Interleukin-10 induces a long-term antigen-specific anergic state in human CD4+ T cells.
TL;DR: Human CD4+ T cells, activated by allogeneic monocytes in a primary mixed lymphocyte reaction in the presence of exogenous interleukin 10, specifically failed to proliferate after restimulation with the same alloantigens, demonstrating that IL-10 induces T cell anergy and therefore may play an important role in the induction and maintenance of antigen-specific T cell tolerance.
read more
Abstract: Human CD4+ T cells, activated by allogeneic monocytes in a primary mixed lymphocyte reaction in the presence of exogenous interleukin (IL) 10, specifically failed to proliferate after restimulation with the same alloantigens. A comparable state of T cell unresponsiveness could be induced by activation of CD4+ T cells by cross-linked anti-CD3 monoclonal antibodies (mAbs) in the presence of exogenous IL-10. The anergic T cells failed to produce IL-2, IL-5, IL-10, interferon gamma, tumor necrosis factor alpha, and granulocyte/macrophage colony-stimulating factor. The IL-10-induced anergic state was long-lasting. T cell anergy could not be reversed after restimulation of the cells with anti-CD3 and anti-CD28 mAbs, although CD3 and CD28 expression was normal. In addition, restimulation of anergized T cells with anti-CD3 mAbs induced normal Ca2+ fluxes and resulted in increased CD3, CD28, and class II major histocompatibility complex expression, indicating that calcineurin-mediated signaling occurs in these anergic cells. However, the expression of the IL-2 receptor alpha chain was not upregulated, which may account for the failure of exogenous IL-2 to reverse the anergic state. Interestingly, anergic T cells and their nonanergic counterparts showed comparable levels of proliferation and cytokine production after activation with phorbol myristate acetate and Ca2+ ionophore, indicating that a direct activation of a protein kinase C-dependent pathway can overcome the tolerizing effect of IL-10. Taken together, these data demonstrate that IL-10 induces T cell anergy and therefore may play an important role in the induction and maintenance of antigen-specific T cell tolerance.
read more
Chat with Paper
AI Agents for this Paper
Find similar papers on Google Scholar, PubMed and Arxiv
Write a critical review of this paper
Analyze citations of this paper to find unaddressed research gaps
Citations
Rough Titanium Oxide Coating Prepared by Micro-Arc Oxidation Causes Down-Regulation of hTERT Expression, Molecular Presentation, and Cytokine Secretion in Tumor Jurkat T Cells.
Igor A. Khlusov,Igor A. Khlusov,Larisa Litvinova,V. V. Shupletsova,Olga Khaziakhmatova,E. S. Melashchenko,Kristina A. Yurova,Vladimir Leitsin,Marina Khlusova,Vladimir F. Pichugin,Yurii P. Sharkeev +10 more
TL;DR: The roughness of the rTOC induces an electrostatic potential and decreases the viability of the immortalized Jurkat T cells through mechanisms unrelated to ROS generation, which may be useful for replacement surgery applications of rough TiO2 implants in cancer patients.
9
Patent
Methods of treating a subject afflicted with an autoimmune disease using predictive biomarkers of clinical response to glatiramer acetate therapy in multiple sclerosis
Suhayl Dhib-Jalbut
- 16 Mar 2011
TL;DR: In this paper, a method for treating a subject afflicted with an autoimmune disease with a pharmaceutical composition comprising glatiramer acetate and a pharmaceutically acceptable carrier was proposed.
9
Regulation of Human CD4 1 ab T-Cell-Receptor-Positive (TCR 1 ) and gd TCR 1 T-Cell Responses to Mycobacterium tuberculosis by Interleukin-10 and Transforming Growth Factor b
Roxana E. Rojas,Kithiganahalli N. Balaji,Ahila Subramanian,W. Henry Boom +3 more
- 01 Jan 1999
TL;DR: IL-10 and TGF-b both inhibited CD4 1 and gd T cells but differed in the mechanism used to inhibit T-cell responses to M. tuberculosis, resulting in fewer than 10% of infected persons developing active tuberculosis.
9
•Dissertation
Propriétés régulatrices des cellules dendritiques humaines traitées par l’acide mycophénolique
Roxane Lemoine
- 15 Dec 2009
TL;DR: In this article, the effets of l'acide mycophenolique (MPA, immunosuppresseur couramment utilise en transplantation) sur les cellules dendritiques (DC) humaines are explored, showing that le MPA diminue la capacite des DC a activer des lymphocytes T CD8+ cytotoxiques allogeniques en diminuant la synthese d'interferon gamma dans les DC.
9
Human recombinant IL-10 reduces xenogenic cytotoxicity via macrophage M2 polarization
TL;DR: Results show that hIL-10 transgenic pig can be used as a model to overcome acute immune rejection in pig-to-human xenotransplantation and suggest that the cytotoxicity of human macrophages was reduced by hil-10 from transgenic cells, inducing M2-like macrophage polarization.
9
References
Loss of CTLA-4 leads to massive lymphoproliferation and fatal multiorgan tissue destruction, revealing a critical negative regulatory role of CTLA-4
Elizabeth A. Tivol,Frank Borriello,A N Schweitzer,W P Lynch,Jeffrey A. Bluestone,Arlene H. Sharpe +5 more
TL;DR: In this article, the authors showed that CTLA-4-deficient mice rapidly develop lymphoproliferative disease with multiorgan lymphocytic infiltration and tissue destruction, with particularly severe myocarditis and pancreatitis, and die by 3-4 weeks of age.
2.9K
Interleukin 10 (IL-10) and viral IL-10 strongly reduce antigen-specific human T cell proliferation by diminishing the antigen-presenting capacity of monocytes via downregulation of class II major histocompatibility complex expression.
R de Waal Malefyt,John B. A. G. Haanen,H Spits,M G Roncarolo,A.A. te Velde,Carl G. Figdor,K E Johnson,Rob A. Kastelein,Hans Yssel,J E de Vries +9 more
TL;DR: It is indicated that IL-10 and v-IL-10 can completely prevent antigen-specific T cell proliferation by inhibition of the antigen-presenting capacity of monocytes through downregulation of class II MHC antigens on monocytes.
A cell culture model for T lymphocyte clonal anergy
TL;DR: The T cell enters an unresponsive state known as clonal anergy in which the T cell is incapable of producing its own growth hormone, interleukin-2, on restimulation.
2K
•Journal Article
IL-10 inhibits macrophage costimulatory activity by selectively inhibiting the up-regulation of B7 expression.
TL;DR: Direct evidence that the lack of B7 is the relevant limiting defect for IL-10-treated macrophage accessory cell function was obtained from studies in which the costimulatory capacity of IL- 10-treatedmacrophages could be completely restored by the addition of B 7 transfected, but not nontransfected and L cells to the assays.
903
Immunosuppression in vivo by a soluble form of the CTLA-4 T cell activation molecule
Peter S. Linsley,Philip M. Wallace,Jennifer S. Johnson,Marylou G. Gibson,Jo Anne L. Greene,Jeffrey A. Ledbetter,Cherry Singh,Mark A. Tepper +7 more
TL;DR: In vitro, when the B7 molecule on the surface of antigen-presenting cells binds to the T cell surface molecules CD28 and CTLA-4, a costimulatory signal for T cell activation is generated.
901