Development of molecular-based techniques for the detection, identification and quantification of food-borne pathogens

Rodríguez Lázaro, David

18 June 2004

La presencia de microorganismos patógenos en alimentos es uno de los problemas esenciales en salud pública, y las enfermedades producidas por los mismos es una de las causas más importantes de enfermedad. Por tanto, la aplicación de controles microbiológicos dentro de los programas de aseguramiento de la calidad es una premisa para minimizar el riesgo de infección de los consumidores. Los métodos microbiológicos clásicos requieren, en general, el uso de pre-enriquecimientos no-selectivos,enriquecimientos selectivos, aislamiento en medios selectivos y la confirmación posterior usando pruebas basadas en la morfología, bioquímica y serología propias de cada uno de los microorganismos objeto de estudio. Por lo tanto, estos métodos son laboriosos, requieren un largo proceso para obtener resultados definitivos y, además, no siempre pueden realizarse. Para solucionar estos inconvenientes se han desarrollado diversas metodologías alternativas para la detección identificación y cuantificación de microorganismos patógenos de origen alimentario, entre las que destacan los métodosinmunológicos y moleculares. En esta última categoría, la técnica basada en la reacción en cadena de la polimerasa (PCR) se ha convertido en la técnica diagnóstica más popular en microbiología, y recientemente, la introducción de una mejora de ésta, la PCR a tiempo real, ha producido una segunda revolución en la metodología diagnóstica molecular, como pude observarse por el número creciente de publicaciones científicas y la aparición continua de nuevos kits comerciales. La PCR a tiempo real es unatécnica altamente sensible -detección de hasta una molécula- que permite la cuantificación exacta de secuencias de ADN específicas de microorganismos patógenos de origen alimentario. Además, otras ventajas que favorecen su implantación potencial en laboratorios de análisis de alimentos son su rapidez, sencillez y el formato en tubo cerrado que puede evitar contaminaciones post-PCR y favorece la automatización y un alto rendimiento. En este trabajo se han desarrollado técnicas moleculares (PCR y NASBA) sensibles y fiables para la detección, identificación y cuantificación de bacterias patogénicas de origen alimentario (Listeria spp., Mycobacterium avium subsp. paratuberculosis y Salmonella spp.). En concreto, se han diseñado y optimizado métodos basados en la técnica de PCR a tiempo real para cada uno de estos agentes: L. monocytogenes, L. innocua, Listeria spp. M. avium subsp. paratuberculosis, y también se ha optimizado yevaluado en diferentes centros un método previamente desarrollado para Salmonella spp. Además, se ha diseñado y optimizado un método basado en la técnica NASBA para la detección específica de M. avium subsp. paratuberculosis. También se evaluó la aplicación potencial de la técnica NASBA para la detección específica de formas viables de este microorganismo. Todos los métodos presentaron una especificidad del 100 % con una sensibilidad adecuada para su aplicación potencial a muestras reales de alimentos. Además, se han desarrollado y evaluado procedimientos de preparación de las muestras en productos cárnicos, productos pesqueros, leche y agua. De esta manera se han desarrollado métodos basados en la PCR a tiempo real totalmente específicos y altamente sensibles para la determinación cuantitativa de L. monocytogenes en productoscárnicos y en salmón y productos derivados como el salmón ahumado y de M. avium subsp. paratuberculosis en muestras de agua y leche. Además este último método ha sido también aplicado para evaluar la presencia de este microorganismo en el intestino de pacientes con la enfermedad de Crohn's, a partir de biopsias obtenidas de colonoscopia de voluntarios afectados.En conclusión, este estudio presenta ensayos moleculares selectivos y sensibles para la detección de patógenos en alimentos (Listeria spp., Mycobacterium avium subsp. paratuberculosis) y para una rápida e inambigua identificación de Salmonella spp. La exactitud relativa de los ensayos ha sido excelente, si se comparan con los métodos microbiológicos de referencia y pueden serusados para la cuantificación de tanto ADN genómico como de suspensiones celulares. Por otro lado, la combinación con tratamientos de preamplificación ha resultado ser de gran eficiencia para el análisis de las bacterias objeto de estudio. Por tanto, pueden constituir una estrategia útil para la detección rápida y sensible de patógenos en alimentos y deberían ser una herramienta adicional al rango de herramientas diagnósticas disponibles para el estudio de patógenos de origen alimentario. / The presence of pathogens in foods is among the most serious public health concerns, and the diseases produced by them are a major cause of morbidity. Consequently, the application of microbiological control within the quality assessment programs in the food industry is a premise to minimize the risk of infection for the consumer. Classical microbiological methods involve, in general, the use of a non-selective pre-enrichment, selective enrichment, isolation on selective media, and subsequent confirmation using morphological, biochemical and/or serological tests. Thus, they are laborious, time consuming and not always reliable (e.g. in viable but non-culturable VBNC forms). A number of alternative, rapid and sensitive methods for the detection, identification and quantification of foodborne pathogens have been developed to overcome these drawbacks. PCR has become the most popular microbiological diagnostic method, and recently, the introduction of a development of this technique, RTi-PCR, has produced a second revolution in the molecular diagnostic methodology in microbiology. RTi-PCR is highly sensitive and specific. Moreover, it allows accurate quantification of the bacterial target DNA. Main advantages of RTi-PCR for its application in diagnostic laboratories include quickness, simplicity, the closed-tube format that avoids risks of carryover contaminations and the possibility of high throughput and automation.In this work, specific, sensitive and reliable analytical methods based on molecular techniques (PCR and NASBA) were developed for the detection, identification and quantification of foodborne pathogens (Listeria spp., Mycobacterium avium subsp. paratuberculosis and Salmonella spp.). Real-time PCR based methods were designed and optimised for each one of these target bacteria: L. monocytogenes, L. innocua, Listeria spp. M. avium subsp. paratuberculosis, and also a real-time PCR basedmethod previously described for Salmonella spp. was optimised and multicenter evaluated. In addition, an NASBA-based method was designed and optimised for the specific detection of M. avium subsp. paratuberculosis. The potential application of the NASBA technique for specific detection of viable M. avium subsp. paratuberculosis cells was also evaluated.All the amplification-based methods were 100 % specific and the sensitivity achieved proved to be fully suitable for further application in real food samples. Furthermore, specific pre-amplification procedures were developed and evaluated on meatproducts, seafood products, milk and water samples. Thus, fully specific and highly sensitive real-time PCR-based methods were developed for quantitative detection of L. monocytogenes on meat and meat products and on salmon and cold smoked salmon products; and for quantitative detection of M. avium subsp. paratuberculosis on water and milk samples. The M. avium subsp. paratuberculosis-specific real-time PCR-based method was also applied to evaluate the presence of this bacterium in the bowelof Crohn's disease patients using colonic biopsy specimens form affected and unaffected volunteers. In addition, fully specific and highly sensitive real-time NASBA-based methods were developed for detection of M. avium subsp. paratuberculosis on water and milk samples.In conclusion, this study reports selective and sensitive amplification-based assays for the quantitative detection of foodborne pathogens (Listeria spp., Mycobacterium avium subsp. paratuberculosis and) and for a quick and unambiguously identification of Salmonella spp. The assays had an excellent relative accuracy compared to microbiological reference methods and can be used for quantification of genomic DNA and also cell suspensions. Besides, in combination with sample pre-amplification treatments,they work with high efficiency for the quantitative analysis of the target bacteria. Thus, they could be a useful strategy for a quick and sensitive detection of foodborne pathogens in food products and which should be a useful addition to the range of diagnostic tools available for the study of these pathogens.

Foodborne pathogens

Detecció microbiana

NASBA

Microbial detection

Detección microbiana

Listeria

Crohn's disease

Enfermedad de Crohn

PCR a tiempo real

Malaltia de Crohn

Patògens d'origen alimentari

Patógenos de origen alimentario

Real-time PCR

577

613

632

Étude sur le rôle de SIGIRR chez les cas pédiatriques dans la maladie de Crohn

Sagala, Patrick

01 1900

No description available.

Sigirr

Sigirr soluble

Maladie de Crohn pédiatrique

Interleukine-37

Interleukine-18

Interleukine-18BP

IL-18Rα

Sigirr

Soluble sigirr

Pediatric Crohn's disease

Interleukin-37

Interleukin-18

Interleukin-18BP

IL-18Rα

Klinické a genetické prediktory lékové závislosti u idiopatických střevních zánětů / Clinical and genetic predictors of drug dependency in inflammatory bowel disease

Ďuricová, Dana

January 2012

IN ENGLISH Drug dependency in inflammatory bowel disease (IBD), Crohn's disease (CD) and ulcerative colitis (UC), is a specific disease phenotype which determines disease prognosis and hence may be used as a prognostic marker for treatment management. Drug dependency in IBD has been well described in corticosteroid treatment and recently also in infliximab (IFX) therapy. The aims of this thesis were: 1) to assess the occurrence of IFX dependency in paediatric and adult patients with CD; further to search for clinical and genetic predictors of IFX outcome and to evaluate the impact of IFX dependency on surgical rate; 2) to assess in CD patients the outcome of the first course of 5-ASA monotherapy with emphasis on 5-ASA dependency and to define clinical predictors of 5-ASA treatment outcome. We found that 66% of children and 29% of adults with CD became IFX dependent. The high frequency in paediatrics is in agreement with previously published studies, while the finding in adult patients indicates a lower rate of IFX dependency in the only study to date. Perianal disease and no bowel surgery prior to IFX start were predicative of IFX dependency in paediatric patients. In adult cohort, 2 genetic variants LTA c.207 A>G and CASP9 c.93 C>T were associated with IFX outcome, whereas no relevant clinical...

The impact of apple peel polyphenols on intestinal and mitochondrial functions in experimental colitis

Rahmani Yeganeh, Pantea

12 1900

Background: We have recently shown that dysregulation of redox-sensitive signaling pathways and oxidative damage to biological structures are major contributors to experimental ulcerative colitis. We also demonstrated the powerful anti-oxidant and anti-inflammatory actions of dietary apple peel polyphenols (DAPP) in the intestine. Objectives: As mitochondria are major sources and target of free radicals, as well as exhibit various important cellular functions, we evaluated their roles in intestinal colitis and their responses to DAPP. Methods: Induction of intestinal inflammation in C57BL6 mice was performed by administration of 3% dextran sulfate sodium (DSS). Two different doses of DAPP (200 and 400 mg/kg/day) were administered by gavage for 10 days (before and during DSS administration) to examine the preventive and curative effects, respectively, on inflammation and oxidative stress (OxS) in the intestine, and on mitochondrial functions. Results: DSS caused a significant weight loss, shortening of the colon, increased OxS (noted by lipid peroxidation), and raised inflammation (verified by infiltration of inflammatory cells, up-regulation of MPO, and elevated TNF-α and COX2 protein expression). Furthermore, DSS induced perturbations in mitochondrial biogenesis, as reflected by alterations of the transcription factor PGC1α and mitochondrial function characterized by diminished Adenosine-5'-Triphosphate (ATP) production, lowered antioxidant defense (GPx and SOD2), amplified apoptosis (as illustrated by the high expression of Cytochrome C and AIF), and defects in DNA integrity (high 8-OHdG). However, DAPP administration improved macroscopic parameters (e.g. weight loss, colon shortening) and reduced DSS-induced clinical signs. DAPP showed an evident capability of reducing inflammation (as noted by decreased TNF-α, iNOS, COX-2 and AP-1) and OxS (as shown by reduced malondialdehyde, hydrogen peroxide levels and increased GPx) in DSS mice. Our findings also revealed that DAPP partially corrected mitochondrial dysfunction related to redox homeostasis, fatty acid β-oxidation, ATP synthesis, apoptosis and regulatory mitochondrial transcription factors (PGC1α, PPARγ and Nrf-2). Conclusion: DAPP have the ability to act on intestinal OxS, inflammation and mitochondrial dysfunction, thereby alleviating colitis progression via the modulation of cellular energy, OxS, antioxidant capacity, apoptosis and mtDNA integrity. / Contexte: L'inflammation et le stress oxydatif (OxS) participent à la pathogenèse de la colite ulcéreuse (CU). Nos résultats récents montrent que les polyphénols de la pelure de pomme (DAPP) jouent un rôle clé dans la prévention de la maladie. Objectifs: Évaluer les effets préventifs et curatifs du DAPP sur la CU et démontrer leur impact sur la dysfonction mitochondriale. Méthode: Une induction de l’inflammation intestinale a été effectuée chez des souris par administration du dextran sulfate sodium (DSS). Des doses de DAPP (200 et 400 mg/kg/j) ont été administrées par gavage pendant 10 jours afin d’évaluer les effets préventifs et curatifs, respectivement, sur l’Inflammation et le OxS au niveau intestinal ainsi que sur les fonctions mitochondriales. Résultats: Le DSS a provoqué une perte de poids, un raccourcissement du côlon, une augmentation du stress oxydant, niveaux de malondialdéhyde et une inflammation documentée par l’infiltration des cellules inflammatoires, la myéloperoxydase et les cytokines inflammatoires. D’autre part, le DSS a induit des désordres au niveau de la biogenèse (PGC1α) et des fonctions de la mitochondrie : diminution de l’ATP, altération des enzymes antioxydantes (SOD2 et GPX1), augmentation de l’apoptose (Bcl 2, Bax et Cytochrome C), et des défauts de l’intégrité de l’ADN (baisse d’OGG1). Cependant, le DAPP a amélioré significativement l’inflammation et le stress oxydant de l’intestin tout en corrigeant les aberrations mitochondriales. Conclusions: Les polyphénols ont la capacité d’agir sur le stress oxydant et le profil inflammatoire de l’intestin ainsi que sur le dysfonctionnement mitochondrial. Ils pourraient donc intervenir efficacement dans la CU.

Mitochondria

Mitochondrial function and dysfunction

Inflammatory bowel disease

Inflammation

Crohn's disease

Experimental colitis

Oxidative stress

Polyphenols

Prevention

Treatment

Stress oxydatif

Mitochondrie

Maladies inflammatoires intestinales

Identification et caractérisation moléculaire et fonctionnelle des cellules tissulaires de l’immunité innée chez les patients atteints de maladies inflammatoires intestinales

Chapuy, Laurence

01 1900

Les maladies inflammatoires intestinales (MII), maladie de Crohn (MC) et colite ulcéreuse (CU), représentent un problème de santé publique majeur en raison de leur prévalence, de leur chronicité et de l’absence de traitement curatif disponible. La physiopathologie de ces maladies implique des facteurs de prédisposition génétique, des facteurs environnementaux et une réponse anormale du système immunitaire. De par leur position à l’interface entre les facteurs environnementaux, les cellules épithéliales et les cellules de l’immunité adaptative, les cellules de l’immunité innée (phagocytes monocucléés (MNPs) et granulocytes) sont des acteurs importants dans l’initiation et le maintien de l’inflammation intestinale. Largement étudiés chez la souris, leur investigation chez l’humain restait parcellaire, souvent contradictoire dans le colon et rarement étudiée dans le ganglion mésentérique (MLN). Nous avons caractérisé par des méthodes de cytométrie de flux multi-couleurs, de cytométrie de masse (CyTOF) et de séquencage de l’ARN (total et à l’échelon de la cellule unique), les MNPs de la muqueuse colique et des ganglions mésentériques chez les patients atteints de MC et de CU. Nous avons également évalué la fonction des MNPs et des basophiles sur les réponses mémoires T CD4+ autologues tissulaires. Notre travail a mis en évidence des similitudes et des différences entre la MC et la CU, dans la distribution des MNPs et le profil de la réponse mémoire T CD4+ dans le colon et le ganglion. La sous-population de MNPs HLADR+SIRPα+CD14+CD64+CD163- qualifiée de monocytes inflammatoires, et non les macrophages HLADR+SIRPα+CD14+CD64+CD163+, s’accumule dans la muqueuse inflammatoire des patients atteints de MC et de CU, et promeut les réponses mémoires de type Th17 et Th17/Th1 d’une manière dépendante de l’IL-1β. La fréquence de cette population corrèle avec le score de sévérité endoscopique en MC. Cependant, la distribution des MNPs ganglionnaires diffère entre la MC et la CU. Nous montrons que, dans les ganglions des patients atteints de CU, les MNPs HLADR+SIRPα+CD14+CD64+ sont enrichis en cellules CD163+, qui incluent principalement des cellules ‘monocyte-like’ HLA-DRdim en plus de macrophages HLA-DRhi. Parmi les cellules dendritiques (DCs) HLADR+SIRPα+CD14-CD64-, les DCs plasmocytoides prédominent dans les deux MII, avec une fréquence supérieure en MC qu’en CU. Par ailleurs, l’IL-1β dans la MC et l’IL-12 dans la CU favorisent un profil pathogénique dans les lymphocytes T CD4+ (IFN-γ, TNF-α, GM-CSF, IL-6) de la muqueuse colique. Par sérendipité, nous avons aussi mis en évidence que l’IL-12 et les monocytes inflammatoires tissulaires induisent la production d’IL-8 par les lymphocytes T CD4+ mémoires de la muqueuse intestinale et des MLNs dans la CU mais pas dans la MC. Au cours de cette étude, nous avons également observé l’accumulation de basophiles, mais pas de mastocytes, dans la muqueuse colique et le MLN en MC et en CU, et montré qu’ils favorisaient également les réponses Th17 et Th17/Th1 et non Th1 dans les lymphocytes T CD4+ mémoires exprimant CCR7. En conclusion, la caractérisation des MNPs de la muqueuse intestinale et des MLNs dans les maladies inflammatoires intestinales (MII) permet de mieux appréhender la physiopathologie de la maladie, dans l’espoir d’optimiser la stratification des MII et de permettre ainsi une prise en charge thérapeutique personnalisée. / Crohn's disease (CD) and ulcerative colitis (UC), two common forms of inflammatory bowel disease (IBD), represent a major public health problem because of their prevalence, chronicity and lack of available curative treatment. The pathophysiology of these diseases involves predisposing genetic factors, environmental triggers, and a dysfunctional immune response. Innate immune cells, including mononuclear phagocytes (MNPs) and granulocytes, are important players in the initiation and maintenance of intestinal inflammation due to their position at the interface between the external environment, epithelium and adaptive immune cells. Although widely studied in mice, their investigation in humans remains fragmentary, often with contradictory findings reported in the colon, and they are rarely studied in the mesenteric lymph nodes (MLNs). MNPs from the colon and MLNs of patients with CD and UC were characterized by multi-color flow cytometry, mass cytometry (CyTOF) and RNA sequencing (bulk and single cell). The function of MNPs and basophils on autologous memory CD4+ T cell responses was also assessed. The results presented here highlight similarities and differences in the distribution of MNPs between CD and UC, and the profile of memory CD4+ T cell response in colon and MLNs. HLADR+SIRPα+CD14+CD64+CD163- MNPs, defined as inflammatory monocytes, but not HLADR+SIRPα+CD14+CD64+CD163+ macrophages, accumulated in the inflammatory mucosa of CD and UC patients, and promoted Th17 and Th17/Th1 memory responses in an IL-1β dependent manner. The frequency of this subpopulation correlated with endoscopic severity in CD. In contrast, the distribution of these two MNP populations in the MLNs differs between CD and UC. HLADR+SIRPα+CD14+CD64+ MNPs were enriched in CD163+ cells that predominantly included HLA-DRdim monocytes-like cells over HLA-DRhi macrophages in UC patients only. Among HLADR+SIRPα+CD14-CD64- dendritic cells (DCs), plasmocytoid DCs predominated in both UC and CD, with higher frequency in CD versus UC. IL-1β in CD and IL-12 in UC favor a pathogenic CD4+ T cell profile (IFN-γ, TNF-α, GM-CSF, IL-6 expression/production) in the colonic mucosa. It was also demonstrated that IL-12 and inflammatory tissue monocytes induced IL-8 production by memory CD4+ T cells in intestinal mucosa and MLNs of UC but not CD. In this study, it was also observed that basophils and not mast cells accumulated, in the colonic mucosa and MLNs of CD and UC patients, and favored Th17 and Th17/Th1, but not Th1, responses in CCR7+ memory CD4+ T cells. In conclusion, characterization of MNPs in the intestinal mucosa and MLNs of IBD patients contributes to a better understanding of IBD pathophysiology and opens avenues to optimize patient stratification, and thus, personalized treatment of IBD patients.

Maladies inflammatoires intestinales

Immunité innée

maladie de Crohn

Colite ulcéreuse

Inflammatory bowel diseases

Ulcerative colitis

Crohn's disease

Innate immunity

Evaluation des facteurs issus de l'efferocytose comme médicament innovant dans le traitement des maladies inflammatoires chroniques de l'intestin / Evaluation of new complex medical biological drug based on apoptotic cell efferocytosis proresolutive factors in the treatment of inflammatory bowel diseases

Martin-Rodriguez, Omayra

10 November 2017

La clairance des cellules apoptotiques par les macrophages est à l’origine d’un microenvironnement pro-résolutif composé de différents facteurs solubles, permettant de stopper la réaction inflammatoire et d’engager la réparation tissulaire. La résolution de l’inflammation est parfois défaillante et concourt au développement de pathologies inflammatoires chroniques, comme les maladies inflammatoires chroniques de l’intestin (MICI), qui regroupent la maladie de Crohn (MC) et la rectocolite hémorragique (RCH). Dans ce contexte, nous proposons d’évaluer l’efficacité thérapeutique de l’injection de ces facteurs pro-résolutifs dans le traitement des MICI. Ce produit issu de la culture de macrophages avec des cellules apoptotiques, appelé SuperMApo (Supernatant issued from Macrophage Apoptotic cell culture) (Brevet # WO2014106666-A1, 2013) contient des facteurs pro-résolutifs semblables à ce qu’on retrouve dans le processus physiologique de résolution de l’inflammation, et qui peuvent être absents ou inefficaces chez ces patients.Lors de ce travail, nous avons mise en évidence une efficacité thérapeutique de SuperMApo à l’aide de deux modèles expérimentaux de colite. Pour évaluer la pertinence de ces modèles par rapport à la pratique clinique, nous avons mise en place la vidéo-endoscopie souple. On a montré que l’efficacité de SuperMApo se traduit par diminution du score clinique, endoscopique et histologique des souris colitiques, accompagnée d’une amélioration de la perméabilité intestinale, et de la cicatrisation muqueuse. Cette efficacité thérapeutique est liée en partie à une reprogrammation des cellules présentatrices d’antigènes (APC) notamment de cDC et de macrophages qui présentent moins de réponse aux ligands de TLR, favorisent l’induction de Treg et inhibent la production de Th1. Par ailleurs, SuperMApo induit une cicatrisation nette de la muqueuse intestinale associée à la fois à une activation des myofibroblastes (la forme active des fibroblastes) et des cellules intestinales épithéliales (IEC). Concrètement, SuperMApo augmente les propriétés de migration, de prolifération et de cicatrisation de ces deux types cellulaire. Cet effet dépend en partie des facteurs de croissance au sein de SuperMApo comme le TGF-β, l’IGF-I et le VEGF. Finalement des résultats préliminaires montrent que SuperMApo induit un profil réparateur sur des fibroblastes issus de patients atteints de MICI. L’ensemble de ces résultats montrent, que l’injection de ces facteurs pro-résolutifs permet de mettre en œuvre des mécanismes capables de mettre en place un processus de résolution de l’inflammation et ouvre vers une utilisation clinique de cette approche dans le traitement de MICI. / Inflammation is a natural body defence reaction in response to injuries. The clearance of apoptotic cells by macrophages is at the origin of a pro-resolving microenvironment composed of various soluble factors, allow the arrest of the inflammatory response and to initiate tissue repair. The resolution of inflammation is sometimes defective and contributes to the development of chronic inflammatory diseases, such as chronic inflammatory bowel disease (IBD), which include Crohn's disease (CD) and ulcerative colitis (UC). In this context, we propose to evaluate the therapeutic effect of these pro-resolving factors in the treatment of IBD. This factors derived from the culture of macrophages with apoptotic cells, and called SuperMApo (Supernatant issued from Macrophage Apoptotic cell culture) (Patent # WO2014106666-A1, 2013) contains pro-resolving factors similar to those found in the physiological process of inflammatory resolution, and which may be absent or ineffective in these patients.In this work, we have demonstrated the therapeutic effect of SuperMApo using two experimental models of colitis. To assess the relevance of these models to clinical practice, we have implemented flexible video endoscopy. The therapeutic effect of SuperMApo has been shown to decrease the clinical, endoscopic and histological score of colitis mice, accompanied by improved intestinal permeability and mucosal healing in vivo. This therapeutic effect is related in part to reprogramming of antigen presenting cells (APC), in particular cDC and macrophages, which exhibit less response to TLR ligands, promote induction of Treg and inhibit Th1 production. In addition, SuperMApo induces a marked tissue repair of the intestinal mucosa associated with activation of myofibroblasts, the active form of fibroblasts, and the epithelial intestinal cells (IEC). In particular, SuperMApo increases the migration, proliferation and wound healing properties of these two cell types. This effect depends in part on the growth factors contained in SuperMApo such as TGF-β, IGF-I and VEGF. Finally, preliminary results show that SuperMApo induces a repairing state on fibroblasts from patients with IBD. This opens widely the use of SuperMApo as a clinically approach to propose this new therapeutic option to refractory patients suffering from IBD

MICI

Rectocolite Hémorragique

Maladie de Crohn

Pro-resol utif

Inflammation

Résolution de l'Inflammation

Réparation tissulaire

Fibroblastes

Cellules intestinales épithéliales

Facteurs de Croissance

IBD

Ulcerative colitis

Crohn's disease

Pro-resolutif

Inflammation

Resolution of inflammation

Tissue repair

Fibroblasts

Intestinal epithelial cells

Growth factors

WI 420

Akvizice, modelování a analýza signálů v ultrazvukovém perfúzním zobrazování / Acquisition, Modeling and Signal Processing in Ultrasound Perfusion Imaging

Mézl, Martin

January 2017

This work deals with possibilities of ultrasound perfusion analysis for the absolute quantification of perfusion parameters. In the theoretical part of this work are discussed possibilities of using of the ultrasound contrast agents and approaches for the perfusion analysis. New methods for the perfusion analysis are suggested and tested in the practical part of this work. The methods are based on convolutional model in which the concentration of the contrast agent is modeled as aconvolution of the arterial input function and the tissue residual function. The feasibility of these methods for the absolute quantification of perfusion parameters is shown on data from phantom studies, simulations and also preclinical and clinical studies. The software for the whole process of the perfusion analysis was developed for using in hospitals.

Patofyziologie idiopatických střevních zánětů.Vztah k primární sklerózující cholangitidě, transplantaci jater a karcinogenezi. / Pathophysiology of inflammatory bowel disease. Relation to primary scklerosing cholangitis, liver transplantation and carcinogenesis.

Bajer, Lukáš

January 2020

Inflammatory bowel disease (IBD) represents a group of multifactorial illnesses with increasing incidence worldwide. Crohn's disease (CD) and ulcerative colitis (UC) are the two most thoroughly defined phenotypes of IBD. IBD associated with primary sclerosing cholangitis (PSC) - a progressive biliary disease leading to cirrhosis and liver failure - is considered as specific IBD phenotype (also referred to as 'PSC - IBD') due to its clinical and pathophysiological characteristics. The aim of the experimental part of this thesis was to define specific features of PSC - IBD in the key areas of IBD pathogenesis. These are: microbiota composition, gut - barrier failure, genetic predisposition and aberrant cellular and antibody immune response. Furthermore, the other goals were to describe relation of IBD status and activity to liver transplantation (LTx) and carcinogenesis based on thorough analysis of clinical data in patients under surveillance at the liver transplantation unit. Using the next-generation parallel sequencing technology, we discovered specific bacterial and mycobial features of gut microbiota composition in PSC - IBD which significantly differed from UC and healthy controls recruited from Czech general population. Moreover, we identified numerous seral biomarkers distinguishing CD, UC...

L’impact de la variation des mesures d’utilité sur le ratio coût-utilité incrémental des traitements indiqués pour la maladie de Crohn

Richard, Marie-Ève

12 1900

Objectifs : La maladie de Crohn (MC) et la colite ulcéreuse (CU) sont associées à un fardeau socio-économique important. Au Canada, les analyses de coûts-utilité (ACU) sont privilégiées afin d’assurer l’allocation optimale des ressources. La mesure d’utilité est essentielle pour réaliser une ACU. L’objectif de ce projet visait à identifier les mesures d’utilité et d’estimer l’impact de ces mesures sur le ratio coût-utilité incrémental (RCUI) des traitements indiqués pour la MC. Méthodes : Un arbre décisionnel a été développé pour mesurer l’impact des valeurs d’utilité du EQ-5D, de l’échelle visuelle analogue (VAS), de l’arbitrage temporel (TTO) et du pari standard (SG), sur le RCUI d’Infliximab (IFX) + Traitements standards (TS) (prednisone, mesalazine (MZ), azathioprine (AZA), 6-mercaptopurine (6-MP)) vs Placébo + TS. Le modèle a porté sur un horizon temporel d’un an, selon les perspectives du système de soins et sociétale. Les moyennes pondérées des mesures d’utilité ont été estimées à partir d’une revue systématique de la littérature. Des analyses de sensibilités déterministes et probabilistes ont également été effectuées. Résultats : L’ensemble des RCUIs, variaient entre 67 068 $/QALY (TTO) et 268 385 $/QALY (EQ-5D). À un seuil de propension à payer de 50 000 $/QALY, la probabilité qu’IFX + TS soit coût efficace était nulle pour l’ensemble des analyses, à l’exception de celle du TTO (4,0%). Conclusion : La variabilité des mesures d’utilité a un impact considérable sur les RCUIs et nécessite une attention particulière de la part des preneurs de décisions, plus précisément au niveau des analyses de sensibilité. / Objectives: Crohn’s disease (CD) and ulcerative colitis are both associated with a high socioeconomic burden. In Canada, cost-utility analyses (CUA) are privileged in order to allocate healthcare spending efficiently. Since utility measures are essential for CUA, the objective of this study was to assess the impact utility values on the incremental cost-utility ratio (ICUR) of CD treatments. Methods: A decision-tree model was developed to assess the impact of utility values derived from the EQ-5D, the visual analogue scale (VAS), the time trade off (TTO) and the standard gamble (SG), on the resulted ICUR of Infliximab (IFX) + Standard of Care (SoC) (prednisone, mesalazine (MZ), azathioprine (AZA), 6-mercaptopurine (6-MP)) versus Placebo (Pbo) + SoC. The model was conducted over a one-year time horizon from the Canadian healthcare and societal perspectives. The weighted averages of utility values were estimated based on a systematic literature evaluation. Both deterministic and probabilistic sensitivity analyses were also conducted. Results: The ICURs ranged from $67,068/QALY (TTO) to $268,385/QALY (EQ-5D). At a $50,000/QALY threshold, the probability of IFX + SoC of being cost-effective was of 0% in most analyses except for the TTO method (4.0%). Conclusion: The variability of utility measures has a considerable impact on the ICURs and requires a special attention from decision-makers, in regards of sensitivity analyses.

Maladies inflammatoires de l’intestin

Maladie de Crohn

Colite ulcéreuse

Utilité

Mesures de préférences

Inflammatory bowel disease

Crohn's disease

Ulcerative colitis

Utility

Preference-based measures

Klinické a genetické prediktory lékové závislosti u idiopatických střevních zánětů / Clinical and genetic predictors of drug dependency in inflammatory bowel disease

Ďuricová, Dana

January 2012

IN ENGLISH Drug dependency in inflammatory bowel disease (IBD), Crohn's disease (CD) and ulcerative colitis (UC), is a specific disease phenotype which determines disease prognosis and hence may be used as a prognostic marker for treatment management. Drug dependency in IBD has been well described in corticosteroid treatment and recently also in infliximab (IFX) therapy. The aims of this thesis were: 1) to assess the occurrence of IFX dependency in paediatric and adult patients with CD; further to search for clinical and genetic predictors of IFX outcome and to evaluate the impact of IFX dependency on surgical rate; 2) to assess in CD patients the outcome of the first course of 5-ASA monotherapy with emphasis on 5-ASA dependency and to define clinical predictors of 5-ASA treatment outcome. We found that 66% of children and 29% of adults with CD became IFX dependent. The high frequency in paediatrics is in agreement with previously published studies, while the finding in adult patients indicates a lower rate of IFX dependency in the only study to date. Perianal disease and no bowel surgery prior to IFX start were predicative of IFX dependency in paediatric patients. In adult cohort, 2 genetic variants LTA c.207 A>G and CASP9 c.93 C>T were associated with IFX outcome, whereas no relevant clinical...