Papel Bim na resposta imune ao Trypanosoma cruzi durante a infecção experimental / Role of Bim protein in the immune response to Trypanosoma cruziduring experimental infection.

Marcela Hernandez Torres

04 December 2015

A proteína Bim é uma potente molécula pró-apoptótica da família Bcl-2 que participa na indução da via intrínseca de apoptose. Pouco se sabe sobre o papel de Bim na resposta imune contra patógenos. Utilizando um modelo murino de infecção pelo T. cruzi, nós observamos um aumento da carga parasitaria e da mortalidade de animais Bim-/-. Macrófagos peritoneais isolados de camundongos Bim-/- no pico de sua parasitemia apresentaram diminuição da produção de NO e da sua atividade microbicida, provavelmente devido a uma deficiência no influxo da subpopulação SPM (small peritoneal macrophages). Ademais, neste mesma fase, esplenócitos apresentaram uma deficiência da produção de NO e das citocinas pró-inflamatórias IFN-γ e IL-6 e os animais Bim-/- apresentaram uma diminuição da citotoxicidade in vivo contra antígenos específicos ao T. cruzi. Em conjunto, nossos resultados sugerem um papel importante da proteína Bim no controle da replicação e eliminação do parasita na fase inicial da infecção. / Bim protein is a potent pro-apoptotic molecule of Bcl-2 family that participates in the induction of intrinsic apoptosis pathway. Little is known about its role on the immune response against pathogens. Using a murine model of T. cruzi infection, we observed an increased parasitemia and mortality in Bim-/- mice. Peritoneal macrophages isolated from these mice at the peak of parasitemia displayed decreased NO production and microbicidal activity, probably due to a defect in the influx of the small peritoneal macrophage (SPM) subpopulation. Moreover, we also observed a deficiency in nitric oxide production, pro-inflammatory cytokines IFN-γ and IL-6 secretion by splenocytes at this period of infection. Finally, Bim-/- mice has an impaired in vivo cytotoxic response against antigens from T. cruzi. Together, our results suggest an important role of Bim in the control of parasite replication and elimination in acute phase of T. cruzi infection.

Trypanosoma cruzi

Bim

IFN-γ

Linfócitos T CD8+

Macrófagos

Óxido nítrico

Trypanosoma cruzi

Bim

CD8+ T lymphocytes

IFN-γ

Macrophages

Nitric oxide

Estudo das populações de linfócitos T e linfócitos B esplênicos e do sangue periférico de camundongos BALB/c imunizados com taquizoítos de Toxoplasma gondii irradiados. / Study of populations T lymphocytes and B lymphocytes in the spleen and peripheral blood of immunized BALB/c mice with irradiated T. gondii tachyzoites.

Nahiara Esteves Zorgi

03 March 2016

Taquizoítos de T. gondii esterilizados por radiação ionizante é uma vacina interessante para induzir uma imunidade semelhante à infecção, mas sem a formação de cistos. Neste estudo avaliamos as populações celulares do sangue e do baço induzidas pela imunização, a resposta imune humoral, celular e a proteção após desafio com parasitas viáveis. Camundongos foram imunizados com taquizoítos de T. gondii irradiados por v.o. ou i.p.. Os animais foram desafiados com 10 cistos da cepa ME-49 ou VEG por via oral e apresentaram altos níveis de proteção com baixa carga parasitária. Camundongos imunizados por i.p. e v.o. apresentaram anticorpos específicos no soro e o aumento das populações de células B, plasmócitos, células TCD4+ e TCD8+ tanto no sangue como no baço. As células esplênicas de camundongos imunizados por i.p. mostraram a produção de IL-10, IFN-γ e IL-4. Células TCD4+ e células B do baço de camundongos imunizados por i.p. proliferaram após a estimulação com antígeno. A imunização com esse modelo vacinal induziu uma resposta imune mediada com células B, TCD4+ e TCD8+, com aumento da resposta imune humoral e celular que são necessárias para proteção do hospedeiro após uma infecção. Essa resposta imune induzida é uma resposta semelhante a uma infecção natural, sendo assim o desenvolvimento de vacinas utilizando a radiação ionizante como uma ferramenta, pode ser um modelo atrativo e eficiente para testar novos imunógenos no futuro. / Tachyzoites of T. gondii sterilized by ionizing radiation is an interesting vaccine for inducing immunity to infection similarly but without the formation of cysts. In this study we evaluated the cell populations from blood and spleen induced by immunization, the humoral immune response, cellular and protection after challenge with viable parasites. Mice were immunized with irradiated tachyzoites of T. gondii by v.o. or i.p.. The animals were challenged with 10 cysts of the ME-49 or VEG strain orally and showed high levels of protection with low worm burden. Immunized mice by i.p. and v.o. present specific antibodies in the serum and increased populations of B cells, plasma cells, CD4+ and CD8+ T cells in blood and spleen. The spleen cells of immunized mice by i.p. showed the production of IL-10, IFN-γ and IL-4. CD4+ T cells and B cells in the spleen of immunized mice i.p. proliferated upon stimulation with antigen. The immunization with this vaccine model induced an immune response mediated by B cells, CD4+ and CD8+ with increased humoral and cellular immune response are necessary for host protection after infection. This induced immune response is a response similar to natural infection, therefore the development of vaccines using ionizing radiation as a tool, can be an attractive and efficient model for testing new immunogens in the future.

Toxoplasma gondii

Linfócitos B

Linfócitos T CD4+

Linfócitos T CD8+

Radiação ionizante

Vacina

Toxoplasma gondii

B-lymphocytes

CD4+ T lymphocytes

CD8+ T lymphocytes

Ionizing radiation

Vaccine

Rôles combinés des cytokines IL-2, IL-15 et IL-21 dans le développement et le maintien des lymphocytes T CD8+ mémoires

Mathieu, Cédric

12 1900

Suite à une infection, des lymphocytes T CD8+ naïfs (LTn CD8+) spécifiques d’un antigène du pathogène sont activés. Après, cette activation, ces lymphocytes se différencient en lymphocytes T effecteurs CD8+ (LTe CD8+) chargés d’éliminer le pathogène. Une fois que l’infection est résolue, la grande majorité des effecteurs meurent par apoptose et les survivants se différencient en lymphocytes T mémoires CD8+ (LTm CD8+). Ces derniers protègeront l’organisme à long terme contre une réinfection par le même pathogène. Il est ainsi primordial d’avoir une meilleure compréhension des mécanismes impliqués dans le développement et la maintenance des LTm CD8+. Plusieurs études ont déjà montré que certaines cytokines de la famille γC (IL-2, IL-7, IL-15 et IL-21) influençaient individuellement le développement des LTe et LTm CD8+. Cependant, nous pensons que ces cytokines ont un impact bien plus grand sur l’homéostasie des LTe et LTm CD8+ que la littérature actuelle le laisse entendre. En effet, nous émettons l’hypothèse que ces cytokines de la famille γC agissent en synergie entre elles afin de promouvoir le développement des LTe et LTm CD8+. Pour tester notre hypothèse, nous avons dans un premier temps étudié l’impact combiné des signaux IL-2 et IL-15 sur la génération des LTe et LTm CD8+ dans un modèle d’infection LCMV Armstrong. Ensuite, dans le même modèle expérimental, nous avons étudié l’effet d’une déficience en signaux IL-2, IL-15 et IL-21 sur le développement des LTe et LTm CD8+. Nos résultats montrent que ces trois cytokines collaborent afin de soutenir l’expansion et la différenciation des LTe CD8+. Plus précisément, l’IL-2, l’IL-15 et l’IL-21 sont essentielles pour l’homéostasie d’une population particulière de LTe CD8+ : les Short-Lived Effector Cells (SLECs). Nous avons également mis en évidence que ces trois cytokines sont toutes les trois requises afin de générer un nombre maximum de LTm CD8+. De plus, la différenciation et le maintien de la population effecteur mémoire (TEM) sont particulièrement réduites en l’absence des signaux combinés de l’IL-2, l’IL-15 et l’IL-21. Nos résultats mettent pour la première fois en lumière les rôles redondants et synergiques de trois cytokines dépendantes de la chaine γc dans le développement et la maintenance des LTe et LTm CD8+. / Over the course of an infection, antigenic signals trigger a specific CD8+ T cells (LTn CD8+) response. Upon antigen recognition, LTn CD8+ are activated and undergo a massive proliferation wave. This leads them to differentiate into effector cells (LTe CD8+) in charge of pathogen elimination. While most effector T cells die after the infection is resolved, a small part of this population persists and differentiates into memory T cells (LTm CD8+). These cells provide long term protection to the organism against the initial infectious agent. It is thus crucial to have a better understanding of all mechanisms governing the development and the maintenance of LTm CD8+. Several studies have already shown that some members of the "C-dependent cytokines family (IL-2, IL-7, IL-15 and IL-21) individually regulate LTe and LTm CD8+ development. However, we believe that these cytokines have a far greater impact on the homeostasis of LTe and LTm CD8+ than the current literature suggests. Indeed, we hypothesized that "C-dependant cytokines act in synergy to promote the development of LTe and LTm CD8+. To assess their effect, we first studied the combined impact of IL-2 and IL-15 signals on the generation of LTe and LTm CD8+ during an LCMV Armstrong infection in mice. In this same experimental model, we also studied the effect of a deficiency in IL-2, IL-15 and IL-21 signals on the development of LTe and LTm CD8+. Our results show that these three cytokines cooperate to support the expansion and differentiation of LTe CD8+. More accurately, IL-2, IL-15 and IL-21 are essential for the homeostasis of a particular LTe CD8+ subset : Short- Lived Effector Cells (SLECs). We also demonstrated that all three cytokines are required to generate a maximal number of LTm CD8+. In addition, differentiation and maintenance of the memory effector population (TEM) are substantially reduced in the combined absence of IL-2, IL-15 and IL-21 signals. These results are the first to our knowledge to highlight redundant and synergistic functions of three "C-dependent cytokines as promoters of the development and maintenance of LTe and LTm CD8+.

Lymphocytes T CD8

Lymphocytes T CD8 mémoires

cytokines gamma c

Migration

redondance

Virus

CD8+ T lymphocytes

c-dépendent cytokines

synergy

redundancy

differentiation

maintenance

secondary infection

migration

L’impact de la grossesse sur l’amplitude et la diversité de la reconnaissance antigénique des lymphocytes T cytotoxiques dirigés contre le VIH-1

Jolette, Elyse

09 1900

La transmission mère-enfant (TME) du VIH-1 est un des enjeux majeurs de la pandémie. Une meilleure compréhension de la réponse des lymphocytes T cytotoxiques CD8+ (LTC) VIH-spécifiques lors de la grossesse facilitera le design de stratégies optimales pour diminuer la TME. Notre objectif est donc de caractériser l’amplitude et la diversité de la reconnaissance antigénique des LTC VIH-spécifiques avant, pendant et après la grossesse chez des femmes infectées par le VIH-1. Nos résultats montrent pour la première fois que l’initiation et la progression de la grossesse, à elles seules, n'ont que peu d’influence sur l’amplitude et la diversité de la reconnaissance antigénique des réponses LTC en termes de production d’IFN‐. Ces résultats indiquent que les femmes infectées par le VIH conservent une immunocompétence durant leur grossesse, du moins dans le contexte d’un traitement antirétroviral efficace. Ceci pourrait éventuellement aider à promouvoir l’immunisation comme stratégie pour prévenir la TME du VIH‐1. / Mother-to-child transmission (MTCT) of HIV-1 is one of the major issues of the pandemic. Characterization of HIV-specific immunity during pregnancy, especially cytotoxic CD8+ T lymphocytes (CTL), will lead to a better understanding of HIV pathogenesis and facilitate design of optimal strategies to prevent MTCT. Our objective is to describe the magnitude and the breadth of antigen recognition of HIV-specific CTL responses before, throughout and after pregnancy in a group of HIV-infected women. Our results revealed for the first time that initiation of pregnancy by itself doesn’t change the magnitude of CTL responses in terms of IFN- production. These findings support the fact that HIV-infected women maintain immunocompetence throughout gestation, at least in the context of effective antiretroviral treatment. These results provide a novel understanding of the dynamics of HIV-specific CTL responses during pregnancy and may help to promote maternal immunization as a strategy to prevent MTCT of HIV-1.

Lymphocytes T cytotoxiques CD8+

Cytotoxic CD8+ T lymphocytes

LTC

CTL

VIH

HIV

Grossesse

Pregnancy

ELISpot

IFN-γ

Gag

Transmission mère-enfant

Mother-to-child transmission

TME

MTCT

Expression des SOCS-1 et SOCS-3 par les lymphocytes T humains en réponse à des cytokines immuno-modulatrices

El-Khoury, Lama

07 1900

Les cytokines jouent un rôle fondamental dans la régulation des processus biologiques via la cascade de signalisation JAK-STAT. Les « Suppressors of Cytokine Signalling » (SOCS), protéines intracellulaires, inhibent la voie JAK-STAT. Plusieurs études supportent leur implication dans des maladies immunitaires, mais peu d’informations sont disponibles sur leur expression par les lymphocytes T humains. Nous postulons que les cytokines Interféron-β(IFN-β) et Interleukine-27 (IL-27), dotées d’un potentiel immuno-régulateur, ont des rôles bénéfiques via l’induction des SOCS. L’impact de l’IFN-β et l’IL-27 sur l’expression des SOCS-1 et SOCS-3 par des cellules T CD8 et CD4 humaines a été étudié en utilisant des cellules sanguines de donneurs sains. L’expression de ces régulateurs a été évaluée aux niveaux de l’ARNm par qRT-PCR et protéique par immunocytochimie. Les SOCS-1 et SOCS-3 ont été rapidement induits en ARNm dans les deux types cellulaires en réponse à l’IFN-β ou l’IL-27 et une augmentation de l’expression a été confirmée au niveau protéique. Afin de mimer les thérapies à base d’IFN-β, les cellules T ont été exposées chroniquement à l’IFN-β. Après chaque ajout de cytokine les cellules T ont augmenté l’expression du SOCS-1, sans moduler le SOCS-3. L’IL-27 a induit les SOCS-1 et SOCS-3 préférentiellement dans les cellules T CD8 ; ceci corrèle avec des résultats du laboratoire démontrant une plus petite expression des récepteurs à l’IL-27 par les lymphocytes T CD4 que les CD8. Notre projet a permis d’élucider l’expression des SOCS dans deux populations de cellules T et de clarifier les mécanismes d’actions de l’IFN-β et l’IL-27. / Cytokines regulate fundamental biological processes via the JAK-STAT signaling pathway. Suppressors of Cytokine Signaling proteins (SOCS), intracellular proteins, inhibit the JAK-STAT pathway. Emerging evidence supports the involvement of SOCS in diseases of the immune system but no data is available regarding their expression in human T cells. We postulate that the cytokines Interferon-β (IFN-β) and Interleukin-27 (IL-27), both potential immuno-regulators, have beneficial roles through the induction of SOCS proteins. The impact of IFN-β and IL-27 on the SOCS-1 and SOCS-3 expression by human CD4 and CD8 T cells was assessed using peripheral blood mononuclear cells from healthy donors. We evaluated the expression of SOCS-1 and SOCS-3 at the mRNA level by qRTPCR and at the protein level by immunocytochemistry. A rapid increase of SOCS-1 and SOCS-3 mRNA levels was observed upon cytokine addition, and such upregulation was confirmed at the protein level. To mimic patients under IFN-β treatment, both T cell subsets were chronically exposed to IFN-β. We observed an increase of SOCS-1 after each stimulation but not for SOCS-3. IL-27 stimulation increased SOCS-1 and SOCS-3 mRNA levels in CD8 T cells but only slightly in CD4 T cells; these observations correlate with previous observations in our laboratory showing less IL-27 receptors on CD4 T cells than CD8 counterparts. Our project determined the distinct expression of SOCS proteins in different human T cells subsets. This study could highlight the mechanism of action of cytokines such as IFN-β and IL-27.

SOCS-1

SOCS-3

lymphocytes T CD8

lymphocytes T CD4

Interféron-béta

Interleukine-27

Sclérose en plaques

SOCS-1

SOCS-3

CD8 T lymphocytes

CD4 T lymphocytes

Interferon-beta

Interleukin-27

Multiple sclerosis

Novo papel da galectina-1 como molécula efetora de células citotóxicas. / New role for galectin-1 as effector molecule of cytotoxic cells.

Machado, Tiago Clemente

18 March 2014

A exocitose de grânulos secretórios é o principal mecanismo efetor de células TCD8+. No entanto, pouco se sabe sobre a composição dos grânulos líticos dessas células. Resultados prévios do nosso grupo identificaram algumas dezenas de novas proteínas desses grânulos. Dentre elas foi identificada Gal-1. A literatura relata que Gal-1 age por via exógena através de sua secreção por via não convencional. Dados iniciais do nosso grupo apontam um novo cenário para esta proteína no qual ela está presente em grânulos citotóxicos. Através das técnicas de microscopia eletrônica e confocal e de ensaios de citotoxicidade, nossos resultados sugerem que Gal-1 participa do papel citotóxico das CTLs modulando a via dos receptores de morte FAS-FASL. Nós também mostramos que Gal-1 interfere com o tempo de contato entre APCs e linfócitos TCD8+, com a ativação dessas células e com o controle da proliferação dos linfócitos. Nossos resultados apontam um novo cenário para Gal-1, no qual ela está presente em grânulos líticos das CTLs e está relacionada a resposta efetora dessas células. / Exocytosis of secretory granules is the main effector mechanism of CD8+ T cells. In particular, little is known about CTLs lytic granules composition. Previous results from our group identified a few dozens of new proteins associated with these granules. Among them, we identified galectin-1. Literature reports the extracellular action of Gal-1. Initial data from our group suggested a new scenario for this protein, since Gal-1 was found inside cytotoxic granules. Here, we show by transmission electron and confocal laser scanning microscopy and cytotoxicity assays that Gal-1 has a role on CTL killing probably mediating the FAS-FASL pathway. We also show that Gal-1 is regulates the time of contact between APCs and TCD8+ lymphocytes, the activation of APCs and the proliferation of CD8 T cells. Taken together, our findings suggest a new scenario, in which Gal-1 is present in CTL granules and participates in cytotoxic effector response.

CD8+ T lymphocytes

Cell proliferation

Cellular cytotoxicity

Célula NK

Células citotóxicas

Citotoxicidade celular

Cytotoxic cells

FAS-FASL

FAS-FASL

Galectin-1

Galectina-1

Linfócito TCD8+

Lisossomos secretórios

NK cell

Proliferação celular

Secretory lysosomes

Infections virales par l’Hépatite E et Zika : pathogenèse à l’interface mère-fœtus et rôle de la réponse immune / Hepatitis E and Zika viral infections : pathogenesis at the maternal-fetal interface and Interplay with the immune response

Gouilly, Jordi

26 November 2018

Durant la grossesse, le fœtus est séparé de la mère par le placenta qui constitue une barrière protectrice efficace. Cependant, cette barrière n’est pas totalement imperméable et permet de nombreux échanges (nutriments, hormones, déchets, ...) dans des zones bien spécifiques nommées interfaces materno-fœtales. Au niveau de ces zones, les cellules fœtales entrent en contact direct avec le sang et les tissus maternels. Parmi ces interfaces, on trouve notamment la decidua basalis (paroi de l’endomètre gestant) où les villosités choriales du placenta s’ancrent profondément et l’espace intervilleux où les villosités flottantes sont baignées par le sang maternel. L’accès au placenta au niveau de ces interfaces est un processus finement régulé par de nombreux mécanismes. Cependant, certains pathogènes qui infectent la mère peuvent détourner ces mécanismes, franchir la barrière placentaire et se disséminer au fœtus. La famille des pathogènes TORCH (Toxoplasmosis, Others, Rubella, Cytomegalovirus et Herpes) est la plus connue pour induire des infections congénitales. Cependant d’autres virus moins connus ou émergents sont aussi capables d’infecter les interfaces mère-fœtus et de causer des complications graves pouvant être fatales pour la mère et le fœtus. Parmi ces virus, on retrouve notamment le virus de l’Hépatite E (VHE) et le virus Zika (ZIKV). C’est dans ce contexte que s’insèrent mes travaux de thèse qui s’articulent autour de trois axes. Dans la première partie de ma thèse, nous nous sommes intéressés à la pathogenèse du VHE et du ZIKV à l’interface mère-fœtus en identifiant les cibles cellulaires des virus et en caractérisant les conséquences fonctionnelles de l’infection. Dans la seconde partie, nous avons étudié la fonction des cellules Natural Killer déciduales (dNK), qui représentent 30% des cellules de la decidua basalis. Ces cellules dNK ne sont pas cytotoxiques durant une grossesse physiologique mais elles sécrètent de nombreux facteurs solubles essentiels au bon déroulement de la grossesse. Nous avons démontré que les fonctions effectrices des cellules dNK sont directement régulées et dictées par le microenvironnement décidual. De plus, nous avons découvert que les cellules dNK sont capables de détecter et de limiter l’infection des cellules stromales déciduales par le ZIKV. Enfin, dans la dernière partie, nous nous sommes intéressés à la pathogenèse de l’infection par le VHE dans un autre groupe de patients à haut risque de formes graves, les personnes âgées. Nous avons alors mis en évidence que le développement de formes sévères est associé à l’émergence d’une population de lymphocytes T CD8 caractérisée par un fort état d’activation associé à des défauts fonctionnels. En conclusion, mes travaux de thèse ont permis de mieux comprendre la pathogenèse du VHE et du ZIKV durant la grossesse et au-delà. De plus, ils ont participé à prouver l’importance du microenvironnement local dans le contrôle de la plasticité des cellules immunitaires. / During pregnancy, the fetus is isolated from the mother by the placenta, which constitutes an efficient protective barrier. However, this barrier is not completely impermeable and allows various exchanges (nutrients, hormones, wastes …) in specific areas called maternal-fetal interfaces. In these areas, fetal cells are in direct contact with maternal blood and tissues. Among these interfaces, we can distinguish the decidua basalis (gestating endometrium wall) where the placental chorionic villi are deeply anchored, and the intervillous space where the floating villi bathe in the maternal blood. The access to the placenta is a process tightly regulated by different mechanisms. However, some pathogens that infect the mother can subvert these mechanisms, cross the placental barrier, and spread to the fetus. The family of TORCH pathogens (Toxoplasmosis, Others, Rubella, Cytomegalovirus and Herpes) is best known for inducing such congenital infections. Alternatively, other less known or emerging viruses like Hepatitis E virus (HEV) and Zika virus (ZIKV) are also able to infect the maternal-fetal interface and cause severe outcomes that can be lethal for both the mother and the fetus. It’s in this context that fit my thesis work, articulated around three research axes. In the first part of my work, we focused on the pathogenesis of HEV and ZIKV at the maternal-fetal interface by identifying the cellular targets of the viruses and deciphering the functional consequences of their infection. Then, we studied the role of the decidual Natural Killer (dNK) cells, which account for 30% of total cells within the decidua basalis. These dNK cells are devoid of cytotoxic function in healthy conditions but they rather secrete various soluble factors that are essential for the success of pregnancy. In the second part of my work, we demonstrated that the decidual microenvironment dictates and regulates the effector functions of dNK cells. Moreover, we found that dNK cells are able to detect and limit the infection of decidual stromal cells by ZIKV. Finally, in a last part, we investigated the pathogenesis of HEV infection in another group of patients at high risk of developing serious forms, the elderly people. Thus, we highlighted that the development of severe forms is associated with the emergence of a population of CD8 T cells characterized by a high activation status associated with functional defects. In conclusion, my thesis work has shed light on the pathogenesis of HEV and ZIKV during pregnancy and beyond. In addition, they helped to demonstrate the importance of the local microenvironment in controlling the plasticity of immune cells.

Interfaces materno-fœtales

Infection congénitale

Réponse immunitaire

Lymphocytes Natural Killer et T CD8

Virus de l’Hépatite E et Zika

Maternal-fetal interfaces

Congenital infection

Immune Response

Natural Killer and CD8 T Lymphocytes

Hepatitis E and Zika viruses

L’impact de la grossesse sur l’amplitude et la diversité de la reconnaissance antigénique des lymphocytes T cytotoxiques dirigés contre le VIH-1

Jolette, Elyse

09 1900

La transmission mère-enfant (TME) du VIH-1 est un des enjeux majeurs de la pandémie. Une meilleure compréhension de la réponse des lymphocytes T cytotoxiques CD8+ (LTC) VIH-spécifiques lors de la grossesse facilitera le design de stratégies optimales pour diminuer la TME. Notre objectif est donc de caractériser l’amplitude et la diversité de la reconnaissance antigénique des LTC VIH-spécifiques avant, pendant et après la grossesse chez des femmes infectées par le VIH-1. Nos résultats montrent pour la première fois que l’initiation et la progression de la grossesse, à elles seules, n'ont que peu d’influence sur l’amplitude et la diversité de la reconnaissance antigénique des réponses LTC en termes de production d’IFN‐. Ces résultats indiquent que les femmes infectées par le VIH conservent une immunocompétence durant leur grossesse, du moins dans le contexte d’un traitement antirétroviral efficace. Ceci pourrait éventuellement aider à promouvoir l’immunisation comme stratégie pour prévenir la TME du VIH‐1. / Mother-to-child transmission (MTCT) of HIV-1 is one of the major issues of the pandemic. Characterization of HIV-specific immunity during pregnancy, especially cytotoxic CD8+ T lymphocytes (CTL), will lead to a better understanding of HIV pathogenesis and facilitate design of optimal strategies to prevent MTCT. Our objective is to describe the magnitude and the breadth of antigen recognition of HIV-specific CTL responses before, throughout and after pregnancy in a group of HIV-infected women. Our results revealed for the first time that initiation of pregnancy by itself doesn’t change the magnitude of CTL responses in terms of IFN- production. These findings support the fact that HIV-infected women maintain immunocompetence throughout gestation, at least in the context of effective antiretroviral treatment. These results provide a novel understanding of the dynamics of HIV-specific CTL responses during pregnancy and may help to promote maternal immunization as a strategy to prevent MTCT of HIV-1.

Lymphocytes T cytotoxiques CD8+

Cytotoxic CD8+ T lymphocytes

LTC

CTL

VIH

HIV

Grossesse

Pregnancy

ELISpot

IFN-γ

Gag

Transmission mère-enfant

Mother-to-child transmission

TME

MTCT

Expression des SOCS-1 et SOCS-3 par les lymphocytes T humains en réponse à des cytokines immuno-modulatrices

El-Khoury, Lama

07 1900

Les cytokines jouent un rôle fondamental dans la régulation des processus biologiques via la cascade de signalisation JAK-STAT. Les « Suppressors of Cytokine Signalling » (SOCS), protéines intracellulaires, inhibent la voie JAK-STAT. Plusieurs études supportent leur implication dans des maladies immunitaires, mais peu d’informations sont disponibles sur leur expression par les lymphocytes T humains. Nous postulons que les cytokines Interféron-β(IFN-β) et Interleukine-27 (IL-27), dotées d’un potentiel immuno-régulateur, ont des rôles bénéfiques via l’induction des SOCS. L’impact de l’IFN-β et l’IL-27 sur l’expression des SOCS-1 et SOCS-3 par des cellules T CD8 et CD4 humaines a été étudié en utilisant des cellules sanguines de donneurs sains. L’expression de ces régulateurs a été évaluée aux niveaux de l’ARNm par qRT-PCR et protéique par immunocytochimie. Les SOCS-1 et SOCS-3 ont été rapidement induits en ARNm dans les deux types cellulaires en réponse à l’IFN-β ou l’IL-27 et une augmentation de l’expression a été confirmée au niveau protéique. Afin de mimer les thérapies à base d’IFN-β, les cellules T ont été exposées chroniquement à l’IFN-β. Après chaque ajout de cytokine les cellules T ont augmenté l’expression du SOCS-1, sans moduler le SOCS-3. L’IL-27 a induit les SOCS-1 et SOCS-3 préférentiellement dans les cellules T CD8 ; ceci corrèle avec des résultats du laboratoire démontrant une plus petite expression des récepteurs à l’IL-27 par les lymphocytes T CD4 que les CD8. Notre projet a permis d’élucider l’expression des SOCS dans deux populations de cellules T et de clarifier les mécanismes d’actions de l’IFN-β et l’IL-27. / Cytokines regulate fundamental biological processes via the JAK-STAT signaling pathway. Suppressors of Cytokine Signaling proteins (SOCS), intracellular proteins, inhibit the JAK-STAT pathway. Emerging evidence supports the involvement of SOCS in diseases of the immune system but no data is available regarding their expression in human T cells. We postulate that the cytokines Interferon-β (IFN-β) and Interleukin-27 (IL-27), both potential immuno-regulators, have beneficial roles through the induction of SOCS proteins. The impact of IFN-β and IL-27 on the SOCS-1 and SOCS-3 expression by human CD4 and CD8 T cells was assessed using peripheral blood mononuclear cells from healthy donors. We evaluated the expression of SOCS-1 and SOCS-3 at the mRNA level by qRTPCR and at the protein level by immunocytochemistry. A rapid increase of SOCS-1 and SOCS-3 mRNA levels was observed upon cytokine addition, and such upregulation was confirmed at the protein level. To mimic patients under IFN-β treatment, both T cell subsets were chronically exposed to IFN-β. We observed an increase of SOCS-1 after each stimulation but not for SOCS-3. IL-27 stimulation increased SOCS-1 and SOCS-3 mRNA levels in CD8 T cells but only slightly in CD4 T cells; these observations correlate with previous observations in our laboratory showing less IL-27 receptors on CD4 T cells than CD8 counterparts. Our project determined the distinct expression of SOCS proteins in different human T cells subsets. This study could highlight the mechanism of action of cytokines such as IFN-β and IL-27.

SOCS-1

SOCS-3

lymphocytes T CD8

lymphocytes T CD4

Interféron-béta

Interleukine-27

Sclérose en plaques

SOCS-1

SOCS-3

CD8 T lymphocytes

CD4 T lymphocytes

Interferon-beta

Interleukin-27

Multiple sclerosis

Valor progn?stico de c?lulas TCD8+ E natural killer em carcinoma epiderm?ide oral e orofaringeano tratado com radioterapia e quimioterapia

Santos, Edilmar de Moura

09 February 2012

Made available in DSpace on 2014-12-17T15:32:21Z (GMT). No. of bitstreams: 1 EdilmarMS_DISSERT.pdf: 790528 bytes, checksum: 570c185c018d55b199d467de6ca18465 (MD5) Previous issue date: 2012-02-09 / Coordena??o de Aperfei?oamento de Pessoal de N?vel Superior / The most common malignant neoplasm of the oral cavity and oropharynx are squamous cell carcinoma. Injuries to the same stage and subjected to the same treatment protocol have sometimes different evolutionary courses. The scope of this study was to investigate, through a retrospective cohort, associations between the number of CD8 + T cells and natural killer, identified immunohistochemically in the inflammatory infiltrate in a series of cases of oral squamous cell carcinoma and orofaringeano, and the level of tumor response to radiotherapy and chemotherapy, overall survival and relapse-free survival of patients. We identified 54 patients with unresectable disease were treated exclusively with radiotherapy and chemotherapy. The median follow-up was 22 months. The sample was characterized by the predominance of male subjects, median age 60 years, all were smokers. The most frequent site was the tongue and 81.5% were in stage IV. Patients with disease in the oral cavity had a worse response to treatment (p = 0.006), worse relapse-free survival (p = 0.007), worse overall survival (p = 0.007). The advanced T stage was shown a negative prognostic factor (p= 0.006) for the clinical treatment response made. Immunohistochemistry was performed to select CD8 + cells (anti-CD8) and NK cells (anti-CD57). Lymphocytes positive and negative markings were counted using the program ImageJ ?. Two groups were created for each marking evaluated: Group I patients with more than 50% cells positive, Group II: less than 50% of labeled cells. For CD8 + cells detected in 38 (70.3%) of Group I were CD8 + and 16 (29.7%) Group II CD8 +. For NK cells, 26 (48.15%) Group I NK and 28 (51.85%) Group II NK. Regarding the clinical response to treatment, we observed that 39% of patients achieved a complete response and 25.9% remained without recurrence at the end of follow-up. These results were better in Group I CD8 + (p = 0.2). Identified that 72.2% of patients progressed to death, this finding had no association with the immunohistochemical data. There was no statistically significant differences between the number of CD8 + and NK cells and the ability of tumor response to radiotherapy and chemotherapy, or with overall survival and relapse-free survival of patients. However, especially in relation to a learned response, we found that this group of patients with advanced disease have a low count of CD8 + T cells active. Believing in the role that the immune response plays in the local fight against neoplastic cells, however, our results do not support the use of quantitative analysis of CD8 + T cells and NK cells as a prognostic factors for oral squamous cell carcinoma and oropharynx / A neoplasia maligna mais frequente da cavidade oral e da orofaringe ? o carcinoma epiderm?ide. Les?es com o mesmo estadiamento e submetidas ao mesmo protocolo terap?utico apresentam, por vezes, cursos evolutivos diferentes. O escopo do presente trabalho foi investigar, atrav?s de um coorte retrospectivo, associa??es entre a quantidade de c?lulas TCD8+ e natural killer, identificadas imuno-histoquimicamente no infiltrado inflamat?rio de uma s?rie de casos de carcinoma epiderm?ide oral e orofaringeano, e o n?vel de resposta tumoral ao tratamento radioter?pico e quimioter?pico, a sobrevida global e sobrevida livre de recidiva dos pacientes. Foram identificados 54 pacientes com doen?a irressec?vel, tratados exclusivamente com radioterapia e quimioterapia. A mediana de seguimento foi de 22 meses. A amostra se caracterizou pelo predom?nio de indiv?duos masculinos, com idade mediana de 60 anos; todos eram tabagistas. O s?tio mais frequente foi a l?ngua oral e 81,5% encontravam-se no est?dio IV. Os pacientes com doen?a na cavidade oral tiveram uma pior resposta ao tratamento (p=0,006), pior sobrevida livre de recidiva (p=0,007), pior sobrevida global (p=0,007). O est?dio T avan?ado se demonstrou um fator progn?stico negativo (p=0,006) para a resposta ao tratamento cl?nico efetuado. Foi realizada imuno-histoqu?mica para marcar c?lulas CD8+ (anti-CD8) e c?lulas NK (anti-CD57). Os linf?citos positivos e negativos para as marca??es foram contados atrav?s do programa ImageJ?. Dois grupos foram criados para cada marca??o avaliada: Grupo I: pacientes com mais de 50% das c?lulas positivas; Grupo II: menos de 50% das c?lulas marcadas. Para as c?lulas CD8+ detectamos que 38 (70,3%) eram do Grupo I CD8+ e 16 (29,7%) do Grupo II CD8+. Para as c?lulas NK, 26 (48,15%) Grupo I NK e 28 (51,85%) Grupo II NK. Em rela??o ? resposta cl?nica ao tratamento, observamos que 39% dos pacientes obtiveram resposta completa e 25,9% permaneceram sem recidiva ao final do seguimento. Esses resultados foram melhores no Grupo I CD8+ (p=0,2). Identificamos que 72,2% dos pacientes evolu?ram para o ?bito, esse achado n?o teve associa??o com os dados imuno-histoqu?micos. N?o se observou diferen?as estatisticamente significantes entre a quantidade de c?lulas CD8+ e NK e a capacidade de resposta tumoral ao tratamento radioter?pico e quimioter?pico, nem com a sobrevida global e sobrevida livre de recidiva dos pacientes. Contudo, principalmente em rela??o a resposta adquirida, detectamos que este grupo de pacientes com doen?a avan?ada tem uma baixa contagem de c?lulas TCD8+ ativas. Acreditando no papel fundamental que a resposta imune exerce no combate local ?s c?lulas neopl?sicas; no entanto, nossos resultados n?o suportam a utiliza??o da an?lise quantitativa das c?lulas TCD8+ e NK como um dos fatores progn?sticos para o carcinoma epiderm?ide oral e de orofaringe

Carcinoma epiderm?ide

C?ncer oral e orofaringeano

Linf?citos TCD8

C?lulas natural killer

Squamous cell carcinoma

Oral and oropharyngeal cancer

CD8 T Lymphocytes

Natural killer cells

CNPQ::CIENCIAS DA SAUDE::ODONTOLOGIA