Longevity of Antigen Presentation and Activation Status of APC Are Decisive Factors in the Balance Between CTL Immunity Versus Tolerance

Encounter of Ag by naive T cells can lead to T cell priming as well as tolerance. The balance between immunity and tolerance is controlled by the conditions of Ag encounter and the activation status of the APC. We have investigated the rules that govern this balance in case an environment that norma...

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Veröffentlicht in:	The Journal of immunology (1950) 2001-09, Vol.167 (5), p.2522-2528
Hauptverfasser:	Th. den Boer, Annemieke, Diehl, Linda, van Mierlo, Geertje J. D, van der Voort, Ellen I. H, Fransen, Marieke F, Krimpenfort, Paul, Melief, Cornelis J. M, Offringa, Rienk, Toes, Rene E. M
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Sprache:	eng
Schlagworte:	Adenovirus E1A Proteins - administration & dosage Adenovirus E1A Proteins - immunology Animals Antigen Presentation Antigen-Presenting Cells - immunology CD40 Antigens - metabolism Humans Immune Tolerance Kinetics Lymphocyte Activation Mice Mice, Inbred C57BL Mice, Transgenic Neoplasms, Experimental - immunology Neoplasms, Experimental - therapy Receptors, Antigen, T-Cell, alpha-beta - genetics Receptors, Antigen, T-Cell, alpha-beta - metabolism T-Lymphocytes, Cytotoxic - immunology
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creator	Th. den Boer, Annemieke Diehl, Linda van Mierlo, Geertje J. D van der Voort, Ellen I. H Fransen, Marieke F Krimpenfort, Paul Melief, Cornelis J. M Offringa, Rienk Toes, Rene E. M
description	Encounter of Ag by naive T cells can lead to T cell priming as well as tolerance. The balance between immunity and tolerance is controlled by the conditions of Ag encounter and the activation status of the APC. We have investigated the rules that govern this balance in case an environment that normally induces tolerance is reverted into a milieu that promotes T cell priming, using a minimal CTL epitope derived from human adenovirus type 5 E1A. Vaccination of mice s.c. with E1A peptide in IFA readily induces CTL tolerance, resulting in the inability to control E1A-expressing tumors. The present study shows that efficient CTL priming is achieved when this peptide vaccine is combined with systemic administration of APC-activating compounds like agonistic anti-CD40 mAb or polyriboinosinate-polyribocytidylate. Surprisingly, this CTL response is not long-lasting and therefore fails to protect against tumor outgrowth. Disappearance of CTL reactivity was strongly associated with systemic persistence of the peptide for >200 days. In contrast, peptide administered in PBS does not persist and generates long term CTL immunity capable of rejecting Ad5E1A-positive tumors, when combined with CD40 triggering. Thus, presentation of CTL epitopes in an appropriate costimulatory setting by activated APC, although being essential and sufficient for CTL priming, eventually results in tolerance when the Ag persists systemically for prolonged times. These observations are important for the development of immune intervention schemes in autoimmunity and cancer.
doi_str_mv	10.4049/jimmunol.167.5.2522
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The present study shows that efficient CTL priming is achieved when this peptide vaccine is combined with systemic administration of APC-activating compounds like agonistic anti-CD40 mAb or polyriboinosinate-polyribocytidylate. Surprisingly, this CTL response is not long-lasting and therefore fails to protect against tumor outgrowth. Disappearance of CTL reactivity was strongly associated with systemic persistence of the peptide for >200 days. In contrast, peptide administered in PBS does not persist and generates long term CTL immunity capable of rejecting Ad5E1A-positive tumors, when combined with CD40 triggering. Thus, presentation of CTL epitopes in an appropriate costimulatory setting by activated APC, although being essential and sufficient for CTL priming, eventually results in tolerance when the Ag persists systemically for prolonged times. 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We have investigated the rules that govern this balance in case an environment that normally induces tolerance is reverted into a milieu that promotes T cell priming, using a minimal CTL epitope derived from human adenovirus type 5 E1A. Vaccination of mice s.c. with E1A peptide in IFA readily induces CTL tolerance, resulting in the inability to control E1A-expressing tumors. The present study shows that efficient CTL priming is achieved when this peptide vaccine is combined with systemic administration of APC-activating compounds like agonistic anti-CD40 mAb or polyriboinosinate-polyribocytidylate. Surprisingly, this CTL response is not long-lasting and therefore fails to protect against tumor outgrowth. Disappearance of CTL reactivity was strongly associated with systemic persistence of the peptide for >200 days. In contrast, peptide administered in PBS does not persist and generates long term CTL immunity capable of rejecting Ad5E1A-positive tumors, when combined with CD40 triggering. Thus, presentation of CTL epitopes in an appropriate costimulatory setting by activated APC, although being essential and sufficient for CTL priming, eventually results in tolerance when the Ag persists systemically for prolonged times. 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subjects	Adenovirus E1A Proteins - administration & dosage Adenovirus E1A Proteins - immunology Animals Antigen Presentation Antigen-Presenting Cells - immunology CD40 Antigens - metabolism Humans Immune Tolerance Kinetics Lymphocyte Activation Mice Mice, Inbred C57BL Mice, Transgenic Neoplasms, Experimental - immunology Neoplasms, Experimental - therapy Receptors, Antigen, T-Cell, alpha-beta - genetics Receptors, Antigen, T-Cell, alpha-beta - metabolism T-Lymphocytes, Cytotoxic - immunology
title	Longevity of Antigen Presentation and Activation Status of APC Are Decisive Factors in the Balance Between CTL Immunity Versus Tolerance
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