Einfluß genetischer Variationen im Tumor Nekrose Faktor-alpha Gen auf die Progession der HIV-Infektion und die Entstehung HIV-assoziierter Krankheiten

Schüttlöffel, Antje

08 January 2002

Fragestellung: Wir gingen der Frage nach, inwieweit genetische Variationen im Gen für den Tumor Nekrose Faktor-alpha einen Einfluß auf die Krankheitsprogression oder die Entstehung bzw. Ausprägung HIV-assoziierter Erkrankungen haben. Methoden: Die Promotorregion sowie die kodierenden Sequenzen des TNF-alpha-Gens wurden mittels SSCP-Analyse auf genetische Variationen untersucht. Anschließend erfolgte die Charakterisierung der häufigsten bekannten Promotorpolymorphismen mittels Restriktionsfragment-Längenpolymorphismus-Analyse (RFLP). Die Bestätigung der Polymorphismen der RFLP-Analyse erfolgte an ausgewählten Proben durch DNA-Fluoreszenzsequenzierung. In sämtlichen Fällen handelte es sich um singuläre Basentransitionen von Guanin zu Adenin. Ergebnisse: Unter Einbeziehung verschiedener Progressionsparameter wie der CD4-Zellzahl, des Zeitraumes vom ARC-Stadium zum AIDS-Stadium und AIDS-assoziierter Krankheiten wie dem Wasting Syndrom und der HIV-Enzephalopathie, erfolgte anschließend die statistische Analyse in Korrelation mit den ermittelten Genotypen. Es zeigte sich bei keiner der statistischen Analysen eine signifikante Assoziation mit einem bestimmten TNF-alpha-Genotyp. Schlußfolgerung: Es ist kritisch anzumerken, daß für einige Subanalysen die Größe der untersuchten Patientengruppe zu gering war, um eine statistische Aussagekraft für seltene Allele zu erreichen. Anhand der hier vorgelegten Ergebnisse hat der TNF-alpha-Genotyp weder einen Einfluß auf die Progression der HIV-Erkrankung noch auf die Ausbildung HIV-assoziierter Erkrankungen wie dem Wasting Syndrom oder der HIV-Enzephalopathie. / Objective: We determined whether variation of the tumor necrosis factor-alpha gene had an impact on HIV disease progression or the prevalence of hiv-associated diseases. Methods: The promotor region of the TNF-alpha gene were examined with SSCP analysis for polymorphisms in the promotor region. The most common promotor polymorphisms were characterized with restriction fragment length polymorphism analysis (RFLP). To confirm RFLP results DNA fluorescence sequenzing analyses were performed with selected samples. In all cases with diagnosis of promotor polymorphisms single base transitions from guanine to adenine were confirmed. Results: Statistical analyses correlated the genotypes with different markers for disease progression e.g. CD4-count, the period from ARC to AIDS and the occurance of HIV associated diseases (wasting syndrome, hiv encephalopathy). In none of the statistical analyses significant association with a certain TNF-alpha genotyp could be demonstrated. Conclusion: For some subanalysis the sample sizes were too small in order to be able to make safe statistical statements concerning rare allels. Regarding our results, none of the examined tumor necrosis factor-alpha promotor polymorphisms had an impact on HIV disease progression or the prevalence of hiv-associated diseases.

Tumor Nekrose Faktor-alpha

TNF-alpha Promotorpolymorphismen

HIV

Krankheitsprogression

tumor necrosis factor-alpha

TNF-alpha promotor polymorphism

HIV

disease progression

610 Medizin und Gesundheit

33 Medizin

YD 8400

ddc:610

Mechanisms underlying the regulatory function of tumor necrosis factor-alpha in skin inflammation

Kumari, Vandana

04 January 2015

Die Haut ist das größte Organ des Menschen und bildet die Barriere gegenüber Einwirkungen aus der Umwelt. Die Störung der Hautbarriere durch exogene und endogene Reize führt zu einer Entzündungsreaktion in der Haut. In der Folge können Hauterkrankungen wie die irritative oder Atopische Dermatitis entstehen. Der Tumor Nekrose Faktor-α (TNF-α) ist ein pleiotrop wirksames Zytokin, das eine zentrale Rolle bei entzündlichen Prozessen spielt. Ziel der vorgelegten Promotionsarbeit war zu untersuchen, ob und wie TNF-α zu Entzündungsgeschehen, ausgelöst durch exogene und endogene Faktoren, beiträgt. Die Bedeutung von TNF-α wurde in TNF-ko Mäusen in verschiedenen Hautmodellen untersucht. Für das Irritationsmodell wurden chemische und physikalische Reize verwendet. TSLP (Thymic stromal lymphopoietin) wurde durch die verschiedenen Stimuli signifikant induziert. Diese Induktion war unabhängig von der endogenen TNF-α Produktion, gezeigt durch den Einsatz von TNF- ko Mäusen . Da endogenes TNF-α für die Hautirritation keine notwendige Bedingung darstellte, wurde die Bedeutung von TNF-α bei der atopischen Dermatitis (AD) untersucht. TNF-α defiziente Mäuse zeigen verstärkt Ekzeme im Vergleich zu Wildtyp Mäusen. Die Behandlung von TNF-ko Mäusen mit einem TSLP Antikörper führte zu einer Verminderung des Ekzems. Mastzellen wurden vermehrt in läsionaler Haut gefunden und korrelierten mit dem Schweregrad des atopischen Ekzems sowie der TSLP-Expression. / The skin is the largest organ of an individuum and builds the barrier for a host against the environment. Skin barrier disruption by exogenous or endogenous stimuli can lead to skin inflammation. As a consequence, irritant or atopic eczema, frequent skin diseases, may evolve. Tumor necrosis factor-α (TNF-α) is a pleiotropic cytokine which plays a central role in inflammatory processes. The main aim of this thesis was to clarify whether and how endogenous TNF-α is contributing to skin inflammation driven by exogenous and endogenous triggers. The role of endogenous TNF-α was studied using TNF knockout (-/-) mice. In an irritation model, chemical and physical stimuli were applied on to mouse skin. Thymic stromal lymphopoietin (TSLP) was significantly induced by the used irritants. This TSLP induction was independent from endogenous TNF-α proven by using TNF-/- mice. Next the role of TNF-α in atopic dermatitis (AD) promoting an allergic skin inflammation was investigated. TNF-/- mice developed more severe AD compared to the wildtype mice and TSLP was significantly increased and correlated with the severity of the eczema. To prove the pathophysiological role of TSLP for AD progression, TNF-/- mice were pretreated with an TSLP antibody. Indeed, these mice developed less AD symptoms compared to the control mice. Mast cells (MCs) were also significantly increased in lesional skin in the AD model and moreover, correlated with AD severity, but also with TSLP expression.

Mastzellen

Tumor Nekrose Faktor-α

Thymic stromal lymphopoietin

Hauterkrankungen

Atopischen Dermatitis

Tumor necrosis factor-α

Thymic stromal lymphopoietin

skin inflammation

Atopic dermatitis

Mast cell

570 Biologie

32 Biologie

YF 2192

ddc:570

Genetic and environmental factors in asthma: a population based European study

Castro Giner, Francesc

20 November 2009

L'asma és una malaltia d'etiologia complexa, formada per factors genètics i ambientals, on la interrelació de ambdós factors mitjançant interaccions gen-ambient juga un paper clau. L'objectiu d'aquesta tesi ha sigut aprofundir en el coneixement del paper dels polimorfismes genètics, i la seva interacció amb factors ambientals, en la ocurrència d'asma, atòpia i hiperreactivitat bronquial. Aquest objectiu ha estat desenvolupat a través de la replicació de variants genètiques prèviament identificades, l'avaluació d'interaccions gen-ambient i la identificació de nous gens de susceptibilitat mitjançant un disseny basat en el genotipatge de variants genètiques all llarg del genoma en pools d'ADN. La tesi ha estat majoritàriament duta a terme dins l'estudi European Community Respiratory Health Survey (ECRHS) que està comprès per 5.000 individus seguits durant 9 anys, pels quals es disposa d'un qüestionari complet sobre símptomes respiratoris, avaluacions clíniques, informació sobre exposicions ambientals i mostres de ADN. Aquesta tesi a replicat l'associació del polimorfismes dels gens TNFA i NPSR1 amb asma. A més s'han establert les interaccions entre TNFA i obesitat, NQO1 i contaminació atmosfèrica, i NPSR1 i edat d'inici d'asma. L'anàlisi de pools d' ADN ha permès associar la regió on es situa el gen SGK493 amb atòpia. Aquesta tesi contribueix al coneixement de l'etiologia d'asma amb la identificació i replicació d'associacions genètiques i interaccions gen-ambient. / Asthma is a disease with a complex etiology, involving multiple genetic and environmental factors, and with an important role of the interplay of these factors through gene-environment interactions. In this thesis I aimed to advance our knowledge on the importance of genetic polymorphisms and their interaction with environmental data for the occurrence of asthma and related phenotypes (atopy and bronchial hyperreactivity). This objective was developed through the replication of genetic associations previously reported, the assessment of gene-environment interactions and the identification of new susceptibility genes using genome-wide analysis based on a pooling DNA strategy. The thesis was, mostly, performed within the European Community Respiratory Health Survey (ECRHS). This cohort has information and DNA samples from approximately 5,000 adult subjects followed-up for 9 years, with extensive questionnaires on respiratory symptoms, clinical evaluations and information on environmental exposures. This thesis replicates previous effects on asthma of polymorphisms in TNFA and NPSR1 genes. In addition, interactions have been established between TNFA and obesity, NQO1 and air-pollution, and NPSR1 and age at onset of asthma. The approach based on genome-wide analysis of DNA pools identified the SGK493 region being associated with atopy. This thesis contributes to the understanding of the etiology of asthma through the identification and replication of genetic associations and gene-environment interactions.

gene-environment interaction

environment

genetic polymorphisms

genetic

epidemiology

bronchial hyperreactivity

atopy

asthma

NQO1 - NAD(P)H:quinine oxidoreductase

NPSR1 - Neuropeptide S-Receptor 1

TNFA - Tumor Necrosis Factor Alpha

estrés oxidatiu

edat d'inici d'asma

diòxid de nitrogen

contaminació

obesitat

interaccions gen-ambient

exposicions ambientals

polimorfismes genètics

genètica

epidemiologia

hiperreactivitat bronquial

atòpia

asma

obesity

air-pollution

nitrogen dioxide

age at onset of asthma

oxidative stress

TNFA - Tumor Necrosis Factor Alpha

NPSR1 - Neuropeptide S-Receptor 1

NQO1 - NAD(P)H:quinine oxidoreductase

57

Tumour necrosis factor alpha induces rapid reduction in AMPA receptor-mediated calcium entry in motor neurones by increasing cell surface expression of the GluR2 subunit: relevance to neurodegeneration

Rainey-Smith, S.R., Andersson, D.A., Williams, R.J., Rattray, Marcus

January 2010

No / The alpha-amino-3-hydroxyl-5-methyl-4-isoxazole-propionate receptor (AMPAR) subunit GluR2, which regulates excitotoxicity and the inflammatory cytokine tumour necrosis factor alpha (TNFalpha) have both been implicated in motor neurone vulnerability in amyotrophic lateral sclerosis/motor neurone disease. TNFalpha has been reported to increase cell surface expression of AMPAR subunits to increase synaptic strength and enhance excitotoxicity, but whether this mechanism occurs in motor neurones is unknown. We used primary cultures of mouse motor neurones and cortical neurones to examine the interaction between TNFalpha receptor activation, GluR2 availability, AMPAR-mediated calcium entry and susceptibility to excitotoxicity. Short exposure to a physiologically relevant concentration of TNFalpha (10 ng/mL, 15 min) caused a marked redistribution of both GluR1 and GluR2 to the cell surface as determined by cell surface biotinylation and immunofluorescence. Using fura-2-acetoxymethyl ester microfluorimetry, we showed that exposure to TNFalpha caused a rapid reduction in the peak amplitude of AMPA-mediated calcium entry in a PI3-kinase and p38 kinase-dependent manner, consistent with increased insertion of GluR2-containing AMPAR into the plasma membrane. This resulted in a protection of motor neurones against kainate-induced cell death. Our data therefore, suggest that TNFalpha acts primarily as a physiological regulator of synaptic activity in motor neurones rather than a pathological drive in amyotrophic lateral sclerosis.

Animals

Biotinylation

Blotting

Western

Calcium

Metabolism

Calcium signaling

Drug effects

Cell survival

Drug effects

Cells

Cultured

Excitatory amino acid agonists

Toxicity

Female

Fluorescent antibody technique

Kainic acid

Antagonists & inhibitors

Toxicity

Mice

Motor neurons

Drug effects

Nerve degeneration

Pathology

Neuroprotective agents

Phosphatidylinositol 3-Kinases

Pregnancy

Receptors

AMPA

Antagonists & inhibitors

Biosynthesis

Genetics

Receptors

Cell surface

Biosynthesis

Receptors

Tumor necrosis factor

Drug effects

Spectrometry

Fluorescence

Tumor necrosis factor-alpha

Pharmacology

p38 mitogen-activated protein kinases

REF 2014

Le rôle de l’inflammation dans le développement des complications neurologiques associées à l’insuffisance hépatique aiguë chez la souris

Chastre, Anne

12 1900

L’insuffisance hépatique aiguë (IHA) se caractérise par la perte soudaine de la fonction hépatique résultant de la nécrose massive des hépatocytes en l’absence de pathologie hépatique préexistante. L’IHA s’accompagne de perturbations métaboliques et immunologiques qui peuvent entraîner l’apparition de complications périphériques et cérébrales telles qu’un syndrome de réponse inflammatoire systémique (SIRS), une encéphalopathie hépatique (EH), un œdème cérébral, une augmentation de la pression intracrânienne, et la mort par herniation du tronc cérébral. Les infections sont une complication fréquente de l’IHA et elles sont associées à un risque accru de développer un SIRS et une aggravation subséquente de l’EH avec un taux de mortalité augmenté. L’ammoniaque joue un rôle majeur dans les mécanismes physiopathologiques qui mènent au développement de l’EH et de l’œdème cérébral, et des études récentes suggèrent que les cytokines pro-inflammatoires sont également impliquées. Le but de cette thèse est d’étudier le rôle des cytokines pro-inflammatoires circulantes et cérébrales dans le développement de l’EH et de l’œdème cérébral lors d’IHA. Dans l’article 1, nous démontrons que l’inhibition périphérique du facteur de nécrose tumorale-α (TNF-α) par l’etanercept retarde la progression de l’EH en diminuant le dommage hépatocellulaire, réduisant l’inflammation périphérique et centrale ainsi que le stress oxydatif/nitrosatif hépatique et cérébral associé chez la souris avec une IHA induite par l’azoxyméthane (AOM). Ces résultats démontrent un rôle important du TNF-α dans la physiopathologie de l’EH lors d’IHA d’origine toxique et suggèrent que l’etanercept pourrait constituer une approche thérapeutique dans la prise en charge des patients en attente de transplantation hépatique. Dans l’article 2, nous simulons la présence d’une infection chez la souris avec une IHA induite par l’AOM pour mettre en évidence une éventuelle augmentation de la réponse inflammatoire. Nous démontrons que l’endotoxémie induite par le lipopolysaccharide (LPS) précipite la survenue du coma et aggrave la pathologie hépatique. Les cytokines pro-inflammatoires systémiques et cérébrales sont augmentées de façon synergique par le LPS lors d’IHA et résultent en une activation accrue de la métalloprotéinase matricielle-9 cérébrale qui s’accompagne d’une extravasation d’immunoglobulines G (IgG) dans le parenchyme cérébral. Ces résultats démontrent une augmentation majeure de la perméabilité de la barrière hémato-encéphalique (BHE) qui contribue à la pathogenèse de l’EH lors d’IHA en condition infectieuse. Les résultats de l’article 3 démontrent que l’augmentation de la perméabilité de la BHE lors d’IHA induite par l’AOM en condition non infectieuse ne résulte pas de l’altération de l’expression des protéines constitutives de la BHE. Dans l’article 4, nous démontrons que l’exposition d’astrocytes en culture à des concentrations physiopathologiques d’ammoniaque ou d’interleukine-1β résulte en l’altération de gènes astrocytaires impliqués dans la régulation du volume cellulaire et dans le stress oxydatif/nitrosatif. Un effet additif est observé dans le cas d’un traitement combiné au niveau des gènes astrocytaires impliqués dans le stress oxydatif/nitrosatif. L’ensemble des résultats de cette thèse démontre un rôle important de l’inflammation périphérique et cérébrale dans la survenue des complications neurologiques lors d’IHA et une meilleure compréhension des mécanismes physiopathologiques impliqués pourrait contribuer à la mise en place de stratégies thérapeutiques chez les patients atteints d’IHA en attente de transplantation. / Acute liver failure (ALF) is the clinical manifestation of an abrupt loss of hepatic function resuting from a massive hepatocyte necrosis in a patient with no preexisting liver disease. ALF is associated with metabolic and immunological disturbances that may lead to peripheral and cerebral complications such as systemic inflammatory response syndrome (SIRS), hepatic encephalopathy (HE), brain edema, increased intracranial pressure (ICP) and ultimately death by cerebral herniation. ALF is frequently complicated by infections, which are known to increase the risk of developing a SIRS with a subsequent worsening of HE and higher mortality rates. Ammonia plays a pivotal role in the pathophysiological mechanisms leading to HE and brain edema, and recent studies suggest that pro-inflammatory cytokines may also be involved. The aim of this thesis is therefore to investigate the role of circulating and cerebral pro-inflammatory cytokines in the setting of HE and brain edema during ALF. In article No. 1, we demonstrated that peripheral inhibition of tumor necrosis factor-alpha (TNF-α) by etanercept delays the progression of HE by reducing hepatocellular damage, decreasing peripheral and cerebral inflammation as well as associated oxidative/nitrosatif stress in mice with ALF induced by azoxymethane (AOM). These findings demonstrate an important role of TNF-α in the pathophysiology of HE during toxic liver injury and suggest that etanercept may provide a therapeutic approach in the management of patient awaiting liver transplantation. In article No. 2, we mimicked infection in mice with AOM-induced ALF in order to better understand the effects of an increased inflammatory response. We demonstrated that endotoxemia induced by lipopolysaccharide (LPS) precipitates the onset of coma and worsens the liver pathology. Peripheral and brain pro-inflammatory cytokines are synergistically raised by LPS during ALF and result in a large increase in cerebral matrix metalloprotease-9 (MMP-9) activity that was associated with immunoglobulin G (IgG) extravasation in the brain parenchyma. These results demonstrate a major increase of blood-brain barrier (BBB) permeability that contributes to the pathogenesis of HE during ALF with superimposed infection. Results from article No. 3 demonstrate that increase of BBB permeability during AOM-induced ALF without superimposed infection is not due to alteration of BBB constitutive proteins. In article No. 4, we demonstrated that exposure of cultured astrocytes to pathophysiological concentrations of ammonia or interleukin-1β results in an alteration of the expression of astrocytic genes implicated in cell volume regulation and oxidative/nitrosative stress. An additive effect on astrocytic genes implicated in oxidative/nitrosative was made evident in case of co-treatment. Taken together, results of the present thesis demonstrate a major role of peripheral and cerebral inflammation in the onset of neurological complications during ALF and a better understanding of the pathophysiological mechanisms implicated may contribute to new therapeutic strategies for ALF patients awaiting transplantation.

Encéphalopathie hépatique

Hepatic encephalopahy

Insuffisance hépatique aiguë

Acute liver failure

Azoxyméthane

Azoxymethane

Astrocytes

Astrocytes

Ammoniaque

Ammonia

Cytokines pro-inflammatoires

Pro-inflammatory cytokines

Neuroinflammation

Neuroinflammation

Facteur de nécrose tumorale-alpha

Tumor necrosis factor-alpha

Infection

Barrière hémato-encéphalique

Blood-brain barrier

Mediadores inflamatórios e metabólicos em pacientes com miocardiopatia dilatada idiopática e chagásica: correlação com disfunção autonômica / Metabolic and inflammatory mediators in patients with idiopathic dilated cardiomyopathy and Chagas\' disease: correlation with autonomic dysfunction

Dabarian, André Luiz

14 December 2017

Alterações metabólicas, inflamatórias e do sistema nervoso autônomo estão presentes em pacientes com insuficiência cardíaca. No entanto, não há até o momento, consenso de que tais alterações são decorrentes da disfunção ventricular ou da síndrome de insuficiência cardíaca. Objetivo: Avaliacão do metabolismo e atividade inflamatória em pacientes com miocardiopatia dilatada chagásica e idiopática e sua correlação com medidas de funcão do sistema nervoso autônomo. Casuística: Foram avaliados 46 pacientes divididos em três grupos: pacientes com miocardiopatia dilatada idiopática, chagásica e controle, pareados entre si de acordo com sexo e idade e índice de massa corpórea. Critérios de inclusão: miocardiopatia chagásica com sorologia positiva em dois métodos diferentes (imunofluorescência indireta e ELISA) e miocardiopatia dilatada idiopática com idade superior a 18 anos; ambos os sexos; Índice de massa corporal (IMC) entre 18,5 e 25 kg/m2 e fração de ejeção < 40% pelo método de Simpson ao ecocardiograma. Metodologia: Todos pacientes foram submetidos a medidas antropométricas: índice de massa corporal e medida da porcentagem de gordura corporal através de bioimpedância. Coletado sangue para dosagens sanguíneas de leptina, adiponectina, interleucina-6, fator de necrose tumoral, glicose, insulina, colesterol total, HDL-Colesterol, LDL-Colesterol e triglicerídeos após jejum de 12 horas e realizados: Holter de 24 horas para avaliação da função autonômica, ecocardiograma transtorácico bidimensional complementado com modo-M, Doppler pulsátil, tecidual e colorido. Resultados: Não houve diferenças entre os grupos com relação a dosagem de glicemia, colesterol total, LDL-colesterol, HDL-colesterol e triglicerídeos. Com relação à leptina e adiponectina e o índice HOMA-IR, não houve diferença entre os grupos. As dosagens de insulina foram menores no grupo chagásico em comparação ao grupo controle e de idiopático (5,4; 8,0; 9,9) respectivamente (p = 0,007). As dosagens de interleucina-6 e fator de necrose tumoral-alfa foram maiores no grupo chagásico em relação aos outros grupos. A insulina correlacionou positivamente no grupo chagásico com leptina (r = 0,579; p = 0,024) e sistema nervoso autônomo ( atividade simpática) BF/AF ( r = 0,562; p = 0,029) e BF (r = 0,562; p = 0,029) e negativamente com adiponectina (r = -0,603; p = 0,017). Na análise multivariada, apenas a adiponectina foi significante. A adição de uma unidade de adiponectina reduziu a média de insulina em 0,332. Conclusões: Os níveis de insulina foram menores nos pacientes com miocardiopatia chagásica em comparação aos pacientes com miocardiopatia dilatada idiopática e controle. Os níveis das citocinas inflamatórias (TNF-alfa e interleucina-6) foram maiores nos pacientes com miocardiopatia chagásica em comparação aos pacientes com miocardiopatia dilatada idiopática e controle. A insulina correlacionou negativamente no grupo chagásico com adiponectina / Metabolic, inflammatory and autonomic nervous system changes are present in patients with heart failure. However, there is so far, consensus that these changes are due to ventricular dysfunction or heart failure syndrome. Objective: Evaluation of metabolism and inflammatory activity in patients with Chagas\' disease and idiopathic dilated cardiomyopathy and its correlation with user function measures the autonomic nervous system. Patients: A total of 46 patients divided into three groups: patients with idiopathic dilated cardiomyopathy, Chagas and control, matched each other according to sex and age and body mass index. Inclusion criteria: serology for Chagas\' disease in two different methods (indirect immunofluorescence and ELISA); idiopathic dilated cardiomyopathy; older than 18 years; both sexes; Body mass index (BMI), ie between 18.5 and 25 kg / m2 and ejection fraction < 40% by Simpson method by echocardiography. Methods: All patients underwent anthropometric measurements: body mass index and measure the percentage of body fat by bioimpedance. Blood was collected for blood leptin dosages, adiponectin, interleukin-6, tumor necrosis factor, glucose, insulin, total cholesterol, HDLcholesterol, LDL-cholesterol and triglyceride levels after fasting for 12 hours and performed: 24 hours for evaluation Holter autonomic function, two-dimensional transthoracic echocardiography complemented by M-mode, pulsed Doppler, tissue and colorful. Results: There were no differences between groups with respect to blood glucose levels, total cholesterol, LDL-cholesterol, HDLcholesterol and triglycerides. With respect to leptin and adiponectin and HOMAIR, there was no difference between groups. Insulin doses were lower in the chagasic group compared to the control group and Idiopathic: 5.4; 8.0; 9.9, respectively (p = 0.007). Dosages of interleukin-6 and tumor necrosis factoralpha were higher in the chagasic group compared to other groups. Insulin positively correlated in the chagasic group with leptin (r = 0.579; p = 0.024) and autonomic nervous system (sympathetic activity) LF / HF (r = 0.562; p = 0.029) and BF (r = 0.562; p = 0.029) and negatively with adiponectin (r = -0.603; p = 0.017). In multivariate analysis, only adiponectin was significant. The addition of an adiponectin unit reduced the average insulin 0.332. Conclusions: Insulin levels were lower in patients with Chagas\' heart disease compared to patients with idiopathic dilated cardiomyopathy and control. The levels of inflammatory cytokines (TNF-alpha and interleukin-6) were higher in patients with Chagas\' heart disease compared to patients with idiopathic dilated cardiomyopathy and control. Insulin negatively correlated with adiponectin in the chagasic group

Adiponectin

Adiponectina

Cardiomiopatia chagásica

Cardiomiopatia idiopática

Chagas cardiomyopathy

Chagas disease

Doença de Chagas

Fator de necrose tumoral alfa

Idiopathic cardiomyopathy

Inflamação

Inflammation

Insulin resistance

Insulin

Insulina

Interleucina-6

Interleukin-6

Lepitina

Leptin

Metabolism

Metabolismo

Resistência a insulina

Sistema nervoso autônomo

Qualidade de vida, qualidade de sono, transporte mucociliar, citocinas inflamatórias e endotipos na rinite alérgica e na rinossinusite crônica / Quality of life, sleep quality, mucociliary transport, inflammatory cytokines and endotypes in allergic rhinitis and chronic rhinosinusitis

Fonseca, Luciana Mazoti Lopes da

05 December 2018

Introdução: A rinite alérgica (RA) e a rinossinusite crônica (RSC) são doenças inflamatórias nasais com prevalência alta e crescente. Estima-se que 15,5% dos norte-americanos tenham RSC, e estudo recente encontrou prevalência de 5,51% na cidade de São Paulo, enquanto a RA acomete entre 10 e 20% da população mundial. Apesar de terem mecanismos fisiopatológicos distintos, em ambas, há recrutamento de células de defesa, principalmente linfócitos T, e produção de citocinas inflamatórias. Esses mediadores variam não apenas entre as doenças, mas também entre as populações acometidas, e seu conhecimento é importante para o diagnóstico correto e direcionamento da terapia escolhida. Objetivos: Mapear os mediadores inflamatórios presentes no lavado nasal e no condensado do ar exalado na RSC e na RA, avaliando possíveis biomarcadores da doença, e analisar o endotipo inflamatório dos pacientes estudados. Além disso, avaliar a qualidade de vida, o nível de obstrução nasal, a qualidade do sono dos pacientes afetados, o transporte mucociliar e coletar material para análise de pH, contagem de células totais e seu diferencial. Pacientes e métodos: Estudo exploratório prospectivo em corte transversal, sendo os pacientes divididos em quatro grupos: 1) Grupocontrole com pacientes sem queixas; 2) Pacientes com RA com prick test positivo; 3) Pacientes com RSC com polipose; e 4) Pacientes com RSC sem polipose. Todos os pacientes responderam a quatro questionários: 20-Item Sino-Nasal Outcome Test (SNOT-20p), Nasal Obstruction Symptom Evaluation (NOSE), o Índice de Qualidade do Sono de Pittsburgh (Pittsburgh Sleep Quality Index - PSQI-BR) e o questionário para triagem e diagnóstico da asma da European Community Respiratory Health Survey (ECRHS). Foi realizado exame físico, incluindo endoscopia nasal (escore de Lund- Kennedy modificado) e, nos pacientes com RSC, avaliação da tomografia computadorizada (TC) de face (escore de Lund-Mackay). Foi também avaliado o transporte mucociliar por meio do teste da sacarina. Coletou-se o condensado do ar exalado para análise do pH e lavado nasal para avaliação do pH, da presença de citocinas e da celularidade (total e diferencial). Foi avaliada a presença de IL-4, IL-5, IL-8, IL-17A, IL-22, TNF-Alfa e IFN-Gama no lavado nasal e IL-5, IL-17A, IL-22 e IFN-Gama no condensado do ar exalado. Resultados: Os pacientes com RSC apresentaram escores significativamente piores nos questionários de obstrução nasal (NOSE, p < 0,01) e qualidade de vida (SNOT-20p, p < 0,01) quando comparados aos controles, e tanto os pacientes com RSC quanto com RA apresentaram pior qualidade do sono (PSQI-BR, p < 0,01). O escore de extensão de Lund- Mackay foi mais elevado nos pacientes com RSC com polipose (p < 0,02). O teste da sacarina apresentou tempo mais prolongado no grupo RSC com polipose (p < 0,01). O pH do condensado do ar exalado não diferiu entre os grupos. O grupo RSC com polipose apresentou tanto diferença do pH (p < 0,01) quanto da contagem de células totais do lavado nasal (p < 0,01) quando comparado ao grupo-controle, porém sem diferença na contagem diferencial. IFN? do condensado foi mais elevado no grupo RA em comparação ao grupo C (p=0,05), enquanto IL-5 foi mais alto no grupo RSC com polipose quando comparado ao grupo RSC sem polipose (p=0,02). Os pacientes foram, então, divididos em endotipos, segundo os grupos descritos por Tomassen et al., sendo que endotipos são os subtipos da doença definidos funcionalmente e patologicamente por mecanismos moleculares distintos. Conclusão: Pacientes com RSC apresentaram escores piores nos questionários de qualidade de vida (SNOT-20p e NOSE), o que, em parte, poderia ser atribuído à pior qualidade do sono apresentada tanto por estes pacientes quanto pelos portadores de RA. O teste da sacarina evidenciou pior transporte mucociliar nos pacientes com RSC com polipose. Não houve diferença do pH do condensado do ar exalado, sugerindo que, apesar de interessante na avaliação das vias aéreas inferiores, este pode não ser um bom teste para análise das vias aéreas superiores. Foram encontradas alterações significantes tanto do pH quanto da contagem de células totais do lavado nasal do grupo com RSC com polipose, sem, no entanto, haver diferença na contagem diferencial. Dos 17 pacientes com RSC com perfil completo de citocinas, 12 se encaixam em endotipos já descritos, sendo que, dos cinco restantes, dois apresentam o mesmo perfil, podendo indicar um novo subgrupo / Introduction: Allergic rhinitis (AR) and chronic rhinosinusitis (CRS) are nasal inflammatory diseases with high and increasing prevalence. It is estimated that 15.5% of Americans have CRS, and a recent study found a prevalence of 5.51% in the city of São Paulo, while AR affects between 10 and 20% of the world population. Although they have distinct pathophysiological mechanisms, in both there is recruitment of defense cells, mainly T lymphocytes, and production of inflammatory cytokines. These mediators vary not only between diseases but also among affected populations, and their knowledge is important for the correct diagnosis and targeting of the therapy chosen. Objectives: To map the inflammatory mediators present in the nasal wash and the exhaled breath condensate in the CRS and AR, evaluating possible biomarkers of this diseases, and to analyze the inflammatory endotype of the patients studied. In addition, assess quality of life, level of nasal obstruction, sleep quality of affected patients, mucociliary transport and collect samples for pH analysis, total cell count and its differential. Patients and Methods: Prospective cross-sectional exploratory study, divided into four groups: 1) Control group with patients without complaints 2) Patients with AR with prick test positive 3) Patients with CRS with polyps 4) Patients with CRS without polyps. All patients responded to four questionnaires: 20-Item Sino-Nasal Outcome Test (SNOT-20p), Nasal Obstruction Symptom Evaluation (NOSE), Pittsburgh Sleep Quality Index (PSQI-BR) and European Community Respiratory Health Survey (ECRHS) questionnaire for screening and diagnosis of asthma. A physical examination was performed, including nasal endoscopy (modified Lund-Kennedy score) and, in patients with CRS, a computerized tomography (Lund-Mackay score) evaluation. The mucociliary transport was also evaluated through the saccharin test. The exhaled breath condensate was collected for pH analysis and the nasal wash for evaluation of pH, cytokines and cellularity (total and differential). The presence of IL-4, IL-5, IL-17, IL-17A, IL-22, TNF-Alfa and IFN-Gama in the nasal wash and IL-5, IL-17A, IL-22 and IFN-Gama in the exhaled breath condensate. Results: Patients with CRS had significantly worse scores in the nasal obstruction questionnaire (NOSE, p < 0.01) and quality of life questionnaire (SNOT-20p, p < 0.01) when compared to controls, and both patients with CRS and AR presented worse sleep quality (PSQI-BR, p < 0.01). The Lund-Mackay extension score was higher in patients with CRS with polyps (p < 0.02). The saccharin test showed longer time in the CSR group with polyps (p < 0.01). The pH of the exhaled breath condensate did not differ between groups. The CRS with polyps group presented both pH difference (p < 0.01) and higher total nasal wash cell count (p < 0.01) when compared to the control group, but with no difference in the differential count (p = 0.05), while IL-5 was higher in the CRS group with polyps when compared to the RSC without polyps group (p = 0.02). Patients were then divided into endotypes according to the groups described by Tomassen et al, Endotypes are the subtypes of the disease defined functionally and pathologically by distinct molecular mechanisms. Conclusions: Patients with CRS presented worse scores on quality of life questionnaires (SNOT-20p and NOSE), which could be attributed in part to the poorer quality of sleep presented by both patients with CRS and AR. The saccharin test evidenced worse mucociliary transport in patients with CRS with polyps when compared with control group. There was no difference in the pH of the exhaled breath condensate, suggesting that, although interesting in the evaluation of the lower airways, this may not be a good test for analyzing the upper airways. Significant alterations were found in both pH and total nasal wash cell count in the CSR group with polyposis, but there was no difference in the differential count. Of the 17 patients with CRS with complete cytokine profile, 12 fit into already described endotypes, and of the remaining five, two have the same profile, which may indicate a new subgroup

Fator de necrose tumoral alfa

Interferon gama

Interferon gamma

Interleucina-17

Interleucina-22

Interleucina-4

Interleucina-5

Interleucina-8

Interleukin-17

Interleukin-22

Interleukin-4

Interleukin-5

Interleukin-8

Nasal obstruction

Obstrução nasal

Qualidade de vida

Quality of life

Rhinitis

Rinite

Sinusite

Sinusitis

Sleep

Sono

Tumor necrosis factor alpha

Análise morfométrica e molecular da alveolite induzida em ratos com diferentes modalidades de tratamento / Molecular and morphometric analysis of induced dry socket in mice with different treatment conditions

Cardoso, Camila Lopes

25 March 2009

A alveolite é uma complicação pós-operatória de carácter inflamatório que acomete alvéolos de dentes recém-extraídos. A incidência dessa complicação varia de 1 a 4% e pode chegar a 30%. O objetivo deste estudo foi analisar os mecanismos biológicos envolvidos no processo de reparo de alvéolos intencionalmente infectados, em ratos; comparar diferentes modalidades de tratamento e correlacionar os resultados encontrados através de duas análises (microscópica e molecular). Foram utilizados 84 ratos, divididos nos grupos: I: alvéolo não infectado; II: alvéolo infectado sem nenhum tratamento; III: alvéolo infectado tratado com irrigação de solução de iodeto de sódio a 2% e peróxido de hidrogênio a 3% na proporção de 1:1; e IV: alvéolo infectado submetido à curetagem, irrigação com soro fisiológico e preenchimento com uma pasta à base de metronidazol. Os animais foram eutanasiados aos 6, 15 e 28 dias pós-operatório. Foi realizada a análise quantitativa da expressão de genes envolvidos no processo de reparo [colágeno tipo I (COL-I), fator de crescimento do endotélio vascular (VEGF), osteocalcina (OCN), fosfatase alcalina (ALP), runt-related transcription factor 2 (RUNX2) e fator de necrose tumoral alfa (TNF-\'alfa\')], através da RealTimePCR, correlacionando sua expressão com as características microscópicas observadas qualitativa e quantitativamente. Com base nos resultados da análise microscópica e molecular, podemos concluir que os marcadores RUNX2, OCN e TNF-\'alfa\' podem ser usados como indicadores para avaliar a neoformação óssea e a quantidade de infiltrado inflamatório em alveolite. Os marcadores ALP e VEGF não representaram adequadamente o que se observou microscopicamente. Embora o tratamento da alveolite com a pasta à base de metronidazol promova maior densidade de neoformação óssea aos 28 dias, não há diferenças entre os tratamentos. / Dry socket is an inflammatory postoperative complication that undertakes sockets of recently extracted teeth. The incidence of such complication varies from 1 to 4% and might reach up to 30%. The objective of this study was to analyze the biological mechanisms involved in the repair process of intentionally infected sockets in mice; compare different treatment conditions and correlate the results of two different analysis (microscopic and molecular). 84 mice were used in this study, divided according the following groups: I: uninfected socket; II: infected socket without any treatment; III: infected socket treated with irrigation of 2% sodium iodide and 3% hydrogen peroxide solution at 1:1 proportion; and IV: infected socket submitted to curettage, physiological saline solution irrigation and fulfillment with metronidazole base paste. The animals were killed at a postoperative period of 6, 15 and 28 days. A quantitative analysis was performed using a RealTimePCR to evaluate the genes expression involved [Collagen Type I (COL-I), vascular endothelial growth factor (VEGF), osteocalcin (OCN), alkaline phosphatase (ALP), runt-related transcription factor 2 (RUNX2) and tumor necrosis factor-alpha (TNF-\'alpha\')], in the repair process, correlating its expression with the microscopic characteristics observed in both qualitative and quantitative manner. Based in the results of the microscopic and molecular analysis, it can be concluded that the RUNX2, OCN and TNF-\'alpha\' markers can be used as indicators to evaluate the dry socket bone neoformation and inflammatory infiltrate quantity. The ALP and VEGF markers did not represented appropriately what was observed microscopically. Although the dry socket treatment with metronidazole base paste promotes an increase in the bone neoformation density at 28 days, no difference was found among the treatments.

Alkaline phosphatase

Alvéolo seco

Cirurgia bucal

Colágeno tipo I

Collagen Type I

Dry socket

Fator de Necrose Tumoral alfa

Fosfatase alcalina

Hydrogen peroxide

Metronidazol. Iodeto de sódio

Metronidazole

Oral surgery

Osteocalcin

Osteocalcina

Peróxido de hidrogênio

Runt-related transcription factor 2

RUNX2

Sodium iodide

Tumor Necrosis Factor-alpha

Vascular Endothelial Growth Factor

Efeito da inflamação no peptídeo natriurético atrial (NT-proBNP) em pacientes com espondilite anquilosante ativa durante terapia anti-TNF / Effect of inflammation on atrial natriuretic peptide (NT-proBNP) levels in active ankylosing spondylitis patients receiving anti-TNF therapy

Moraes, Júlio César Bertacini de

21 October 2013

Introdução: O fragmento amino-terminal do pró-peptídeo natriurético do tipo B (NT-proBNP) é um forte marcador de doença cardiovascular com evidências recentes de que a inflamação também pode influenciar seus valores. A diferenciação dessa variável de confusão é de particular interesse nas doenças reumáticas. Objetivos: Avaliar o comportamento dos valores de NT-proBNP em pacientes com espondilite anquilosante (EA) pré e pós uso de bloqueadores de TNF para determinar a possível associação entre os valores de NT-proBNP e os parâmetros inflamatórios. Métodos: Quarenta e cinco pacientes consecutivos com EA sem evidência prévia ou atual de doença cardiovascular ou disfunção miocárdica sistólica e que eram elegíveis para terapia anti-TNF foram incluídos prospectivamente. Todos os pacientes receberam bloqueadores de TNF e foram avaliados para concentrações circulantes de NT-proBNP, parâmetros clínicos e laboratoriais de atividade de doença, fatores de risco cardiovasculares tradicionais e ecodopplercardiografia convencional e tecidual no momento da inclusão e após seis meses de tratamento. Resultados: No momento da inclusão, todos os pacientes tinham EA ativa, os valores de NT-proBNP tinham uma mediana de 36 (20-72) pg/mL e 11% dos valores estavam altos mesmo na ausência de alteração miocárdica sistólica. A análise de regressão linear múltipla revelou que esse peptídeo estava independentemente correlacionado com o VHS (p < 0,001), com a idade dos pacientes (p = 0,01) e com a pressão de pulso (p = 0,01) no momento da inclusão. Após seis meses, todos os parâmetros relacionados a doença de base melhoraram e os valores de NT-proBNP se reduziram significativamente [24 (16-47) pg/mL, p = 0,037] quando comparados com os valores do momento da inclusão. As mudanças nos valores de NT-proBNP correlacionaram-se positivamente com as mudanças nos valores do VHS (r = 0,41, p = 0.006). Os fatores de risco cardiovasculares avaliados permaneceram estáveis durante o seguimento. Conclusão: As elevações nos valores de NT-proBNP devem ser interpretadas com cuidado nos pacientes com EA ativa e sem evidência de doença cardiovascular. A redução no curto prazo dos valores de NT-proBNP nesses pacientes recebendo terapia anti-TNF parece refletir uma melhora do estado inflamatório / Introduction: N-terminal pro-brain natriuretic peptide (NT-proBNP) is a strong marker of cardiovascular disease with recent evidence that inflammation may also influence its levels; discrimination of this confounding variable is of particular interest in rheumatic diseases. Objectives: to evaluate NT-proBNP in ankylosing spondylitis (AS) patients pre- and post-TNF blocker to determine the possible association between NT-proBNP levels and inflammatory parameters. Methods: Forty-five consecutive AS patients without previous/current cardiovascular disease or systolic myocardial dysfunction, who were eligible to anti-TNF therapy, were prospectively enrolled. All patients received TNF blockers and they were evaluated for circulating NT-proBNP levels, clinical and laboratory parameters of disease activity, traditional cardiovascular risk factors, and conventional and tissue Doppler imaging echocardiography at baseline (BL) and six months after (6M) treatment. Results: At BL, all patients had active AS, NT-proBNP levels had a median of 36 (20-72) pg/mL and 11% were high in spite of no systolic alteration. Multiple linear regression analysis revealed that this peptide, at BL, was independently correlated with ESR (p < 0.001), age (p = 0.01) and pulse pressure (p = 0.01). After 6M, all disease parameters improved and NT-proBNP levels were significantly reduced [24 (16-47) pg/mL, p = 0.037] compared to BL. Changes in NT-proBNP were positively correlated with ESR changes (r = 0.41, p = 0.006). Cardiovascular risk factors remained stable during follow-up. Conclusion: our data suggests that elevations of NT-proBNP should be interpreted with caution in active AS patients with no other evidence of cardiovascular disease. The short-term reduction of NT-proBNP levels in these patients receiving anti-TNF therapy appears to reflect an improvement in inflammatory status

Adalimumab

Adalimumabe

Atrial natriuretic factor

Cardiovascular diseases

Doenças cardiovasculares

Espondilite anquilosante

Etanercept

Etanercepte

Fator natriurético atrial

Inflamação

Inflammation

Infliximab

Infliximabe

Proteína de fusão TNFR-Fc

Spondylitis ankylosing

TNFR-FC fusion protein

Concentrações de mediadores inflamatórios em crianças com idade inferior a três meses e infecção do trato respiratório inferior pelo vírus sincicial respiratório / Concentrations of inflammatory mediators in children less than three months of age with respiratory syncytial virus lower respiratory tract infection

Vieira, Renata Amato

20 August 2009

INTRODUÇÃO: A elevada frequência e morbimortalidade das infecções do trato respiratório inferior (ITRI) pelo vírus sincicial respiratório (VSR) na infância, além da ausência de estudos no Brasil que correlacionam evolutivamente a resposta inflamatória no epitélio respiratório e no sangue periférico à gravidade da doença respiratória pelo VSR, estimularam a realização desta pesquisa. OBJETIVOS: Avaliar se as concentrações dos mediadores inflamatórios (MI) (RANTES, sICAM-1, TNF-,IL -6 e IL-10) e suas razões na secreção nasofaríngea e no sangue de crianças com idade inferior a 3 meses e ITRI pelo VSR correlacionam-se à gravidade da doença; determinar a frequência dos grupos A e B do VSR nas crianças internadas na Unidade de Cuidados Intensivos Neonatal (UCINE) do Instituto da Criança do HCFMUSP; avaliar se há diferença na gravidade da doença respiratória pelo VSR entre as crianças internadas na UCINE e infectadas pelos grupos A e B do vírus; comparar as concentrações dos MI na secreção nasofaríngea e no sangue à admissão hospitalar ou por ocasião do diagnóstico de ITRI pelo VSR adquirida durante a internação, no terceiro e sétimo dias de evolução ou à alta (se antes do sétimo dia); comparar as concentrações dos MI na secreção nasofaríngea e no sangue dos pacientes à admissão, de acordo com grupos A e B do VSR; e descrever a evolução das concentrações de RANTES, sICAM-1, TNF-, IL-6 e IL-10 na secreção nasofaríngea e no sangue durante a doença pelo VSR. MÉTODOS: Foram incluídas no estudo prospectivo, de coorte, observacional, de julho de 2004 a dezembro de 2005, 30 crianças com idade inferior a três meses portadoras de ITRI pelo VSR internadas na UCINE. Foram medidas as concentrações dos MI na secreção nasofaríngea e no soro de todas as crianças à admissão no estudo, no terceiro e sétimo dias de evolução ou à alta hospitalar (se antes do sétimo dia) através da técnica ELISA sanduíche. Utilizamos para avaliar a gravidade da doença respiratória os seguintes marcadores clínicos: sistema de escore clínico modificado de De Boeck et al. (1997), tempos de oxigenoterapia e de ventilação mecânica e duração da internação. RESULTADOS: Houve correlação positiva significante entre a gravidade da doença pelo sistema de escore clínico modificado à admissão hospitalar e as concentrações na secreção nasofaríngea de sICAM-1 (r=0,401, p=0,028) e IL-10 (r=0,412, p=0,024) e de IL-6 no soro (r=0,469, p=0,009). Houve também correlação positiva significante entre as concentrações de IL-6 no soro e o tempo de oxigenoterapia (r=0,445, p=0,023) e a duração da internação (r=0,572, p=0,001). Das razões dos MI estudadas, a IL-10/IL-6 (primeiras amostras de soro), a IL-6/TNF- e a IL -6/IL-10 (segundas amostras de soro) foram associadas de forma mais consistente (p<0,001) à gravidade da ITRI pelo VSR. Não ocorreram óbitos entre as crianças envolvidas neste estudo. Os dois grupos de VSR causaram ITRI nas crianças internadas na UCINE, sendo que o grupo A foi o mais frequente (57%). No entanto, foram as crianças infectadas pelo grupo B do VSR as que evoluíram com maior morbidade (p<0,001). As medianas das concentrações de RANTES, sICAM-1 e IL-10 foram maiores nas três amostras de soro (p<0,001); enquanto as medianas das concentrações de IL-6 predominaram nas três amostras de secreção nasofaríngea (p<0,001). A mediana das concentrações de TNF- foi maior apenas nas primeiras amostras de secreção nasofaríngea (p<0,001). Houve diferença estatisticamente significante entre os dois grupos do VSR apenas em relação à mediana das concentrações de IL-10 na secreção nasofaríngea à admissão hospitalar, que foi mais elevada nas crianças com infecção pelo grupo B (p=0,039). As concentrações de RANTES, sICAM-1, IL-6 e IL-10 na secreção nasofaríngea e de TNF-,IL -6 e IL-10 no soro variaram, de forma significante, durante a evolução da ITRI pelo VSR. Os demais níveis de MI na secreção nasofaríngea e no soro mantiveram-se estáveis durante o período de estudo. CONCLUSÕES: Níveis de RANTES, sICAM-1, TNF-,IL -6 e IL-10 foram detectados em todas as amostras de secreção nasofaríngea e de soro das crianças com ITRI pelo VSR internadas na UCINE, confirmando o papel destes MI na patogênese da doença. Nossos resultados sugerem que as concentrações de sICAM-1 e IL-10 na secreção nasofaríngea e IL-6 no soro à admissão, bem como as razões IL-10/IL-6 (primeiras amostras de soro), IL-6/TNF- e IL -6/IL-10 (segundas amostras de soro), poderiam ser usadas como marcadores de gravidade da doença respiratória pelo VSR. Os níveis de IL-6 determinados no soro admissão também poderiam ser usados para predizer tempo de oxigenoterapia e duração da internação mais prolongados. Os grupos A e B do VSR cocircularam durante o período do estudo, com o grupo A sendo dominante nestes pacientes. Entretanto, foram as crianças infectadas com o grupo B do vírus que evoluíram com maior morbidade. As concentrações de IL-10 na secreção nasofaríngea à admissão hospitalar foram significantemente maiores nos pacientes com ITRI pelo grupo B do VSR. O tempo de evolução da doença pelo VSR foi significante para os níveis de RANTES, sICAM-1, IL-6 e IL-10 na secreção nasofaríngea e de TNF-,IL -6 e IL-10 no soro destas crianças. / INTRODUCTION: The high frequency and morbimortality of respiratory syncytial virus (RSV) lower respiratory tract infections (LRTI) in children, besides the lack of studies in Brazil that evolutionally correlate the inflammatory response in respiratory epithelium and in peripheral blood with RSV respiratory disease severity, have stimulated this research. OBJECTIVES: To assess whether the concentrations of inflammatory mediators (IM) (RANTES, sICAM-1, TNF- , IL-6 and IL-10) and their ratios in nasopharyngeal secretion and in blood of children less than 3 months of age and RSV LRTI correlate with disease severity; to determine the frequency of RSV groups A and B in children admitted to Unidade de Cuidados Intensivos Neonatal (UCINE) do Instituto da Criança do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo; to assess whether there is difference in RSV respiratory disease severity, according to RSV groups A and B; to compare the concentrations of IM in nasopharyngeal secretion and in blood at the time of hospital admission or by occasion of a diagnosis of RSV LRTI acquired during the stay, on third and seventh days of evolution or at the hospital discharge (should it had happened before the seventh day); to compare the concentrations of IM in nasopharyngeal secretion and in blood of patients at the hospital admission, according to RSV groups A and B; to describe the evolution of RANTES, sICAM-1, TNF-, IL-6 and IL-10 concentrations in nasopharyngeal secretion and in blood. METHODS: Thirty children less than 3 months of age with RSV LRTI admitted to UCINE were included in the prospective cohort observational study, from July 2004 to December 2005. The concentrations of IM were measured through the sandwich ELISA technique in nasopharyngeal secretion and in serum of all children at the hospital admission, and on the third and seventh days of evolution or at the hospital discharge (if before the seventh day). We used the following markers to assess the severity of respiratory illness: the modified clinical scoring system by De Boeck et al. (1997), the days of oxygen supplementation and of mechanical ventilation and duration of hospitalization. RESULTS: There was a significant positive correlation between severity of disease by modified clinical scoring system at the time of hospital admission and nasopharyngeal secretion sICAM-1 (r=0.401, p=0.028) and IL-10 concentrations (r=0.412, p=0.024) and serum IL-6 concentrations (r=0.469, p=0.009). There was also a significant positive correlation between serum IL-6 concentrations and the days of oxygen supplementation (r=0.572, p=0.001), as well as the days of hospital stay (r=0.572, p=0.001). Of IM ratios studied, IL-10/ IL-6 (first samples of serum), IL-6/TNF- and IL-6/IL-10 (second samples of serum) were associated to severity of RSV LRTI with greatest consistency (p<0.001). No fatal cases occurred among the children enrolled in this study. The two groups of RSV caused LRTI in 30 children less than 3 months of age hospitalized in UCINE, being group A the most frequent (57%). However, the children infected by RSV group B were the ones that evolved with a greater need of mechanical ventilation (p<0.001). Medians RANTES, sICAM-1 and IL-10 concentrations were greater in all the three serum samples (p<0.001); whereas medians IL-6 concentrations were predominant in the three nasopharyngeal secretion samples (p<0.001). Median TNF- concentration was greater only in the first nasopharyngeal secretion samples (p<0.001). There was a statistically significant difference between the two groups of RSV only relative to the median IL-10 concentrations on first nasopharyngeal secretion samples, which was more elevated in children infected by RSV group B (p=0.039). The nasopharyngeal secretion RANTES, sICAM-1, IL-6 and IL-10 and serum TNF- , IL-6 and IL-10 concentrations varied significantly during the evolution of RSV LRTI. The other nasopharyngeal secretion and serum IM levels remained stable during the period of study. CONCLUSIONS: Levels of RANTES, sICAM-1, TNF- , IL-6 and IL-10 were detected in all nasopharyngeal secretion and serum samples of children with RSV LRTI admitted to UCINE, therefore confirming the role of these IM in pathogenesis of illness. Our results suggest that nasopharyngeal secretion sICAM-1 and IL-10 and serum IL-6 concentrations determined at hospital admission, as well as the ratios IL-10/IL-6 (first samples of serum), IL-6/TNF- and IL-6/IL-10 (second samples of serum), could be used as markers of RSV respiratory disease severity. The levels of IL-6 found in serum at the time of hospital admission could also be used to predict prolonged oxygen supplementation and hospital stay. RSV groups A and B co-circulated during the period of the study, with group A being dominant in these patients. However, the children infected by RSV group B were the ones that evolved with a greater morbidity. Nasopharyngeal secretion IL-10 concentrations at admission were significantly greater in patients with RSV group B LRTI. The duration of RSV disease evolution was significant to nasopharyngeal secretion RANTES, sICAM-1, IL-6, IL-10 levels and to serum TNF- , IL-6 and IL-10 concentrations of these children.

Bronchiolitis

Bronquiolite

Chemokine CCL5

Children

Crianças

Fator de necrose tumoral alfa

Inflammation mediators

Intercellular adhesion molecule-1

Interleucina-10

Interleucina-6

Interleukin-10

Interleukin-6

Lung/secretion

Mediadores da inflamação

Molécula 1 de adesão intercelular

Pneumonia

Pneumonia

Pulmão/secreção

Quimiocina CCL5

Respiratory syncytial virus

Serum

Soro

Tumor necrosis factor-alpha

Vírus sincicial respiratório