Immunobiology of IFRD1, a Novel Genetic Modifier of Cystic Fibrosis Lung Disease

Gu, Yuanyuan

06 November 2009

No description available.

Molecular Biology

Cystic Fibrosis

Modifier gene

IFRD1

neutrophil

HDAC

INFLAMMATORY PROTEASES AND CARDIAC REPAIR POST MYOCARDIAL ISCHEMIA

Qi, Zhao

January 2013

Neutrophils are thought to orchestrate myocardial remodeling during the early progression to cardiac failure through the release of reactive oxygen species, antimicrobial peptides, and proteases. Although neutrophil activation may be beneficial at early stages of disease, excessive neutrophil infiltration detrimentally leads to cardiomyocyte death and tissue damage. The neutrophil-derived serine protease cathepsin G (CG) has been shown to induce neonatal rat cardiomyocyte detachment and apoptosis by anoikis1. However the role of inflammatory serine proteases in cardiac remodeling and cardiac regeneration in-vivo is still unknown. We showed that cardiac injection of neutrophil derived protease led to early cardiac dilatation and dysfunction characterized by an increase in matrix metalloprotease (MMP) activation and extracellular matrix degradation along with an increase in myocyte death by apoptosis. To assess the role of these serine proteases, we used mice lacking dipeptidyl peptidase I (DPPI), an enzyme involved in major inflammatory protease activation. DPPI deficient mice demonstrated a more robust functional recovery after ischemia reperfusion (IR) and myocardial infarction (MI) injury, as well as significantly reduced myocyte apoptosis, cardiac dilatation, infarct size and mortality rate. Meanwhile, our data showed increased groups of cardiac stem cells and proliferating cardiac cells in the MI 7-days DPPI knockout mice. We also found enhanced DPPI expression in response to pathological stress stimuli in mice. These findings reveal an unrecognized role of DPPI as a key mediator of post-ischemia cardiac injury and show that inflammatory derived proteases may contribute to the pathological cardiac remodeling and cardiac regeneration, and may be considered as novel target for future therapies. / Physiology

Physiology

Dppi

Inflammatory Protease

Ischemia Reperfusion

Myocardial Infarction

Neutrophil

Regeneration

HYPERHOMOCYSTEINEMIA ACCELERATES STROKE-INDUCED BRAIN INJURY VIA PROMOTING ENDOTHELIAL ACTIVATION AND INFLAMMATORY CELL INFILTRATION: THE ROLE OF ICAM1-MEDIATED NEUTROPHIL AND MONOCYTE INFILTRATION

Zhang, Lixiao

January 2017

Background: Epidemiology, clinical trials and meta-analysis studies have established that Hyperhomocysteinemia (HHcy) is an independent risk factor for stroke. However, the exact molecular mechanism underlying the HHcy-induced risk of stroke is unclear. Our study aims to investigate the role of HHcy in stroke. Methods and results: We established a mice mode of focal ischemic stroke, termed transient Middle Cerebral Artery Occlusion (tMCAO) and conducted surgery on a mice model of HHcy (plasma homocysteine level ~150μM), in which a Zn2+ inducible human cystathionine β-synthase (CBS) transgene was introduced to circumvent the neonatal lethality of the CBS gene deficiency (Tg-hCBS Cbs-/- mice). Fourteen-week-old male mice were used in the experiment. A student’s t-test was used for the evaluation of the statistical significance between the two groups. For the comparison across multiple groups, one-way ANOVA was used. We found that HHcy 1) increased the infarction volume from 42.3 ± 4.9 mm / Pharmacology

Health Sciences

Pharmacology

Biology

Homocysteine

Icam1

Ly6c

Monocyte

Neutrophil

Stroke

Modulation of Innate Immune Cell Signaling Pathways by Staphylococcus aureus and Omnigen-AF®

Johnson, Anne Caitlin

08 November 2013

Staphylococcus aureus causes chronic mastitis in bovines that is difficult to treat with current therapeutics. The goal of this research is to provide information about and improve innate immune responses to infection. Infection can result in host cell apoptosis or programmed cell death. Many pathogens can inhibit apoptosis; thereby acquiring a replicative niche, a reprieve from immune responses, and an escape from treatments. We hypothesize that S. aureus inhibits apoptosis in dendritic cells (DC). To investigate our hypothesis, DC were infected with live S. aureus (LSA), γ-irradiated S. aureus (ISA), or Streptococcus agalactiae (Strep ag.) for 2 hours. Stimulations of DC included ultraviolet light (UV) and lipoteichoic acid (LTA). Results indicate that γ-irradiated S. aureus can inhibit UV-induced apoptosis by upregulating LTA. This research provides information about S. aureus infections, but further research is needed to improve responses to this type of infection. One way to improve innate immune responses to infection is by supplementing bovines with OmniGen-AF®, a probiotic that restores neutrophil function during immunosuppression. To determine the mechanism by which OmniGen-AF® functions, wildtype, MyD88 KO, and TLR4 KO mice were fed either normal chow or supplemented with OmniGen-AF® for two weeks. Mice were immunosuppressed with dexamethasone and challenged with LTA. LTA overcame immunosuppression in a TLR4-depenent manner regardless of supplementation with OmniGen-AF®. Overall this research supplies knowledge about S. aureus inhibition of apoptosis in DC and S. aureus LTA activation of PMN regardless of immunosuppression or supplementation with OmniGen-AF®. / Master of Science

Staphylococcus aureus

dendritic cell

Apoptosis

OmniGen-AF®

immunosuppression

neutrophil

MyD88

O papel dos marcadores imunoinflamatórios no prognóstico e ressecabilidade do adenocarcinoma pancreático

Eyff, Tatiana Falcão

January 2017

Introdução: O adenocarcinoma pancreático é responsável pela maioria das neoplasias pancreáticas e está associado a um prognóstico extremamente pobre tanto devido à alta taxa de diagnósticos em estágio avançado quanto ao elevado índice de recidiva mesmo nos pacientes submetidos à ressecção com intenção curativa. Uma ferramenta que possa predizer adequadamente o prognóstico da doença é fundamental para uma melhor estratificação de risco. Evidências tem mostrado que a resposta inflamatória sistêmica está associada ao prognóstico de diversos tipos de câncer, sendo que a razão neutrófilos/linfócitos (NLR) e suas adaptações e a razão plaquetas/linfócitos (PLR) tem se mostrado promissores para este fim. Objetivo: O objetivo do presente estudo é avaliar o valor prognóstico das razões NLR, NLR derivada (dNLR) e PLR determinados por exames coletados no momento da internação e após tratamento quimioterápico paliativo numa população de pacientes com diagnóstico de adenocarcinoma pancreático, analisando ainda qual o valor de ponto de corte mais adequado para cada parâmetro. Além disso, pretendemos investigar se essas razões podem ter algum valor como fator preditivo de ressecabilidade no adenocarcinoma pancreático. Métodos: Foram coletados dados de pacientes com diagnóstico de adenocarcinoma pancreático confirmado por exame histopatológico atendidos no Hospital de Clínicas de Porto Alegre entre 2003 e 2013. As razões estudadas foram determinadas com base nos hemogramas coletados na internação dos pacientes e após dois ciclos de quimioterapia naqueles que foram submetidos a tratamento paliativo. Resultados: Na análise combinada de todos os pacientes incluídos no estudo, NLR basal, dNLR basal e PLR basal não mostraram evidência de ter impacto prognóstico na sobrevida (P= 0,394, P= 0,152, P= 0,177 respectivamente). No subgrupo de pacientes submetidos a quimioterapia paliativa, NLR, dNLR e PLR calculados pelos exames realizados após 2 ciclos de tratamento mostraram-se fatores prognósticos para sobrevida global (P=0,003, P=0,009 e P=0,001 respectivamente). Os pontos de corte mais adequados encontrados foram 4,11 para NLR (sensibilidade 83% e especificidade 75%), 362 para PLR (sensibilidade 91% e especificidade 62,5%) e 2,8 para dNLR (sensibilidade 87% e especificidade 62,5%). Nenhuma das razões se mostrou estatisticamente significativa como preditor para ressecabilidade (NLR, P=0,88; dNLR, P=0,99; PLR, P=0,64). Conclusões: As razões NLR, dNLR e PLR são úteis como marcadores prognósticos de sobrevida global em pacientes com adenocarcinoma pancreático submetidos a quimioterapia paliativa. Seu uso como preditor de ressecabilidade das lesões pancreáticas não foi demonstrado. / Background: Pancreatic adenocarcinoma is responsible for most of the pancreatic neoplasias and it is associated to an extremely poor prognosis due to diagnosis in advanced stage and the recurrence even among patients treated with curative intention. A prognostic tool is essential for a better risk stratification. Evidence has shown that systemic inflammatory response is associated to the prognosis of a variety of cancers and the neutrophil/lymphocyte ratio (NLR) and adaptations and the platelet/lymphocyte (PLR) ratio seem promising for this purpose. Objetive: The objective of this study is to evaluate the prognostic value of NLR, derived NLR (dNLR) and PLR determined by blood counts collected at hospital admission and after palliative chemotherapy in patients with pancreatic adenocarcinoma, analyzing the ideal cutoff value for each parameter. Also, we intend to investigate if those ratios have some role in predicting the resectability of pancreatic adenocarcinoma. Methods: Data were collected of patients who had diagnosis of pancreatic adenocarcinoma confirmed by histopathologic exam in Hospital de Clínicas de Porto Alegre between 2003 and 2013. The studied ratios were determined by blood counts collected at hospital admission and after two cycles of chemotherapy in patients submitted to palliative treatment. Results: In the combined analysis including all patients, basal NLR, dNLR and PLR did not have prognostic impact in overall survival (P=0,394, P=0,152, P=0,177 respectively). In subgroup analysis of patients submitted to palliative chemotherapy, NLR, dNLR and PLR determined by blood count collected after two cycles of chemotherapy were prognostic for overall survival (P=0,003, P=0,009, P=0,001 respectively). The ideal cutoff values found were 4,11 for NLR (sensibility 83%, specificity 75%), 2,8 for dNLR (sensibility 87%, specificity 62,5%) and 362 for PLR (sensibility 91%, specificity 62,5%). None of these ratios has shown to be able to predict resectability (NLR, P=0,88; dNLR, P=0,99; PLR, P=0,64). Conclusions: NLR, dNLR and PLR are useful as prognostic markers of overall survival in patients with pancreatic adenocarcinoma submitted to palliative chemotherapy. Its use as resectability predictor could not be demonstrated.

Neutrófilos

Linfócitos

Neoplasias da próstata

Prognóstico

Neutrophil/lymphocyte ratio

Platelet/lymphocyte rati

Derived neutrophil/lymphocyte ratio

Prognosis

Pancreatic adenocarcinoma

O papel dos marcadores imunoinflamatórios no prognóstico e ressecabilidade do adenocarcinoma pancreático

Eyff, Tatiana Falcão

January 2017

Introdução: O adenocarcinoma pancreático é responsável pela maioria das neoplasias pancreáticas e está associado a um prognóstico extremamente pobre tanto devido à alta taxa de diagnósticos em estágio avançado quanto ao elevado índice de recidiva mesmo nos pacientes submetidos à ressecção com intenção curativa. Uma ferramenta que possa predizer adequadamente o prognóstico da doença é fundamental para uma melhor estratificação de risco. Evidências tem mostrado que a resposta inflamatória sistêmica está associada ao prognóstico de diversos tipos de câncer, sendo que a razão neutrófilos/linfócitos (NLR) e suas adaptações e a razão plaquetas/linfócitos (PLR) tem se mostrado promissores para este fim. Objetivo: O objetivo do presente estudo é avaliar o valor prognóstico das razões NLR, NLR derivada (dNLR) e PLR determinados por exames coletados no momento da internação e após tratamento quimioterápico paliativo numa população de pacientes com diagnóstico de adenocarcinoma pancreático, analisando ainda qual o valor de ponto de corte mais adequado para cada parâmetro. Além disso, pretendemos investigar se essas razões podem ter algum valor como fator preditivo de ressecabilidade no adenocarcinoma pancreático. Métodos: Foram coletados dados de pacientes com diagnóstico de adenocarcinoma pancreático confirmado por exame histopatológico atendidos no Hospital de Clínicas de Porto Alegre entre 2003 e 2013. As razões estudadas foram determinadas com base nos hemogramas coletados na internação dos pacientes e após dois ciclos de quimioterapia naqueles que foram submetidos a tratamento paliativo. Resultados: Na análise combinada de todos os pacientes incluídos no estudo, NLR basal, dNLR basal e PLR basal não mostraram evidência de ter impacto prognóstico na sobrevida (P= 0,394, P= 0,152, P= 0,177 respectivamente). No subgrupo de pacientes submetidos a quimioterapia paliativa, NLR, dNLR e PLR calculados pelos exames realizados após 2 ciclos de tratamento mostraram-se fatores prognósticos para sobrevida global (P=0,003, P=0,009 e P=0,001 respectivamente). Os pontos de corte mais adequados encontrados foram 4,11 para NLR (sensibilidade 83% e especificidade 75%), 362 para PLR (sensibilidade 91% e especificidade 62,5%) e 2,8 para dNLR (sensibilidade 87% e especificidade 62,5%). Nenhuma das razões se mostrou estatisticamente significativa como preditor para ressecabilidade (NLR, P=0,88; dNLR, P=0,99; PLR, P=0,64). Conclusões: As razões NLR, dNLR e PLR são úteis como marcadores prognósticos de sobrevida global em pacientes com adenocarcinoma pancreático submetidos a quimioterapia paliativa. Seu uso como preditor de ressecabilidade das lesões pancreáticas não foi demonstrado. / Background: Pancreatic adenocarcinoma is responsible for most of the pancreatic neoplasias and it is associated to an extremely poor prognosis due to diagnosis in advanced stage and the recurrence even among patients treated with curative intention. A prognostic tool is essential for a better risk stratification. Evidence has shown that systemic inflammatory response is associated to the prognosis of a variety of cancers and the neutrophil/lymphocyte ratio (NLR) and adaptations and the platelet/lymphocyte (PLR) ratio seem promising for this purpose. Objetive: The objective of this study is to evaluate the prognostic value of NLR, derived NLR (dNLR) and PLR determined by blood counts collected at hospital admission and after palliative chemotherapy in patients with pancreatic adenocarcinoma, analyzing the ideal cutoff value for each parameter. Also, we intend to investigate if those ratios have some role in predicting the resectability of pancreatic adenocarcinoma. Methods: Data were collected of patients who had diagnosis of pancreatic adenocarcinoma confirmed by histopathologic exam in Hospital de Clínicas de Porto Alegre between 2003 and 2013. The studied ratios were determined by blood counts collected at hospital admission and after two cycles of chemotherapy in patients submitted to palliative treatment. Results: In the combined analysis including all patients, basal NLR, dNLR and PLR did not have prognostic impact in overall survival (P=0,394, P=0,152, P=0,177 respectively). In subgroup analysis of patients submitted to palliative chemotherapy, NLR, dNLR and PLR determined by blood count collected after two cycles of chemotherapy were prognostic for overall survival (P=0,003, P=0,009, P=0,001 respectively). The ideal cutoff values found were 4,11 for NLR (sensibility 83%, specificity 75%), 2,8 for dNLR (sensibility 87%, specificity 62,5%) and 362 for PLR (sensibility 91%, specificity 62,5%). None of these ratios has shown to be able to predict resectability (NLR, P=0,88; dNLR, P=0,99; PLR, P=0,64). Conclusions: NLR, dNLR and PLR are useful as prognostic markers of overall survival in patients with pancreatic adenocarcinoma submitted to palliative chemotherapy. Its use as resectability predictor could not be demonstrated.

Neutrófilos

Linfócitos

Neoplasias da próstata

Prognóstico

Neutrophil/lymphocyte ratio

Platelet/lymphocyte rati

Derived neutrophil/lymphocyte ratio

Prognosis

Pancreatic adenocarcinoma

O papel dos marcadores imunoinflamatórios no prognóstico e ressecabilidade do adenocarcinoma pancreático

Eyff, Tatiana Falcão

January 2017

Introdução: O adenocarcinoma pancreático é responsável pela maioria das neoplasias pancreáticas e está associado a um prognóstico extremamente pobre tanto devido à alta taxa de diagnósticos em estágio avançado quanto ao elevado índice de recidiva mesmo nos pacientes submetidos à ressecção com intenção curativa. Uma ferramenta que possa predizer adequadamente o prognóstico da doença é fundamental para uma melhor estratificação de risco. Evidências tem mostrado que a resposta inflamatória sistêmica está associada ao prognóstico de diversos tipos de câncer, sendo que a razão neutrófilos/linfócitos (NLR) e suas adaptações e a razão plaquetas/linfócitos (PLR) tem se mostrado promissores para este fim. Objetivo: O objetivo do presente estudo é avaliar o valor prognóstico das razões NLR, NLR derivada (dNLR) e PLR determinados por exames coletados no momento da internação e após tratamento quimioterápico paliativo numa população de pacientes com diagnóstico de adenocarcinoma pancreático, analisando ainda qual o valor de ponto de corte mais adequado para cada parâmetro. Além disso, pretendemos investigar se essas razões podem ter algum valor como fator preditivo de ressecabilidade no adenocarcinoma pancreático. Métodos: Foram coletados dados de pacientes com diagnóstico de adenocarcinoma pancreático confirmado por exame histopatológico atendidos no Hospital de Clínicas de Porto Alegre entre 2003 e 2013. As razões estudadas foram determinadas com base nos hemogramas coletados na internação dos pacientes e após dois ciclos de quimioterapia naqueles que foram submetidos a tratamento paliativo. Resultados: Na análise combinada de todos os pacientes incluídos no estudo, NLR basal, dNLR basal e PLR basal não mostraram evidência de ter impacto prognóstico na sobrevida (P= 0,394, P= 0,152, P= 0,177 respectivamente). No subgrupo de pacientes submetidos a quimioterapia paliativa, NLR, dNLR e PLR calculados pelos exames realizados após 2 ciclos de tratamento mostraram-se fatores prognósticos para sobrevida global (P=0,003, P=0,009 e P=0,001 respectivamente). Os pontos de corte mais adequados encontrados foram 4,11 para NLR (sensibilidade 83% e especificidade 75%), 362 para PLR (sensibilidade 91% e especificidade 62,5%) e 2,8 para dNLR (sensibilidade 87% e especificidade 62,5%). Nenhuma das razões se mostrou estatisticamente significativa como preditor para ressecabilidade (NLR, P=0,88; dNLR, P=0,99; PLR, P=0,64). Conclusões: As razões NLR, dNLR e PLR são úteis como marcadores prognósticos de sobrevida global em pacientes com adenocarcinoma pancreático submetidos a quimioterapia paliativa. Seu uso como preditor de ressecabilidade das lesões pancreáticas não foi demonstrado. / Background: Pancreatic adenocarcinoma is responsible for most of the pancreatic neoplasias and it is associated to an extremely poor prognosis due to diagnosis in advanced stage and the recurrence even among patients treated with curative intention. A prognostic tool is essential for a better risk stratification. Evidence has shown that systemic inflammatory response is associated to the prognosis of a variety of cancers and the neutrophil/lymphocyte ratio (NLR) and adaptations and the platelet/lymphocyte (PLR) ratio seem promising for this purpose. Objetive: The objective of this study is to evaluate the prognostic value of NLR, derived NLR (dNLR) and PLR determined by blood counts collected at hospital admission and after palliative chemotherapy in patients with pancreatic adenocarcinoma, analyzing the ideal cutoff value for each parameter. Also, we intend to investigate if those ratios have some role in predicting the resectability of pancreatic adenocarcinoma. Methods: Data were collected of patients who had diagnosis of pancreatic adenocarcinoma confirmed by histopathologic exam in Hospital de Clínicas de Porto Alegre between 2003 and 2013. The studied ratios were determined by blood counts collected at hospital admission and after two cycles of chemotherapy in patients submitted to palliative treatment. Results: In the combined analysis including all patients, basal NLR, dNLR and PLR did not have prognostic impact in overall survival (P=0,394, P=0,152, P=0,177 respectively). In subgroup analysis of patients submitted to palliative chemotherapy, NLR, dNLR and PLR determined by blood count collected after two cycles of chemotherapy were prognostic for overall survival (P=0,003, P=0,009, P=0,001 respectively). The ideal cutoff values found were 4,11 for NLR (sensibility 83%, specificity 75%), 2,8 for dNLR (sensibility 87%, specificity 62,5%) and 362 for PLR (sensibility 91%, specificity 62,5%). None of these ratios has shown to be able to predict resectability (NLR, P=0,88; dNLR, P=0,99; PLR, P=0,64). Conclusions: NLR, dNLR and PLR are useful as prognostic markers of overall survival in patients with pancreatic adenocarcinoma submitted to palliative chemotherapy. Its use as resectability predictor could not be demonstrated.

Neutrófilos

Linfócitos

Neoplasias da próstata

Prognóstico

Neutrophil/lymphocyte ratio

Platelet/lymphocyte rati

Derived neutrophil/lymphocyte ratio

Prognosis

Pancreatic adenocarcinoma

Characterisation of chromatin extracellular traps in rainbow trout (Oncorhynchus mykiss)

Van, Andre P.

January 2018

One of the greatest challenges in finfish aquaculture is combating losses caused by infectious bacterial diseases, and a better understanding of the interactions between the host immune system and pathogens is essential for developing new methods to manage infections and outbreaks. Extracellular traps (ETs) are decondensed nuclear chromatin released by neutrophils into the extracellular matrix that can ensnare and kill microbes. Since the discovery of ETs in humans, these innate immune effectors have been characterised across the animal kingdom, including in some fish species, though their existence the salmonids has yet to be confirmed. Therefore, the aim of this thesis was to confirm and characterise the release of ETs in the rainbow trout (Oncorhynchus mykiss) and investigate the interaction of these structures with fish pathogenic bacteria. To do this, a triple-layer Percoll gradient technique was employed to give highly enriched cell suspensions of polymorphonuclear cells (PMNs) derived from head-kidney tissue preparations. Treatment of PMN-enriched cell suspensions with the nucleic-acid-specific stain, SYTOX Green, revealed the presence of ET-like structures that had been released without stimulation. These ET-like structures were confirmed by immunostaining techniques to contain the diagnostic proteinaceous markers of ETs: neutrophil elastase, myeloperoxidase and the H2A histone. Previously characterised inhibitors and inducers of ET release from phagocytic immune cells in other animals confirmed that calcium ionophore (CaI), flagellin, and cytochalasin D shared similar activities for ET-release by rainbow trout PMNs. However, interestingly, as the common ET-inducer phorbol-myristate acetate (PMA) and ET-inhibitor diphenyleneiodonium (DPI) did not exert their expected potency in ET release assays with the PMNs, perhaps indicating that these fish cells are less dependent on NADPH oxidase signalling for ET release compared to mammals and most invertebrate species. The PMN-derived ETs were demonstrated to bind to and trap the extracellular nuclease-deficient bacterial fish pathogen, Vibrio anguillarum (Vib 87) when co-cultured. Finally, extracellular nuclease activity produced by a V. anguillarum isolate (Vib 6) during culture was able to degrade ETs released by rainbow trout PMNs in a dose-dependent manner. Moreover, viable colony counts, fluorescent and phase contrast microscopy demonstrated that V. anguillarum Vib 6 eluded trapping by ETs, while an extracellular nuclease-deficient isolate did not. These observations are consistent with the suggestion that nucleases are a microbial virulence factor during host infection. Confirming the existence and antimicrobial potential of extracellular traps released by rainbow trout PMNs may provide a platform towards the development of novel therapeutics to reduce mortalities in finfish aquaculture caused by infectious microbial pathogens.

Modulation fonctionnelle des cellules dendritiques par les « Neutrophil Extracellular Traps » / Functional modulation of dendritic cells by « Neutrophil Extracellular Traps »

Barrientos, Lorena

04 November 2013

Les polynucléaires neutrophiles (PN) sont des cellules essentielles au cours de la réponse immunitaire innée ; recrutés rapidement au site inflammatoire où ils participent à la phase aigüe, ils vont aussi contribuer à la résolution de l’inflammation. Ils peuvent en effet moduler la réponse adaptative par interaction avec les lymphocytes (Ly) ou les cellules dendritiques (DC) via des médiateurs solubles ou des interactions cellulaires directes. Les Neutrophil Extracellular Traps (NETs) libérés par les PN activés pourraient jouer un rôle important dans ce contexte. Les NETs sont des filaments de chromatine décondensée associés à des protéines issues principalement des granulations et du cytoplasme. Ils sont essentiels dans la réponse anti-infectieuse mais semblent également impliqués dans la physiopathologie de certaines maladies auto-immunes et inflammatoires. L’objectif de ce travail a été d’évaluer les effets des NETs sur la maturation des DC dans un contexte inflammatoire au cours duquel les PN et les DC peuvent co-exister, assurant ainsi un pont entre immunité innée et immunité adaptative. La première partie de ce travail a consisté à développer un modèle de production, isolement et caractérisation des NETs issus de PN sanguins humains. L’ionophore de calcium A23187 a été choisi pour induire les NETs et l'enzyme de restriction AluI a permis la récupération de fragments de NETs de taille hétérogène. Certains des composants de ces NETs sont quantifiables (ADN, élastase, histone 3 en particulier), et nous avons montré qu’ils conservaient leurs capacités bactéricides in vitro. Ces échantillons de NETs constituent donc un outil biologique standardisé, permettant d’évaluer leurs effets sur des cellules ou des tissus. Dans la deuxième partie de ce travail, nous avons mis en évidence que ces NETs purifiés régulaient négativement la maturation de moDC induites par le LPS (expression de HLA-DR, CD80, CD83, CD86 et production de TNFα, IL-12, IL-6, IL-23). De plus, les NETs diminuent la capacité de ces moDC à induire la prolifération des LyT, et leur polarisation est modulée en favorisant la production de cytokines de type Th2 (IL-5 et IL-13) aux dépens de cytokines de types Th1 (INFγ) et Th17 (IL-17). De manière intéressante, la capacité de migration des moDC activées par le LPS n’est pas modifiée en présence de NETs. En résumé, ces résultats suggèrent que les NETs pourraient jouer un rôle immunorégulateur sur la maturation des moDC dans des conditions inflammatoires. Les NETs produits par les PN activés pourraient ainsi participer à la régulation indispensable de la réponse inflammatoire. / Polymorphonuclear neutrophils (PMN) are innate immune cells rapidly recruited to the inflammatory sites where they play a major role during the acute phase response but also contribute to resolution and repair. They can also modulate the adaptive response by interacting with lymphocytes (Ly) or dendritic cells (DC) via soluble mediators or cell-cell contacts. Activated PMN release Neutrophil Extracellular Traps (NETs) that could play a role in this context. NETs are decondensed chromatin fibers associated with granule and cytoplasmic proteins. As they are mainly involved in host defense against infection, they contribute to some autoimmune and inflammatory diseases. The aim of this work was to evaluate NET effects on DC maturation in an inflammatory context where PMN and DC co-exist, thus bridging innate and adaptive immunity. We first developed a model to induce, isolate and characterize NETs from human PMN. Calcium ionophore A23187 was chosen to induce NETs and the restriction enzyme AluI allowed the recovery of heterogeneous-sized fragments of NETs. Some of their components were quantified (DNA, elastase, histone 3, in particular) and we found that they retained their bactericidal activity. These NETs samples thus constitute a new and important biological tool to study their effects on immune cells or tissues. In the second part of this work, we found that isolated NETs were able to down-regulate LPS-induced moDC maturation as evidenced by the expressions of HLA-DR, CD80, CD83, CD86 and cytokine release (TNFα, Il-6, IL-12, Il-23). Moreover, the presence of NETs during moDC maturation lead to a decrease capacity of these moDC to induce T lymphocyte proliferation and modulated polarization by promoting the production of Th2 cytokines (IL-5 and IL-13) and decreasing Th1 cytokines (INFγ) and Th17 (IL- 17). Interestingly, moDC migration capacity was not modified when moDC maturation was done in the presence of NETs. In summary, these data suggest that NETs could downregulate DC activation. NETs produced by activated PMN could thus participate to the regulation of inflammation.

Neutrophil Extracellular Traps

Polynucléaire neutrophile

Cellule dendritique

Inflammation

Lymphocyte T

Réponse immune

Interaction cellulaire

Neutrophil Extracellular Traps

Neutrophils polymorphonuclear

Dendritique cell

Inflammation

T lymphocyte

Immune response

Cellular intéraction

Dynamics of Neutrophil Extracellular Trap (NET) Formation

Neubert, Elsa

07 May 2019

No description available.

610

Neutrophil granulocytes

Innate immunity