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Characterization of virus-primed CD8+ T cells with a type 1 cytokine profile
Authors:Christensen  Jan Pravsgaard; Stenvang  Jens Peter; Marker  Ole; Thomsen  Allan Randrup
Institution:Institute of Medical Microbiology and Immunology, The Panum Institute 3C Blegdamsvej, 2200 N, Copenhagen, Denmark
1 The Bartholin Institute, Kommunehospitalet 5Øster Farimagsgade, 1399K Copenhagen, Denmark
Abstract:Infection with lymphocytic chorlomeningitis virus is associatedwith marked polyclonal activation of the CD8+ T cell subpopulation.In this report the cytokine production of virus-activated Tcells is analyzed and the producing cells subset is characterizedphenotypically. CoinciB. A. Askonasding with other parametersof cell-mediated immunity, splenic T cells appear which areable to release high amounts of IFN-{gamma}, but not IL-5, IL-10 ortumor necrosis factor-{alpha} upon short-term stimulation with anti-CD3in vitro. A similar profile is observed analyzing T cells takenfrom an inflammatory site. Phenotypically, the main cytokine-producingcell subset is found to be CD8+ cells targeted for homing toinflammatory sites (VLA-4hiL-selectinlo) of which 30–40%were positive by intracellular staining for IFN-{gamma}. This subsetalso contains all T cells with a cytotoxic potential as measuredby redirected killing. An enhanced cytotoxic potential as wellas an increased capacity to produce IFN-{gamma} is observed for atleast 2 months after infection and cell sorting analysis revealedthat this could be ascribed to a long-standing increase in thefrequency of CD8+Pgp-1hi cells. Therefore, these results demonstratethat systemic virus infection may exert marked perturbationof the CD8+ T cell population resulting in generation of a long-livedsubset of primed cells with important effector potential.
Keywords:CD8+ T cells  cytokines  inflammation  virus infection
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