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Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells

CD4 T-cell help is required for the induction of efficient CD8 T-cells responses and the generation of memory cells. Lack of CD4 T-cell help may contribute to an exhausted CD8 phenotype and viral persistence. Little is known about priming of CD4 T-cells by liver-derived antigen. We used TF-OVA mice...

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Autores principales: Derkow, Katja, Müller, Anja, Eickmeier, Ira, Seidel, Daniel, Rust Moreira, Marcos Vicinius, Kruse, Nils, Klugewitz, Katja, Mintern, Justine, Wiedenmann, Bertram, Schott, Eckart
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3136477/
https://www.ncbi.nlm.nih.gov/pubmed/21779338
http://dx.doi.org/10.1371/journal.pone.0021847
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author Derkow, Katja
Müller, Anja
Eickmeier, Ira
Seidel, Daniel
Rust Moreira, Marcos Vicinius
Kruse, Nils
Klugewitz, Katja
Mintern, Justine
Wiedenmann, Bertram
Schott, Eckart
author_facet Derkow, Katja
Müller, Anja
Eickmeier, Ira
Seidel, Daniel
Rust Moreira, Marcos Vicinius
Kruse, Nils
Klugewitz, Katja
Mintern, Justine
Wiedenmann, Bertram
Schott, Eckart
author_sort Derkow, Katja
collection PubMed
description CD4 T-cell help is required for the induction of efficient CD8 T-cells responses and the generation of memory cells. Lack of CD4 T-cell help may contribute to an exhausted CD8 phenotype and viral persistence. Little is known about priming of CD4 T-cells by liver-derived antigen. We used TF-OVA mice expressing ovalbumin in hepatocytes to investigate CD4 T-cell priming by liver-derived antigen and the impact of CD4 T-cell help on CD8 T-cell function. Naïve and effector CD4 T-cells specific for ovalbumin were transferred into TF-OVA mice alone or together with naïve ovalbumin-specific CD8 T-cells. T-cell activation and function were analyzed. CD4 T-cells ignored antigen presented by liver antigen-presenting cells (APCs) in vitro and in vivo but were primed in the liver-draining lymph node and the spleen. No priming occurred in the absence of bone-marrow derived APCs capable of presenting ovalbumin in vivo. CD4 T-cells primed in TF-OVA mice displayed defective Th1-effector function and caused no liver damage. CD4 T-cells were not required for the induction of hepatitis by CD8 T-cells. Th1-effector but not naïve CD4 T-cells augmented the severity of liver injury caused by CD8 T-cells. Our data demonstrate that CD4 T-cells fail to respond to liver-derived antigen presented by liver APCs and develop defective effector function after priming in lymph nodes and spleen. The lack of CD4 T-cell help may be responsible for insufficient CD8 T-cell function against hepatic antigens.
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spelling pubmed-31364772011-07-21 Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells Derkow, Katja Müller, Anja Eickmeier, Ira Seidel, Daniel Rust Moreira, Marcos Vicinius Kruse, Nils Klugewitz, Katja Mintern, Justine Wiedenmann, Bertram Schott, Eckart PLoS One Research Article CD4 T-cell help is required for the induction of efficient CD8 T-cells responses and the generation of memory cells. Lack of CD4 T-cell help may contribute to an exhausted CD8 phenotype and viral persistence. Little is known about priming of CD4 T-cells by liver-derived antigen. We used TF-OVA mice expressing ovalbumin in hepatocytes to investigate CD4 T-cell priming by liver-derived antigen and the impact of CD4 T-cell help on CD8 T-cell function. Naïve and effector CD4 T-cells specific for ovalbumin were transferred into TF-OVA mice alone or together with naïve ovalbumin-specific CD8 T-cells. T-cell activation and function were analyzed. CD4 T-cells ignored antigen presented by liver antigen-presenting cells (APCs) in vitro and in vivo but were primed in the liver-draining lymph node and the spleen. No priming occurred in the absence of bone-marrow derived APCs capable of presenting ovalbumin in vivo. CD4 T-cells primed in TF-OVA mice displayed defective Th1-effector function and caused no liver damage. CD4 T-cells were not required for the induction of hepatitis by CD8 T-cells. Th1-effector but not naïve CD4 T-cells augmented the severity of liver injury caused by CD8 T-cells. Our data demonstrate that CD4 T-cells fail to respond to liver-derived antigen presented by liver APCs and develop defective effector function after priming in lymph nodes and spleen. The lack of CD4 T-cell help may be responsible for insufficient CD8 T-cell function against hepatic antigens. Public Library of Science 2011-07-14 /pmc/articles/PMC3136477/ /pubmed/21779338 http://dx.doi.org/10.1371/journal.pone.0021847 Text en Derkow et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Derkow, Katja
Müller, Anja
Eickmeier, Ira
Seidel, Daniel
Rust Moreira, Marcos Vicinius
Kruse, Nils
Klugewitz, Katja
Mintern, Justine
Wiedenmann, Bertram
Schott, Eckart
Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells
title Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells
title_full Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells
title_fullStr Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells
title_full_unstemmed Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells
title_short Failure of CD4 T-Cells to Respond to Liver-Derived Antigen and to Provide Help to CD8 T-Cells
title_sort failure of cd4 t-cells to respond to liver-derived antigen and to provide help to cd8 t-cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3136477/
https://www.ncbi.nlm.nih.gov/pubmed/21779338
http://dx.doi.org/10.1371/journal.pone.0021847
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