Global ETD Search

11	Role of group 2 innate lymphoid cells in the pathogenesis of bone marrow fibrosis / Roll av medfödda lymfoida celler i grupp 2 i patogenesen av benmärgsfibros Piñero Garasa, Maria Angeles January 2022 (has links) Primär myelofibros (PMF) är en typ av myeloproliferativ neoplasm (MPN) som leder till en progressiv och irreversibel benmärgsfibros. En somatisk mutation, Jak2V617F, har hittats hos 50 % av patienterna med MPN i hematopoetiska stamceller. Nyligen har man upptäckt grupp 2 av medfödda lymfoida celler (ILC2) som tillhör det medfödda systemet. De är T-cellernas motsvarighet men saknar TCR-receptorn. ILC2 reagerar på IL-33 och producerar Il-13. Under de senaste åren har man upptäckt att dessa två cytokiner är inblandade i PMF. För att undersöka ILC2:s roll i utvecklingen av benmärgsfibros in vivo producerade vi retrovirus som uttrycker Jak2 vildtyp (JAK2_WT) eller Jak2V617F (JAK2_V617F) och transducerade benmärg vildtyp (BM_WT) eller benmärg ILC2KO (BM_ILC2KO). Benmärgen transplanterades till subletalt bestrålade immunbristande möss (NOG). Klinikopatologiska drag som är karakteristiska för sjukdomens första stadier, som förhöjda hemoglobinnivåer, megakaryocythyperplasi och betydande trombocytos, uppstod inte under studieperioden. Ökade vita blodkroppar uppstod dock på grund av avsaknaden av ILC2 i JAK2_V617F-expressiva möss. Flödescytometeranalys visade ursprunget till den markerade leukocytosen som ett resultat av expansionen från lymfocytlinjen, mer specifikt B-celler, men resultaten är inte entydiga eftersom de förhöjda nivåerna av B-celler kan vara en följd av ILC2 knock-out fenotypen som förvärras av närvaron av mutationen. Granulocytnivåerna från de inympade cellerna hölls låga till följd av att stamcellerna i värdens benmärg var inblandade på grund av subletal bestrålning. Vi drar slutsatsen att frånvaron av ILC2 i JAK2_V617F-uttryckta benmärgsprogenitorer har en tendens att förvärra den myeloproliferativa fenotypen i sjukdomens tidiga skeden, vilket tyder på en möjlig skyddande roll för ILC2 vid utvecklingen av MPN. / Primary myelofibrosis (PMF) is one type of myeloproliferative neoplasm (MPN) that leads to a progressive and irreversible bone marrow fibrosis. A somatic mutation, Jak2V617F has been found in 50% of patients with MPN in hematopoietic stem cells. Group 2 innate lymphoid cells (ILC2) belonging to the innate system has been recently discovered. They are the counter part of T cells but lacking the TCR receptor. ILC2 response to IL-33 producing Il-13. In recent years, the involvement of these two cytokines in the PMF has been uncovered. To investigate the role of ILC2 in the progression of bone marrow fibrosis in vivo we produced retrovirus expressing Jak2 wild-type (JAK2_WT) or Jak2V617F (JAK2_V617F) and transduced bone marrow wild type (BM_WT) or bone marrow ILC2KO (BM_ILC2KO). The bone marrow was transplanted into sub-lethally irradiated immunodeficient mice (NOG). Clinicopathologic features characteristic from the first stages of the disease, as elevated hemoglobin levels, megakaryocyte hyperplasia and significant thrombocytosis did not emerge during the study period. However, increased in white blood cells arise from the absence of ILC2 in JAK2_V617F expressing mice. Flow cytometer analysis revealed the origin of the marked leukocytosis as a result of the expansion from the lymphocyte lineage, more specifically B cells, but the results are inconclusive as the elevated levels of B-cells could be a consequence of the ILC2 knock-out phenotype aggravated by the presence of the mutation. Granulocyte levels from engrafted cells were kept low because of the involvement of host bone marrow stem cells due to sublethal irradiation. We conclude that the absence of ILC2 in JAK2_V617F-express bone marrow progenitors has a tendency to aggravate the myeloproliferative phenotype in the early stages of the disease, indicating a possible protective role of ILC2 in the development of MPNs. Myeloproliferative neoplasms Primary myelofibrosis Group 2 innate lymphoid cells JAK2 leukocytosis Cell Biology Cellbiologi
12	Humanized Mice as Models to study Human Innate Immunity and Immunotherapies / Les souris humanisées comme modèles d'étude de l'immunité innée humaine et des immunothérapies Lopez-Lastra, Silvia 17 February 2017 (has links) Les modèles animaux ont largement contribué à notre compréhension de l’immunologie humaine et des mécanismes pathologiques associés au développement des maladies. Cependant, les modèles murins ne permettent pas de reproduire toute la complexité des pathologies humaines. Les souris à système immunitaire humain (HIS), par leur capacité à récapituler l’hématopoïèse humaine et à être infectées par des pathogènes humains, constituent une solution de choix pour combler ce fossé inter-espèce. Après greffe de cellules souches hématopoïétiques humaines, des souris hôtes sévèrement immunodéprimées permettent un haut niveau de développement du système hémato-lymphoïde humain tout au long de leur vie. Cependant, certains types cellulaires, comme les cellules lymphoïdes innées, ne parviennent pas à se différencier et à fonctionner normalement dans les modèles murins HIS actuels. Ici, nous décrivons le développement d’un modèle souris HIS original, nommé BRGSF, montrant une amélioration de la maturation, de la fonction et de l’homéostasie des cellules natural killer (NK) humaines et des autres ILCs. De plus, en récapitulant les différentes étapes du développement des ILCs humaines, ce modèle souris BRGSF nous a permis d’identifier pour la première fois un précurseur d’ILC (ILCP) présent à la fois dans notre modèle HIS ainsi que dans le sang périphérique et plusieurs organes lymphoïdes et non-lymphoïdes humains. Cette population circulante d’ILCPs pourrait constituer un substrat pour la production d’ILCs matures dans les tissus périphériques en réponse à des stress environnementaux, inflammatoires et/ou infectieux. Dans une seconde partie de ce travail de thèse, nous avons utilisé ces souris BRGS afin de tester l’efficacité de deux immunothérapies reposant sur les lymphocytes innés pour le traitement d’un carcinome colorectal exprimant EGFR et muté pour KRAS. La première approche a consisté en la co-administration des cellules NK dérivées de sang de cordon ombilical et d'anticorps monoclonal cetuximab afin de promouvoir le mécanisme de cytotoxicité cellulaire dépendante des anticorps (ADCC) contre la tumeur. La seconde stratégie a reposé sur l’injection de nanobodies VHH combinant l’inhibition de l’EGFR et l’activation spécifique du récepteur Vγ9Vδ2 des cellules T effectrices. Les résultats de cette étude soulignent l’importance des modèles murins HIS pour la compréhension du développement des lymphocytes innés humains et pour mieux les mettre à profit dans les thérapies anti-tumeurs / Animal models have extensively contributed to our understanding of human immunobiology and to uncover the underlying pathological mechanisms occurring in the development of the disease. However, mouse models do not always reproduce the genetic complexity inherent in human disease conditions. Human immune system (HIS) mouse models that are susceptible to human pathogens and can recapitulate human hematopoiesis provide one means to bridge the interspecies gap. Severely immunodeficient host mice support life-long, high level human hematolymphoid development after engraftment with human hematopoietic stem cells (HSC). However, the differentiation and function of some blood cell types, including innate lymphoid cells (ILCs), is poorly characterized in current HIS mice. Here we describe the development of a novel HIS mouse model, named BRGSF, which demonstrate enhanced maturation, function and homeostasis of human natural killer (NK) cells and other ILCs. Furthermore, the BRGSF-based HIS mouse model recapitulated the developmental stages of human ILCs. We could identify for the first time an ILC precursor (ILCP) population that is present both in HIS mice and in human peripheral blood as well as in several lymphoid and non-lymphoid human tissues. This circulating human ILCP population may provide a substrate to generate mature ILCs in tissues in response to environmental stressors, inflammation and infection. In a second part of the thesis we used BRGS immunodeficient mice to assess two innate lymphocyte-based immunotherapeutic approaches for treating EGFR-expressing KRAS-mutated colorectal carcinoma in vivo. The first model used a combination of umbilical cord blood (UCB)-derived NK cells and the monoclonal antibody cetuximab to promote antibody dependent cell cytotoxicity (ADCC) against the tumors. In a second model, we evaluated the therapeutic suitability of novel bispecific VHH constructs that combine inhibition of the EGFR with the target-specific activation of effector Vγ9Vδ2-T cells. These studies highlight the utility for HIS-based mouse models to understand human innate lymphocyte development and to harness these potent effectors for anti-tumor therapies. Souris humanisées Natural Killer Cellules lymphoïdes innées Immunothérapies Human immune system mice Natural killer Innate lymphoid cells Immunotherapy
13	Rôle des éosinophiles et des cellules lymphoïdes innées dans l'asthme / Role of eosinophils and innate lymphoid cells in asthma Barnig, Cindy 22 October 2014 (has links) Dans la première partie de cette thèse, nous avons cherché à déterminer le rôle de l’éosinophile circulant dans l’asthme par une approche transcriptomique. Nos résultats suggèrent que l’éosinophile recruté sur un site inflammatoire présente des fonctions immunomodulatrices, importantes dans la réparation tissulaire et le retour à l’homéostasie. Dans la deuxième partie de cette thèse, nous avons étudié le rôle des cellules NK et des cellules lymphoïdes innées de type 2 (ILC2) dans l’inflammation asthmatique. Les cellules NK circulantes sont fortement activées dans l’asthme sévère et ont la capacité d’induire l’apoptose d’éosinophiles autologues in vitro. La PGD2 induit la production d’IL-13 par les ILC2 en synergie avec les cytokines épithéliales IL-25 et IL-33. Enfin, ces fonctions sont régulées par la LXA4. En conclusion, notre travail de thèse met en lumière de nouveaux rôles pour l’éosinophile et les cellules lymphoïdes innées dans l’immunopathologie de l’asthme. / In the first part of the thesis, we adopted a transcriptomic-based approach to investigate the activation state of circulating eosinophils in patients with asthma and other unrelated hypereosinophilic diseases. Taken together, our results, which suggest that esoinophils, recruited to inflammatory sites exhibit non-specific immunomodulatory functions important for tissue repair and homeostasis. In the second part of the thesis, we investigated the role of NK cells and type 2 innate lymphoid cells (ILC2) in asthma inflammation. Circulating NK cells are highly activated in severe asthma and promote apoptosis of autologous eosinophils in vitro. ILC2 generate interleukin-13 in response to prostaglandin D2 alone and in a synergistic manner with the airway epithelial cytokines IL-25 and IL-33. Finally, these functions are regulated by lipoxine A4. In conclusion, this thesis highlights new roles for eosinophils and innate lymphoid cells in asthma immunopathology. Asthme Éosinophiles Cellules NK Cellule lymphoïde innée de type 2 Lipoxine A4 Asthma Eosinophils NK cells Type 2 innate lymphoid cells Lipoxine A4 572.8 616.2
14	Disease Tolerance, Epigenetic Inheritance, and Surviving Pathogenic Viral Infections Silverstein, Noah J. 18 August 2021 (has links) Health is often defined in terms of absence of disease or pathological processes, but this is a definition of exclusion and incomplete. For example, SARS-CoV-2 viral load does not reliably predict disease severity, and so individuals must vary in their ability to control inflammation and maintain normal tissue homeostasis. This host defense strategy is called disease tolerance, and better understanding of disease tolerance mechanisms could change the way that we treat disease and work to maintain health. The first project presented in this dissertation found that after accounting for effects of age and sex, innate lymphoid cells (ILCs), but not T cells, were lower in adults and children sick with COVID-19 or MIS-C, independent of lymphopenia. Furthermore, abundance of ILCs, but not of T cells, correlated inversely with disease severity. These blood ILCs were shown to produce amphiregulin, a protein implicated in disease tolerance and tissue homeostasis, and the percentage of amphiregulin-producing ILCs was lower in males. These results suggest that, by promoting disease tolerance, homeostatic ILCs decrease morbidity and mortality associated with SARS-CoV-2 infection, and that lower ILC abundance accounts for increased COVID-19 severity with age and in males. The second project describes a novel mouse model of epigenetic inheritance wherein paternal influenza A virus (IAV) infection results in less severe influenza disease in IAV infected offspring. This offspring phenotype was not attributable to differences in viral load, indicating a possible difference in disease tolerance. Paternal caloric deprivation decreased, and influenza B virus infection increased, offspring influenza disease severity, and in vitro fertilization demonstrated sperm are sufficient to transfer IAV-associated epigenetic inheritance phenotypes. These findings represent a foundation for further work that, by continuing to elucidate the mechanisms of disease tolerance and epigenetic inheritance, could provide novel therapeutic interventions to help promote and maintain health. SARS-CoV-2 COVID-19 MIS-C lymphocytes innate lymphoid cells disease tolerance amphiregulin AREG epigenetic inheritance influenza Biology Immunology and Infectious Disease Virus Diseases
15	The Tec kinase ITK is required for homeostasis and anti-viral immune protection in the intestine Cho, Hyoung-Soo 10 October 2018 (has links) The Tec kinase ITK is activated by TCR stimulation and also required for TCR downstream signaling. Previous studies have reported differential roles of ITK and another Tec family kinase RLK in CD4+ TH differentiation and effector function. However, these findings are confounded by the complex T cell developmental defects in Itk-/- mice. Furthermore, the function of ITK in tissue-resident T cells in the intestine and anti-viral immune response to a persistent infection has not been studied previously. In addition to T cells, recent studies have indicated an expression of ITK in ILC2, but not in other ILC subsets. Yet, the role of ITK in ILC2 has not been characterized. Here, I have examined the role of ITK and RLK in CD4+ TH subsets using a small molecule inhibitor PRN694. I found that PRN694 impaired TH1 differentiation in vitro, and PRN694 administration prevented TH1-mediated colitis progression in vivo. In an MHV68 infection model, Itk-/- mice failed to control viral replication in the intestine, while gut-homing of CD8+ T cells was greatly impaired. Finally, I found that ILC2 number was markedly reduced in the intestine of Itk-/- mice. Gut-specific defect of Itk-/- ILC2 is associated with a low availability of IL-2 in the intestine of Itk-/- mice. Collectively, these data suggest that ITK is important in T cell migration to the intestine and ILC2 homeostasis in the intestine, thereby contributing to the protective response to a latent virus and intestinal tissue homeostasis. T cells Mucosal Immunology CD4 T helper cells T helper cell differentiation PRN694 CD8 T cells Intestine Innate Lymphoid Cells ILC2 Tissue Homeostasis Immunity Immunology of Infectious Disease Immunopathology
16	T-bet and RORa control lymph node formation by regulating embryonic innate lymphoid cell differentiation Stehle, Christina 10 December 2021 (has links) Angeborene lymphoide Zellen (ILCs) bilden eine Familie von Effektorzellen des angeborenen Immunsystems, denen somatisch rekombinierte Antigenrezeptoren fehlen und die in drei Hauptgruppen eingeteilt werden. In der Embryonalentwicklung spielen Typ 3 ILCs, sogenannte LTi (Lymphoid Tissue inducer) Zellen, eine zentrale Rolle in der Entwicklung von Lymphknoten. ILC3, einschließlich LTi Zellen sind abhängig von dem Master-Transkriptionsfaktor RORgt, was sich in RORgt-defizienten Mäuse durch die Abwesenheit aller ILC3, und auch durch fehlende Lymphknoten äußert. Während postnatale Ko-expression der Transkriptionsfaktoren T-bet und RORgt in ILC3-Subpopulationen fest etabliert ist, ist der Einfluss von T-bet in fötalen ILC3 und auf die Generation von Lymphknoten noch unbekannt. Um diese Mechanismen genau zu untersuchen, wurden fötale ILCs mittels Einzelzell-RNA-Sequenzierung charakterisiert, wodurch eine unerwartete Heterogenität innerhalb der ILC3 mit T-bet-exprimierenden Zellen aufgedeckt wurde. Außerdem wurden PLZF+ ILC-Vorläufer (ILCP) im sich entwickelnden Darm nachgewiesen. Weiterhin, bestätigen diverse Mausmodelle eine Schlüsselrolle für T bet in der Regulation der ILC-Differenzierung und der Entstehung von Lymphknoten. Die zusätzliche genetische Ablation von T-bet in RORgt-defizienten Mäusen beeinflusste Differenzierungsentscheidungen in fötalen ILCP und ermöglichte die Akkumulation von ILCP mit LTi-Aktivität, wodurch die Organogenese von Lymphknoten, unabhängig von RORgt wiederhergestellt wurde. PLZF+ ILCP von RORgt/T-bet-Doppeldefizienten Mäusen bestanden bis ins Erwachsenenalter, wo diese Zellen die Darmbarrierefunktionen durch Produktion von IL-22 wiederherstellten. Darüber hinaus erwies sich RORa als entscheidend für die Entwicklung von PLZF+ ILCP und die damit verbundene Bildung von Lymphknoten. / Innate lymphoid cells (ILCs) represent a family of innate effector cells lacking rearranged antigen receptors, which are classified into three main groups based on their lineage-specifying transcription factors (TF) and effector functions. During embryonic development, the formation of lymphoid organs critically relies on a specific member of group 3 innate lymphoid cells (ILC3), expressing the master transcription factor RORgt and exhibiting lymphoid tissue inducer (LTi) functions. Accordingly, RORgt-deficient mice lack ILC3 and do not generate lymph nodes (LN). While it is established that T-bet is co-expressed with RORgt in a subset of ILC3 emerging postnatally and influencing their differentiation, phenotype and functions, the effect of T-bet on fetal ILC3 biology and its impact on LN generation remains completely unknown. In order to study the role of T-bet in fetal ILC3 differentiation and functions as well as in LN formation, single-cell RNA sequencing and flow cytometry were applied to characterize fetal ILC subsets revealing an unanticipated heterogeneity within embryonic ILC3 and identifying T-bet+ ILC3 subsets within the fetal intestine and mesenteric LN anlage for the first time. Furthermore, PLZF+ ILC progenitors (ILCP) were exposed in the developing mouse intestine. Importantly, using multiple mouse models, a key role for T-bet in regulating ILC differentiation and LN formation was discovered. Specifically, additional deficiency of T-bet in RORgt-deficient mice skewed lineage fate decisions in differentiating fetal ILCP and allowed accumulation of ILCP with LTi activity, thereby rescuing LN organogenesis in a RORgt-independent fashion. PLZF+ ILCP of RORgt/T-bet double deficient mice persisted into adulthood where these cells restored intestinal barrier functions through reinstalled IL-22 production. Moreover, RORa was found to be critical for the development of PLZF+ ILCP and associated LN formation. Lymphknoten Organogenese RORgt lymph nodes innate lymphoid cells Organogenesis RORgt 570 Biologie WX 6503 WW 9123 ddc:570
17	Immunogenetic regulation of Natural Killer cell function in pregnancy Gaynor, Louise Michelle January 2017 (has links) Uterine NK (uNK) cells are a distinct subset of NK cells in the decidua of humans and rodents during pregnancy, which are essential for remodelling of the spiral arteries supplying the feto-placental unit. Similarly to peripheral NK cells, uNK cells express Natural Killer receptors (NKRs) that engage MHC class I molecules. Evidence from human genetic association studies suggests that, in the presence of allogeneic cognate paternal MHC class I ligands, inhibitory uterine NKRs are associated with disorders of pregnancy arising from impaired decidual vascular remodelling. Conversely, enhancement of human uNK cell activity through activating NKRs is associated with high birth weight. Evidence from mouse models corroborates that uNK cell activity is modulated by interactions between NKRs and MHC class I, but has largely focussed on the effect of paternal MHC. In this study, the contribution of maternal immunogenetic regulation of NK cell function to reproductive outcome was assessed independently of parental MHC disparity in mice. To evaluate the role of NKR genes in isolation, I used congenic B6.BALB-TC1 (TC1) mice that differ from C57BL/6 (B6) mice only within the region of chromosome six encoding NKRs that recognise MHC class I. Absence of a major inhibitory NKR for self-MHC, Ly49I, in TC1 mice causes a compensatory shift in the NKR repertoire expressed and preserves a majority subpopulation of educated NK cells. B6 and TC1 splenic and uterine NK cells are similarly functionally reactive and mature, and no significant differences could be detected in spiral arterial remodelling or fetal growth between these strains in MHC-syngeneic matings. This supports data from human immunogenetic studies showing that maternal uterine NKRs are not associated with differences in pregnancy outcome in the absence of novel paternal MHC class I ligands, and highlights the importance of maternal and paternal co-regulation of uNK cell activity during pregnancy. No mouse models of uNK cell activation are currently available with which to corroborate human immunogenetic associations between activating uterine NKRs and high birth weight. Male m157-transgenic (m157-Tg) mice, which ubiquitously express viral m157 glycoprotein ligands for the activating NKR Ly49H, were mated with B6 females. Exclusive expression of m157 glycoprotein by trophoblast improved placental efficiency, but did not enhance fetal growth. Some fertility clinics surmise that uNK cell activation initiates the pathogenesis of spontaneous abortion. It has been suggested that this may occur due to reduced expression by human uNK cells of miR-483-3p, which stimulates endogenous insulin-like growth factor (IGF)-1 production and uNK cell cytotoxicity in vitro. It is demonstrated here that neither miR-483-3p nor IGF-1 regulate murine NK cell development, maturation or function. No discernible reproductive phenotype is evident in miR-483 deficient females. It can be inferred that post-transcriptional control by miR-483 is not biologically relevant to murine NK cell function. Although m157-Tg mice may provide an interesting model to further study uNK cell-mediated placental adaptations, it remains important to identify a murine model of enhanced uNK cell function to corroborate human immunogenetic associations with high birth weight and to challenge the supposition that uNK cell activation is harmful to pregnancy.
18	Rôle des cellules lymphoïdes innées chez l'homme : analyse au cours de déficits immunitaires, pathologies auto-immunes et inflammatoires / Roles of innate lymphoid cells in human : analysis in primary immunodeficiencies, autoimmune and inflammatory diseases Ebbo, Mikaël 19 October 2017 (has links) Les cellules lymphoïdes innées (ILCs) sont des populations cellulaires d’identification récente, mais leur rôle in vivo chez l’homme reste mal connu. Dans une 1ère étude, nous avons pu montrer qu’un déficit sévère en NK au cours de déficits immunitaires communs variables est associé à un risque accru de manifestations non infectieuses et infectieuses bactériennes sévères, suggérant un rôle protecteur non redondant des cellules NK lorsque le système immunitaire adaptatif n’est pas fonctionnel. Dans une 2ème étude, nous avons montré que des patients atteints de déficits immunitaires combinés sévères ɣc et JAK3 déficients n’ont pas d’ILCs. Après allogreffe de moelle osseuse, le nombre d’ILCs circulantes reste indétectable, sans manifestation clinique notable associée. Ces résultats sont en faveur d’une redondance des fonctions des ILCs chez l’homme, lorsque les fonctions T et B sont conservées. Nous avons ensuite étudié les modifications phénotypiques et fonctionnelles des cellules NK au cours du purpura thrombopénique immunologique, et observé un défaut de production d’interféron-ɣ par les cellules NK circulantes et une augmentation de la cytotoxicité dépendante des anticorps des cellules NK spléniques. Une inhibition des fonctions des cellules NK par les immunoglobulines polyvalentes est également mise en évidence. Enfin, une étude des ILCs circulantes au cours de la maladie associée aux IgG4 ainsi qu’une revue de la littérature sur l’étude des ILCs au cours des pathologies inflammatoires sont rapportées. En conclusion, l’apparente redondance des ILCs chez l’homme ainsi que leur implication en pathologies inflammatoires en font de potentielles cibles thérapeutiques. / Innate lymphoid cells (ILCs) are recently identified components of the immune system, but their functions in vivo in humans are still elusive. In a first study, we show in patients with common variable immunodeficiency that non-infectious inflammatory complications and severe bacterial infections were more frequent in patients with severe NK cell lymphopenia, indicating potential non-redundant immune functions of NK cells when the adaptive immune response is not optimal. In a second study, we observe that in patients with ɣc and JAK3 severe combined immunodeficiencies, all ILC subsets are absent. After hematopoietic stem cell transplantation, ILCs remain indetectable with no susceptibility to disease, suggesting that ILCs might be redundant and dispensable in humans, if T and B cells functions are preserved. In the second part of this thesis, we study phenotypic and functional modifications of NK cell compartment in primary immune thrombocytopenia. Interferon gamma production by the peripheral blood NK cells of ITP patients is decreased. In contrast, splenic NK cells of ITP patients tend to be more efficient in antibody-dependent cell cytotoxicity. Intravenous polyvalent immunoglobulins lead to the inhibition of blood NK cell activation. Finally, we present the preliminary results of a study investigating the modifications of circulating ILCs in IgG4-related disease, and present an extensive litterature review concerning the role of ILCs in inflammatory diseases. In conclusion, the apparent redundancy of ILCs for protective immunity and their pathogenic role in inflammatory diseases make their targeting in humans for therapeutic purposes particularly promising. Cellules Natural Killer (NK) Cellules lymphoïdes innées (ILC) Déficit immunitaire primitif Pathologies inflammatoires Homme Natural Killer (NK) cells Innate lymphoid cells Primary immunodeficiency Immune thrombocytopenia (ITP) Inflammatory diseases Human
19	Einfluss des lymphatischen Systems auf die Entwicklung einer Herzinsuffizienz durch Erhöhung der Nachlast / Effect of lymphoid cells on the progression of pressure overload-induced heart failure Sasse, André 06 December 2017 (has links) No description available. 610 heart failure transverse aortic constriction innate lymphoid cells HFrEF HFpEF Cytokine Kardiologie (PPN619875755)
20	Les lymphocytes MAIT induisent l'inflammation, la dysbiose et le diabète de type 2 au cours de l'obésité / Mucosal Associated Invariant T (MAIT) cells induce inflammation, gut dysbiosis, and type 2 diabetes during obesity Kiaf, Badr 29 September 2017 (has links) Le surpoids et l’obésité touchent plus de 1,9 milliard d’adultes à travers le monde et pourraient atteindre 3,3 milliards de personnes dans une dizaine d’année. L’obésité est associée à une inflammation tissulaire et systémique chronique de bas grade, qui contribuent à l’apparition de la résistance à l’insuline. Récemment, notre laboratoire a mis en évidence des anomalies d’une nouvelle population de lymphocytes T innés, les cellules MAIT (Mucosal Associated Invariant T) chez des patients obèses et/ou ayant un diabète de type 2 (T2D). Les cellules MAIT sont des lymphocytes T non conventionnels, qui expriment un récepteur des cellules T (TCR) avec une chaîne alpha invariante. Leur TCR reconnait la molécule d’histocompatibilité de classe 1 non classique MR1, présentant des métabolites dérivés de la voie de biosynthèse des vitamines B, notamment les vitamines B2 et B9. Dans cette étude, nous utilisons les modèles murins pour analyser le rôle des cellules MAIT dans le developpement du T2D. Au cours de l’obésité induite par un régime riche en graisse, les cellules MAIT du tissu adipeux viscéral (TA) et de l’iléon sont activées de façon précoce et anormale et produisent plus de cytokines pro-inflammatoires (i.e. IL-17, TNFa et l’IFN?). De plus, l’augmentation de la fréquence tissulaire des MAIT chez des souris Va19 transgéniques conduit à l’apparition de la résistance à l’insuline et à une intolérance au glucose, au cours de l’obésité. A l’inverse, les souris obèses déficientes en MAIT, MR1-/-, sont protégées contre ces anomalies métaboliques. Une fréquence élevée de MAIT est associée au changement de macrophages M2 (anti-inflammatoires) en M1 (inflammatoires) et à une infiltration des cellules NK et des LTaß-CD8 au niveau du TA. Par ailleurs, les MAIT contrôlent la fréquence des Treg, ILC2 et ILC3 dans l’iléon et des Treg, ILC2 et éosinophiles dans le tissu adipeux. La modification de la fréquence des ILC2 et ILC3 est associée à la production intestinale d’IL-33 et d’IL-25. De plus, nous montrons que le rôle délétère des MAIT dans le développement du T2D est associé à une dysbiose intestinale. Finalement, des expériences de transfert de flores intestinales montrent que cette dysbiose intestinale est en partie responsable des anomalies immunitaires et métaboliques. / Obesity and type 2 diabetes are associated with low-grade chronic inflammation. Immune cells are recruited and activated in several tissues, including adipose tissue, thereby contributing to insulin-resistance and diabetes. Recent studies described gut microbiota dysbiosis as a consequence as well as a driver of obesity and type 2 diabetes. Mucosaassociated invariant T cells (MAIT) are innate-like T cells expressing a semi-invariant T-cell receptor restricted by the non-classical MHC class I molecule MR1 presenting bacterial ligands. In obese/T2D patients MAIT cells in blood and adipose tissue exhibit a pro-inflammatory profile. In the present study, we show that during high fat diet-induced obesity MAIT cells produce inflammatory cytokines in adipose tissue and the ileum and induce inflammation in these tissues by modifying other immune cell populations (i.e. macrophages, CD8 Taß cells, NK cells, LTreg, eosinophils and ILC2 in the adipose tissue and ILC2, ILC3 and LTreg in the ileum). These changes impair the function of both tissues leading to insulin resistance, glucose intolerance, impaired lipid metabolism and increased gut permeability. MAIT cells also impact gut microbiota dysbiosis during obesity and microbiota transfer experiments highlight a bidirectional crosstalk between MAIT cells and the gut microbiota leading to inflammation and gut leakage. Altogether these results reveal the major role of MAIT cells in promoting the development of type 2 diabetes during obesity. Diabète de type 2 Microbiote gastrointestinal Cellule lymphoïde innée Insulinorésistance Mucosal Associated Invariant T Cells Diabetes mellitus, type 2 Gastrointestinal Microbiotas Innate lymphoid cells Insulin resistance

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