Global ETD Search

291	On the pathophysiological significance of CD154/CD40-mediated leukocyte-endothelial cell interaction / On the pathophysiological significance of CD154/CD40-mediated leukocyte-endothelial cell interaction Gao, Dingcheng 07 May 2003 (has links) No description available. 32 Biologie WHC 700 Mathematics and Natural Science CD40 antisense-Oligonukleotide Endothelzellen CD40 antisense oligonucleotide endothelial cell chronic inflammatory bowel disease 42.15
292	Neue Biomarker zur Überwachung der zellulären Immunität chronisch-entzündlicher Darmerkrankungen / New biomarkers for monitoring of cellular immunity of chronic inflammatory bowel disease Weigand, Sebastian 24 June 2013 (has links) Zurzeit existieren keine validen Biomarker, welche die Krankheitsaktivität oder das Rezidiv-Risiko von chronisch-entzündlichen Darmerkrankungen objektivierbar machen. Im Rahmen dieser Arbeit wurden neue Biomarker des Immunmonitorings auf ihren Nutzen bei der Beurteilung der Krankheitsaktivität von Patienten mit chronisch-entzündlichen Darmerkrankungen (CED) untersucht. Hierzu wurde bei 98 Patienten mit CED, nach positivem Votum der Ethikkommission, die intrazelluläre ATP-Konzentration der CD4+-Zellen gemessen, um diese mit der Krankheitsaktivität der Patienten in Bezug zu setzen. Die Patientendaten wurden zuvor mithilfe von standardisierten Fragebögen erhoben, um daraufhin die Krankheitsaktivitätsindices CDAI, HBI und SCCAI aus den klinischen Daten zu ermitteln. Es wurde keine signifikante Korrelation zwischen der ATP-Konzentrationen und der Krankheitsaktivität der Patienten festgestellt. Dies führte zu der Schlussfolgerung, dass Einzelmessungen der intrazellulären ATP-Konzentration von Lymphozyten nicht die Krankheitsaktivität von Patienten mit chronisch-entzündlichen Darmerkrankungen widerspiegeln. Ein signifikanter Unterschied der intrazellulären ATP-Konzentration CD4+-Zellen wurde allerdings zwischen Patienten mit und ohne Infliximab-Therapie nachgewiesen. Die Patienten, die unter einer Infliximab-Therapie standen, hatten signifikant niedrigere intrazelluläre ATP-Konzentrationen der Lymphozyten (p<0,01, Mann-Whitney-U). Dieses Ergebnis verdeutlicht, dass Infliximab als TNF-α-Blocker die Immunantwort bzw. die Aktivität von Lymphozyten inhibiert. Mithilfe der intrazellulären ATP-Konzentration wäre somit evtl. ein Werkzeug gegeben, um die Effektivität der Inhibierung der lymphozytären Immunreaktion durch TNF-α-Blocker zu kontrollieren. Weiterhin wurde bei 99 CED-Patienten die Anzahl regulatorischer T-Zellen im peripheren Blut bestimmt. Hierfür wurden die Zellen mithilfe von CD4-, CD25-, CD127- und FoxP3-Antikörpern angefärbt und mittels der FACS-Analytik quantifiziert. Anschließend wurde die so ermittelte Anzahl regulatorischer T-Zellen (CD4+CD25highCD127-FoxP3+-Zellen) mit der Krankheitsaktivität der Patienten korreliert. Auch dabei wurde keine signifikante Korrelation nachgewiesen. Bei der Unterteilung der Patienten in Gruppen mit erhöhter und erniedrigter Krankheitsaktivität deutete sich ein Unterschied bezüglich der Anzahl regulatorischer T-Zellen an, der jedoch nicht signifikant war (p=0,073, Mann-Whitney-U-Test). Diese Ergebnisse führten zu der Annahme, dass sich die durchflusszytometrisch quantifizierte Anzahl regulatorischer T-Zellen ebenfalls nicht als Surrogatmarker für die Krankheitsaktivität von Patienten mit chronisch-entzündlichen Darmerkrankungen eignet. Zudem wurde postuliert, dass die Quantifizierung von Tregs keine Hilfe bei der Unterscheidung zwischen den beiden Erkrankungen Morbus Crohn und Colitis ulcerosa liefern kann. Der tendenzielle Unterschied in der Anzahl von Tregs zwischen Patienten mit niedriger und erhöhter Krankheitsaktivität zeigt jedoch, dass regulatorische T-Zellen bei der Pathogenese von chronisch-entzündlichen Darmerkrankungen eine Rolle zu spielen scheinen. Allerdings deutet sich auch eine Abhängigkeit von weiteren pathogenen Faktoren in der komplexen Ätiologie von chronisch-entzündlichen Darmerkrankungen an. Bei 35 der CED-Patienten wurde zusätzlich eine weitere Methode zur Quantifizierung regulatorischer T-Zellen angewendet. Hierbei handelte es sich um einen DNA-Methylierungsassay, welcher die regulatorischen T-Zellen anhand einer spezifischen Demethylierungsregion der DNA (TSDR) ermittelt. Diese TSDR ist bei den Tregs demethyliert, während sie bei allen anderen Zellen des Blutes methyliert ist. Die Ergebnisse dieses Assays korrelierten jedoch nicht mit der Krankheitsaktivität der Patienten und korrelierten auch nicht mit den Ergebnissen für die Anzahl regulatorischer T-Zellen aus der FACS-Analytik. Diese Tatsache könnte zum einen darauf beruhen, dass in der FACS-Analytik im Gegensatz zum DNA-Methylierungsassay auch aktivierte T-Effektorzellen quantifiziert werden, welche nur transient FoxP3 exprimieren. Zum anderen werden mittels des DNA-Methylierungsassays auch CD8+FoxP3+-Zellen quantifiziert, welche keine oder geringe regulatorischen Eigenschaften besitzen und in der Durchflusszytometrie nicht quantifiziert werden. Zudem könnte eine fehlende Korrelation zwischen den Ergebnissen der beiden Verfahren auch daran liegen, dass sich die quantifizierten Tregs aus der Durchflusszytometrie auf die Gesamtheit der CD4+-Zellen beziehen, während sich die Tregs des DNA-Methylierungsassays auf die gesamten DNA-haltigen Zellen des Vollblutes beziehen. Zur besseren Vergleichbarkeit könnte in zukünftigen Studien ein Quotient aus Tregs und CD4+-Zellen gebildet werden. Zusammenfassend hat sich im Rahmen dieser Arbeit gezeigt, dass sich weder mithilfe der intrazellulären ATP-Konzentrationen von Lymphozyten noch der Anzahl regulatorischer T-Zellen eine Aussage bezüglich der Krankheitsaktivität oder des Rezidivrisikos von CED-Patienten treffen lässt. Da die chronisch-entzündlichen Darmerkrankungen derzeit nicht heilbar sind, werden weitere Surrogatmarker zum Objektivieren der Krankheitsaktivität benötigt, um Krankheitsrezidiven zeitnah entgegenwirken zu können. 610 Treg regulatory t cell inflammatory bowel disease intracellular ATP concentration biomarkers
293	The potential of proton magnetic resonance spectroscopy (1H MRS) in detecting early colonic inflammation and assessing the effect of various dietary fatty acids on modulation of inflammatory bowel disease in an animal model Varma, Sonal 14 May 2008 (has links) The objectives of our study were to determine the potential of 1H MRS in detecting (1) early colonic inflammation, (2) effects of various fatty acids on normal colon and (3) their effects on IBD. Sprague dawley rat fed with 2% carrageenan was used as a model of IBD. Flaxseed oil served as ω-3, corn oil as ω-6 and beef tallow as saturated fatty acid sources. Control group animals were fed 5% corn oil, whereas, those in high-fat diet groups received an additional 7% of the respective fatty acids. After 2 weeks, 1H MRS and histology were conducted on excised colonic mucosa. Statistical classification strategy (SCS) used for analyzing 1H MRS data achieved an accuracy of 82 % in stage 1, 90-100% in stage 2 and 96-100% in stage 3. This implies that 1H MRS is a sensitive tool to diagnose early IBD and the effects of dietary fat on IBD. Beef tallow Colon cancer Corn oil Flaxseed oil Inflammatory bowel disease Proton magnetic resonance spectroscopy Statistical classification strategy ω-3 polyunsaturated fatty acids
294	Microbial etiology of Inflammatory Bowel Disease: Microbial diversity and the role of Escherichia coli SEPEHRI, SHADI 12 April 2010 (has links) Inflammatory bowel disease (IBD), comprises Crohn’s disease (CD) and ulcerative colitis (UC), and is a chronic relapsing inflammation of gastrointestinal tract without any known cause or cure. Currently, it is accepted that IBD is a result of a dysfunctional immune response to commensal bacteria in a genetically susceptible host, and that environmental factors can trigger the onset or reactivation of the disease. This thesis considers the possibility of a specific pathogenic agent as well as an imbalance in the composition of the normal microflora in the pathogenesis of IBD. Gut biopsy tissues were taken from a population-based case-control tissue bank held at the University of Manitoba. Automated ribosomal intergenic spacer analysis (ARISA) and terminal restriction fragment length polymorphisms (T-RFLP) were employed to assess the diversity of gut microbiota. The phylogenetic, virulence and biochemical characteristics of Escherichia coli isolated from IBD biopsies were examined using multi-locus sequence typing (MLST), DNA microarray technology and API 20E system. Utilizing ARISA and T-RFLP, a remarkable increase in the order of unclassified Clostridia was detected in inflamed tissues, particularly in CD patients (P < 0.05). Moreover, species richness and diversity were the highest in non-inflamed IBD biopsies. Culture-based quantification detected a significantly higher number of E. coli in IBD tissues (P < 0.05). Phylogenetic analysis revealed the tendency of E. coli isolated from IBD patients to be grouped into separate clonal clusters based on their allelic profiles (P = 0.02). A link was detected between uropathogenic E. coli (UPEC) CFT073 and strains isolated from IBD, with regards to gene distribution and virulence, using microarray technology. Amino acid substitutions N91S and S99N in FimH, the adhesive subunit of E. coli type I fimbria, were significantly associated to IBD (P < 0.05). This study demonstrated an increase in the microbial diversity of non-inflamed IBD tissues and suggested a recruitment phase of bacterial adherence and colonization, before the inflammation sets in. Furthermore, E. coli isolated from IBD tissues were distinct from commensal strains in both clonal and virulence characteristics and shared remarkable traits with extraintestinal pathogenic E. coli. Features involved in bacterial adhesion to epithelial cells may hold the key to E. coli pathogenesis in IBD. Inflammatory Bowel Disease Crohn's Disease Ulcerative colitis Microbial diversity Escherichia coli MLST ARISA T-RFLP Microarray gene content Virulence factors Phylogenetic analysis fimH AIEC UPEC APEC Nissle 1917
295	Human intestinal alkaline phosphatase : tissue expression and serum levels Domar, Ulla January 1992 (has links) Human alkaline phosphatase (ALP) comprises four isozymes, viz liver/bone/ kidney or tissue unspecific (AP), intestinal (LAP), placental (PLAP) and germ cell or PLAP-like alkaline phosphatase, with their main expression in specific tissues as indicated by their names. The isozymes are coded by different genes, but they are closely related, with more than 50% amino acid sequence homologies. Their biological function is unclear. In certain malignant and benign diseases, serum elevations of one or more of the isozymes occur, which is of diagnostic importance. In this study, the special expression of the intestinal isozyme in human tissues and sera, in normal as well as in pathological conditions, has been investigated by use of isozyme specific monoclonal antibodies. Monoclonal antibodies against the AP, IAP and PLAP isozymes were prepared, and specific assays developed, based on these monoclonal antibodies and the catalytic activity of the isozymes. By use of these assays the basal levels of all three isozymes were examined in selected normal organs. The isozymes were found to be expressed in measurable amounts in all the examined organs. IAP was immunohistochemically localized to the epithelial cells of membranes lining the ducts and tubules of the kidney, liver, pancreas and small intestine. Normal human serum contained all three isozymes. The AP isozyme constituted about 90% of the total ALP activity, the IAP isozyme less than 10% and the PLAP isozyme about 1%. Considerable interindividual variations of the serum IAP activity were observed. The serum activities of the IAP isozyme were related to the individual ABO blood group and secretor status. Non-secretors had low levels of IAP activity amounting to about one tenth of the activity in sera from blood group B or 0 secretors, while blood group A secretors had serum IAP activities in the same order as non-secretors. High individual day to day variations were observed. Fat absorption caused serum IAP to increase significantly for all persons, but it was rapidly cleared from the blood. We found that the release of IAP into the blood was linked to lipid absorption, but removal from the blood was not linked to lipoprotein clearance. Certain tumors of the testis expressed elevated levels of all three ALP isozymes. The highest activitiy of LAP was observed in one yolk sac tumor, in agreement with the endodermal origin of this tumor. In seminoma tissue the AP and PLAP isozymes were significantly, and IAP moderately elevated. Cirrhosis of the liver caused significantly increased serum levels of IAP besides the AP isozyme. In inflammatory diseases of the small intestine, normal serum IAP activities were observed. / <p>Diss. (sammanfattning) Umeå : Umeå universitet, 1992, härtill 7 uppsatser.</p> / digitalisering@umu Human alkaline phosphatase intestinal alkaline phosphatase blood blood group lipid monoclonal antibody immunohistochemistry liver kidney pancreas liver disease inflammatory bowel disease
296	Les systèmes microparticulaires pour la libération colonique / Multiparticulate colon drug delivery systems Bautzova, Tereza 17 September 2012 (has links) La maladie de Crohn et la rectocolite hémorragique font partie des maladies inflammatoires chroniques de l'intestin (MICI). Le principal objectif des traitements anti-inflammatoires est de favoriser la délivrance du principe actif localement, spécifiquement sur les zones enflammées et de limiter les effets indésirables. Ainsi, plusieurs systèmes à libération colonique de molécules actives ont été développés. Parmi eux, les pellets présentent de nombreux avantages par rapport aux formes solides unitaires conventionnelles. Dans un premier temps, des pellets comptant une substance anti-inflammatoire naturelle et nutritive, la rutine, ont été développés. L'intérêt de cette molécule est de réduire considérablement les effets secondaires qui constituent un véritable problème dans les traitements actuels des MICI. Les pellets ont été enrobé avec les polysaccharides naturels se dégradant avec la flore colonique. Les études in vitro ont démontré une libération minimale du principe actif au niveau de l'estomac et du petit intestin. Par contre, une libération rapide et totale a été observée lors de l'exposition des pellets dans les conditions du milieu colonique. Les résultats des tests in vivo ont démontré que la rutine a atténué considérablement l'inflammation au niveau de colon et les pellets enrobés ont été aussi efficaces que les pellets d'acide 5-aminosalicylique (5-ASA) commercialisés. L'administration orale de rutine via les pellets enrobés et préparés avec le chitosan semble être une approche prometteuse, permettant la libération du principe actif au niveau des zones enflammées, pour le traitement des MICI tout en réduisant les effets secondaires. Le deuxième but de notre travail était d'élucider l'impact du chitosan, un polymère mucoadhésif, sur l'efficacité thérapeutique. Les pellets de 5-ASA ont été préparés à partir de cellulose microcristalline avec ou sans chitosan. Un enrobage constitué d'un polymère pH dépendant,1' Eudragit® FS, a ensuite été réalisé autour du noyau. Les tests de dissolution ont montré que le principe actif n'était pas libéré du pellet après 2 h en milieu acide. En revanche,la libération était rapide dans un milieu simulant l'environnement colonique. Les tests ex vivo avec les pellets contenant le chitosan ont montré des propriétés mucoadhésives importantes qui ont été confirmées par la concentration élevée du métabolite de 5-ASA dans les tissus coloniques des rats. De plus, nous avons a démontré que les pellets permettaient d'atténuer de façon significative l'inflammation du côlon. Ainsi, les pellets bioadhésifs enrobés possèdent des propriétés bénéfiques supplémentaires pour la libération du 5-ASA au niveau du côlon par rapport à des formes multidoses commercialisées pour le traitement des MICI. / Crohn's disease and ulcerative colitis are two related but distinct chronic inflammatory disorders of gastrointestinal tract (GIT), commonly denoted as inflammatory bowel disease(IBD). The main goal of the anti-inflammatory treatment of this disorder is to achieve maximal drug concentration in inflamed area and reduce systemic adverse effects. For this purpose several colon-spécifie drug delivery systems have been investigated. In addition, the design of pellets as oral drug delivery systems may provide many advantages over single unit preparations and thus improve patient compliance. It is well known that most existing treatments of IBD are associated with significant side effects and for this reason the formulation with a " food like " composition was designed. In the first part of our study, therapeutic efficiency of rutin/chitosan pellets with coatings based on natural polysaccharides degraded by colonie microbiota compared to commercialized 5-aminosalicylic acid (5-ASA) pellets was investigated. Release profiles ofcoated pellets showed a minimal drug release in simulated stomach and small intestine following by rapid drug release upon exposure to the colonie fluid. The results from in vivo testing showed that rutin attenuated efficiently inflammation in the colon and coated pellets were as effective as 5-ASA pellets in mitigating experimental colitis. The studies demonstrated that rutin administration via chitosan core coated pellets seems to be apromising approach for colon-specific delivery since they could interact easily with the mucin layer and deliver drug especially to the inflamed colonie area to relieve symptoms of IBD omitting side effects related to conventional treatment. The second objective of this thesis was to explore the impact of additional mucoadhesive polymer chitosan in the pellets core on the therapeutic efficiency. For this purpose, 5-ASA loaded pellets were produced by extrusion/spheronisation method and subsequently coated with pH-sensitive polymer Eudragit® FS. No drug release at pH 1.2within 2 h, and release as intended in the simulated distal ileum and colon was observed. Chitosan-core pellets showed efficient mucoadhesive properties in ex vivo bioadhesion testing which were also confirmed by increased concentration of 5-ASA metabolite in the colonie tissues in rats. The pellets were tested in preexisting colitis and the results revealed significant attenuation of the colonie inflammation. We can conclude, that bioadhesive chitosan-corepellets showed additional beneficial properties for colonie 5-ASA delivery in the treatment of IBD over marketed dosage formulation. 5-ASA (5-aminosalicylique) Pellets Colon drug delivery Inflammatory bowel disease Rutin Chitosan WI 512
297	Att leva med inflammatorisk tarmsjukdom (IBD) : En litteraturöversikt om vuxna människors upplevelser i vardagen / Living with inflammatory bowel disease (IBD) : A literature review of adults’ experience in their daily lives Petterqvist, Anders, Rosenberg-Persson, Sandra January 2014 (has links) Background: Inflammatory bowel disease (IBD) includes Crohn´s disease (CD) and ulcerative colitis (UK). The diseases are chronic and have a pattern of relapses interspersed with relatively symptom-free periods. Common symptoms during relapse are diarrhea, abdominal pain and weight loss. Since you have IBD for life it is important to find ways to relate to and cope with the disease. In that process a nurse can be of great help. Aim: The purpose of this literature review was to increase the understanding of how adult patients with inflammatory bowel disease experience their daily lives. Method: The method used was a literature review. A literature search was performed in two separate databases which resulted in eleven examined and analyzed articles on the subject. Results: After the analyze of the articles three different themes emerged: Limitations in daily life, Self-image and self-esteem and finally Self-care and strategies. Several individuals felt limited one way or the other in their daily life. They also described how their self-esteem was affected. Some positive changes due to the disease were also described. For example some changed their exercise and food habits for the better. Discussion: The results are discussed through the perspective of Antonovsky’s (1991/2005) salutogenic view and were connected to how the SOC (Sense of Coherence) was affected. The importance of relatives’ support and self-care was also discussed. Inflammatory bowel disease Crohn’s disease ulcerative colitis patient experience nursing quality of life Inflammatorisk tarmsjukdom Crohns sjukdom ulcerös kolit patientupplevelse omvårdnad livskvalitet
298	The potential of proton magnetic resonance spectroscopy (1H MRS) in detecting early colonic inflammation and assessing the effect of various dietary fatty acids on modulation of inflammatory bowel disease in an animal model Varma, Sonal 14 May 2008 (has links) The objectives of our study were to determine the potential of 1H MRS in detecting (1) early colonic inflammation, (2) effects of various fatty acids on normal colon and (3) their effects on IBD. Sprague dawley rat fed with 2% carrageenan was used as a model of IBD. Flaxseed oil served as ω-3, corn oil as ω-6 and beef tallow as saturated fatty acid sources. Control group animals were fed 5% corn oil, whereas, those in high-fat diet groups received an additional 7% of the respective fatty acids. After 2 weeks, 1H MRS and histology were conducted on excised colonic mucosa. Statistical classification strategy (SCS) used for analyzing 1H MRS data achieved an accuracy of 82 % in stage 1, 90-100% in stage 2 and 96-100% in stage 3. This implies that 1H MRS is a sensitive tool to diagnose early IBD and the effects of dietary fat on IBD. Beef tallow Colon cancer Corn oil Flaxseed oil Inflammatory bowel disease Proton magnetic resonance spectroscopy Statistical classification strategy ω-3 polyunsaturated fatty acids
299	Microbial etiology of Inflammatory Bowel Disease: Microbial diversity and the role of Escherichia coli SEPEHRI, SHADI 12 April 2010 (has links) Inflammatory bowel disease (IBD), comprises Crohn’s disease (CD) and ulcerative colitis (UC), and is a chronic relapsing inflammation of gastrointestinal tract without any known cause or cure. Currently, it is accepted that IBD is a result of a dysfunctional immune response to commensal bacteria in a genetically susceptible host, and that environmental factors can trigger the onset or reactivation of the disease. This thesis considers the possibility of a specific pathogenic agent as well as an imbalance in the composition of the normal microflora in the pathogenesis of IBD. Gut biopsy tissues were taken from a population-based case-control tissue bank held at the University of Manitoba. Automated ribosomal intergenic spacer analysis (ARISA) and terminal restriction fragment length polymorphisms (T-RFLP) were employed to assess the diversity of gut microbiota. The phylogenetic, virulence and biochemical characteristics of Escherichia coli isolated from IBD biopsies were examined using multi-locus sequence typing (MLST), DNA microarray technology and API 20E system. Utilizing ARISA and T-RFLP, a remarkable increase in the order of unclassified Clostridia was detected in inflamed tissues, particularly in CD patients (P < 0.05). Moreover, species richness and diversity were the highest in non-inflamed IBD biopsies. Culture-based quantification detected a significantly higher number of E. coli in IBD tissues (P < 0.05). Phylogenetic analysis revealed the tendency of E. coli isolated from IBD patients to be grouped into separate clonal clusters based on their allelic profiles (P = 0.02). A link was detected between uropathogenic E. coli (UPEC) CFT073 and strains isolated from IBD, with regards to gene distribution and virulence, using microarray technology. Amino acid substitutions N91S and S99N in FimH, the adhesive subunit of E. coli type I fimbria, were significantly associated to IBD (P < 0.05). This study demonstrated an increase in the microbial diversity of non-inflamed IBD tissues and suggested a recruitment phase of bacterial adherence and colonization, before the inflammation sets in. Furthermore, E. coli isolated from IBD tissues were distinct from commensal strains in both clonal and virulence characteristics and shared remarkable traits with extraintestinal pathogenic E. coli. Features involved in bacterial adhesion to epithelial cells may hold the key to E. coli pathogenesis in IBD. Inflammatory Bowel Disease Crohn's Disease Ulcerative colitis Microbial diversity Escherichia coli MLST ARISA T-RFLP Microarray gene content Virulence factors Phylogenetic analysis fimH AIEC UPEC APEC Nissle 1917
300	Leva med en kronisk sjukdom : En litteraturöversikt om inflammatorisk tarmsjukdom och hälsorelaterad livskvalitet / To live with a chronic disease : A literature review about inflammatory bowel disease and health-related quality of life Hansen, Linda, Lindh, Louise January 2014 (has links) Bakgrund: Inflammatorisk tarmsjukdom (IBD) inkluderar ulcerös kolit och Crohns sjukdom. De är kroniska och uppkommer i skov då tarmslemhinnan blir inflammerad och sårig vilket ger en komplex symtombild med akuta diarréer, rektalblödning och buksmärtor. Behandlingen går ut på att minska symtom och förebygga uppkomst av skov. Då dessa sjukdomar påverkar det dagliga livet så påverkas också den individuella hälsorelaterade livskvaliteten, vilket mäter den fysiska, psykiska och sociala aspekten av ett hälsoproblem. Syfte: Syftet var att beskriva upplevelsen av hälsorelaterad livskvalitet hos personer med inflammatorisk tarmsjukdom. Metod: En litteraturöversikt har gjorts där tolv vetenskapliga artiklar har utgjort grunden till resultatet och skapat en översikt på befintlig forskning. De har lästs, sammanfattats och analyserats där likheter och skillnader har hittats och teman bildats. Resultat: Resultatets fyra huvudteman är Fysisk funktion, Psykisk funktion, Social funktion och Att återställa sin livskvalitet. Det framkom i resultatet att de fysiska symtomen och sjukdomsaktiviteten är det som i huvudsak styr såväl det psykiska välmåendet som de sociala restriktionerna. Detta visade sig även ha en negativ inverkan på den hälsorelaterade livskvaliteten. Men med tiden blev dock sjukdomen en normal del av livet och en bättre livskvalitet upplevdes. Diskussion: Metodens tillvägagångssätt samt fördelar och nackdelar diskuteras och analyseras. Vid diskussion av resultatet tas främst kunskap, utbildning och tidsperspektivet upp samt återkopplas till Orems egenvårdsteori. / Background: Inflammatory bowel disease (IBD) encompasses ulcerative colitis and Crohn's disease. They are chronic and occur in relapses when the mucosal becomes inflamed and ulcerated, causing complex symptoms such as acute diarrhoea, rectal bleeding and abdominal pain. The treatment aims to reduce symptoms and prevent the occurrence of relapses. As these diseases affect the daily life it also affects the individual health-related quality of life, which measures the physical, psychological and social aspects of a health problem. Aim: The purpose was to describe the experience of health-related quality of life in people with inflammatory bowel disease. Method: A literature review has been done where twelve original articles have formed the basis of the results, this creates an overview of existing research. They have been read, summarized and analysed where the similarities and differences were found and themes were formed. Results: The four main themes of the result is Physical function, Psychological function, Social function and Rebuilding their quality of life. It emerged in the results that physical symptoms and disease activity are those which essentially controls the psychological well-being as well as social constraints. This was shown in studies to have a negative impact on the health-related quality of life. But overtime the disease became a normal part of one's life and gave a better quality of life experience. Discussions: The method approach, benefits and weaknesses will be discussed and analysed. When discussing the results of the current study mainly knowledge, education, and time perspective will be addressed and analysed with Orem’s self-care theory. Inflammatory bowel disease IBD Ulcerative colitis Crohn’s disease Quality of life Health-related quality of life Inflammatorisk tarmsjukdom IBD Ulcerös kolit Crohns sjukdom Livskvalitet Hälsorelaterad livskvalitet

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