das Ausbleiben der Darmentzündung bei keimfrei gehaltenen Interleukin-2 defizienten Mäusen stützt die Hypothese einer Fehlaktivierung von T-Zellen durch luminale Antigene. In weiterführenden Experimenten haben wir den Beweis erbracht, daß primäre mukosale Epithelzellen das Potential zur Antigenpräsentation besitzen. Ihre Funktion besteht jedoch offenbar in der aktiven, reversiblen Hemmung von CD4+ T-Zellantworten. Da sie in unmittelbarem Kontakt mit den luminalen Antigenen stehen, kommt ihnen zumindest im Kolon eine regulatorische, tolerogene Rolle zu. Eine Störung dieses Prozesses trägt möglicherweise zur Ausbildung und Aufrechterhaltung unkontrollierter Entzündung bei chronisch entzündlichen Darmerkrankungen und insbesondere bei Colitis ulcerosa bei. Dendritische Zellen sind die am längsten bekannten und potentesten antigenpräsentierenden Zellen. Wir konnten zeigen, daß bei Patienten in Remission bereits ein Mangel an zirkulierenden unreifen, d.h. potentiell tolerogenen, dendritischen Zellen besteht, der bei akuten Schüben stark zunimmt. Dendritische Zellen von Patienten reagieren auf mikrobielle Modellstimuli im Gegensatz zu dendritischen Zellen von Gesunden mit der Ausbildung eines aktivierten Phänotyps und der Sekretion pro-inflammatorischer Zytokine. Unsere Daten lassen vermuten, daß ihre tolerogene Rolle gestört ist und sie möglicherweise aktiv zum Entzündungsgeschehen durch eine Fehlreaktion auf die kommensale Flora beitragen. Die klinische Relevanz der gestörten T-Zellaktivierung wird durch klinische Daten deutlich. Wir haben gezeigt, daß der T-Zellaktivierungshemmer Tacrolimus zur überbrückenden Therapie refraktärer chronisch entzündlicher Darmerkrankungen bis zum Wirkeintritt konventioneller Immunmodulatoren, wie zum Beispiel Azathioprin oder 6-Mercaptopurin, zur raschen Induktion einer Remission und auch bei Therapieversagen konventioneller Immunmodulatoren geeignet ist. Weiterhin demonstrierten wir seine Wirksamkeit bei refraktären extraintestinalen Komplikationen chronisch entzündlicher Darmerkrankungen, wie dem Pyoderma gangrenosum. / The etiology of inflammatory bowel disease is still unknown. Patients with inflammatory bowel disease have an inappropriate T-cell response to antigenic components of their indigenous gut flora and/or food stream. This breakdown in "oral tolerance" is poorly understood. However, this phenomenon likely relates to how antigen presenting cells, such as dendritic cells and epithelial cells, process and present antigen(s) to T-cells. Our data in the interleukin-2 knock out mouse model of ulcerative colitis underscores the central role of T-cells for the inflammatory process in inflammatory bowel disease and particularly ulcerative colitis. Adoptive transfer experiments showed that T-cells from diseases animals can transmit the ulcerative like disease onto healthy controls. T-cells are among the main producers of pro-inflammatory cytokines. The absence of the ulcerative colitis like disease in gnotobiotic interleukin-2 mice supports the hypothesis of an inappropriate T-cell response towards the indigenous flora. In additional studies we were able to show, that intestinal epithelial cells are capable to present antigen. However, their major role is apparently the reversible silencing of activated CD4+ T-cell responses. Their close proximity with luminal antigens suggest a regulatory, tolerogenic role at least in the colon. A disturbance of this process probably contributes to the occurrence and perpetuation of uncontrolled inflammation in inflammatory bowel disease and particularly UC. Dendritic cells are the longest known most potent antigen presenting cells. We have demonstrated that inflammatory bowel disease patients lack circulating, immature, and thereby potentially tolerogenic dendritic cells. Cultured dendritic cells from inflammatory bowel disease patients showed a more vigorous response to microbial surrogate stimuli compared with healthy controls. Our data suggest that the normally tolerogenic role of circulating dendritic cells is impaired in inflammatory bowel disease patients. It appears that they actively contribute to the inflammatory process by a false response to the indigenous flora. The clinical relevance of an uncontrolled T-cell activation is supported by our clinical data. We demonstrated that the T-cell activation inhibitor tacrolimus is suitable for the management of refractory inflammatory bowel disease. Low dose oral tacrolimus was also effective in refractory extraintestinal complications of inflammtory bowel disease such as pyoderma gangrenosum. The concepts and available data of current and evolving biologic therapies are extensively discussed. Morbus Crohn T-Zellen Colitis ulcerosa Epithelzellen Dendritische Zellen Antigenpräsentation Immunmodulatoren Crohn''s disease ulcerative colitis T-cells epithelial cells dendritic cells antigen presentation immunomodulators 610 Medizin 33 Medizin XG 7554 XG 7563 XG 7572 WF 9900 ddc:610
240	Effect of Coconut Oil on Ulcerative Colitis in the Mouse Model Alok, Pranav Chandra 01 May 2013 (has links) Ulcerative colitis (UC) is a chronic disease of the colon or large intestine that causes inflammation and ulceration of the inner lining of the colon and rectum. In patients with ulcerative colitis, the body’s immune system overreacts and the body mistakes food, bacteria or other internal materials in the colon for an invading substance. The immune system attacks the material, thus irritating the colon. Limited knowledge of inflammatory conditions coupled with a narrow range of therapeutic options necessitates investigating the role of natural products. This study describes the effect of natural coconut oil on chemically-induced acute and chronic disease in mice. Ulcerative colitis was induced in four groups (5 mice per group) of 10-week-old female C57BL/6 mice by exposing them to 2.5-3% dextran sulfate sodium (DSS) for 5 and 29 days in the acute and chronic models, respectively. Coconut oil treatment was given via food containing 5% coconut oil to three diseased groups in three different regimens: one, preventive group receiving treatment prior to disease induction (14 d in acute; 28 d in chronic); two, simultaneous group receiving treatment simultaneous to disease induction; and three, regular treatment group receiving treatment after the disease induction –until termination of the experiment (14 d in acute; 60 d in chronic). Coconut food was replaced by the regular chow in the disease and water control groups. Clinical symptoms (diarrhea, occult blood, anal bleeding and body weight change) and the size of the isolated colon were recorded for comparison between experimental and control groups. Groups receiving coconut food displayed remissions in clinical markers of the disease. Improvements in clinical symptoms, histopathology, as well as cytokine activities were observed in both models, but the effects were more significant on the basis of standard error in the chronic model. Ulcerative Colitis Coconut Medium-Chain Fatty Acids Gastrointestinal Ulcers Inflammatory Bowel Diseases Natural Fatty Acids Virgin Coconut Oil Coconut Supplements Biology Digestive, Oral, and Skin Physiology Medical Immunology

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