Eosinophil Apoptosis

Seton, Kristina

January 2003

<p>Apoptosis or programmed cell death is crucial for the resolution of inflammation, and phagocytosis of apoptotic cells initiates the release of actively anti-inflammatory responses from the phagocytes. Eosinophils are one of the most potent inflammatory cells in the body and is involved in a number of diseases, most commonly associated with parasitic infections and allergic diseases. Apoptosis in eosinophils is therefore one of the most important systems to avoid inflammation. This aim of the present investigation was to examine the mechanisms behind, and the consequences of this process in eosinophils. Apoptotic eosinophils have a unique surface receptor expression that indicates abilities to communicate with T-, B- and antigen presenting cells. They have a novel expression of CD49f, indicating an importance for binding to laminin or unknown functions of the VLA-6 receptor, possibly in the concept of phagocytosis of the apoptotic cell. </p><p>In apoptotic eosinophils the granules are translocated to the periphery of the cell, probably through a disruption of the cytoskeleton. This translocation makes the granules easily accessible and the apoptotic eosinophil can release considerable amounts of granule proteins in response to specific stimuli. The spontaneous release however, is decreased as compared with living cells. </p><p>Furthermore, the survival of eosinophils in response to an allergen challenge is increased in healthy subjects, but not in allergic patients. Mechanistically, this needs further investigation, but one theory is that it is due to the presence of specific IgE in patients in combination with differences in the response from the epithelial cells.</p>

Cell biology

Apoptosis

Programmed Cell Death

Survival

Eosinophils

Inflammatory Diseases

Resolution of inflammation

Functions

Flow cytometry

Cellbiologi

Cell biology

Cellbiologi

Eosinophil Apoptosis

Seton, Kristina

January 2003

Apoptosis or programmed cell death is crucial for the resolution of inflammation, and phagocytosis of apoptotic cells initiates the release of actively anti-inflammatory responses from the phagocytes. Eosinophils are one of the most potent inflammatory cells in the body and is involved in a number of diseases, most commonly associated with parasitic infections and allergic diseases. Apoptosis in eosinophils is therefore one of the most important systems to avoid inflammation. This aim of the present investigation was to examine the mechanisms behind, and the consequences of this process in eosinophils. Apoptotic eosinophils have a unique surface receptor expression that indicates abilities to communicate with T-, B- and antigen presenting cells. They have a novel expression of CD49f, indicating an importance for binding to laminin or unknown functions of the VLA-6 receptor, possibly in the concept of phagocytosis of the apoptotic cell. In apoptotic eosinophils the granules are translocated to the periphery of the cell, probably through a disruption of the cytoskeleton. This translocation makes the granules easily accessible and the apoptotic eosinophil can release considerable amounts of granule proteins in response to specific stimuli. The spontaneous release however, is decreased as compared with living cells. Furthermore, the survival of eosinophils in response to an allergen challenge is increased in healthy subjects, but not in allergic patients. Mechanistically, this needs further investigation, but one theory is that it is due to the presence of specific IgE in patients in combination with differences in the response from the epithelial cells.

Cell biology

Apoptosis

Programmed Cell Death

Survival

Eosinophils

Inflammatory Diseases

Resolution of inflammation

Functions

Flow cytometry

Cellbiologi

Cell biology

Cellbiologi

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

Alard, Jeanne

19 September 2017

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

Probiotiques

Obésité

MICI

Modèles animaux

Techniques in vitro

TNBS

In vivo

Colite

In vitro model

Obesity

Chronic inflammatory diseases

Probiotics

Understanding and Exploiting Wnt5a and GSK3 Signaling in Inflammatory Disease

Bhatt, Pooja

07 June 2013

No description available.

Biomedical Research

Cellular Biology

Molecular Biology

Atherosclerosis

Wnt5a

Alzheimer's disease

inflammation

GSK3

cytokines

beta catenin

inflammatory diseases

Vliv vybraných zánětlivých agens na proces osteoklastogeneze / Effect of selected inflammatory agents on the osteoclastogenesis

Škubica, Patrik

January 2018

Introduction: Bone is a highly active tissue throughout life and is a subject to constant remodelling. Main cells responsible for continuous resorption and de novo synthesis of bone matrix are osteoclast, osteoblasts and osteocytes. Osteoclasts are the only known type of cells able to resorb bone. These cells are formed by fusion of precursor cells in bone marrow or peripheral blood in a process called osteoclastogenesis. Formation of osteoclasts may be of importance concerning chronic inflammatory diseases that are linked with higher risk of developing osteoporosis during lifespan. Celiac disease is one of those diseases, which is characterized by destruction of intestinal mucosa after ingestion of gluten by susceptible individuals followed by induction of chronic inflammation. In this work, we focused on the potential role of osteoclastogenesis in the development of osteoporosis in patients with celiac disease and we studied roles of selected inflammatory agents (TNF-α, IL-6, IFN-γ a cfDNA) with supposed or hypothesised effects on osteoclastogenesis. Material & Methods: We obtained plasma and serum samples from newly diagnosed patients with celiac disease, patients on gluten free diet and healthy controls and analysed concentrations of cfDNA and inflammatory cytokines TNF-α, IL-6 and IFN-γ in...

Immunisation active à base de peptides, dérivés de l’IL-6 et de l’IL-1β, dans les maladies inflammatoires chroniques / Peptide-based active immunization against IL-6 and IL-1β in chronic inflammatory diseases

Desallais, Lucille

13 May 2013

Les anticorps monoclonaux anti-cytokine ont constitué une révolution dans le traitement des maladies inflammatoires chroniques, mais leur utilisation présente des inconvénients (non réponse, résistance, effets secondaires, coûts élevés).Notre équipe développe une stratégie alternative originale, l’immunisation active à base de peptides de cytokines. Elle a pour but de faire synthétiser, par l’organisme même du patient, des anticorps neutralisant les effets pathogènes dus à l’excès de cytokines.Durant ma thèse, j’ai montré que l’immunisation active contre un peptide dérivé de l’IL-6 murine est protectrice dans un modèle murin de sclérodermie systémique. L’immunisation de singes avec l’équivalent humain entraîne une réduction significative des réactions inflammatoires locales suite à l’induction d’une réaction d’HSR. De plus, l’immunisation active contre deux peptides dérivés de l’IL-1β et de l’IL-23 conduit à la réduction de la sévérité de l’EAE.Ces résultats confortent l’intérêt de cibler les cytokines par l’approche d’immunisation active à base de peptides, qui pourra permettre de diversifier l’offre thérapeutique actuellement disponible. / Monoclonal antibodies have been a revolution for the treatment of chronic inflammatory diseases, but their use shows major drawbacks (non-response, resistance, side effects and prohibitive costs).Our team develops an original alternative strategy: anti-cytokine peptide-based active immunization.The aim of the approach is to make the patient’s own organism produce antibodies capable of neutralizing the pathogenic effects of cytokine overproduction.During my PhD, I have demonstrated that active immunization against an IL-6 murine peptide confers clinical protection in a murine model of systemic sclerosis. Monkeys immunized against the human peptide also showed a significant decrease of local inflammatory reactions following a delayed-type hypersensitivity reaction. Moreover, active immunization against an IL-1β and an IL-23 murinepeptide led to a reduction of the severity of the EAE in mice.These results comfort the interest of anti-cytokine peptide-based active immunization, which should eventually widen the choice of therapeutics available for the patients.

Immunisation active

Interleukine-6

Interleukine-1β

Peptide

Maladies inflammatoires chroniques

Active immunization

Interleukin-6

Interleukin-1β

Peptide

Chronic inflammatory diseases

610

Infectious and Inflammatory Diseases of Salivary Glands

Al-Abbadi, Mousa A., Zakaria, Wael N., Eltoum, Isam A.

09 March 2011

No description available.

acute bacterial parotitis

an infrequent illness - in the elderly

in dehydrated

malnourished and intubated patients

an uncommon cause of parotitis

Facteurs génétiques de prédisposition à la maladie coeliaque et l'oesophagite éosinophilique

Cherief, Freha Nour el Hayet

12 1900

Les maladies immunitaires chroniques incluant les maladies auto-immunes et inflammatoires touchent 20 à 25% de la population des pays occidentaux. La comparaison des taux de concordance chez les jumeaux ou l’histoire familiale de sujets atteints de la maladie cœliaque (maladie auto-immune de l’intestin) ou de l’œsophagite éosinophilique (maladie inflammatoire de l’œsophage) indiquent que des facteurs génétiques et environnementaux interviennent dans la susceptibilité à ces maladies. Cependant, ces études ne distinguent pas de manière claire la prédisposition génétique selon l’hétérogénéité clinique (enfants versus adultes) ou ethnique (stratification des populations). Méthodes. Les haplotypes HLA de prédisposition à la maladie cœliaque et les polymorphismes des gènes candidats IL-13 (R130Q), IL-5 (-746 T/G) et IL-5R (-80A/G) impliqués dans la physiopathologie de l’œsophagite éosinophilique, ont été caractérisés par la technique PCR-SSP sur l’ADN génomique. Résultats: Nos études familiales et cas-contrôles réalisées chez une population Québécoises avec un fond génétique très homogène nous a permis : i) d’éviter le problème de stratification des populations, ii) de confirmer que les gènes HLA sont également associés à la maladie cœliaque (enfants et adultes) au Québec comme dans les autres populations Caucasiennes, iii) de mettre en évidence le rôle du gène IL-13 dans la prédisposition à l’œsophagite éosinophilique (garçons et filles) et d’exclure les gènes IL-5 et IL-5R comme facteurs de susceptibilité dans notre population. Conclusion: Ce travail confirme pour la première fois l’impact des gènes HLA dans la prédisposition à la maladie cœliaque et le rôle du facteur génétique dans l’œsophagite éosinophilique chez une population Canadienne Française avec un fond génétique ayant un fort effet fondateur. / Chronic immune diseases including autoimmune and inflammatory diseases affect 20 to 25% of Western country population. The higher concordance of disease in twins or in first-degree relative of patients with celiac disease (bowel autoimmune disease) or eosinophilic esophagitis (inflammatory disease of the esophagus) indicate that genetic and environmental factors are involved in susceptibility to these diseases. However, these studies do not distinguish clearly genetic predisposition according to clinical heterogeneity (children versus adults) or ethnicity (population stratification). Methods: HLA haplotypes predisposing to celiac disease and polymorphisms of candidate genes IL-13 (R130Q), IL-5 (-746 T / G) and IL-5R (-80A / G) involved in physiopathology of eosinophilic esophagitis, have been evaluated by PCR-SSP on genomic DNA. Results: Our familial and case-control studies performed in populations having a very similar genetic background with a strong founder effect, allowed us: i) to avoid the problem of population stratification, ii) to confirm that HLA genes are also associated with celiac disease in Quebec (children and adults) as in other Caucasian populations, iii) to identify the role of IL-13 gene in susceptibility to eosinophilic esophagitis (boys and girls) and to exclude IL-5 and IL-5R genes as susceptibility factor in our population. Conclusion: This study confirms for the first time the impact of HLA genes in predisposition to celiac disease and the role of genetic factors in eosinophilic esophagitis in a French Canadian population with a strong founder effect.

Maladies immunitaires

Maladies auto-immunes

Maladies inflammatoires

Maladie cœliaque

HLA –II

Œsophagite à éosinophile

Immune diseases

auto-immune diseases

inflammatory diseases

Celiac disease

HLA-II

Eosinophilic esophagitis

Rôle des cellules lymphoïdes innées chez l'homme : analyse au cours de déficits immunitaires, pathologies auto-immunes et inflammatoires / Roles of innate lymphoid cells in human : analysis in primary immunodeficiencies, autoimmune and inflammatory diseases

Ebbo, Mikaël

19 October 2017

Les cellules lymphoïdes innées (ILCs) sont des populations cellulaires d’identification récente, mais leur rôle in vivo chez l’homme reste mal connu. Dans une 1ère étude, nous avons pu montrer qu’un déficit sévère en NK au cours de déficits immunitaires communs variables est associé à un risque accru de manifestations non infectieuses et infectieuses bactériennes sévères, suggérant un rôle protecteur non redondant des cellules NK lorsque le système immunitaire adaptatif n’est pas fonctionnel. Dans une 2ème étude, nous avons montré que des patients atteints de déficits immunitaires combinés sévères ɣc et JAK3 déficients n’ont pas d’ILCs. Après allogreffe de moelle osseuse, le nombre d’ILCs circulantes reste indétectable, sans manifestation clinique notable associée. Ces résultats sont en faveur d’une redondance des fonctions des ILCs chez l’homme, lorsque les fonctions T et B sont conservées. Nous avons ensuite étudié les modifications phénotypiques et fonctionnelles des cellules NK au cours du purpura thrombopénique immunologique, et observé un défaut de production d’interféron-ɣ par les cellules NK circulantes et une augmentation de la cytotoxicité dépendante des anticorps des cellules NK spléniques. Une inhibition des fonctions des cellules NK par les immunoglobulines polyvalentes est également mise en évidence. Enfin, une étude des ILCs circulantes au cours de la maladie associée aux IgG4 ainsi qu’une revue de la littérature sur l’étude des ILCs au cours des pathologies inflammatoires sont rapportées. En conclusion, l’apparente redondance des ILCs chez l’homme ainsi que leur implication en pathologies inflammatoires en font de potentielles cibles thérapeutiques. / Innate lymphoid cells (ILCs) are recently identified components of the immune system, but their functions in vivo in humans are still elusive. In a first study, we show in patients with common variable immunodeficiency that non-infectious inflammatory complications and severe bacterial infections were more frequent in patients with severe NK cell lymphopenia, indicating potential non-redundant immune functions of NK cells when the adaptive immune response is not optimal. In a second study, we observe that in patients with ɣc and JAK3 severe combined immunodeficiencies, all ILC subsets are absent. After hematopoietic stem cell transplantation, ILCs remain indetectable with no susceptibility to disease, suggesting that ILCs might be redundant and dispensable in humans, if T and B cells functions are preserved. In the second part of this thesis, we study phenotypic and functional modifications of NK cell compartment in primary immune thrombocytopenia. Interferon gamma production by the peripheral blood NK cells of ITP patients is decreased. In contrast, splenic NK cells of ITP patients tend to be more efficient in antibody-dependent cell cytotoxicity. Intravenous polyvalent immunoglobulins lead to the inhibition of blood NK cell activation. Finally, we present the preliminary results of a study investigating the modifications of circulating ILCs in IgG4-related disease, and present an extensive litterature review concerning the role of ILCs in inflammatory diseases. In conclusion, the apparent redundancy of ILCs for protective immunity and their pathogenic role in inflammatory diseases make their targeting in humans for therapeutic purposes particularly promising.

Cellules Natural Killer (NK)

Cellules lymphoïdes innées (ILC)

Déficit immunitaire primitif

Pathologies inflammatoires

Homme

Natural Killer (NK) cells

Innate lymphoid cells

Primary immunodeficiency

Immune thrombocytopenia (ITP)

Inflammatory diseases

Human

Avaliação do estado nutricional de pacientes com doença inflamatória intestinal / Nutrition status of patients with inflammatory bowel disease

Beatriz Peixoto Ramos

28 July 2011

A doença Inflamatória Intestinal (DII) é uma desordem caracterizada pela inflamação crônica do trato gastrointestinal. Os dois principais tipos de DII são a Retocolite Ulcerativa (RCU) e a Doença de Crohn (DC) e ambas cursam com importantes alterações no estado nutricional (EN). O objetivo deste estudo foi identificar as diferenças na composição corporal entre pacientes com DC, RCU e indivíduos saudáveis, além de comparar o estado nutricional dos três grupos de pacientes, ajustando para fatores que podem interferir no EN, como o uso atual de corticosteróides, a atividade física, a atividade de doença, a idade e o sexo. Foi realizado um estudo transversal que incluiu 101 pacientes com DII (50 com DC e 51 com RCU) e 35 indivíduos saudáveis, selecionados no Ambulatório do Hospital Universitário Pedro Ernesto (HUPE) da Universidade do Estado do Rio de Janeiro (UERJ). Foram colhidas informações sócio-demográficas e pessoais, tais como: prática de atividade física, tabagismo, doenças pregressas e procedimentos cirúrgicos prévios. Outras informações necessárias à pesquisa foram coletadas em prontuário médico. A avaliação antropométrica foi realizada por meio das seguintes medidas: peso corporal; altura; circunferências do braço, da cintura (CC) e do quadril; dobras cutâneas do tríceps, subescápula, supra-ilíaca e da coxa; e circunferência muscular do braço (CMB). A análise da composição corporal foi realizada por meio da bioimpedância elétrica (BIA), utilizando-se o aparelho Biodynamics modelo 450. As variáveis laboratoriais analisadas foram: glicose, hemograma completo, perfil lipídico, proteínas totais, albumina, globulina, velocidade de hemossedimentação e proteína C reativa. O peso, o índice de massa corporal, a CC e o percentual de gordura corporal calculado a partir da aferição das dobras cutâneas, foram menores nos pacientes com DC, quando comparados aos indivíduos saudáveis e/ou aos pacientes com RCU. A CMB foi menor nos pacientes com DC e RCU quando comparados aos indivíduos saudáveis, porém sem apresentar diferenças entre os dois grupos de pacientes. Por BIA, verificou-se que os pacientes com DC apresentaram valores de massa magra, massa celular corpórea, massa extracelular, água corporal total e água extracelular menores quando comparados aos indivíduos saudáveis. Os níveis séricos de colesterol total, proteínas totais e albumina, e a contagem total de hemácias foram menores nos indivíduos com DC quando comparados aos indivíduos do grupo controle e/ou aos indivíduos do grupo da RCU. Os pacientes com RCU exibem composição corporal semelhante à da população saudável. Em contraposição, os pacientes com DC apresentam EN amplamente comprometido com depleção de gordura corporal e massa magra em relação aos demais indivíduos / Inflammatory Bowel Disease (IBD) is a disorder characterized by diffuse inflammation of the gastrointestinal tract. The two main types of IBD are ulcerative colitis (UC) and Crohn's disease (CD), both coursing with important changes in nutritional status (NS). The objective of this study was to identify differences in body composition between patients with CD, UC, and healthy subjects and to compare the NS of these three groups of patients, adjusting for factors that can interfere in NS such as current use of corticosteroids, physical activity, disease activity, age and sex. It was conducted a cross-sectional study which included 101 patients with IBD (50 with CD and 51 with UC) and 35 healthy subjects, selected at the Ambulatory of Pedro Ernesto University Hospital (HUPE) of the Rio de Janeiro State University (UERJ). Socio-demographic and personal information such as physical activity, smoking, prior diseases and previous surgical procedures were collected. Other necessary information for the research were collected from medical records. The anthropometric evaluation was carried out through the following measures: body weight; height; mid-arm, waist and hip circumferences; skinfold thickness of the triceps, subscapular, suprailiac, and thigh; and mid-arm muscle circumference (MAMC). The body composition analysis was performed by bioelectrical impedance (BIA) using the equipment Biodynamics model 450. The laboratory variables analyzed, included: glucose, complete blood count, lipid profile, total protein, albumin, globulin, erythrocyte sedimentation rate, and C-reactive protein. Weight, body mass index, waist circumference, and percentage body fat calculated from skinfold measurements were lower in CD patients compared to healthy subjects and/or the patients with UC. The MAMC was lower in patients with CD and UC compared to healthy subjects, but without showing differences between the two groups of patients. Through BIA, it was found that CD patients had values of lean body mass, body cell mass, extracellular mass, total body water, and extracellular water smaller when compared to healthy subjects. Seric levels of total cholesterol, total protein, and albumin, as well as red blood cell count and relative count of lymphocytes were lower in the individuals with CD than the individuals of the control group and/or the patients with UC. Patients with UC exhibit body composition similar to that of the healthy population. In contrast, CD patients have widely NS committed with depletion of body fat and lean mass in relation to other individuals.

Gastroenterologia - Teses

Avaliação nutricional

Bioimpedância elétrica

Composição corporal

Retocolite ulcerativa

Doença de Crohn

Doença inflamatória intestinal

Crohn, Doença de - Teses

Proctocolite

Inflammatory bowel disease

Ulcerative colitis

Body composition

Nutrition status

Bioelectrical impedance analysis

Nutritional assessment

Gastroenterology - Theses

Crohn's Disease - Theses

4. Proctocolitis

NUTRICAO