Influência da poluição do ar na inflamação das vias aéreas e na atividade de doença de pacientes com lúpus eritematoso sistêmico juvenil / Influence of air pollution on airway inflammation and disease activity in childhood-systemic lupus erythematosus

Andressa Guariento Ferreira Alves

28 August 2018

Lúpus eritematoso sistêmico juvenil é uma doença inflamatória autoimune multifatorial com elevação de citocinas inflamatórias e com gravidade variável. Estudos observaram associação entre exposição a poluição do ar e aumento do número de internações hospitalares devido à exacerbação das doenças reumáticas pediátricas e aumento no risco de crianças portadoras de lúpus eritematoso sistêmico juvenil apresentarem atividade de doença moderada /grave após exposição a material particulado e dióxido de nitrogênio. Exposição à poluição do ar pode acarretar agravo agudo em doenças reumatológicas pediátricas, incluindo lúpus eritematoso sistêmico juvenil. Objetivos: Avaliar o efeito da exposição real a poluentes atmosféricos sobre biomarcadores inflamatórios em condensado do ar exalado e sobre a fração de monóxido de nitrogênio em ar exalado em pacientes com lúpus eritematoso sistêmico juvenil. Avaliar ainda, a correlação entre os biomarcadores inflamatórios no ar exalado e atividade da doença. Métodos: Estudo longitudinal de painel de medidas repetidas realizado em 108 visitas consecutivas de pacientes com diagnóstico de lúpus eritematoso sistêmico juvenil sem doenças respiratórias. Por 4 semanas consecutivas, medidas diárias individuais de dióxido de nitrogênio, material particulado fino, temperatura ambiental e humidade relativa do ar foram obtidos. Este ciclo foi repetido a cada 2,5 meses ao longo de um ano, além disso, citocinas do condensado do ar exalado (interleucinas 6, 8, 17 e fator de necrose tumoral-alfa), fração exalada de monóxido de nitrogênio e parâmetros de atividade de doença foram coletados semanalmente. Modelos específicos de equação estimada generalizada foram usadas para avaliar o impacto destes poluentes no risco de Systemic Lupus Erythematosus Disease Activity Index 2000 >= 8, citocinas no condensado do ar exalado e fração exalada de monóxido de nitrogênio, considerando o efeito fixo para medidas repetidas. Os modelos foram ajustados para provas de fase aguda, índice de massa corpórea, infecções, medicações e variáveis meteorológicas. Resultados: Efeito positivo nas medidas de desfechos foi observado para um aumento do intervalo interquartil do material particulado fino (18.12 ?g/m3). Um aumento do intervalo interquartil na média móvel de 7 dias no material particulado fino (lag0 to lag6) foi associado a um aumento de 0.1pg/ml (95%IC:0.01;0.19) e 0.9pg/ml (95%IC:0.05;0,12) nos níveis de interleucina 17 e fator de necrose tumoral-? do condensado do ar exalado, respectivamente. Também foi observado um aumento no risco de Systemic Lupus Erythematosus Disease Activity Index 2000 >= 8 de 1.47(95%CI:1.10;1.84) associado ao aumento da média móvel de material particulado fino. Em adição, um efeito a curto prazo na fração exalada de monóxido de nitrogênio foi evidenciado, medida móvel de 3 dias do material particulado fino foi associada com um aumento de 0.75ppb (95%IC:0.38;1.29) na fração exalada de monóxido de nitrogênio. Conclusão: Exposição a partículas finas inaláveis pode aumentar a inflamação das vias aéreas e posterior inflamação sistêmica nos pacientes com lúpus eritematoso sistêmico juvenil / Systemic lupus erythematosus is an inflammatory multisystem, autoimmune disease with elevated inflammatory interleukins levels. Exposure to air pollution may trigger pulmonary inflammation/systemic inflammation. Objective: The objective of this study was to investigate the association between daily individual exposure to air pollutants and airway inflammation and disease activity in childhood-onset systemic lupus erythematosus patients. A longitudinal panel study was carried out in 108 consecutive appointments with childhood-onset systemic lupus erythematosus patients without respiratory diseases. Methods: Over four consecutive weeks, daily individual measures of nitrogen dioxide, fine particulate matter, ambient temperature, and humidity were obtained. This cycle was repeated every 2.5 months along 1 year, and cytokines of exhaled breath condensate (interleukins 6, 8, 17 and tumoral necrose factor-alpha), fractional exhaled nitrogen monoxide, and disease activity parameters were collected weekly. Specific generalized estimation equation models were used to assess the impact of these pollutants on the risk of Systemic Lupus Erythematous Disease Activity Index 2000 >= 8, exhaled breath condensate cytokines, and fractional exhaled nitrogen monoxide, considering the fixed effects for repetitive measurements. The models were adjusted for inflammatory indicators, body mass index, infections, medication, and weather variables. Results: An interquartile range increase in fine particulate matter 4-day moving average (18.12ug/m3) was associated with an increase of 0.05 pg/ml (95% CI 0.01; 0.09, p = 0.03) and 0.04 pg/ml (95% CI 0.02; 0.06, p = 0.01) in interleukin 17 and tumoral necrosis factor-alpha exhaled breath condensate levels, respectively. Additionally, a short-term effect on fractional exhaled nitrogen monoxide was observed: the fine particulate matter 3-day moving average was associated with a 0.75 ppb increase (95% CI 0.38; 1.29, p = 0.03) in fractional exhaled nitrogen monoxide. Also, an increase of 1.47 (95% CI 1.10; 1.84) in the risk of Systemic Lupus Erythematous Disease Activity Index 2000 >= 8 was associated with fine particulate matter 7-day moving average. Conclusion: Exposure to inhalable fine particles increases airway inflammation/pulmonary and then systemic inflammation in childhood-onset systemic lupus erythematosus patients

Adolescente

Atividade de doença

Citocinas

Condensado do ar exalado

Criança

Dióxido de nitrogênio

Fator de necrose tumoral alfa

Lúpus eritematoso sistêmico

Material particulado

Poluição do ar

Adolescent

Air pollution

Child

Cytokines

Disease activity

Exhaled breath condensate

Nitrogen dioxide

Particulate matter

Systemic lupus erythematosus

Tumor necrosis factor-alpha

Etude des mécanismes de rupture de tolérance lymphocytaire au cours des déficits immunitaires primitifs de l'adulte avec manifesations auto-immunes / Study of lymphocyte tolerance breakdown in adults primary immunodeficiencies with autoimmunity

Guffroy, Aurélien

01 April 2019

L’association entre déficits immunitaires primitifs (DIPs) et manifestations auto-immunes peut sembler paradoxale lorsque l’on aborde les DIPs comme des défauts d’immunité opposés à l’autoimmunité vue comme excès d’immunité adaptative à l’encontre du soi. Néanmoins, loin de se résumer à un simple défaut d’une ou plusieurs composantes du système immunitaire qui prédispose aux infections par divers agents pathogènes, les DIPs sont fréquemment associés à une autoimmunité; parfois révélatrice. Ainsi, les données épidémiologiques issues de registres ou de larges séries de patients atteints de DIPs s’accordent sur une prévalence globale de 25 à 30% de complications auto-immunes (au premier rang desquelles figurent les cytopénies auto-immunes). Différentes hypothèses sont avancées pour rendre compte de l’auto-immunité dans les DIPs. On peut citer : 1°) une perturbation profonde de l’homéostasie lymphocytaire, en particulier dans les déficits immunitaires combinés sévères (CID) avec lymphopénies T et B ; 2°) des défauts intrinsèques des lymphocytes B permettant une rupture de tolérance précoce des LB auto réactifs ; 3°) un comportement aberrant des LT (défaut de maturation, excès d’activation) ; 4°) une absence de lymphocytes T ou de B régulateurs ; 5°) une production inappropriée de certaines cytokines proinflammatoires comme dans les interféronopathies. Ces hypothèses concernent surtout les DIPs pédiatriques sévères. Mon travail de thèse explore la rupture de tolérance immunitaire adaptative au cours des DIPs de l’adulte par différentes approches. Nous nous sommes en particulier attachés au plus fréquent, le DICV (Déficit Immunitaire Commun Variable), déficit immunitaire humoral pas toujours bien défini sur le plan génétique et physiopathologique qui constitue un défi thérapeutique lorsqu’il est compliqué d’une auto-immunité nécessitant un traitement immunosuppresseur. / The association between primary immune deficiency (PID) and autoimmunity may seem paradoxical when PID is considered only as an immune response defect against pathogens and autoimmunity only as an excess of immunity. Nevertheless, far from being simple immune defects increasing the risk of infections, DIPs are frequently associated with autoimmunity. Even more, autoimmunes manifestations can sometimes reveal a PID. Thus, epidemiological data from registers or large series of patients with PIDs agree on an overall prevalence of 25 to 30% of autoimmune complications (with auto-immune cytopenias as first causes). Several hypotheses have been proposed with different underlying mechanisms to explain the tolerance breakdown in PIDs. We can cite : 1°) a severe disturbance of lymphocyte homeostasis, for example in severe combined immunodeficiencies ; 2°) an impaired B-cell developpement with earlystage defects of tolerance ; 3°) a dysregulation of T cells (developpement or activation impairments) ; 4°) a dysfunction of T-reg (or B-reg) ; 5°) an excess of production of proinflammatory cytokines. These hypotheses are especially true for early-onset PIDs (in infancy). In this work (PhD), we explore the mechanisms of tolerance breakdown involved in adults PIDs. We use several approaches to describe the pathways leading to autoimmunity, focusing on the most common PID in adult : CVID (common variable immunodeficiency). This syndrome is not well defined on the genetic and physiopathological level. It is still a therapeutic challenge when complicated by autoimmunity (requiring immunosuppressive therapy).

Tolérance

Auto-immunité

Déficit immunitaire primitif

Lymphocyte B

Lymphocyte T

Génétique

WES

NGS

Cohortes

Cytopénies auto-immunes

PTI AHAI

Syndrome d’EVANS

Neutropénie

Tolerance

Autoimmunity

Primary immune deficiency

B lymphocytes

T lymphocytes

Whole Exome Sequencing

Next Generation Sequencing

Systemic lupus erythematosous (SLE)

EVANS syndrome

Neutropenia

Autoimmune cytopenia

571.96

616.97

Clinical and molecular characterisation of type I interferonopathies / Caractérisation clinique et moléculaire des interféronopathies de type I

Melki, Isabelle

29 November 2017

Les interférons de type I (IFN I) sont des cytokines antivirales aux propriétés puissantes. L’induction, la transmission et la résolution de la réponse immunitaire engendrée par les IFN I est minutieusement régulée. Le concept d’interféronopathie de type I, récemment individualisé par notre équipe, repose sur l’hypothèse que certaines pathologies seraient secondaires au déséquilibre de ces voies de signalisation complexes et à la sécrétion excessive et inappropriée d’IFN I. L’inhibition de celle-ci par des thérapeutiques ciblées permettrait de valider cette hypothèse, si les symptômes allégués s’amélioraient, voire disparaissaient. Ce travail de thèse s’est initialement concentré sur la caractérisation clinique et biologique des interféronopathies monogéniques et polygéniques, et secondairement sur l’identification moléculaire de nouvelles mutations du gène TMEM173 à l’origine de l’interféronopathie liée à STING, également appelée SAVI (STING associated vasculopathy with onset in infancy), syndrome auto-inflammatoire associant une atteinte sévère cutanée et pulmonaire. De nouvelles techniques ont permis la sélection de patients présentant une augmentation de l’IFN I en comparaison à des contrôles sains : la signature IFN I, qPCR de 6 gènes stimulés par l’IFN (IFN stimulated genes – ISGs) et le dosage d’IFN alpha sérique ou plasmatique par méthode du SIMOA (single molecule array) permettant la détection de molécules d’IFN de l’ordre du femtogramme (10-18g). Ces méthodes nous ont ainsi permis d’élargir le spectre clinique phénotypique des interféronopathies de type I, initialement considéré comme essentiellement neurologique. Les patients atteints du syndrome d’Aicardi-Goutières, première interféronopathie monogénique décrite, présentaient les signes suivants : dystonie, spasticité, décalage des acquisitions, calcifications intra-cérébrales et anomalies de la substance blanche. Cependant, l’utilisation systématique de nos méthodes de criblage associée à l’avènement des technologies de séquençage à haut débit (next generation sequencing – NGS) a permis de révéler un phénotype plus large, caractéristique des interféronopathies de type I : sur le plan cutané (engelures, vascularite nécrosante des extrémités, sclérodermie), pulmonaire (pneumopathie interstitielle isolée ou non), musculo-squelettique (arthralgies, arthrites, arthropathie de Jaccoud, myalgies et myosites), ophtalmologique (glaucome), néphrologique (néphropathies lupiques), gastro-entérologique (maladies inflammatoires chroniques intestinales précoces), associées à de l’auto-immunité ou un déficit immunitaire inconstants. Notre méthode de sélection nous a notamment permis d’identifier des patients présentant de manière variable des signes cardinaux de SAVI et une de trois nouvelles mutations activatrices dans une région spécifique du gène TMEM173 (codant pour STING). Ces mutations circonscrivent une région de la protéine à ce jour encore jamais impliquée dans le contrôle de la voie de l’IFN I. STING est une protéine du réticulum endoplasmique qui agit comme adaptateur cytosolique de senseurs intracellulaires d’ADN viral dans une voie de signalisation de l’IFN I. STING active TBK1 (TANK-binding kinase) et permet la transcription des IFN I par la phosphorylation d’IRF3. La Janus Kinase 1 (JAK1) et la tyrosine kinase 2 (TYK2) sont activées suite à la stimulation des récepteurs de l’IFN I et phosphorylent les facteurs de transcription STAT1 et STAT2, conduisant à l’expression de nombreux ISGs. Les analyses génétiques, de conformation tridimensionnelle, sur un modèle cellulaire in vitro (HEK293T) et ex vivo sur cellules mononuclées périphériques des patients nous ont ainsi permis de mettre en évidence pour ces mutations un caractère constitutionnellement activé, indépendant de la liaison au ligand cGAMP, mais transmettant ce signal à travers la voie d’aval par TBK1. (...) / Type I interferons (IFN I) are antiviral cytokines with potent properties. Hence, the induction, transmission and resolution of the immune response generated by IFN I is tightly regulated. The concept of the type I interferonopathies, recently formulated by our team, rests on the assumption that some diseases arise from a disturbance of this complex signalling pathway, leading to excessive and inappropriate IFN I secretion. On this basis, targeted therapeutics should improve or cure features of such type I interferonopathies, thereby providing a validation of the underlying hypothesis. This PhD project initially focused on the clinical and biological characterisation of monogenic and polygenic interferonopathies, and secondarily on the molecular identification of novel mutations in the gene TMEM173 causing the interferonopathy called STING associated vasculopathy with onset in infancy (SAVI), an auto-inflammatory syndrome with severe cutaneous and pulmonary features. Our selection of patients in comparison to healthy controls was made possible through the use of novel screening tools: IFN signature (qPCR of 6 IFN stimulated genes – ISGs), and measurement of IFN alpha protein levels in serum or plasma (SIMOA-single molecule array - enabling the detection of molecules of IFN in the femtogram [10-18g]) range. In this way, we have been able to expand the phenotypic spectrum of the interferonopathies, which was initially considered as primarily neurological. Patients with Aicardi-Goutières syndrome (AGS), the first described of the monogenic interferonopathies, exhibit dystonia, spasticity, developmental delay, intra-cranial calcifications and white matter abnormalities. However, the systematic use of our interferon screening assays, plus the advent of next-generation sequencing technology, has revealed a much broader set of features relevant to this novel disease grouping – involving the skin (chilblains, necrotising vasculitis, scleroderma), lungs (isolated lung interstitial disease or associated with other signs), musculoskeletal system (joint pain, arthritis, Jaccoud’s arthropathy, muscle pain and myositis), eyes (glaucoma), kidneys (lupus nephritis) and gastro-intestinal tract (early inflammatory bowel disease), as well features of autoimmunity and immunodeficiency. Using our screening assays enabled us to identify three patients variably exhibiting the core features of SAVI, all of whom were found to harbour distinct novel activating mutations in STING. These mutations highlight a protein domain not previously implicated in the control of IFN I signalling. STING is an endoplasmic reticulum protein, acting as a cytosolic adaptor of intracellular sensors of viral DNA in the type I IFN signalling pathway. STING activates TANK-binding kinase (TBK1), allowing transcription of IFN I through phosphorylation of IRF3. Janus kinase 1 (JAK1) and tyrosine kinase 2 (TYK2) are activated following stimulation of the IFN I receptor, leading to phosphorylation of the transcription factors STAT1 and STAT2 and the subsequent induction of a large number of ISGs. Genetic analysis, conformational studies, an in vitro cellular model (HEK293T) and ex vivo experimental data (using patient peripheral blood mononuclear cells - PBMCs) enabled us to confirm the constitutive activating nature of these variants, and show that this activation did not require binding with cGAMP, but was dependent on signalling through TBK1. Ruxolitinib, a JAK1/2 inhibitor, could antagonise this constitutive activation ex vivo. These results indicate a promising therapeutic approach in such patients, and more widely in the monogenic, and perhaps even, polygenic, interferonopathy context.

Interféron de type I

Lupus systémique juvénile

Dermatomyosite juvenile

TMEM173

STING

MDA5

Type I interferon

Autoinflammatory diseases

Autoimmune diseases

Juvenile systemic lupus erythematosus

Juvenile dermatomyositis

TMEM173

STING

MDA5

571.96

Dissecting the Genetic Basis of Systemic Lupus Erythematosus : The Pursuit of Functional Variants

Delgado Vega, Angélica María

January 2013

Systemic lupus erythematosus (SLE) is a chronic and systemic autoimmune disease that primarily affects women during the childbearing years. SLE is characterized by the production of autoantibodies against nucleic acids and their interacting proteins. The exact molecular mechanisms leading to the breakdown of self-tolerance remain to a large extent unknown, but it is well established that they are influenced by both non-genetic (i.e. environmental and hormonal) and genetic factors. SLE is a complex, polygenic disease. Several susceptibility variants have been identified in SLE. However, the functional role in disease pathogenesis for the majority of them remains largely unknown. This thesis includes case-control association studies where the role of the genes TNFSF4 (Paper I), STAT4 (Paper II), CD226 (Paper III), and BLK (Papers IV and V) in the susceptibility of developing SLE was investigated. The primary focus was on the identification of the functional variants underlying the association. For each of these genes, fine mapping was performed using single nucleotide polymorphisms (SNPs), the linkage disequilibrium (LD) was characterized, and the association was narrowed down to specific haplotypes by means of several different statistical genetic strategies. Candidate variants were prioritized for further functional analysis on the basis of their potential effect on the gene function, their association, and/or biological plausibility. In Paper I, the association of TNFSF4 with SLE was validated and attributed to a risk haplotype tagged by SNPs rs1234317-T and rs12039904-T. Paper II provides evidence supporting the presence of at least two independent genetic effects within the STAT4 gene represented by rs3821236-A and rs7574865-A, which correlated with increased levels of gene expression. In Paper III, a functional allele in CD226 (rs727088-C) was identified, which was responsible for decreased levels in both mRNA and protein expression. In Paper IV, two independent genetic effects in the BLK gene were demonstrated. The first one comprised multiple regulatory variants in high LD that were enriched for NFκB and IRF4 binding sites and correlated with low BLK mRNA levels. The second was a low-frequency missense substitution (Ala71Thr) that decreased the BLK protein half-life. In Paper V, a genetic epistatic interaction between BANK1 rs10516487 (GG) and BLK rs2736340 (TT+TC) was demonstrated. Additional molecular analyses established that these molecules interact physically.   These studies have contributed to the dissection of the genetic architecture of SLE. They highlight the allelic heterogeneity of the disease and provide functional links to the associated variants, which has significantly aided in the understanding of SLE disease pathogenesis.

Systemic Lupus Erythematosus

SLE

Genetic Mapping

Association Studies

Functional Variants

TNFSF4

STAT4

IRF5

CD226

BLK

BANK1

Systemisk Lupus Erythematosus

SLE

Genetik

Genetisk Association

Funktionella Varianter

TNFSF4

STAT4

IRF5

CD226

BLK

BANK1

Lupus Eritematoso Sistémico

LES

Estudios de Asociación Genética

Variantes Funcionales

TNFSF4

STAT4

IRF5

CD226

BLK

BANK1

Avaliação da adesão à terapêutica medicamentosa em pacientes com Lúpus Eritematoso Sistêmico atendidos em Hospital Universitário na cidade do Rio de Janeiro, Brasil / Assessment of adherence to medication Lupus Erythematosus Systemic treated at University Hospital in Rio de Janeiro, Brazil

Santos, Marise Oliveira dos

January 2009

Made available in DSpace on 2011-05-04T12:36:24Z (GMT). No. of bitstreams: 0 Previous issue date: 2009 / INTRODUÇÃO: Um dos aspectos importantes que frequentemente prejudica a obtenção dos resultados pretendidos com a terapêutica medicamentosa é a não adesão à prescrição médica. Segundo a Organização Mundial de Saúde, os portadores de doenças crônicas são potenciais candidatos ao seguimento inadequado à terapêutica medicamentosa. Estudos relatam que a baixa adesão no Lúpus Eritematoso Sistêmico (LES) pode conduzir à recaídas e potenciais danos ao organismo, aumento da frequência às consultas e admissões hospitalares, conclusões erradas sobre a eficácia da terapêutica e perda de recursos das instituições de saúde. Em países em desenvolvimento existem poucas informações a cerca de quais fatores estariam mais relacionados à adesão no LES. OBJETIVOS: Estimar a prevalência da adesão à terapêutica medicamentosa e analisar associações com as características do regime de tratamento, da doença, das questões demográficas, sociais e econômicas, e dos profissionais e serviços de saúde em pacientes com LES. MATERIAL/MÉTODO: Desenvolveu-se estudo com delineamento transversal em amostra aleatória composta de 246 mulheres com LES atendidas em hospital universitário na cidade do Rio de Janeiro. Os dados foram coletados entre março e agosto/2008, por meio de entrevistas individuais e revisão de prontuários. Utilizaram-se os critérios de Morisk para avaliar a adesão. A análise considerou as variáveis de exposição em três níveis de hierarquia: distal, intermediário e proximal. Na análise bivariada utilizou-se a regressão logística e na multivariada a regressão logística hierarquizada. (...)CONCLUSÃO: Os dados do estudo realizado indicaram que a adesão à terapêutica medicamentosa no LES é um fenômeno complexo e multifatorial. A análise hierarquizada revelou-se uma boa alternativa para avaliar a adesão, pois permitiu visualizar as diversas etapas da análise. A identificação e análise dos fatores que podem levar à não adesão à terapêutica medicamentosa, nos pacientes com LES, permitirão desenvolver ações de saúde pública para reduzir as barreiras no tratamento, assim como os custos assistenciais e, principalmente promover melhor qualidade de vida dos pacientes. / INTRODUCTION: Nonadherence to medication is one of the critical aspects that may very often jeopardize the intended results of treatment based on medical prescriptions. According to the World Health Organization chronic disease patients are potential candidates to inadequate follow up in therapeutic medication. Some studies reported that a low adherence to medication in Systemic Lupus Erythematosus (SLE) may lead to residiva and potential harm to patients, raise the frequency of visits to medical offices and hospital admissions, may lead to wrong conclusions about the efficacy of therapeutics and significant losses of health resources. There are only a few studies in developing countries about intervening factors related to SLE medical adherence. OBJECTIVES: To estimate adherence to medications in Systemic Lupus Erythematosus and analyze associations with characteristics of treatment, with illness, with social, economic and demographic factors and with caracteristics of medical professional and health services in patients of SLE. METHODS: a cross-seccional study was conducted in a random sample of 246 women patients with SLE attending a University Hospital in the city of Rio de Janeiro. Data were collected between March and August 2008 using face-to-face interviews and medical records review. Morisk’s criteria were used to evaluate adherence to medication. The analysis included exposure variables divided into 3 hierarchical levels: distal, intermediate and proximal. The bivariate analysis used logistic regression and multivariate analysis used hierarchized regression model. RESULTS: Demographic and social data showed predominance of black and mestizo women aged 41 ± 12.35 years with completed secondary school, per capita income of 1.27 ± 1.35 average minimum wage. The number of medications in use was 5 ± 2.48, prednisone being the most used. In the interviewed group 31.7% were classified as adherent to medication. Reasons for nonadherence were careless with the time of taking the medications (52.43%), orgetting (38.21%), side effects (13.8%) and stopping the medication when feeling better (7.72%).The multivariate hierarchical regression showed that the factors associated with adherence were: behavior to side effects, hematological changes, mucocutaneous manifestations, legibility of medical prescriptions, education and family support. CONCLUSION: Data from the study indicated that adherence to medication in SLE is a complex, multi-factorial phenomenon. Hierarchized model analysis seemed to be a valuable method to evaluate adherence to medication because it allowed to view the various stages of analysis. Identification and analysis of the various factors that may interfere with adherence to medication in patients with SLE will permit to develop public health actions to reduce barriers in the treatment as well as to reduce health costs and, most important, to improve patients life quality.

Adesão à terapêutica medicamentosa

Lúpus Eritematoso Sistêmico

Análise multivariada hierarquizada

Lupus Eritematoso Sistêmico/terapia

Cooperação do Paciente

Recusa do Paciente ao Tratamento

Análise Multivariada

Modelos Estatísticos

Entrevista

Adherence to medication

Systemic Lupus Erythematosus

Hierarchized Multivariate Analysis

Lupus Eritematoso Sistêmico/Terapia

Cooperação do Paciente

Recusa do Paciente ao Tratamento

-Brasil

Análise Multivariada

Modelos Estatísticos

Imunogenetické a hormonální predispoziční markery systémových revmatických onemocnění,zejména systémového lupus erythematodu / Immunogenetic and hormonal markers of predisposition to systemic rheumatic diseases particularly systemic lupus erythematosus

Fojtíková, Markéta

January 2011

Fojtikova 2011 INTRODUCTION: Several factors like genetic susceptibility is required for systemic rheumatic diseases development. Immunomodulatory PRL effect supports autoimmunity. AIMS: 1. To detect the immunogenetic background (alleles HLA class I, II and microsatellite polymorphism of the transmembrane part exon 5 of MIC-A gene) of SLE and PsA. 2. To detect PRL serum and synovial fluid with regard to clinical and laboratory RA activity. 3. To find the role of the functional polymorphism -1149G/T SNP PRL of extrapituitary promoter of PRL gene in SLE, RA, PsA, SSc and inflammatory myopathies development. METHODS: Genetic analyses of pateints with SLE (n=156), RA (n=173), PsA (n=100), SSc (n=75), PM (n=47) a DM (n=68) and 123 healthy individuals: PCR-SSP (HLA clase I and II), PCR-fragment analysis (MIC-A) a PCR-RFLP (-1149 G/T SNP PRL). In 29 RA a 26 OA PRL serum and synovial fluid concentrations were detected using immunoradiometric assay. RESULTS: 1. The allele HLA-DRB1*03 (pc=0.008; OR 2.5) and haplotype HLA-DRB1*03-DQB1*0201 (pc <0.001; OR 4.54) were determined as risk immunogenetic markers for SLE in Czech population. In SLE versus controls allele MIC-A5.1 was increased (pc =0.005; OR 1.88). MIC-A5.1 together with HLA-DRB1*03 increases the risk for SLE development, pc <0.000001; OR 9.71....

Correlação clínico-laboratorial e de imagem do lúpus eritematoso sistêmico e da esclerose múltipla no HC/FM/UFG em Goiânia/Goiás de 2009 a 2010: ênfase nas manifestações neurológicas / Correlation of clinical-laboratorial and image of lupus erythematosus and multiple sclerosis in HC/FM/UFG at Goiânia/Goiás, 2009 to 2010: emphasis on neurological manifestations

DINIZ, Denise Sisterolli

12 September 2011

Made available in DSpace on 2014-07-29T15:28:57Z (GMT). No. of bitstreams: 1 Tese Denise Sisterolli Diniz.pdf: 6293055 bytes, checksum: d5c5b19907b7602ca5e99aa0414271f7 (MD5) Previous issue date: 2011-09-12 / Systemic Lupus Erythematosus - LES is an autoimmune disease involving multiple systems. In the Central nervous system-SNC is one of his more severe manifestations. One of the frames of Lupus neuropsychiatric - LES-NP, is a Demyelinating Syndrome - SD. SD in rare cases, may be the first manifestation of LES, resembling multiple sclerosis - MS in their symptoms. MS is autoimmune disease with involvement of SNC with components, degenerative and inflammatory, which can produce autoantibodies and general symptoms that make your final diagnosis. The disease occurs more in young women than in men, typically evolve with outbreaks and remissions. In order to contribute to the diagnosis of these two illnesses, we proposed a comparative analysis, considering clinical, laboratory, and image aspects. As there is a lack of definition of SD, aims to contribute to the definition and establishment of standards of compromise of the SNC by SD of LES-NP, comparing patients with LES-NP and MS (the prototype of CNS demyelinating disease), attended in rheumatology and neurology of the HC/FM/UFG, Goiania. GO, from 2009 to 2010, according to the demographic aspects (sex and age), clinical (time of illness, functional systems and EDSS), laboratory (Autoantibodies and liquid Cerebroespinhal - LCR), image (Conventional magnetic resonance - RM) and Neuropsychological - NPS (cognitive and emotional). It is one epidemiological, analytical and comparative cross-sectional study of LES-NP and MS, which was approved by the CEP/HC/UFG. Were used in the survey questionnaires: an analysis of demographic and personal and family background; other symptoms; Neurological exams and NPS; Analysis: image by RM, laboratory of autoantibodies and LCR; and symptoms of depression and anxiety by Beck inventory (BAI and BDI). The results demonstrated an increased frequency in patients of age; time of disease; Visual symptoms; changes of sensitivity; of coordination; of the March; retention and urinary incontinence; changes of speech and swallowing; depressive and psychotic symptoms in family and personal history; WMHs in parietal and frontal lobes, occipitais, corpus callosum, periventricular, justacortical, brain stem; the cerebellum; spinal cord and the Barkhof and Tintoré criteria - CBT. Other findings in the RM were: infarcts; Vasculitis; menigioma and thrombosis in patients with LES-NP. The involvement of SNC in LES was measured by clinical symptomatology, neurological examination, EDSS, image findings and neuropsychological tests. RM was predictive analytics to relate workload post-lesional adaptation in brain regions typically involved in in. The application of CBT in patients with SD of LES-NP, associated with the qualitative assessment of WMHs may define the differences of neurological involvement pattern of injury of the SD of LES-NP, those at. The dosage of autoantibodies was predictive analytics for the diagnosis of LES, especially the anti DNA, the anti-ENA and the LAC, which were unique in the LES-NP. The clinical examination and laboratory research, neurological autoantibodies antinuclear antibodies and image by RM offers great security in diagnosis of the two diseases.Show that there are aspects of the involvement of the SD in LES needing new assessments, using the markers of neuronal injury, the more specific and with studies of Immunogenetics compared with in, the prototype of CNS demyelinating disease. / Lúpus Eritematoso Sistêmico - LES é a doença auto-imune que envolve vários sistemas. No Sistema Nervoso Central - SNC é uma de suas manifestações mais graves. Um dos quadros neurológicos do Lúpus Neuropsiquiátrico - LES-NP, é a Síndrome Desmielinizante - SD. Em raros casos, SD pode ser a primeira manifestação do LES, se assemelhando a Esclerose Múltipla - EM em sua sintomatologia. EM é doença autoimune com envolvimento do SNC com componentes, inflamatório e degenerativo, que pode apresentar auto-anticorpos e sintomas gerais que dificultam seu diagnóstico final. As doenças ocorrerem mais em mulheres jovens que em homens, evoluem tipicamente com surtos e remissões. Com o intuito de contribuir para o diagnóstico dessas duas enfermidades, propusemos uma análise comparativa, considerando aspectos clínicos, laboratoriais e de imagem. Como há uma carência de definição da SD, pretende-se contribuir com a definição e o estabelecimento de padrões de comprometimento do SNC pela SD do LES-NP, comparando os pacientes com LES-NP e EM (o protótipo da doença desmielinizante), atendidos no serviço de reumatologia e neurologia do HC/FM/UFG, Goiânia/GO, de 2009 a 2010, segundo os aspectos demográficos (sexo e idade), clínicos (tempo de doença, sistemas funcionais e EDSS), laboratoriais (Autoanticorpos e Líquido Cerebroespinhal - LCR), de imagem (Ressonância Magnética Convencional - RM) e Neuropsicológicos - NPS (cognitivo e emocional). É um estudo epidemiológico, analítico, transversal, comparativo de LES-NP e EM, que foi aprovado pelo CEP/HC/UFG. Foram utilizados na pesquisa análise de questionários: um demográfico e de antecedentes pessoais e familiares; outro de sintomas; exames: neurológico e de NPS; avaliações: imagem por RM e laboratorial de auto-anticorpos e LCR; e sintomas de depressão e ansiedade pelo inventário de Beck (BAI e BDI). Os resultados demonstraram uma frequência aumentada nos pacientes de EM, em idade; tempo de doença; sintomas visuais; alterações de sensibilidade; da coordenação; da marcha; retenção e incontinência urinária; alterações da fala e deglutição; sintomas depressivos e psicóticos na história pessoal e familiar; alterações focais da substância branca (WMHs) nos lobos frontais, parietais e occipitais, corpo caloso, periventricular, justacortical, tronco encefálico; cerebelo; medula espinhal e os critérios de Barkhof e Tintoré - CBT. Outros achados na RM foram: infartos cerebrais; vasculites; meningioma e trombose nos pacientes com LES-NP. O envolvimento do SNC no LES foi mensurado pela sintomatologia clínica, exame neurológico, EDSS, achados de imagem e testes neuropsicológicos. RM foi preditiva em relacionar carga lesional em regiões cerebrais tipicamente envolvidas na EM. A aplicação dos CBT nos pacientes com SD do LES-NP, associado à avaliação qualitativa das WMHs pode definir as diferenças de padrão de envolvimento neurológico da lesão da SD do LES-NP, daquelas da EM. A dosagem de autoanticorpos foi preditiva para o diagnóstico de LES, especialmente o anti DNA, o anti-ENA e o LAC, os quais foram exclusivos no LES-NP. O exame clínico e neurológico, da investigação laboratorial de auto-anticorpos antinucleares e da imagem por RM oferece segurança no diagnóstico das duas enfermidades. Mostram que há aspectos do envolvimento da SD no LES que necessitam de novas avaliações, utilizando os marcadores de lesão neuronal, mais específicos e com estudos de imunogenética comparados com a EM, o protótipo da doença desmielinizante do SNC.

Lúpus Eritematoso Sistêmico

Esclerose Múltipla

Imagem por Ressonância Magnética

Anticorpos Antinucleares

Líquido Cefalorraquidiano

Cognição

Transtornos Depressivos e Ansiosos

Systemic Lupus Erythematosus

Multiple Sclerosis

Magnetic resonance imaging

Anti-nuclear Antibodies

Cerebrospinal Fluid

Cognition

Anxious and depressive disorders

CNPQ::CIENCIAS DA SAUDE

The Effects of Immune Regulation and Dysregulation: Helper T Cell Receptor Affinity, Systemic Lupus Erythematosus and Cancer Risk, and Vaccine Hesitancy

Johnson, Deborah K.

03 June 2020

Helper T cells direct the immunological response to foreign pathogens and cancer. To become activated, helper T cells must recognize unique peptides presented on major histocompatibility complex II (pMHCII) by antigen presenting cells (APCs) with their T cell receptor (TCR). While much is known about helper T cell activation signaling cascades and the subsequent roles of helper T cell subsets, the initiation of helper T cell activation by the TCR and other co-receptors is less well understood. Specifically, the affinity of the TCR for its pMHCII can change helper T cell subset fate, proliferation, and alter the risk for activation induced cell death. High affinity TCRs are attractive targets for immunotherapies, but little is known about how helper T cells respond to high affinity TCRs. Here we describe high affinity TCR activation thresholds for both full length TCRs and chimeric antigen receptor TCRs both with and without the presence of the coreceptor CD4 and propose a mechanism whereby CD4 inhibits T cell activation via Lck sequestration and a CD4-independent method. Dysregulated helper T cells play critical roles in the development and perpetuation of systemic lupus erythematosus (SLE), a systemic autoimmune disease that causes widespread inflammation and organ damage throughout the body. Chronic inflammation in SLE affects the immune response to viruses and the risk of developing cancer. However, in SLE patients, it is unclear if viruses initiate the development of cancer directly or if the effects are non-interacting and concomitant. Here we describe the interactions between SLE, viruses, and cancer risk revealing that viruses and SLE do interact to increase the both the overall cancer risk and the risk for hematological malignancies. Due to vaccine efficacy, vaccine preventable diseases (VPDs) are no longer commonly experienced or understood by the public. Vaccines are a victim of their own success and according to the World Health Organization (WHO), vaccine hesitancy (VH) is one of the top threats to global health. VH is the refusal to accept vaccinations and the reasons for VH vary across time, place, and vaccine. Refuting VH is difficult as directly confronting false assumptions can cause individuals to become more entrenched in their position resulting in confirmation bias. Adults with VH attitudes are often motivated by concerns over personal liberty, harm, independence, and body purity. Here we describe the results of a VPD interview- and education-based intervention geared towards promoting positive vaccine attitudes for young adults and demonstrate that education focused on VPDs is more effective than vaccine safety.

Helper T cell

CD4+ T cell

CD4

T cell receptor (TCR)

Lck

IL-2

T cell activation

TCR single chain signaling (TCR-SCS)

chimeric antigen receptor (CAR)

full length TCR (flTCR)

high affinity TCRs

systemic lupus erythematosus (SLE)

cancer-risk

viruses

vaccine hesitancy (VH)

vaccine preventable diseases (VPDs)

vaccines

Life Sciences

Imunogenetické a hormonální predispoziční markery systémových revmatických onemocnění,zejména systémového lupus erythematodu / Immunogenetic and hormonal markers of predisposition to systemic rheumatic diseases particularly systemic lupus erythematosus

Fojtíková, Markéta

January 2011

Fojtikova 2011 INTRODUCTION: Several factors like genetic susceptibility is required for systemic rheumatic diseases development. Immunomodulatory PRL effect supports autoimmunity. AIMS: 1. To detect the immunogenetic background (alleles HLA class I, II and microsatellite polymorphism of the transmembrane part exon 5 of MIC-A gene) of SLE and PsA. 2. To detect PRL serum and synovial fluid with regard to clinical and laboratory RA activity. 3. To find the role of the functional polymorphism -1149G/T SNP PRL of extrapituitary promoter of PRL gene in SLE, RA, PsA, SSc and inflammatory myopathies development. METHODS: Genetic analyses of pateints with SLE (n=156), RA (n=173), PsA (n=100), SSc (n=75), PM (n=47) a DM (n=68) and 123 healthy individuals: PCR-SSP (HLA clase I and II), PCR-fragment analysis (MIC-A) a PCR-RFLP (-1149 G/T SNP PRL). In 29 RA a 26 OA PRL serum and synovial fluid concentrations were detected using immunoradiometric assay. RESULTS: 1. The allele HLA-DRB1*03 (pc=0.008; OR 2.5) and haplotype HLA-DRB1*03-DQB1*0201 (pc <0.001; OR 4.54) were determined as risk immunogenetic markers for SLE in Czech population. In SLE versus controls allele MIC-A5.1 was increased (pc =0.005; OR 1.88). MIC-A5.1 together with HLA-DRB1*03 increases the risk for SLE development, pc <0.000001; OR 9.71....