Expressão ex vivo de fatores antivirais em mães infectadas por HIV-1 e recém-natos. / Ex vivo expression of antiviral factors in mothers infected by HIV-1 and newborns.

Natalli Zanete Pereira

16 April 2013

A transmissão vertical mãe-recém-nato é a principal fonte de infecção pediátrica. O tratamento antirretroviral vem reduzindo a transmissão vertical, mas também tem elevado o número de infantes expostos não infectados, os quais vêm mostrando maior risco de morbidade e mortalidade. Este dado salienta a importância de avaliar as características imunológicas, relacionadas à resposta inata no binômio mãe e recém-nato. A proposta do trabalho foi avaliar a expressão de fatores antivirais em células mononucleares (CMN), tecido placentário e no colostro de mães infectadas por HIV e cordão umbilical (RN), comparadas com mães-RN controle não infectadas. Os dados mostram que há uma ativa expressão dos fatores antivirais, sejam constitutivos ou induzíveis por IFN, nas mães infectadas por HIV e nos RN expostos. No sítio de interface materno-fetal, decídua e face fetal da placenta, foi detectado um perfil alterado de expressão dos fatores antivirais, especialmente da proteína APOBEC3G. Apesar da relativa imaturidade imunológica dos RNs, a infecção materna por HIV gerou um perfil semelhante de expressão dos fatores antivirais nos RN, por uma complexa interação de fatores relacionados a gestação e a infecção. / Vertical transmission mother-newborn is the main source of pediatric infection. The antiretroviral therapy has reduced vertical transmission, but also has increased the number of exposed uninfected infants, which have shown increased risk of morbidity and mortality. This finding emphasizes the importance of evaluating the immunological characteristics, related to innate response in both the mother and newborn. The purpose of this study was to evaluate the expression of antiviral factors in mononuclear cells (MNC), placental tissue and colostrum of HIV-infected mothers and umbilical cord (RN), compared with control mothers-uninfected infants. The data show that the active expression of antiviral factors, are constitutive or inducible by IFN in HIV-infected mothers and newborns exposed. At the site of maternal-fetal interface, decidua and placental villi, a profile was detected altered expression of antiviral factors, especially the APOBEC3G protein. Despite the relative immunological immaturity of the newborn, maternal HIV infection generated a similar profile of expression of antiviral factors in RN, by a complex interaction of factors related to pregnancy and infection.

Fatores imunológicos

Gravidez

Imunidade natural

Infecções por HIV

Interferons

Recém-nascido

HIV infections

Immune factors

Interferons

Natural immunity

Newborn

Pregnancy

Efeitos da separação materna sobre o comportamento, a imunidade inata e o crescimento tumoral / Maternal separation effects on the behavior, innate immunity and tumor growth

Milena Lobão Pinheiro

14 March 2008

Um modelo de indução de estresse/ansiedade é a separação materna. Sabe-se, a este respeito, que o desenvolvimento do comportamento emocional normal em mamíferos jovens depende da interação entre a mãe e o filhote. Além disso, eventos estressantes na infância e interrupções no cuidado materno podem levar a efeitos deletérios na resposta imune e na resistência a doenças ao longo da vida. Buscamos neste trabalho estudar os efeitos da separação materna sobre o comportamento, imunidade inata e crescimento tumoral de uma prole de camundongos machos adultos. Nossos resultados mostraram que a separação materna, em camundongos A/J, (1) não produziu alterações robustas no comportamento e em parâmetros hematológicos (antes e após o crescimento tumoral), (2) aumentou a atividade de neutrófilos sanguíneos e macrófagos alveolares (antes e após o crescimento tumoral), (3) aumentou os níveis estriatais de serotonina, seu metabólito 5-HIAA e o turnover de dopamina, (4) diminuiu os níveis séricos de corticosterona e (5) não influenciou a incidência tumoral. Em camundongos C57BL/6, a separação materna produziu um comportamento ansioso e um aumento na atividade de neutrófilos sanguíneos. Tomados em seu conjunto, parece-nos possível afirmar que a separação materna tenha produzido alterações na atividade neuroimune dos animais, modificando, nos mesmos a atividade do eixo HPA e essas alterações foram influenciadas pelas características individuais das linhagens. / Maternal separation is one model of stress/anxiety induction. We know about it that the mammals normal emotional behavior development depends on the interaction between mother and younglet. Beside this, early life stressed events can induce deletery effects in immune response and to illness resistance for all life long. In this work we searched for the maternal separation effects on the behavior, innate immunity and tumor growth in an adult male mice offspring. Our results showed that the maternal separation, in A/J mice (1) had no big effects in the behavior and in the hematological parameters (before and after the tumor growth), (2) increased the neutrophil and alveolar macrophages activity (before and after the tumor growth), (3) increased the serotonin striatum levels, the 5-HIAA metabolite and the dopamine turnover (4) decreased the corticosterone serum levels and (5) had no effects on tumor incidence. In the C57BL/6 mice, the maternal separation induced an anxiety behavior and increased the neutrophil activity. These results suggest that the maternal separation could have produced alterations in neuroimmune activity, modifying the HPA axis activity and these alterations could be influenced by individual strains characteristics.

Ansiedade de separação

Citometria de fluxo

Imunidade natural

Labirintos

Neuroimunomodulação

Stress

Flow citometry

Mazes

Natural immunity

Neuroimmunomodulation

Separation anxiety

Stress

Efeitos da alga Chlorella vulgaris sobre a resposta hematopoética e capacidade funcional de neutrófilos em ratos submetidos ao estresse agudo físico e psicogênico e infectados com Listeria monocytogenes / Effects of the algae Chlorella vulgaris on hematopoietic response and functional activity of neutrophils in rats submitted to physical and psychogenic acute stress and infected with Listeria monocytogenes

Julia de Souza-Queiroz

21 June 2006

Evidências experimentais sugerem que uma variedade de estressores ativa o controle hipotalâmico das respostas neuroendócrinas e autonômicas que estão envolvidas na produção de células do sangue e na liberação destas células da medula óssea para a circulação. A alga Chlorela vulgaris (CV) exibe várias atividades imunomoduladoras como, por exemplo, a capacidade de estimulação das células hematopoéticas e de ativação de leucócitos maduros. No presente trabalho analisamos o efeito imunoprotetor da CV em animais submetidos aos estressores físicos (estresse por choque escapável - CE e inescapável - CI) e ao estressor psicogênico (grupo de animais que testemunhou a exposição ao choque inescapável - T) e inoculados com a bactéria Listeria monocytogenes (LM). Os parâmetros imunológicos observados foram: 1) Crescimento e diferenciação de progenitores hematopoéticos para granulócitos e macrófagos (CFU-GM) da medula óssea; 2) Atividade funcional (burst e fagocitose) de neutrófilos circulantes avaliados por citometria de fluxo; 3) Sobrevida de animais inoculados com dose letal de LM e/ou submetidos aos estressores físicos e psicogênico. Nos grupos CI e T observamos uma redução no número de CFU-GM na medula óssea. Por outro lado, não houve redução deste parâmetro nos animais do grupo CE quando comparado ao medido no grupo controle. Observamos uma maior susceptibilidade do organismo a infecção por LM quando o estresse foi aplicado previamente à inoculação com dose subletal desta bactéria. No entanto, o tratamento com 200 mg/Kg/dia de CV por 5 dias consecutivos mostrou uma ação protetora, restabelecendo a mielossupressão induzida pelo choque inescapável ou pelo estressor psicogênico e/ou pela infecção. A aplicação de choques escapáveis não alterou significativamente o perfil da resposta hematopoética produzida pela infecção. O estudo da eficácia terapêutica de alga, avaliada pelo tratamento de animais infectados com dose letal de LM, demonstrou uma sobrevida de 50% no grupo infectado e de 20% nos grupos infectados e submetidos aos diferentes tipos de estresse, inclusive naquele exposto ao estresse escapável. Ao considerarmos os efeitos dos estressores sobre a atividade funcional de neutrófilos sanguíneos, observamos uma redução na capacidade de fagocitose nos grupos CI e T, e um aumento do burst induzido pela fagocitose. No grupo CE houve um aumento na capacidade de fagocitose destas células, enquanto que o burst não foi alterado. O estudo dos efeitos da CV sobre a atividade funcional de neutrófilos demonstrou uma capacidade da alga de impedir a redução da fagocitose produzida pelo estresse físico por choque inescapável e psicogênico, sem interferir com o burst oxidativo, que estava aumentado nestes grupos. Impediu também o aumento da capacidade de fagocitose verificado no grupo CE. Esses resultados sugerem que a CV possua propriedades protetoras contra os efeitos induzidos pelo diferentes tipos de estressores sobre a série granulocítica/macrofágica, a atividade funcional de neutrófilos e sobre a sobrevida de animais estressados e infectados com dose letal de LM. / Evidence suggests that a variety of stressors can activate the hypothalamic control of the neuroendocrine and autonomic responses involved in the production´s control of blood cells and their release from bone marrow to circulation. The algae Chlorella vulgaris (CV) has several imunomodulatory activities, as the stimulation of hematopoietic cells and the activation of mature leukocytes. The present study evaluated the mieloprotective effects of CV in rats exposed to physical stressors (inescapable - CI and escapable footshock - CE) and to psychogenic stressors (animals that witnessed the inescapable shock application - T), which were inoculated or not with a sublethal dose of the bacterium Lysteria monocytogenes (LM). The immunologic parameters observed were: 1) The growth and differentiation of bone marrow progenitors into granulocytes and macrophages (CFU-GM); 2) the functional activity (oxidative burst and phagocytosis) of blood neutrophils, using flow citometric methods; 3) The rate of survival of animals infected with lethal dose of LM and submitted or not to the stressors. The CI and T groups were mielossupressed. On the other hand, in the CE group, no differences in the number of CFU-GM were observed, when compared to controls. An increase in the susceptibility of the organism was observed when the animals received the inescapable shock application and the psychogenic stressor before the inoculatium of sublethal dose (7,8x108) of the 15 bacterium. However, this mielopoietic response was recovered with the pre-treatment with 200 mg/Kg/day for 5 consecutive days of CV, reestablishing the mielossupression caused by the stress and the infection. The escapable shock didn´t produce any significant difference in the hematopoetic response observed in the infection. The study of the survival rate of rats infected with the letal dose of LM showed that the pre-treatment with CV protected 50% of the animals that were only infected with LM, whereas in the group previously stressed the protection was of 20%. Here, the same response was observed in the animals submitted to the different types of stressors evaluated in this work. To assess the effect of CV treatment in the response of mature blood cells, we considered the functional activity of neutrophils of animals submitted to the stressors. We observed a reduction in phagocytosis in the CI and T groups, and an increase in the oxidative burst induced by the phagocytosis. In the CE group there was an increase in the blood neutrophil phagocytosis, while the production of oxidative burst remained equal to that of control group. The treatment with CV reestablished the changes in phagocytosis to normal values in all the groups, but it produced no changes in the respiratory burst, which was increased in the circunstances of the inescapable shock and of the psychogenic stressor, when compared to the values of control group. Considering our results, we suggest that CV has protective properties against the effects produced by the different types of stressors on the CFU-GM, the functional activity of neutrophils and on the rate of survival of animals stressed and infected with lethal dose of LM.

choque escapável

choque inescapável

citometria de fluxo

imunidade natural

mielopoiese

neuroimunomodulação

escapable footschok

flow cytometry

inescapable footshock

mielopoyesis

natural immunity

neuroimmunomodulation

Prospecção gênica e atividade antimicrobiana de b-defensina-símiles em viperídeos. / Gene survey and antimicrobial activity of beta-defensin-like in viperid.

Poliana Garcia Corrêa

30 October 2013

As b-defensinas são pequenos peptídeos catiônicos com estrutura rica em folhas b pregueadas e seis cisteínas conservadas. São bastante estudadas em mamíferos, mas pouco em serpentes. Utilizando a PCR foram descritos 13 genes b-defensina-símiles em serpentes do gênero Bothrops e Lachesis . Eles se organizam em três éxons e dois íntrons; há alta similaridade no éxon1, íntron 1 e 2, mas os éxons 2 e 3 estão sob evolução acelerada. A análise filogenética por máxima parcimônia revelou que o gene ancestral de b-defensina-símile pode ter três éxons em vertebrados e sua evolução ocorreu de acordo com o modelo de nascimento-e-morte. Peptídeos b-defensina-símiles reduzidos, testados por ensaio de inibição de crescimento em meio líquido, apresentaram atividade inibitória contra Escherichia coli, Citrobacter freundii, Micrococcus luteus e Staphylococcus aureus. A crotamina reduzida foi mais ativa que a forma nativa. Os resultados indicam que a carga líquida era a característica bioquímica mais importante na atividade antibiótica dos peptídeos b-defensina-símiles. / b-defensins are small basic cationic peptides with b-sheet-rich fold plus six conserved cysteines. They are fully studied in mammals, but scarce in snakes. Using a PCR approach, we described 13 b-defensin-like sequences in Bothrops and Lachesis snakes. They are organized in three exons and two introns; they show high similarities in exon 1, intron 1 and intron 2, but exons 2 and 3 have undergone accelerated evolution. Phylogenetic analysis was done using maximum parsimony indicate that the ancestral b-defensin-like gene may have three exons in vertebrates and that their evolution occurred according to a birth-and-death model. Reduced b-defensin-like peptides were tested by microbroth dilution assay, showed inhibitory activity against Escherichia coli, Citrobacter freundii, Micrococcus luteus e Staphylococcus aureus. The reduced form of crotamine was more active than native. The results indicate that the positive net charge is the most important biochemical characteristic of b-defensin-like peptides to antibiotic activity.

Agentes antimicrobianos

Evolução molecular

Filogênia

Imunidade natural

Polimorfismo

Viperidae

Antimicrobial agents

Molecular evolution

Natural immunity

Phylogeny

Polymorphism

Viperidae

Caractérisation des mécanismes de régulation de la synthèse du Tumor Necrosis Factor-alpha par le nicotinamide

Goffette, Nicolas

13 September 2013

Dans le cadre de l’étude de la régulation de la synthèse de la cytokine pro-inflammatoire TNF-alpha dans les cellules myéloïdes stimulées aux lipopolysaccharides, nous avons pu mettre en évidence que l’effet anti-inflammatoire du nicotinamide (NAM) sur la production de cette cytokine s’opère au niveau de l’état de phosphorylation de la MAPK p38. Une diminution de la concentration intracellulaire de NAD entraine également une inhibition de la phosphorylation de la MAPK p38 en réponse aux lipopolysaccharides. De plus, une étude pharmacologique plus ciblée suggère que les sirtuines, une famille d’enzymes consommatrices de NAD, sont impliquées dans cette régulation. Nos résultats indiquent que ce processus s’effectuerait par un contrôle de l’expression des gènes mkp-1 et pac-1 codant pour des « dual-phosphatases » modulant l’état de phosphorylation des MAPKs. Enfin, nos données indiquent que l’effet anti-inflammatoire du NAM s’opère aussi par une régulation de l’efficacité traductionnelle du messager du TNF-alpha impliquant un raccourcissement de la queue poly(A) du messager. En conclusion, l’ensemble de nos données montre une complexité importante dans la régulation de la production de TNF-alpha dans les cellules myéloïdes par des enzymes consommatrices de NAD, dont les sirtuines. / Doctorat en sciences, Spécialisation biologie moléculaire / info:eu-repo/semantics/nonPublished

Sciences exactes et naturelles

Biologie

Nicotinamide

Natural immunity

Genetic regulation

Nicotinamide

Immunité naturelle

Régulation génétique

TNF; nicotinamide

Hormones and dendritic cells influences on the initiation of the autoimmune disease experimental autoimmune encephalomyelitis /

Papenfuss, Tracey L.

January 2007

Thesis (Ph. D.)--Ohio State University, 2007. / Full text release at OhioLINK's ETD Center delayed at author's request

Adaptations of Trypanosoma brucei to the innate immunity proteins TNF-gas and ApoL-1 / Adaptations de Trypanosoma brucei aux protéines de l'immunité innées TNF-gas et ApoL-1

Vanwalleghem, Gilles

06 March 2012

This work allowed the first characterization of the three members of the chloride channel CLC family in T.brucei. The TbCLCs are expressed in the two proliferative stages of the parasite and two of their members appear non-essential. The three TbCLCs act as chloride transporters in X.laevis oocytes and some of their biophysical properties were determined. Furthermore, TbCLC-b appeared to be involved in lysis by the human innate immunity protein apoL-1<p>A novel function of T.brucei adenylate cyclases was discovered in their ability to suppress expression of the innate immunity protein TNF-α. The suppression of the innate response occurs before the first peak of parasitemia and reduces the host ability to control the parasite.<p> / Doctorat en Sciences / info:eu-repo/semantics/nonPublished

Sciences exactes et naturelles

Biologie

Trypanosoma brucei

Host-parasite relationships

Natural immunity

Trypanosoma brucei

Relations hôte-parasite

Immunité naturelle

Host-parasite interactions

Étude du niveau de B Lymphocyte Stimulator (BLyS) et de son impact sur les lymphocytes B en relation avec l’infection et la résistance au virus d’immunodéficience humaine (VIH) chez des travailleuses du sexe au Bénin

Sabourin-Poirier, Catherine

04 1900

L’infection au VIH s’accompagne souvent de dérégulations du compartiment des lymphocytes B qui nuisent à la génération de réponses efficaces. En effet, détectées tôt après l’infection, ces dérégulations perdurent, ne sont pas totalement restaurées par la thérapie, et mènent souvent à des manifestations auto-immunes et lymphomes. Une étude longitudinale de notre groupe, effectuée avec des cellules mononucléées du sang circulant provenant de patients VIH+ avec différents types de progression clinique, a démontré qu’un niveau élevé de BLyS chez des individus VIH+ progresseurs était associé à une dérégulation des fréquences de populations de cellules B avec augmentation de cellules innées de la zone marginale (MZ) présentant des caractéristiques d’immaturité et d’activation. Au contraire, chez des individus VIH+ non-progresseurs avirémiques ou contrôleurs d’élite, les niveaux de BLyS étaient dans la normale et ce sont les fréquences de cellules B MZ plus matures qui étaient diminuées. La résistance au VIH pourrait aussi impliquer le contrôle de BLyS et son impact sur les cellules B. De ce fait, nous avons préalablement recruté une cohorte de travailleuses du sexe (TS) à Cotonou (Bénin) dans laquelle nous avons identifié des femmes qui demeurent séronégatives malgré une exposition soutenue au virus. Nous avons mesuré les niveaux de BLyS dans le sang et dans les lavages cervico-vaginaux (CVL) de TS VIH- et les avons comparés à ceux mesurés chez des TS VIH+ et un groupe contrôle de non-TS VIH- . Nous avons trouvé que les niveaux de BLyS dans le sang et le CVL des TS VIH- étaient inférieurs à ceux des TS VIH+ et des non-TS VIH-. Le niveau d’expression de BLyS à la surface des lymphocytes T, monocytes et cellules dendritiques de TS VIH- était augmenté, mais à un niveau moindre que les TS VIH+. Chez les TS VIH+, les hauts niveaux de BLyS étaient concomitants avec une dérégulation du compartiment B caractérisée par une hyperglobulinémie, une augmentation de la fréquence de populations avec un profil immature/inné et une plus grande proportion de plasmablastes IgG vs IgA. Au contraire, les niveaux inférieurs de BLyS dans le sang des TS VIH- coïncident avec un compartiment B préservé, révélant que les lymphocytes B MZ peuvent être impliqués dans l’immunité naturelle au VIH. Ces résultats démontrent l’importance du contrôle des niveaux de BLyS et du maintien de l’intégrité du compartiment B dans la résistance au VIH. / HIV infection leads to B cell dysregulations that disrupt efficient immune responses. Detected early after infection, these dysregulations are lasting, are not totally resolved by therapy and often lead to auto-immune defects. We have shown that excess BLyS in plasma and on the surface of blood dendritic cells (DC) of HIV-infected progressors coincides with B cell dysregulation and increased frequency of “precursor” innate marginal zone (MZ)-like B cells. In contrast, BLyS levels were normal in elite-controllers and frequency of precursor MZ-like B cells was unaltered. Instead, percentages of MZ-like B-cells presenting a more “mature” profile were decreased in the blood of these individuals, suggesting peripheral recruitment of these cells could be beneficial to the control of disease progression. Based on this, we hypothesize that control of BLyS status and innate B cells could be relevant to the understanding of natural immunity to HIV. We previously established an ongoing cohort of heavily HIV-exposed female commercial sex workers (CSWs) in Cotonou (Benin) and identified individuals who remain HIV-uninfected after several years of active prostitution. Herein, we have measured BLyS levels in the blood and cervico-vaginal lavages (CVLs) of HIV-uninfected CSWs and have compared them to those of HIV-infected CSWs and control uninfected non-CSWs. We found that BLyS levels in the blood and CVLs of HIV-uninfected CSWs were lower when compared to HIV-infected CSWs and even to controls. BLyS surface expression on T-cells, monocytes, and DC of HIV-uninfected CSWs was increased, but to a significantly lower extent than those measured in HIV-infected CSWs, albeit higher than controls. In HIV-infected CSWs, high BLyS levels were concomitant with a dysregulated blood B-cell compartment, characterized by hyperglobulinemia, increased frequency of populations presenting immature and/or innate profiles and a higher proportion of IgG+ than IgA+ plasmablasts. In contrast, contained BLyS levels in the blood of HIV-uninfected CSWs coincided with a rather preserved B-cell compartment, which reveals that “mature” MZ-like B-cells could be involved in natural immunity against HIV. These results highlight the importance of a better understanding of B cell populations and BLyS in the context of HIV resistance.

VIH

Lymphocyte B

BLyS

BAFF

zone marginale

Bénin

Travailleuse du sexe

Résistance

HIV

B cell

Marginal zone

Commercial sex worker

Immunité naturelle

natural immunity

Insight into the activation mechanism of Toll-like receptor 4 by diC14-amidine

Schmidt, Boris

12 September 2014

SUMMARY:<p>The bacterial lipopolysaccharide (LPS)-sensing machinery with the innate immune system receptor Toll-like receptor 4 (TLR4) at its centre has been the subject of extensive research but while TLR4 and myeloid differentiation factor 2 (MD2) were both shown to be essential, the role of other, so-called "accessory", molecules is much less clear. The co-receptor cluster of differentiation 14 (CD14) has been widely perceived as being a mere facilitator for the capture and transfer of LPS to TLR4, until recent studies suggested it might have a determining influence on which TLR4-dependent signaling cascades are triggered in response to LPS. The TLR4 receptor complex was shown to be specifically activated by diC14 amidine, a cationic lipid originally synthesized for its carrier properties. The lipid's immunostimulatory activity extends to both TLR4-dependent signaling cascades, the MyD88 and TRIF pathways.<p>The aim of this work was to gain more insight into how diC14 amidine is able to trigger these cascades and to contribute to the general understanding of the TLR4 machinery and its activation by non-LPS ligands. More precisely we were interested in the role of CD14 in the activation of both MyD88 and TRIF pathways by diC14-amidine and in potential consequences of possible divergent requirements of diC14 amidine and LPS for this co receptor.<p>Our study of the role of the membrane-associated and the soluble form of CD14 in the activation of the TLR4-dependent pathways by diC14 amidine revealed that – unlike LPS – the cationic lipid does not require CD14 to exercise its immunostimulatory activity, although the presence of the co receptor modulates the TLR4 activation and infrared spectroscopy experiments suggest a direct interaction.<p>In the case of sensing LPS, CD14 is required for the endocytosis of TLR4 and the subsequent activation of the TRIF pathway. By blocking the endocytosis mechanism at different stages we found that diC14-amidine generally enters the cell via endocytosis and that it activates – unlike LPS – both signaling cascades from inside endosomal vesicles, albeit at different stages of the endocytosis process.<p>Although the eventual immunological responses caused by diC14 amidine and LPS resemble each other or are even identical, our research revealed differences in the actual mechanism of activating TLR4, the receptor responsible for the corresponding innate immune response. These findings illustrate the uniqueness of diC14 amidine and the potential of further exploring its intriguing properties and mechanisms as a tool to decipher the TLR4 signaling machinery and with the perspective of designing new immunomodulators for vaccination and therapy.<p><p><p>RÉSUMÉ:<p>Le mécanisme de reconnaissance des lipopolysaccharides bactériens (LPS) par le récepteur de l'immunité innée Toll-like receptor 4 (TLR4) a fait l'objet d'une recherche intensive ces dernières années. Alors que TLR4 et son co-récepteur myeloid differentiation factor 2 (MD2) ont été démontrés comme étant essentiels pour la détection du LPS, le rôle des molécules dites "accessoires" est beaucoup moins évident. Le co-récepteur cluster of differentiation 14 (CD14) a largement été considéré comme un simple facilitateur pour la capture et le transfert des LPS à TLR4, mais des études récentes suggèrent qu'il pourrait avoir une influence déterminante sur les cascades de signalisation dépendantes de TLR4 induites en réponse au LPS. La diC14-amidine, un lipide cationique synthétisé initialement pour ses qualités en tant que vecteur de transfection, a révélé récemment une activité immunostimulatrice dépendante du récepteur TLR4, impliquant les deux cascades de signalisation dépendantes de TLR4, les voies MyD88 et TRIF.<p>Le but de ce travail était de mieux comprendre le mécanisme par lequel la diC14¬ amidine induit ces cascades et de contribuer à la compréhension générale du fonctionnement du complexe récepteur TLR4 et son activation par des ligands non-LPS. Plus précisément nous nous sommes intéressés au rôle de CD14 dans l'activation des voies MyD88 et TRIF par la diC14-amidine et des conséquences potentielles d’éventuelles divergences en termes d’exigence pour ce co-récepteur entre la diC14-amidine et le LPS. <p>Notre étude sur le rôle de la forme membranaire ou soluble de CD14 dans l'activation des voies dépendantes de TLR4 par la diC14-amidine a révélé que - contrairement au LPS - le lipide cationique ne nécessite pas de CD14 pour exercer son activité immunostimulatrice. Cependant, la présence du co-récepteur module l'activation de TLR4 et des expériences de spectroscopie infrarouge suggèrent une interaction directe entre le lipide et le CD14. <p>Dans le cas de la détection de LPS, le CD14 est nécessaire pour l'endocytose de TLR4 et l'activation subséquente de la voie TRIF. En bloquant le mécanisme d'endocytose à différents stades, nous avons montré que la diC14-amidine active - contrairement au LPS - les deux cascades de signalisation depuis l'intérieur des vésicules endosomiales, mais à des stades différents du processus d'endocytose.<p>En conclusion, bien que les réponses immunologiques causées par la diC14-amidine et le LPS se ressemblent, notre recherche a mis en évidence des différences substantielles dans leurs modes d'action. Ces différences illustrent le caractère unique de la diC14-amidine et son potentiel comme outil pour explorer la complexité du système de signalisation du TLR4 et en tirer des enseignements qui permettront de contribuer à la conception de nouveaux immunomodulateurs pour la vaccination et la thérapie. / Doctorat en Sciences / info:eu-repo/semantics/nonPublished

Chimie

Sciences exactes et naturelles

Endotoxins

Natural immunity

Amidines

Endocytosis

Endotoxines

Immunité naturelle

Amidines

Endocytose

lipopolysaccharides

cationic lipid

diC14-amidine

lipopolysaccharide

endocytose

endocytosis

cluster of differentiation 14

LPS

Toll-like receptor 4

TLR-4

TLR4

MyD88

lipide cationique

TRIF

CD-14

CD14

immunité innée

innate immunity

L’immunité naturelle contre le VIH-1 est associée à un profil tolérogénique dans la muqueuse génitale des travailleuses du sexe béninoises hautement exposées et séronégatives (HESN)

Fourcade, Lyvia

01 1900

La plupart des infections par le VIH-1 sont acquises lors de rapports hétérosexuels. En Afrique subsaharienne on observe 71 % des infections mondiales et 60 % des nouvelles infections par le VIH-1 touchent les femmes. Le tractus génital féminin (TGF) constitue la principale porte d’entrée pour le VIH-1 et joue un rôle important dans la défense de l’organisme contre les microorganismes pathogènes tout en maintenant une tolérance de la flore commensale. On y trouve les cellules épithéliales qui participent à l’élaboration des réponses immunes en collaboration avec les cellules dendritiques (DCs), mais également d’autres types de cellules immunitaires qui confèrent une protection à la muqueuse vaginale, notamment à travers la production de cytokines et de chimiokines. Nous avons établi une cohorte de travailleuses du sexe (CSWs) au Bénin et nous avons identifié des femmes hautement exposées et séronégatives au VIH-1 (HESN), qui demeurent séronégatives après plus de sept années actives dans le travail du sexe. Les personnes HESN étant un excellent modèle d’immunité naturelle contre le VIH-1, le but de notre projet consiste donc à étudier les cellules immunitaires impliquées dans la protection de l’hôte face au VIH-1, au niveau du tractus génital féminin. Nous émettons l’hypothèse que le maintien de faibles conditions inflammatoires dans le TGF des femmes HESN préviendrait une activation immunitaire excessive en préservant l’intégrité de la barrière de la muqueuse vaginale et contribuerait ainsi à maintenir une protection contre l’infection par le VIH-1. Des études antérieures sur les HESN béninoises et kenyanes ont démontré que ces femmes présentent de faibles niveaux d’inflammation dans leur TGF inférieur. En accord avec cela, nous avons observé de faibles niveaux de BLyS/BAFF dans la muqueuse vaginale des HESN comparativement aux travailleuses du sexe séropositives (CSWs+ HIV+). BLyS/BAFF est une molécule importante pour la différenciation des cellules B et pour la sélection de cellules B de première ligne de la zone marginale (MZ). De ce fait, nous rapportons pour la première fois la présence de cellules B CD1c+ de type MZ qui sont capables de se lier naturellement à la gp120 glycosylée, au niveau de la muqueuse vaginale. Or, des cellules B CD1c+ exprimant IgG sont augmentées chez les CSWs+ HIV+ comparativement aux HESN, ce qui pourrait contribuer à l’hyperglobulinémie observée dans le TGF inférieur des CSWs+ HIV+. Les faibles niveaux de BLyS/BAFF retrouvés dans la muqueuse vaginale des HESN semblent donc préserver une homéostasie au sein du compartiment B et des cellules B CD1c+ du TGF. De plus, nous y détectons une réactivité des IgG1 avec la gp-41 de l’enveloppe virale, qui pourrait contribuer à leur immunité naturelle. Avec les cellules épithéliales, les DCs sont l’une des premières à être en contact avec le virus dans le TGF. Elles jouent un rôle essentiel dans l’orchestration des réponses immunitaires. Nous pensons que les DCs contribuent au maintien de faibles conditions inflammatoires dans le TGF des HESN, prévenant ainsi l’activation immunitaire excessive et préservant l’intégrité de la barrière muqueuse de façon à maintenir une protection/contrôle contre le virus. Nous avons caractérisé une population myéloïde endocervicale « tolérogénique » HLA-DR+CD14+CD11c+ exprimant HLA-G, ILT4, CD103 et de forts taux d’IFN-α et d’IL-10 dont la fréquence relative était augmentée au niveau du col de l’utérus des HESN comparativement aux CSWs+ HIV+. De plus, des populations Tregs/Tr1 étaient aussi augmentées chez les HESN. Ces données reflètent à la fois une réponse antivirale et une contribution au contrôle des conditions inflammatoires dans le TGF des HESN. Afin de mieux comprendre la nature des cellules myéloïdes tolérogéniques, nous avons voulu dériver des monocytes en cellules dendritiques (MoDCs). Toutefois, nous avons remarqué que la différenciation des MoDCs des HESN était altérée. Suite à cela, nous avons caractérisé le profil transcriptomique des monocytes. Les résultats préliminaires mettent en lumière l’éventuel rôle des récepteurs nucléaires NR4A dans la modulation des MoDCs et, possiblement, sur le plan des cellules myéloïdes tolérogéniques chez les HESN. Dans l’ensemble, ces résultats nous ont permis d’acquérir de nouvelles connaissances sur les mécanismes mis en place chez les HESN dans l’immunité naturelle contre le VIH-1. / Most HIV-1 infections are acquired through heterosexual intercourse. In sub-Saharan Africa, 71% of global infections are observed and 60% of new HIV-1 infections affect women. The female genital tract (FGT) constitutes a main portal of entry for HIV-1 and plays an important role in protecting the host against pathogens while maintaining a tolerance to a commensal flora. FGT immunity involves genital epithelial cells as well as dendritic cells (DCs) and many other types of immune cells which confer protection, through the production of chemokines and cytokines. We established a cohort of commercial sex workers (CSWs) in Benin and identified HIV-1 highly exposed seronegative (HESN) individuals, who remain uninfected after more than seven years of active prostitution. These HESN individuals being an exceptional model of natural immunity against HIV-1, the aim of our project is to characterize immune cells involved in protection from HIV-1 infection, in the female genital tract. We hypothesize that maintenance of low inflammatory conditions in the FGT of HESN women helps to prevent excessive immune activation likely preserving the mucosal barrier integrity and would help to maintain a protection against HIV infection. Previous studies of Beninese and Kenyan HESN have shown that these women have a low inflammatory profile in their lower FGT. Accordingly, we found that vaginal mucosa of HESN had lower soluble BLyS/BAFF levels when compared to HIV-infected CSWs (CSWs+ HIV+). BLyS/BAFF is highly recognized for its role in B-cell ontogenesis, as well as cell fate decision towards the innate marginal zone (MZ) B-cell pool. For the first time, we report the presence of genital MZ-like CD1c+ B-cells that naturally bind to fully glycosylated gp120 in the vaginal mucosa. However, CD1c+ B-cells expressing IgG are increased in the lower FGT of CSWs+ HIV+ when compared to HESN, suggesting that these cells could contribute to the hyperglobulinemia observed in the lower FGT of CSWs+ HIV+. The low levels of BLyS/BAFF found in the vaginal mucosa of HESN thus appear to preserve homeostasis of the FGT B cell compartment and CD1c+ B-cells. In addition, we detect a reactivity of IgG1 to HIV-gp41 in cervico-vaginal lavages (CVL) supernatants of HESN, which could contribute to their natural immunity. Epithelial cells and DCs are one of the earliest cell types to sense the virus in the FGT. They play a key role in the orchestration of immune responses. We characterized a "tolerogenic" endocervical myeloid HLA-DR+CD14+CD11c+ population expressing HLA-G, ILT4, CD103 and high levels of IFN-α and IL-10, that was increased in the cervix of HESN when compared to CSWs+ HIV+. In addition, frequencies of Tregs/Tr1 cells were also increased in HESN. We believe that DCs contribute to maintaining low inflammatory conditions in the FGT of HESN, preventing excessive immune activation and preserving the integrity of the mucosal barrier to maintain a protection/control against the virus. These data reflect both an antiviral response and a contribution to the control of inflammatory conditions in the FGT of HESN. To better understand the nature of tolerogenic myeloid cells, we wanted to derive monocyte-derived dendritic cells (MoDCs). However, derivation of blood MoDCs was impaired in HESN. As a result, we decided to characterize the transcriptomic profile of total blood monocytes. Preliminary results appear to demonstrate the possible role of NR4A nuclear receptors in MoDCs modulation, and possibly in tolerogenic myeloid cells in HESN. Overall, our results contribute to a better understanding of the mechanisms established by HESN in natural immunity to HIV-1.

VIH-1

HESN

tractus génital féminin

immunité naturelle

BLyS/BAFF

isotype

DCs tolérogéniques

Tregs/Tr1

IFN-α

MoDCs

HIV-1

HESN

Female genital tract

Natural immunity

BLyS/BAFF

CD1c+ B-cells MZ

"tolerogenic" DCs