Global ETD Search

221	Células Natural Killer na modulação da imunidade celular em humanos. / Natural Killer cells in the modulation of cell-mediated immunity in humans. Salomon, Maria Alejandra Clavijo 17 August 2016 (has links) Células dendríticas (DCs) são componentes centrais da imunidade celular, responsáveis pelo priming de linfócitos T naïve. A polarização de linfócitos T é restrita aos sinais fornecidos durante a apresentação do antígeno. Além desses sinais, a origem e natureza de DCs que induzem diferentes perfis de linfócitos T não é totalmente compreendida. Foi investigada a capacidade de células Natural Killer (NK) de modular estágios iniciais da diferenciação de monócitos em DCs e de impactar na sua função de primar e polarizar linfócitos T naïve. DCs derivadas de monócitos pré-co-cultivados com células NK favorecem o priming de linfócitos T CD8 do tipo Tc1/Tc17, com potente capacidade de produção de IFN-γ. Este fenômeno foi dependente de interações longas via NKp30 e da maquinaria citotóxica de células NK desencadeada nas etapas inicias da sua interação com monócitos. Esta interação pode ter implicações na compreensão da imunidade mediada por linfócitos T CD8 e pode ser explorada para imunoterapia em que a produção de IFN-γ por células T CD8 é necessária ou exacerbada. / Dendritic cells (DCs) are central components of cellular immunity, responsible for the priming of naïve T cells. The polarization of T cells is restricted to signals provided during antigen presentation. Besides such signals, the origin and nature of DCs that induce different T cell profiles is not fully understood. The ability of natural killer cells (NK) to modulate early stages of monocytes differentiation into DCs and to impact on DCs function to prime and polarize naïve T cells was investigated. DCs derived from monocytes co-cultured with NK cells support the priming of type Tc1/Tc17 CD8 T cells with potent IFN-γ production capacity. NK cell-mediated cytotoxicity triggered at early stages of NKp30-dependent long-lasting monocytes-NK-cells interactions, mediated the mechanism by which this phenomenon occurred. This interaction may have implications in the understanding of CD8 T cell-mediated immunity and can be exploited for immunotherapy in which IFN-γ production by CD8 T cells is required or exacerbated. CD8 T cells Células dendríticas Células Natural Killer Dendritic cells IFN-γ IFN-γ Linfócitos T CD8 Monócitos Monocytes Natural Killer cells NKp30 NKp30
222	Avaliação de aspectos inatos e adaptativos do sistema imune na psoríase: análise fenotípica e funcional de células natural killer e células T / Innate and adaptive features of the immune system in psoriasis: phenotypic and functional analyses of natural killer cells and T cells Batista, Mariana Dias 06 December 2012 (has links) INTRODUÇÃO: A psoríase é doença inflamatória hiperproliferativa da pele, na qual mecanismos imunológicos são cruciais para o processo patogênico. O marcador CD57 denota inabilidade de replicação e imuno-senescência de células T CD8+, e sua expressão foi demonstrada em diversas condições inflamatórias. CD57 também pode ser expresso por células natural killer (NK), nas quais é considerado marcador de maturidade, por ser em geral adquirido pelas formas mais diferenciadas CD56+CD16+. A expressão de CD57 e outros receptores de células NK não foi amplamente investigada na psoríase. OBJETIVOS: Este estudo buscou examinar o fenótipo de células NK em biópsias de pele e células mononucleares do sangue periférico (CMSP) de pacientes com psoríase em relação a controles sadios. Este estudo investigou também o fenótipo e características funcionais de células T isoladas da pele lesional e não afetada de pacientes com psoríase. MÉTODOS: Foram isoladas células NK dos subtipos CD56+CD16- e CD56+CD16+ de pele lesional, não afetada e CMSP de pacientes com psoríase, comparadas com pele normal e CMSP de controles sadios. A expressão de CD57, NKG2A e NKG2C foi determinada nesses subtipos de células por citometria de fluxo. Células T CD4+ e CD8+ foram isoladas da pele lesional e não afetada de pacientes com psoríase, e a expressão de CD57 foi avaliada. Características funcionais de células T foram estudadas através da análise da secreção de diversas citocinas inflamatórias (IL-17A, IFN-\", IL-2, IL-33, TNF- #, IL-21, IL-22 and IL-27) produzidas por células T CD4+ e CD8+ isoladas por sorting celular, a partir de amostras de pele lesional e não afetada de pacientes com psoríase. RESULTADOS: Células NK isoladas das lesões de psoríase apresentaram um fenótipo particular, caracterizado por baixa expressão de CD57 e alta expressão de NKG2A na pele lesional e não afetada em relação aos controles. Em relação às células T, encontrouse frequência de células T CD4+CD57+ e CD8+CD57+ significativamente maior na pele não afetada em relação à pele lesional de pacientes com psoríase. Células T CD4+ isoladas por sorting celular a partir de amostras de pele lesional produziram níveis maiores de IL-17A, IL-22 e IFN-\" em relação às amostras de pele não afetada. Células T CD8+ isoladas da pele lesional secretaram maiores níveis de IL-17A, IFN-\", TNF-# e IL- 2 em relação à pele não afetada. CONCLUSÕES: Esses dados sugerem que células NK presentes nas lesões de psoríase apresentam fenótipo imaturo, que foi previamente associado a maiores capacidades funcionais, e poderiam ser implicadas na patogênese da psoríase. Em relação às células T, as características fenotípicas sugerem menor sobrevivência de células com baixa capacidade replicativa na pele lesional, pelo ambiente inflamatório local ou pelo alto turnover celular da psoríase / INTRODUCTION: Psoriasis is a hyper-proliferative inflammatory disease of the skin in which immunological mechanisms play a direct role in disease pathogenesis. CD57 is a marker of replicative inability and immunosenescence on CD8+ T cells and its expression is increased in a number of inflammatory conditions. CD57 is also expressed by NK cells and is considered a marker of NK cell maturity, being acquired by more differentiated CD56+CD16+ NK cells. The expression of CD57 and other NK cell markers in psoriasis has not been thoroughly investigated. OBJECTIVES: This study sought to examine the phenotype of NK cells in skin biopsies and peripheral blood mononuclear cells (PBMC) from patients with psoriasis and healthy controls. We also investigated the phenotype and functional characteristics of T cells from psoriasis patients, comparing lesional and unaffected skin. METHODS: CD56+CD16- and CD56+CD16+ NK cells were isolated from lesional skin, unaffected skin and PBMC of psoriasis patients, and normal skin and PBMC from healthy controls. The expression of CD57, NKG2A, and NKG2C was assessed by flow cytometry. CD57 expression was also determined on T cells from lesional and unaffected skin by flow cytometry. We assessed functional characteristics of T cells by evaluating the secretion of several inflammatory cytokines (IL-17A, IFN-\", IL- 2, IL-33, TNF-#, IL-21, IL-22 and IL-27), from cell-sorted purified CD4+ and CD8+ T cells isolated from lesional and unaffected skin of psoriasis patients, by multiplex assays. RESULTS: NK cells in psoriasis skin lesions exhibited a distinct phenotype, with CD57 expression significantly reduced and NKG2A expression increased on NK cells in lesional and unaffected skin compared to controls. In relation to T cells, we observed that the frequency of CD57+CD4+ and CD57+CD8+ T cells was significantly increased in unaffected skin of psoriasis patients compared to lesional skin. Sorted CD4+ T cells from psoriasis lesional skin produced higher levels of IL-17A, IL-22 and IFN-\" compared to unaffected skin. CD8+ T cells isolated from lesional skin produced higher levels of IL- 17A, IFN-\", TNF-# and IL-2 compared to unaffected skin. CONCLUSIONS: These data suggest that NK cells in psoriasis lesions exhibit an immature phenotype, that has been previously associated with higher functional abilities, and could implicate NK cells in psoriasis pathogenesis. For T cells, the findings of this study suggest lower survival of cells with low replicative ability in lesional skin, due to the local inflammatory environment or to the high cellular turnover in psoriasis Adaptive immunity Antígenos CD57 CD57 Células natural-killer Citocinas Cytokines Imunidade adaptativa Imunidade inata Innate immunity Natural killer cells NKG2A NKG2A Psoríase Psoriasis
223	Mechanism and efficacy of a GD2-specific immunotherapy using NK cells Seidel, Diana 27 February 2015 (has links) Das Neuroblastom (NB) ist ein solider, extrakranieller Tumor neuroektodermalen Ursprungs, der sich im Kleinkindalter manifestiert. Ein etabliertes Zielantigen für die passive Immuntherapie beim NB ist das Disialogangliosid GD2. Aufgrund der geringen oder fehlenden Expression von MHC Klasse I Molekülen sowie der Tatsache, dass die Lyse von NB-Zellen durch verschiedene Mechanismen der natürlichen Zytotoxizität von NK-Zellen vermittelt werden kann, stellt eine auf NK-Zellen basierende Therapie einen vielversprechenden Ansatz zur Behandlung dieser Erkrankung dar. Auf dieser Grundlage wurde eine NK-Zelllinie generiert, die einen GD2-spezifischen chimären Antigenrezeptor (CAR) exprimiert (NK-92-scFv(ch14.18)-zeta). Die Hauptbestandteile dieses CARs sind ein Einzelkettenantikörper, welcher die variablen Regionen des GD2-spezifischen Antikörpers ch14.18 enthält, und die CD3ζ-Kette als signaltransduzierende Komponente. Im Rahmen dieser Arbeit konnte gezeigt werden, dass NK-92-scFv(ch14.18)-zeta in der Lage sind, auch Chemotherapie-resistente GD2-positive NB-Zelllinien effektiv abzutöten und dass dabei die Interaktion des CARs mit GD2 den Hauptmechanismus darstellt. Die anti-tumorale Wirkung von NK-92-scFv(ch14.18)-zeta in vivo wurde in einem Chemotherapie-resistenten GD2-positiven Xenograft-Mausmodell gezeigt. Die wiederholte Applikation von NK-92-scFv(ch14.18)-zeta in Kombination mit IL-2 resultierte in einem signifikant verlangsamten Tumorwachstum und einem verbesserten Überleben. Die Ergebnisse dieser Arbeit belegen, dass GD2-spezifische NK-92 das Potential für eine zukünftige klinische Anwendung besitzen. Demnach stellt der Einsatz einer solchen GD2-spezifischen NK-Zelllinie, die unter GMP-Bedingungen expandiert werden kann und zu jeder Zeit in einer standardisierten Qualität verfügbar wäre, eine vielversprechende Alternative zur Behandlung von Hochrisikopatienten dar, deren Erkrankung nicht mehr auf die Standardtherapie anspricht. / Neuroblastoma (NB) is a solid extracranial childhood malignancy of neuroectodermal origin. The Disialoganglioside GD2 is an established antigen for passive immunotherapy of NB. Cellular therapy of NB with natural killer (NK) cells is especially appealing because MHC class I expression is absent or low in most NB, rendering this tumor sensitive to NK cell recognition. Additionally, natural cytotoxicity of NK cells, mediated by interaction of activating NK cell receptors and their respective ligands on tumor cells, has been shown to play a role in lysis of NB cells. It is therefore tempting to assume that a combination of passive immunotherapy with GD2-specific antibodies and adoptive transfer of NK effector cells would result in an improved NB therapy. To achieve this goal an NK cell line expressing a GD2-specific chimeric antigen receptor (CAR) was engineered: NK-92-scFv(ch14.18)-zeta. This CAR consists of a GD2-specific scFv-fragment, which was generated from ch14.18, and the CD3ζ-chain as intracellular signal-transducing domain. Within this thesis, GD2-specificity of NK-92-scFv(ch14.18)-zeta as well as efficacy towards GD2-expressing NB cell lines, including relapse cell lines that exhibit partial or multidrug resistance were demonstrated. Blocking the interaction between the CAR and GD2 resulted in almost complete abrogation of NK-92-scFv(ch14.18)-zeta-mediated lysis of GD2-positive NB cell lines in vitro, indicating that this interaction is the main mechanism of activation of NK-92-scFv(ch14.18)-zeta. Importantly, repeated application of NK-92-scFv(ch14.18)-zeta in combination with IL-2 significantly decreased tumor growth and prolonged survival of mice in an aggressively growing drug-resistant xenograft NB mouse model. These findings suggest that GD2-specific NK-92 has potential for a future clinical application as NB-specific effector cells that would be ready on demand in a standardized quality. Neuroblastom Immuntherapie Disialogangliosid Natürliche Killer-Zellen immunotherapy neuroblastoma Disialoganglioside natural killer cells 570 Biowissenschaften, Biologie 32 Biologie XH 2393 ddc:570
224	Interações entre orcas Orcinus orca (Linnaeus, 1758) e falsas orcas Pseudorca crassidens (Owen, 1846) com a pesca de espinhel pelágico monofilamento no Atlântico Oeste Tropical CHARLES, William Dantas 15 February 2007 (has links) Submitted by (edna.saturno@ufrpe.br) on 2017-02-23T12:25:14Z No. of bitstreams: 1 Williams Dantas Charles.pdf: 2829415 bytes, checksum: bf5d0ed2319bb047d509bf6837ebad7e (MD5) / Made available in DSpace on 2017-02-23T12:25:14Z (GMT). No. of bitstreams: 1 Williams Dantas Charles.pdf: 2829415 bytes, checksum: bf5d0ed2319bb047d509bf6837ebad7e (MD5) Previous issue date: 2007-02-15 / Since 50`s, industrial fisheries have been damaged by cetaceans in all oceans, with different intensity levels. According to specialists, this behavior is named depredation, which occurs when the animals eat the fishes caught by a fishing gear. Killer whale has been cited as an animal that shows this kind of behavior often, otherwise other species as a false killer whale or sperm whale have been recorded doing fishing gear interactions. After the creation of the On Board Observers Program (PROBORDO) it was possible to cover all tuna fleet working in northeast of Brazil, based on Natal-RN, Cabedelo-PB and Recife-PE ports. The covering was made by board observers that get important information to the fisheries dynamic knowledge made by pelagic long line. Interactions between false killer whales and killer whales are cited as an important scientific subject, in relation to these fisheries type, that the present study pretends to show up. Factors like interactions type, groups’ size, qualitative and quantitative descriptions of depredated fishes and spatial location of the interactions were analyzed. The false killer whale showed greater occurrence on the study area than other species, generally within groups of few individuals, however, there were situations that the group was composed by hundreds of individuals. This species showed food preference about the target species of this fisheries kind, in other words, tuna and swordfishes instead of others catched, but in case of low productivity, they feed with squid used as a bait on the hooks. Killer whales were observed in the Tropical Western Atlantic, interacting with the fisheries. Also, there were accidental catches of the cited cetaceans by the fishing gear, what can bring serious damage to the individuals caughted. / Desde a década de 50, a indústria pesqueira vem sofrendo perdas provocadas por cetáceos, em todos os oceanos, com diferentes níveis de intensidade, num comportamento denominado pelos especialistas como depredação, que ocorre quando esses animais se alimentam do peixe capturado pela arte de pesca. Orcas verdadeiras têm sido citadas como as que exibem esse comportamento com maior freqüência, porém outras espécies como as falsas orcas e cachalotes, são registradas interagindo com a pesca. Com a criação do Programa de Observadores de Bordo (PROBORDO) foi possível a cobertura de toda a frota atuneira arrendada que opera no nordeste, sediada nos portos de Natal-RN, Cabedelo-PB e Recife-PE por observadores de bordo, que coletam informações relevantes para o conhecimento da dinâmica da pesca realizada com espinhel pelágico monofilamento. Dentre os assuntos de grande valor científico cita-se a ocorrência de interações entre as falsas orcas e as orcas verdadeiras, com esse tipo de pescaria, que o presente trabalho pretende apresentar. Fatores como o tipo de interação, tamanho de grupo, descrição quali-quantitativa dos peixes depredados e localização espacial das interações, foram analisados. A falsa orca apresentou maior ocorrência na área de estudo, geralmente em grupos de poucos indivíduos, porém houve situações em que o grupo era composto por centenas de espécimens. Elas demonstraram preferência alimentar pelas espécies-alvo deste tipo de pescaria, ou seja, atuns e espadartes em detrimento da fauna acompanhante, mas no caso de produtividade baixa, também se alimentavam das lulas, utilizadas nos anzóis como isca. Orcas verdadeiras também foram observadas na região do Atlântico oeste tropical, interagindo com a pesca. Também houveram capturas dos referidos cetáceos pelo espinhel, o que pode causar danos sérios aos espécimens capturados. Orca Falsa - orca Espinhel Cetáceo Interação Orcinus orca Pseudorca crassidens Killer whales False killer whales Interaction Longline
225	Estudo do polimorfismo dos genes KIR na esclerose sistêmica Salim, Patrícia Hartstein January 2009 (has links) As células Natural Killer (NK) fazem parte da resposta imune inata, sendo a primeira linha de defesa do organismo contra vírus, bactérias, tumores e microorganismos. Estas células induzem a morte da célula-alvo quando não há o reconhecimento das moléculas de antígenos leucocitários humanos (HLA) de classe I, através de seus receptores, chamados Killer cell Immunoglobulin-like Receptor (KIR). Vários estudos demonstram o envolvimento dos genes KIR na patogênese das doenças auto-imunes. Acredita-se que combinações desses genes possam ser favoráveis para o desenvolvimento da esclerose sistêmica (ES). Portanto, o conhecimento destes genes relacionados às células NK poderiam ser úteis para o entendimento da patogênese da ES. O objetivo deste estudo é investigar o polimorfismo dos genes KIR em um grupo de pacientes com ES, incluindo a forma difusa e limitada da doença. A freqüência do receptor inibidor KIR2DL2 foi significantemente menor nos pacientes comparada com a do grupo controle (28,7% versus 65,2%; P<0,001; OR=0,21; IC95% 0,11–0,38). Quando analisamos a combinação do receptor inibidor 2DL2, com a presença do ativador 2DS2 (KI2DS2+/KIR2DL2-), encontramos uma maior freqüência nos pacientes (26,1% versus 1,7%; P<0,001; OR=19,94; IC95% 4,7–175,1). Por outro lado, a presença de ambos KIR2DL2 e KIR2DS2 foi mais freqüente no grupo controle (26,9% versus 57,3%; P<0,001; OR=0,27; 95%CI 0,1–0,4). Nenhuma diferença estatística no polimorfismo dos genes KIR foi encontrada entre a forma difusa e a forma limitada. A combinação KIR2DS2+/KIR2DL2– parece ser um fator de risco para o desenvolvimento da ES enquanto a alta freqüência do gene inibidor KIR2DL2 no grupo controle parece ter uma função protetora. Estes resultados indicam um potencial papel dos genes KIR na patogênese da ES. / Natural killer (NK) cells have an important role in the early responses to viral infections. They kill diverse target cells with decreased or absent expression of major histocompatibility complex (MHC) class I molecules through the Killer Cell Immunoglobulin-Like Receptors (KIR). Many studies have reported association of KIR genes with autoimmune diseases. The objective of this study is to investigate possible associations of KIR polymorphisms with systemic sclerosis (SSc), including the limited (lSSc) and diffuse (dSSc) forms of the disease. The frequency of inhibitory KIR2DL2 was significantly decreased among patients with SSc compared with healthy controls (28.7% versus 65.2; P<0.001, odds ratio [OR] 0.21, 95% confidence interval [95% CI] 0.11–0.38). When activatory and inhibitory KIR genes were analyzed in combination, the concomitant presence of KIR2DS2 and absence of KIR2DL2 (KI2DS2+/KIR2DL2-) phenotype was more frequent in SSc patients than in the control group (26.08% versus 1.75%; P<0.001, OR=19.94, 95%CI [4.78–175.10]). On the other hand, the presence of both KIR2DS2 and KIR2DL2 was more frequent in the control group (26.96% versus 57.39%; P=0.000005, OR=0.27, 95%CI [0.15–0.49]). No significant difference in KIR genes polymorphisms was found between lSSc and dSSc disease subsets. The combination of KIR2DS2+/KIR2DL2– may be a risk factor for development of SSc while the higher frequency of the inhibitory KIR2DL2 gene in the control group suggest to a protective effect. These results indicate a potential role of KIR genes in the SSc pathogenesis. Escleroderma sistêmico Polimorfismo genético Receptores KIR Células matadoras naturais Autoimunidade Natural killer cell Systemic sclerosis Autoimmunity
226	Estudo do polimorfismo dos genes KIR e HLA em pacientes com câncer de mama e grupo controle Jobim, Maria Regina Sampaio Leite January 2014 (has links) O presente estudo tem como objetivo investigar a frequência dos diversos polimorfismos dos genes KIR (Killer Immunoglobulin-like Receptors) e HLA C1 e C2 em um grupo de pacientes com câncer de mama e comparar com um grupo controle de indivíduos sadios. As células natural killer (NK) são linfócitos que diferem das células T e B e que fazem parte da imunidade natural, reconhecendo as moléculas HLA (Antígenos Leucocitários Humano) de classe I em células infectadas por vírus ou em células tumorais, através de seus receptores de membrana. Os principais receptores das células NK são conhecidos como receptores KIR, sendo codificados por genes localizados no cromossomo 19q13.4 e classificados em grupos funcionais supressores e ativadores. Neste estudo, analisamos 15 genes KIR e alelos do sistema HLA de classe I em 230 pacientes caucasóides e em 278 controles, usando a técnica de PCR com primers específicos (PCR-SSO e PCR-SSP). Nossos resultados demonstraram uma frequência maior do genótipo supressor 2DL2 (P<0,001) em pacientes com câncer de mama, quando comparados ao grupo controle. Os genes HLA-C2 e HLA-BW4 não apresentaram diferenças significantes entre os grupos. Contudo, o gene HLA-C1 foi observado em maior frequência nos pacientes com câncer de mama. Considerando que estes achados sugerem uma potencial associação entre o sistema de genes KIR, HLA classe I e o câncer de mama, estudos adicionais sobre este tema são necessários. / We investigated the frequency of various KIR (Killer Immunoglobulin-like Receptors) and HLA C1 and C2 gene polymorphisms in a group of patients with breast cancer and healthy controls. Natural Killer (NK) cells are lymphocytes that differ from T and B cells and are part of the innate immune system, recognizing class I Human Leukocyte Antigens (HLA) molecules on target cells (virus-infected as well as cancer cells), through specific cell surface receptors. KIR comprises the main class of NK receptors, being encoded by genes located in chromosome 19q13.4. They possess both suppressor and activating functional groups. Fifteen KIR genes and class I HLA alleles obtained from 230 Caucasians patients, as well as 278 controls were studied, using PCR techniques with specific primers (PCR-SSO and PCR-SSP). Our results showed a higher frequency of suppressor genotype 2DL2 (P<0,001) in patients with breast cancer as compared to controls. No significant difference between HLA-C2 and HLA-BW4 alleles were observed between the study groups. Notably, a higher frequency of HLA-C1 gene was noted in patients with breast cancer. Our results suggest a potential association between KIR genes, HLA class I and breast cancer, deserving further investigation. Poliformismo genético Receptores KIR Antígenos HLA Neoplasias da mama Grupos de controle Human leukocyte antigen Natural killer cell Killer cell immunoglobulin-like receptor Breast cancer
227	Regulation of natural killer and cd4+T cell function by NKG2 C-type lectin-like receptors Sáez Borderias, Andrea 20 February 2009 (has links) This work is centered on the study of the NKG2 C-type lectin-like receptors on NK and CD4+T cells. We provide evidence supporting that CD4+T cells specific for Human Cytomegalovirus (HCMV) may express different NK cell receptors, and demonstrate that the C-type lectin-like receptor NKG2D is expressed on cytotoxic CD4+T cells with an effector/memory phenotype, enhancing their TCR-dependent proliferation and cytokine production. A second part of the work is centered on the study of the CD94/NKG2 receptors on NK cells. We show that NKG2A can be induced on NKG2C+ NK cells upon activation with rIL-12 or when cocultured with HCMV-infected dendritic cells, and that NKG2A expression inhibits the response of NKG2C+NK clones against HLA-E-expressing targets, providing a potential regulatory feedback mechanism to control cell activation. Altogether, our results support that expression of NKG2 C-type lectin like receptors may be shaped during the course of viral infections, providing mechanisms to finely regulate both NK and CD4+T cell functions. / Aquesta tesi es centra en l'estudi dels receptors lectina de tipus C NKG2 en cèl·lules Natural Killer i T CD4+. Demostrem que les cèl·lules T CD4+ específiques pel Cytomegalovirus Humà poden expressar diferents receptors NK, i que el receptor lectina tipus C NKG2D s'expressa en cèl·lules citotòxiques i de memòria, potenciant la proliferació i secreció de citocines depenent del TCR. La segona part d'aquesta tesi es centra en l'estudi de l'expressió dels receptors CD94/NKG2 en cèl·lules NK. Mostrem com l'expressió de CD94/NKG2A s'indueix en cèl·lules CD94/NKG2C+ estimulades amb IL-12 o cultivades amb cèl·lules dendrítiques infectades pel Cytomegalovirus Humà, i que l'expressió de CD94/NKG2A inhibeix la resposta de clons NK CD94/NKG2C+ envers dianes HLA-E+, constituint un possible mecanisme de feedback negatiu per controlar l'activació cel·lular. En resum, els nostres resultats demostren que l'expressió dels receptors lectina tipus C NKG2 pot ser modificada durant les infeccions víriques consitutint un possible mecanisme per regular la resposta tant de cèl·lules NK com T CD4+. Human Cytomegalovirus CD94/NKG2 KIR ILT2 NKG2D C-type lectin-like receptors Natural Killer cell Receptors CD4+T cells Natural Killer cells 57
228	Actual and potential host range of Arsenophonus nasoniae in an ecological guild of filth flies and their parasitic wasps Taylor, Graeme Patrick 30 April 2010 (has links) The gammaproteobacterium Arsenophonus nasoniae infects Nasonia vitripennis (Hymenoptera: Pteromalidae), a parasitic wasp that attacks filth flies. This bacterium kills virtually all male offspring of infected females. Female wasps transmit A. nasoniae both vertically (from mother to offspring) and horizontally (to unrelated Nasonia developing in the same fly). This latter mode may enable the bacterium to colonize novel species and spread throughout a filth fly-parasitoid guild. This spread may be important for maintenance of the bacterium. The ecology of novel hosts may be significantly impacted by infection. The actual and potential host range of A. nasoniae was assessed. I used Arsenophonus-specific primers to screen a large sample of filth flies and their parasitoids. The bacterium infects a wide range of wasp species in the environment. The potential host range was determined by inoculating three wasp and one fly species with an isolate of A. nasoniae from Lethbridge, AB. The bacterium successfully infected all insects and was transmitted by two wasp species. It reduced host longevity, but did not kill males, in Trichomalopsis sarcophagae. It also caused pupal mortality in Musca domestica. Arsenophonus nasoniae Nasonia vitripennis horizontal transmission host range house fly endosymbiont male-killer son-killer APSE bacteriophage
229	Etudes pré-clinique et clinique de l'anticorps immunomodulateur Lirilumab visant à augmenter la réponse anti-tumorale des cellules NK / Preclinical and clinical studies of anti-KIR antibody aiming at enhancing anti-tumoral NK cell activity. Thielens, Ariane 17 December 2013 (has links) L’activité anti-tumorale des cellules NK est régulée par des récepteurs de surface activateurs et inhibiteurs qui reconnaissent des ligands exprimés par les cellules cibles. Afin d’augmenter le potentiel cytotoxique des cellules NK face à des cellules cancéreuses autologues, Innate Pharma a développé des Ac bloquant les interactions entre certains récepteurs inhibiteurs de la cellule NK, les KIRs, et leurs ligands, des molécules du CMH de classe I.Dans un premier temps, nous avons mis en place un modèle tumoral d’efficacité des Ac anti-KIR dans des souris transgéniques pour l’expression d’un KIR. Ce modèle nous a permis de démontrer l’efficacité thérapeutique anti-tumorale du blocage des interactions entre les KIRs exprimés par les cellules NK et les molécules HLA exprimées par la tumeur. Ce modèle nous a également permis de tester la combinaison de l’Ac anti-KIR avec un Ac thérapeutique utilisé dans le traitement des lymphomes B non-hodgkiniens, rituximab. Utilisé en combinaison, ces deux Ac augmentent significativement la survie de souris greffées avec une lignée tumorale d’origine B humaine par rapport à chacun des deux traitements seuls.Ces données précliniques nous amènent à proposer une stratégie thérapeutique pour le traitement de tumeurs hématologiques, basée sur la combinaison d’un Ac anti-KIR avec un Ac induisant de l’ADCC afin de potentialiser la réponse anti-tumorale des cellules NK. / NK cell anti-tumoral activity is regulated by inhibitory and activating receptors interacting with target cell ligands. Innate Pharma has developed anti-KIR Abs (IPH2101 and lirilumab), directed against inhibitory NK cell receptors interacting with HLA molecules, in order to increase NK cell activity against autologous tumor cells.We have set up a preclinical model to assess anti-KIR anti-tumoral efficacy in transgenic mice expressing a KIR receptor. With this model, we have also shown the therapeutic benefit of combining lirilumab with rituximab, a therapeutic Ab mediating ADCC.These results support the rationale of combining anti-KIR Ab with Ab mediating ADCC as a therapeutic strategy for hematological malignancies. Cellules NK KIR (Killer Ig-Like Receptors) Immuno-modulation Ac thérapeutique NK cells KIR (Killer Ig-Like Receptors) Immunomodulation Therapeutic Ab 571
230	Role of the actin cytoskeleton in breast cancer cell resistance to natural killer cells / Rôle du cytosquelette d'actine dans la résistance des cellules de cancer du sein à la lyse induite par les cellules "natural killers" Al Absi, Antoun 06 July 2018 (has links) L'évasion immunitaire tumorale joue un rôle central dans la progression tumorale et représente un obstacle majeur au succès des immunothérapies. Dans cette Thèse nous avons étudié le rôle du cytosquelette d’actine dans la résistance des cellules de cancer du sein à la lyse induite par les cellules "natural killers" (NKs). Nous avons trouvé que les cellules de cancer du sein résistantes échappent à l’attaques des cellules NKs par une accumulation importante et rapide d’actine près de la synapse immunologique, un processus que nous avons nommé "réponse actine". Nos analyses mécanistiques suggèrent que la réponse actine induit la polarisation d’autophagosomes vers la synapse immunologique et facilite ainsi la dégradation des molécules cytotoxiques sécrétées par les cellules NKs, tel que le ganzyme B, par autophagie. De plus, la réponse actine est associée au regroupement de ligands inhibiteurs à la synapse, suggérant qu’elle est au centre de plusieurs mécanismes de résistance. Dans leur ensemble, nos résultats constituent une base pour le développement d’approches thérapeutiques visant à interférer avec la réponse actine et à restaurer une réponse immunitaire anti tumorale efficace. / Tumor immune evasion plays a central role in cancer progression and is a major hurdle to effective immunotherapy. In this Thesis, we examine the role of the actin cytoskeleton in breast cancer cell resistance to natural killer (NK) cell-mediated cell lysis. We found that resistant breast cancer cells escape from NK-cell attack through a rapid and prominent accumulation of actin near the immunological synapse, a process we termed the “actin response”. Our mechanistic investigations suggest that the actin response drives autophagosome polarization toward the immunological synapse and thereby facilitates the autophagy-mediated degradation of NK cell-derived cytotoxic molecules such as granzyme B. In addition, the actin response was associated with inhibitory ligand clustering at the immunological synapse, suggesting that it is a common driver of different immune evasion mechanisms. Taken together, our data lays the groundwork for therapeutic approaches aimed at interfering with the actin response and restoring an effective anti-tumor immune response. Cellules Natural Killer Cytosquelette d’actine Cytotoxicité Évasion immunitaire Granzyme B Actin cytoskeleton Breast cancer Cytotoxicity Granzyme B Immune escape Natural killer 572.8 616.99

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