963 resultados para lymphocyte T CD8
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Le diabte auto-immun rsulte de la destruction des cellules bta pancratiques scrtrices dinsuline par les lymphocytes T du systme immunitaire. Il sensuit une dficience hormonale qui peut tre comble par des injections quotidiennes dinsuline dorigine exogne, toutefois il demeure ce jour impossible de gurir les patients atteints de la maladie. De faon gnrale, un systme immunitaire sain reconnat une multitude dantignes diffrents et assure ainsi notre dfense lgard de diffrents pathognes ou encore de cellules tumorales. Il arrive cependant que, pour des raisons gntiques et/ou environnementales, les lymphocytes T puissent sactiver de faon aberrante suite la reconnaissance dantignes provenant du soi. Cest ce bris de tolrance qui mne au dveloppement de pathologies auto-immunes telles que le diabte auto-immun. Afin de limiter lauto-immunit, des mcanismes de slection stricts permettent dliminer la majorit des lymphocytes T prsentant une forte affinit envers des antignes du soi lors de leur dveloppement dans le thymus. Certains de ces lymphocytes russissent toutefois chapper lapoptose et migrent en priphrie afin dy circuler en qute dun antigne spcifiquement reconnu. Il est alors primordial que des mcanismes priphriques assurent le maintien de la tolrance immunitaire en faisant obstacle lactivation et la prolifration des lymphocytes T auto-ractifs. Lune des avenues afin dinhiber le dveloppement de rponses immunitaires aberrantes est la gnration de lymphocytes T rgulateurs. Ces cellules, dorigine thymique ou priphrique, peuvent arborer diffrents phnotypes et agissent via de multiples mcanismes afin dinactiver et/ou liminer les cellules impliques dans lapparition de pathologies auto-immunes. Lutilisation de modles murins transgniques a permis la mise en vidence dune population peu caractrise de lymphocytes T au potentiel rgulateur. En effet, la proportion de ces cellules T nexprimant pas les corcepteurs CD4 et CD8 (double ngatives, DN) a t inversement corrle la prdisposition lauto-immunit chez ces ii souris. Lobjectif principal de cette thse est de dmontrer la fonction immuno-rgulatrice des lymphocytes T DN, tout en investiguant les facteurs gntiques responsables du maintien de cette population cellulaire. Nous avons observ que les lymphocytes T DN exercent une activit cytotoxique lgard des lymphocytes B de faon spcifique lantigne, via la libration de granules cytolytiques contenant du granzyme B et de la perforine. Par ailleurs, nous avons tabli quun unique transfert adoptif de ces cellules est suffisant afin dinhiber le dveloppement du diabte auto-immun chez des htes transgniques prdisposs la maladie. Le recours des souris dficientes pour lexpression du gne CD47 a permis de constater que la voie de signalisation CD47-Sirp est essentielle dans le maintien de la proportion des lymphocytes T DN. De plus, le locus murin de prdisposition au diabte auto-immun Idd13, qui contient le gne Sirp, a t identifi pour son rle dans la rgulation de la proportion de ces cellules. Finalement, une analyse gntique a rvl que dautres intervalles gntiques sont impliqus dans le contrle de la population des lymphocytes T DN. Parmi ceux-ci, un locus situ en rgion proximale du chromosome 12 a t valid grce la cration de souris congniques. Grce aux rsultats prsents dans cette thse, notre comprhension de la biologie ainsi que de la rgulation des lymphocytes T DN est approfondie. Ces connaissances constituent un pas important vers la cration de thrapies cellulaires novatrices permettant de prvenir et de gurir diverses pathologies auto-immunes.
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Lors dune infection par un pathogne, des lymphocytes T CD8+ nafs (LTn) spcifiques de lantigne sont activs, prolifrent et se diffrencient en LT effecteurs (LTe). Les LTe produisent diffrentes cytokines et acquirent une activit cytotoxique menant llimination du pathogne. Seulement 5 10 % des LTe survivront et se diffrencieront en LT mmoires (LTm), qui sont capables de rpondre plus rapidement lors dune seconde infection par le mme pathogne, contribuant au succs de la vaccination. Toutefois, la comprhension de lensemble des mcanismes rgulant le dveloppement des LTe et des LTm demeure incomplte. Afin de mieux comprendre les signaux requis pour la diffrenciation des LT CD8+ lors de la rponse immune, nous avons pos deux hypothses. Nous avons dabord propos que diffrentes cellules prsentatrices dantigne (CPA) fournissent diffrents signaux au moment de la reconnaissance antignique influenant ainsi le devenir des LT CD8+. Vu leur potentiel dutilisation en immunothrapie, nous avons compar la capacit dactivation des LT CD8+ par les lymphocytes B activs via le CD40 (CD40-B) et les cellules dendritiques (CD). Nous avons montr que limmunisation avec des CD40-B induit une rponse effectrice mais, contrairement limmunisation avec des CD, pratiquement aucun LTm nest gnr. Les LTe gnrs sont fonctionnels puisquils scrtent des cytokines, ont une activit cytotoxique et contrlent une infection avec Listeria monocytogenes (Lm). Nous proposons quune scrtion plus faible de cytokines par les CD40 B ainsi quune interaction plus courte et moins intime avec les LT CD8+ comparativement aux CD contribuent au dfaut de diffrenciation des LTm observ lors de la vaccination avec les CD40-B. Ensuite, nous pos lhypothse que, parmi les signaux fournis par les CPA au moment de la reconnaissance antignique, la voie de signalisation Notch influence le dveloppement des LTe, mais aussi des LTm CD8+ en instaurant un programme gntique particulier. Dabord, grce un systme in vitro, le rle de la signalisation Notch dans les moments prcoces suivant lactivation du LT CD8+ a t tudi. Ce systme nous a permis de dmontrer que la voie de signalisation Notch rgule directement lexpression de la molcule PD-1. Ensuite, grce des souris o il y a dltion des rcepteurs Notch1 et Notch2 seulement chez les LT CD8+ matures, un rle de la voie de signalisation Notch dans la rponse immune des LT CD8+ a t dmontr. Nos rsultats dmontrent que suite une infection avec Lm ou une immunisation avec des CD, la signalisation Notch favorise le dveloppement de LTe, exprimant fortement KLRG1 et faiblement CD127, destins mourir par apoptose. Toutefois, la signalisation Notch na pas influenc la gnration de LTm. De faon trs intressante, lexpression des rcepteurs Notch influence la production dIFN- en fonction du contexte dactivation. En effet, suite une infection avec Lm, labsence des rcepteurs Notch naffecte pas la production dIFN- par les LTe, alors quelle est diminue suite une immunisation avec des CD suggrant un rle dpendant du contexte pour la voie de signalisation Notch. Nos rsultats permettent une meilleure comprhension des signaux fournis par les diffrentes CPA et de la voie de signalisation Notch, donc des mcanismes molculaires rgulant la diffrenciation des LT CD8+ lors de la rponse immunitaire, ce qui pourrait ultimement permettre damliorer les stratgies de vaccination.
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Une petite population de lymphocytes T exprimant les deux corcepteurs CD4 et CD8 et appele double positive (DP), a t dtecte dans le sang priphrique de donneurs sains et de patients atteints de diverses pathologies dont la sclrose en plaques (SEP). Nous avons mis lhypothse quil sagissait de lymphocytes T hautement activs pouvant contribuer linflammation chronique prsente dans la SEP. Nous avons compar les cellules T DP obtenues du sang de donneurs sains et de patients atteints de la SEP et non traits. La frquence des cellules DP tait similaire chez les patients et les donneurs sains. La proportion de lymphocytes T DP qui exprimaient les chaines du rcepteur de linterleukine-15 (IL-15) tait plus leve que pour les autres populations lymphocytaires. Des mesures dinduction de la phosphorylation du STAT5 (signal transducer and activator of transcription) ont dmontr que les cellules DP ont rpondu des doses plus faibles et pour de plus longues priodes lIL-15 comparativement aux autres lymphocytes T. Le pourcentage de lymphocytes T DP ayant la capacit de produire linterfron-gamma et des enzymes lytiques tait lev chez les tmoins sains mais ces niveaux taient significativement rduits chez les patients atteints de la SEP. La caractrisation phnotypique de cellules DP a suggr que ces cellules ont des proprits similaires aux lymphocytes T activs. Bien quil ne sagisse que dune caractrisation partielle, il semble que les lymphocytes T DP perdent une partie de leurs proprits chez les patients atteints de la SEP.
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The clonal expansion of antigen-specific CD8+ T cells in response to microbial infections is essential for adaptive immunity. Although IL-2 has been considered to be primarily responsible for this process, quantitatively normal expansion occurs in the absence of IL-2 receptor signaling. Here, we show that ligating CD27 on CD8+ T cells that have been stimulated through the T cell receptor causes their expansion in the absence of IL-2 by mediating two distinct cellular processes: enhancing cell cycling and promoting cell survival by maintaining the expression of IL-7 receptor alpha. This pathway for clonal expansion of the CD8+ T cell is not associated with the development of a capacity either for production of IFN-gamma or for cytotoxic T lymphocyte function and, therefore, is uncoupled from differentiation. Furthermore, ligating CD27 increases the threshold concentration at which IL-2 induces IFN-gamma-producing capability by the CD8+ T cell, suggesting that CD27 signaling may suppress effector differentiation. Finally, CD8+ T cells that have been stimulated by the TCR/CD27 pathway maintain their capacity for subsequent expansion and effector differentiation in response to a viral challenge in vivo. Thus, the TCR/CD27 pathway enables the CD8+ T cell to replicate by a process of self-renewal, which may contribute to the continuous generation of new effector CD8+ T cells in persistent viral infections.
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Gastrointestinal complications in AIDS patients with diarrhoea are common clinical manifestations, frequently diagnosed by colonoscopy as non-specific colitis. We retrospectively study colon biopsies diagnosed as chronic colitis associated with HIV (CCH). Biopsies were sorted as patients with AIDS (serum CD4 < 200 cell/mm(3)) but without any clear infectious process (n = 12) and patients without HIV infection (n = 24). There are low numbers of CD4+ T lymphocytes in lamina propria of AIDS patients, but CD8+ T populations in this area appear to be similar in all studied groups, regardless of HIV infection or laboratory evidence of a specific agent. We found the clear evidence of CD8+ T cells infiltration in colonic mucosa in HIV patients with microscopic colitis. An imbalance of lymphocyte subpopulations in the colon, both in the lamina propria and epithelium, could result in an intraepithelial CD8 infiltration, involved in the pathogenesis of CCH in AIDS patients.
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Fish oil supplementation has been shown to improve the cachectic state of tumor-bearing animals and humans. Our previous study showed that fish oil supplementation (1 g per kg body weight per day) for 2 generations had anticancer and anticachetic effects in Walker 256 tumor-bearing rats as demonstrated by reduced tumor growth and body weight loss and increased food intake and survival. In this study, the effect of fish oil supplementation for 2 generations on membrane integrity, proliferation capacity, and CD4/CD8 ratio of lymphocytes isolated from mesenteric lymph nodes, spleen, and thymus of Walker 256 tumor-bearing animals was investigated. We also determined fish oil effect on plasma concentration and ex vivo production of cytokines [tumor necrosis factor-alpha (TNF-alpha), interferon-gamma (IFN-gamma), interleukin-4 (IL-4), IL-6, and IL-10]. Lymphocytes from thymus of tumor-bearing rats presented lower viability, but this change was abolished by fish oil supplementation. Tumor growth increased proliferation of lymphocytes from all lymphoid organs, and fish oil supplementation abolished this effect. Ex vivo production of TNF-alpha and IL-6 was reduced in supplemented animals, but IL-4 and IL-10 secretion was stimulated in both nontumor and tumor-bearing rats. IL-10 and IFN-gamma plasma levels was also decreased in supplemented animals. These results suggest that the anticachetic effects of fish oil supplementation for a long period of time (2 generations) in Walker 256 tumor-bearing rats may be associated to a decrease in lymphocyte function as demonstrated by reduced viability, proliferation capacity, and cytokine production.
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Lymphotoxin alpha (LTA) is a member of the TNF cytokine superfamily, produced principally by lymphocytes. It plays an important role in immune and inflammatory responses. Many TNF superfamily members have functionally important isoforms generated by alternative splicing but alternative splicing of LTA has never been studied. The known LTA protein is encoded by a transcript containing four exons. Here we report seven new LTA splice variants, three of them evolutionary conserved. We demonstrate their presence in cytoplasmic RNA suggesting that they could be translated into new LTA isoforms. We observed that their expression is differentially regulated upon activation of peripheral blood mononuclear cells and lymphocyte subpopulations (CD4+, CD8+, and CD19+). Our data suggest that the new LTA splice variants might play a role in the regulation of the immune response. (C) 2007 Elsevier Ltd. All rights reserved.
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Fundao de Amparo Pesquisa do Estado de So Paulo (FAPESP)
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A DNA vaccine based on the heat-shock protein 65 Mycobacterium leprae gene (pHSP65) presented a prophylactic and therapeutic effect in an experimental model of tuberculosis. In this paper, we addressed the question of which protective mechanisms are activated in Mycobacterium tuberculosis-infected mice after immune therapy with pHSP65. We evaluated activation of the cellular immune response in the lungs of infected mice 30 days after infection (initiation of immune therapy) and in those of uninfected mice. After 70 days (end of immune therapy), the immune responses of infected untreated mice, infected pHSP65-treated mice and infected pCDNA3-treated mice were also evaluated. Our results show that the most significant effect of pHSP65 was the stimulation of CD8+ lung cell activation, interferon- recovery and reduction of lung injury. There was also partial restoration of the production of tumour necrosis factor-. Treatment with pcDNA3 vector also induced an immune stimulatory effect. However, only infected pHSP65-treated mice were able to produce significant levels of interferon- and to restrict the growth of bacilli.
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Infected dogs are urban reservoirs of Leishmania chagasi, which is a causative agent of visceral leishmaniasis (VL). Dogs exhibit immune suppression during the course of this disease, and lymphocyte apoptosis is involved in this process. To investigate apoptosis and the expression levels of FAS-FAS-associated death domain protein (CD95 or APO-1), FASL-FAS ligand protein (CD178), and TRAIL-TNF-related apoptosis-inducing ligand (CD253) receptors in peripheral blood mononuclear cells and spleen leukocytes from 38 symptomatic dogs with moderate VL and 25 healthy dogs were evaluated by flow cytometry. The apoptosis rate of blood and splenic CD4+ and CD8+ cells was higher in infected dogs than in healthy dogs. The expression levels of FAS and FASL in blood and splenic CD4+ cells were lower in infected dogs than in healthy dogs. FAS expression in CD8+ cells was higher in infected dogs than in healthy dogs; in contrast, FASL expression was lower in infected dogs. The expression of the TRAIL receptor increased only in splenic CD8+ cells from infected dogs. The FAS and FAS-L blocking antibodies confirmed the importance of these receptors in apoptosis. Our results enhance the current understanding of the immune response in dogs infected with L. chagasi, facilitating the future development of therapeutic interventions to reduce lymphocyte depletion. 2013 Elsevier B.V.
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Fundao de Amparo Pesquisa do Estado de So Paulo (FAPESP)
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Ps-graduao em Biocincias e Biotecnologia Aplicadas Farmcia - FCFAR
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Fundao de Amparo Pesquisa do Estado de So Paulo (FAPESP)
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The expression of immune response as a leukocytic infiltrate by CD4+ and CD8+ cells in the epithelium and in the intestinal lamina propria of chicks fed Lactobacillus spp or cecal microflora (CM) and experimentally challenged or not with Salmonella enterica serovar Enteritidis (SE) was studied using immunohistochemistry. Three hundred and twenty day-of-hatch broiler chicks were divided into four groups of 80 birds each and orally received L. reuteri, L. salivarius, L. acidophilus, or CM. Each group was subdivided into four subgroups of 20 birds each, classified as follows: a subgroup did not receive any oral treatment (negative control), subgroup treated with L. spp or CM, subgroup treated with L. spp or CM and challenged with SE, and subgroup only challenged with SE (positive control). The results show that the oral treatment with L. reuteri, L. salivarius, L. acidophilus, or CM and challenge or not with SE stimulated bird immune response as determined by the leukocytic infiltrate by CD8+ lymphocytes followed by CD4+ in the epithelium and in the lamina propria of the duodenum, jejunum, and cecum of chicks up to 12 days of age. CD8+ lymphocyte number was significantly higher in the intestine of chicks receiving CM and challenged with SE. The duodenum, followed by the jejunum, were the segments in which the immune response, as shown by T, CD4+ and CD8+ cells, was stimulated with the greatest intensity.
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Fundao de Amparo Pesquisa do Estado de So Paulo (FAPESP)
