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Endogenous Memory CD8 T Cells in Cardiac TransplantationSu, Charles 02 September 2014 (has links)
No description available.
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CD8 MEMORY T CELL FUNCTION DURING THE 72 HOURS IMMEDIATELY FOLLOWING CARDIAC ALLOGRAFT REPERFUSIONSchenk, Austin David 08 July 2008 (has links)
No description available.
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CD4+ T cell responses to myelin autoantigens : activation, memory and toleranceChung, Chen-Yen January 2009 (has links)
Experimental autoimmune encephalomyelitis (EAE) is a CD4+ T cell mediated autoimmune disease of the central nervous system and shares many characteristics with multiple sclerosis (MS). Induction of EAE is mediated by myelin reactive CD4+ T helper (Th) cells, particularly Th1 and Th17 cells, which can be provoked by the immunization with myelin derived protein (or peptide) and Toll-like receptor (TLR) stimulus (eg, complete Freund¡s adjuvant, CFA). If given an injection of soluble peptide before immunization, mice do not develop EAE (they are tolerant). This approach has been widely applied, evoking tolerance in primary responses (i.e., in naive T cells). Therefore the first hypothesis of this thesis is that peptide induced protection from EAE is a result from T cell deletion or / and anergy. As MS patients have ongoing disease and over 85% of MS patients develop a relapsing-remitting course, memory T cells are key targets when considering peptide-induced tolerance as a therapeutic strategy. Thus, a model for ¡memory EAE¡ was established to test a second hypothesis that the myelin reactive memory T cells can be controlled by the administration of soluble peptide. Here, adoptive transfer of T cells from T cell receptor transgenic mice (2D2) recognizing myelin oligodendrocyte glycoprotein 35-55 (pMOG) was used to investigate the pMOG-reactive memory responses. Soluble pMOG administration could induce a transient expansion of 2D2 T cells followed by their loss through apoptosis. A model using double immunization was established by immunizing mice first with pMOG together with unmethylated CpG oligonucleotide (CpG) as an adjuvant, and subsequently immunizing with pMOG in CFA. This produced EAE with early onset and high incidence compared to mice which received pMOG/CFA only. Cells from mice that received the double immunization protocol produced high levels of IFN-γ, suggesting that memory T cell responses have been triggered in the mice. Administration of soluble peptide before secondary immunization could ameliorate EAE, indicating that memory T cells are susceptible to tolerance induction. pMOG-reactive memory T cells were further assessed by isolating CD4+ CD25- CD44high CD62Llow cells from pMOG-experienced 2D2 mice. These cells showed early and high production of IFN-γ, and early but transient production of IL-2, compared with naive population. These data provide basic information relevant to translating peptide-induced T cell tolerance from mice to humans.
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Dissecting the Role of 4-1BB and its Ligand in Enhancing CD8 Effector and Memory T Cell ResponsesLin, Gloria Hoi Ying 19 January 2012 (has links)
The Tumor necrosis factor receptor (TNFR) family member 4-1BB and its TNF family ligand, 4-1BBL, are important in modulating multiple stages of the CD8 T cell response. Here I show that during a mild influenza infection, 4-1BBL is completely dispensable for initial T cell responses, viral clearance and mouse survival. In contrast, during severe influenza infection with prolonged viral load, 4-1BB expression is sustained on lung T cells and 4-1BBL is upregulated in the lung compared to mild influenza infection. Under these conditions, 4-1BBL-deficiency results in a decreased CD8 T cell response in the lungs, higher viral load, impaired lung function and increased mortality. These findings suggest that the sustained expression of 4-1BB and its ligand as a function of viral load fine-tunes the CD8 T cell response to a level appropriate for the severity of infection. 4-1BBL is also important for maintaining CD8 memory T cell survival following the clearance of an infection. I found that 4-1BB is selectively expressed on a subset of memory CD8 T cells in the bone marrow. I further showed that the TNFR family member GITR is intrinsically required on CD8 memory T cells for 4-1BB expression in vivo, and that 4-1BB on CD8 T cells interacting with 4-1BBL on a radio-resistant cell in the bone marrow contributes to CD8 memory T cell survival. Immunotherapy with 4-1BB agonists has shown efficacy in eradication of tumors in several mouse models. These effects have been attributed to 4-1BB on multiple cell types. I found that 4-1BB either on transferred T cells or on host T cells was necessary and sufficient for inducing regression of established tumors when anti-4-1BB is combined with adoptive T cell therapy. This thesis highlights the importance of the CD8 T cell intrinsic role of 4-1BB in the immune system.
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Dissecting the Role of 4-1BB and its Ligand in Enhancing CD8 Effector and Memory T Cell ResponsesLin, Gloria Hoi Ying 19 January 2012 (has links)
The Tumor necrosis factor receptor (TNFR) family member 4-1BB and its TNF family ligand, 4-1BBL, are important in modulating multiple stages of the CD8 T cell response. Here I show that during a mild influenza infection, 4-1BBL is completely dispensable for initial T cell responses, viral clearance and mouse survival. In contrast, during severe influenza infection with prolonged viral load, 4-1BB expression is sustained on lung T cells and 4-1BBL is upregulated in the lung compared to mild influenza infection. Under these conditions, 4-1BBL-deficiency results in a decreased CD8 T cell response in the lungs, higher viral load, impaired lung function and increased mortality. These findings suggest that the sustained expression of 4-1BB and its ligand as a function of viral load fine-tunes the CD8 T cell response to a level appropriate for the severity of infection. 4-1BBL is also important for maintaining CD8 memory T cell survival following the clearance of an infection. I found that 4-1BB is selectively expressed on a subset of memory CD8 T cells in the bone marrow. I further showed that the TNFR family member GITR is intrinsically required on CD8 memory T cells for 4-1BB expression in vivo, and that 4-1BB on CD8 T cells interacting with 4-1BBL on a radio-resistant cell in the bone marrow contributes to CD8 memory T cell survival. Immunotherapy with 4-1BB agonists has shown efficacy in eradication of tumors in several mouse models. These effects have been attributed to 4-1BB on multiple cell types. I found that 4-1BB either on transferred T cells or on host T cells was necessary and sufficient for inducing regression of established tumors when anti-4-1BB is combined with adoptive T cell therapy. This thesis highlights the importance of the CD8 T cell intrinsic role of 4-1BB in the immune system.
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Étude des interactions ostéoimmunologiques dans les maladies inflammatoires chroniques de l’intestin / Osteoimmunological interaction in inflammatory bowel diseasesBoucoiran, Agathe 29 September 2016 (has links)
Les maladies inflammatoires chroniques sont associées à un maintien de la réponse immunitaire et notamment la présence de cellules T CD4+ mémoires. Les maladies inflammatoires chroniques de l’intestin ont pour conséquence une perte osseuse due à une augmentation du nombre et de l'activité des ostéoclastes, les cellules responsables de la résorption osseuse. Les cellules CD4+ ont été décrites comme participant à la différenciation des ostéoclastes mais la nature exacte de ces cellules reste encore indéterminée. Des études in vivo et in vitro chez la souris et chez l’Homme nous ont permis de décrire une population inflammatoire Th17 TNFα CD4+ présente dans la moelle osseuse participant à la différenciation des ostéoclastes. Ces cellules Th17 participent au recrutement et à la différenciation des monocytes en ostéoclastes en agissant sur les cellules stromales mésenchymateuses. De plus, les maladies inflammatoires chroniques de l’intestin sont associées à une augmentation de la prolifération et de la différenciation des cellules souches hématopoïétiques en cellules myéloïdes. Suite à un stress chimique ou mécanique, les ostéoclastes participent à la mobilisation des cellules souches hématopoïétiques depuis la moelle osseuse. Nous avons montré qu’au cours des maladies inflammatoires de l’intestin, l’augmentation de l’activité des ostéoclastes participe à la prolifération et la différenciation des cellules souches en cellules myéloïdes. Ainsi, les ostéoclastes sont devenus une nouvelle cible thérapeutique intéressante dans la lutte des maladies inflammatoires chroniques de l’intestin / Chronic inflammatory diseases are associated to maintain of memory response and the presence of memory CD4+ T cells. Inflammatory bowel diseases are associated with bone loss due to an increase of the number and activity of osteoclasts, the bone-resorbing cells. CD4+ T cells participated to osteoclasts differentiation, but their nature is still undetermined. In vivo and in vivo studies in mice and human allow us to describe an inflammatory Th17 TNFα CD4+ T cells in the bone marrow that participated to osteoclast differentiation and link inflammation and bone loss. Th17 T cells induce the recruitment and the differentiation of monocytes into osteoclasts acting on mesenchymal stromal cells. Moreover, inflammatory bowel diseases are associated in an increase of hematopoietic stem cell (HSC) mobilization. In stress condition, osteoclasts act on HSC niches and induce their mobilization. We have shown that in inflammatory bowel disease, increase osteoclast activity is involved in the proliferation and differentiation of stem cells into myeloid cells. These myeloid cells are responsible for the intestinal inflammation. Thus, osteoclasts have become an exciting new therapeutic target in the fight of inflammatory bowel diseases
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Protein Arginine MethylTransferase 5 (PRMT5) Drives Inflammatory T cell Responses and AutoimmunityWebb, Lindsay M., Webb January 2018 (has links)
No description available.
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Maintenance and re-activation of antigen-specific CD8+ and CD4+ memory T lymphocytes in the bone marrowSiracusa, Francesco 17 August 2018 (has links)
Das Knochenmark (BM) beherbergt wesentliche Komponenten des adaptiven Immunsystems, die einen langfristigen Schutz gegen wiederkehrende Pathogene vermitteln können, sodass es sich als Reservoir für ein immunologisches Gedächtnis qualifiziert. Neben langlebiger Antikörper-produzierender Plasmazellen bleiben auch Antigen (Ag)-spezifische CD8+ und CD4+ T-Gedächtniszellen dauerhaft im Knochenmark erhalten, auch wenn sie in den sekundären lymphoiden Organen (SLOs) und im Blut abwesend sind. Es wird angenommen, dass diese T-Gedächtniszellen bei erneutem Kontakt mit den gleichen systemischen Pathogenen schnell reagieren können. Allerdings sind die biologischen Mechanismen für ihre langfristige Aufrechterhaltung immer noch umstritten und demnach ungeklärt. Unklar ist auch, wie die T-Gedächtniszellen des Knochenmarks bei erneuter Konfrontation mit demselben Antigen reagieren. Hier wird dieser Frage begegnet, indem durch klassiche Immunisierung mit definieren Antigenen eine stabile Population Ag-spezifischer CD8+ und CD4+ T-Gedächtniszellen im Knochenmark erzeugt wird. / The bone marrow (BM) harbors critical components of the adaptive immune system being able to provide long-lasting protection against previously encountered pathogens, thus qualifying as a reservoir of immunological memory. In addition to long-lived antibody producing plasma cells, antigen (Ag)-specific CD8+ and CD4+ memory T lymphocytes are maintained long-term in the BM even when they are absent from secondary lymphoid organs (SLOs) and blood. Those memory T cells are thought to respond fast upon re-encounter of systemic pathogens. However, the biological mechanisms behind their long-term maintenance in the BM are still a matter of debate and thus remain unclear. Similarly, it is also unclear how the memory T cells of the BM react to antigenic re-challenge. Here we address these issues by generating a stable pool of Ag-specific CD8+ and CD4+ memory T lymphocytes in the BM by classical immunizations with defined antigens.
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Charakterizace naivních a virtuálně paměťových T lymfocytárních klonů / Characterization of T-cell clones from naïve and virtual memory compartmentPřibíková, Michaela January 2019 (has links)
Virtual memory (VM) CD8+ T cells represent a population of antigen-inexperienced T cells with an apparent memory phenotype. In lymphoreplete germ-free mice VM CD8+ T cells represent 10-20% of all peripheral CD8+ T cells. Their origin correlates with the levels of self-reactivity where the main factor that determinates the T-cell fate decision is the strength of homeostatic signals. In the first part of this thesis, we demonstrated that VM CD8+ T cells and naïve CD8+ T cells had distinct TCR repertoire and T-cell subsets contained different clonotypes. Moreover, 'VM clones' were enriched among VM T cells and were also present in naïve T cells. In contrast, 'naïve clones' were almost exclusively detected in naïve T cells. Next, we characterized the signaling of particular OVA-reactive TCRs from both naïve and VM subsets. We confirmed that 6 out of 8 tested TCRs were responsive to Kb-OVA. In the last part of the thesis, we developed and optimized a qPCR-based method for the relative quantification of specific T-cell clonotypes prior to and during the immune response. This method will serve as a tool for studying the biology of particular VM and naïve T-cell subsets and their role during the immune response. Keywords: T-cell receptor, homeostatic signaling, self-reactivity, virtual memory cells, T cells
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Effet de la surexpression du gène Hoxb4 sur la prolifération homéostatique des cellules T mémoiresFrison, Héloïse 08 1900 (has links)
Les cellules T mémoires (Tm) protègent l’organisme contre les réinfections de pathogènes qu’il a déjà combattu. Les Tm possèdent plusieurs propriétés en commun avec les cellules souches hématopoïétiques (CSH), notamment la capacité de se différencier, de s’auto-renouveler et de maintenir une population relativement constante au sein de l’organisme via des mécanismes homéostatiques. Il a été démontré que Hoxb4, un membre de la famille des facteurs de transcription Hox, était capable d’induire l’expansion des CSH in vivo et in vitro de façon rapide. Au vu de ces parallèles, nous avons posé l’hypothèse que la surexpression de Hoxb4 pourrait induire l’expansion de populations de Tm. Nous avons analysé les populations de Tm et lymphocytes T naïfs (Tn) dans les organes lymphoïdes de souris transgéniques surexprimant Hoxb4 et les avons comparées à des souris de type sauvage (wt). Alors que la fréquence des cellules T matures Hoxb4 diminuait avec l’âge, leur phénotype ainsi que leur viabilité demeuraient inchangés. Ensuite, nous avons procédé à des transplantations en compétition de Tm (CD4+CD44hi) Hoxb4 et wt chez des hôtes dépourvus de lymphocytes T (CD3-/-) dans le but d’évaluer leur contribution à la reconstitution du compartiment T après 2 mois. Au final, les Tm wt avait contribué un peu plus que les Tm Hoxb4 à la reconstitution (~60%). Des analyses fonctionnelles et phénotypiques ont montré que les Tm Hoxb4 possédaient une fonctionnalité normale, mais se distinguaient des Tm wt par la présence d’une faible population qui présentait un phénotype « mémoire central » (Tcm), conférant habituellement une longévité accrue. Les cellules des ganglions lymphatiques totaux des hôtes furent transplantées de façon sérielle chez trois générations de nouveaux hôtes. Le phénotype Tcm observés chez les Tm Hoxb4 était récapitulé chez les hôtes secondaires uniquement. Les ratios sont demeurés en faveur des Tm wt lors des deux transplantations suivantes, mais les Tm Hoxb4 ont commencé à montrer un avantage compétitif chez certains hôtes quaternaires. Une transplantation en compétition à court terme de Tm Hoxb4 et wt marqués avec un marqueur cytoplasmique ont démontré la présence chez les Tm Hoxb4 seulement d’une faible population CD62Lhi proliférant lentement. Ainsi, l’expansion préférentielle de Tcm CD4 par le biais d’une sélection ou d’une différenciation induite par la surexpression de Hoxb4 pourrait potentiellement leur permettre de maintenir un état de quiescence leur permettant de persister plus longtemps suite à des transplantations sérielles. / Memory T cells (Tm) protect the organism against reinfection from pathogens they’ve already encountered. Tm share characteristics with hematopoietic stem cells (HSC), such as the capacity to differentiate, self-renew and maintain a relatively constant population via homeostatic mechanisms. Hoxb4, a member of the Hox genes family of transcription factors, has been shown to expand HSCs rapidly in vivo and in vitro. Thus, drawing from these parallels we hypothesise that Hoxb4 overexpression could lead to expansion of Tm populations. Tm and naïve T cell (Tn) populations were analysed in the lymphoid organs of young and aged transgenic mice overexpressing Hoxb4 in comparison with wild type (wt) mice. While the frequencies of mature Hoxb4 T cells in lymphoid organs seemed to decline with age, the phenotype or the cell viability remained unaffected. Next, CD4+CD44hi Hoxb4 Tm were transferred into T cell deficient (CD3-/-) hosts in competition with wt CD4+CD44hi Tm and evaluated for their contribution to T cell reconstitution after 2 months. Engraftment of wt Tm in secondary lymphoid organs was slightly higher than Hoxb4 Tm (~60%). Functional assays and phenotypic analysis showed that Hoxb4 Tm exhibited normal functionality, but in contrast to wt Tm, a fraction of Hoxb4 Tm exhibited a more central memory (Tcm) phenotype, indicative of a longer lifespan. Total lymph nodes from hosts were serially re-transplanted for three generations. The Tcm phenotype of the Hoxb4 Tm present in the primary hosts was recapitulated in the secondary but not in the tertiary hosts. The ratios remained in favor of the wt Tm after two subsequent expansion rounds, but Hoxb4 Tm showed a competitive advantage over wt Tm in some quaternary hosts. Cell tracking of a short term transplantation of Hoxb4 and wt Tm in competition exposed a small population of CD62Lhi cells displaying slow proliferation in the Hoxb4 Tm only. Thus preferential CD4+ Tcm expansion by selection or differentiation could potentially allow Hoxb4 Tm to persist longer following serial transplantations due to a more quiescent state.
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