Anatomical and Cellular Requirements for the Activation and Migration of Virus-Specific CD8+T Cells to the Brain during Theiler's Virus Infection
Open Access
- 1 March 2005
- journal article
- Published by American Society for Microbiology in Journal of Virology
- Vol. 79 (5) , 3063-3070
- https://doi.org/10.1128/jvi.79.5.3063-3070.2005
Abstract
Theiler's murine encephalomyelitis virus (TMEV) infection of the brain induces a virus-specific CD8+T-cell response in genetically resistant mice. The peak of the immune response to the virus occurs 7 days after infection, with an immunodominant CD8+T-cell response against a VP2-derived capsid peptide in the context of the Dbmolecule. The process of activation of antigen-specific T cells that migrate to the brain in the TMEV model has not been defined. The site of antigenic challenge in the TMEV model is directly into the brain parenchyma, a site that is considered immune privileged. We investigated the hypothesis that antiviral CD8+T-cell responses are initiated in situ upon intracranial inoculation with TMEV. To determine whether a brain parenchymal antigen-presenting cell is responsible for the activation of virus-specific CD8+T cells, we evaluated the CD8+T-cell response to the VP2 peptide in bone marrow chimeras and mutant mice lacking peripheral lymphoid organs. The generation of the anti-TMEV CD8+T-cell response in the brain requires priming by a bone marrow-derived antigen-presenting cell and the presence of peripheral lymphoid organs. Although our results show that activation of TMEV-specific CD8+T cells occurs in the peripheral lymphoid compartment, they do not exclude the possibility that the immune response to TMEV is initiated by a brain-resident, bone marrow-derived, antigen-presenting cell.Keywords
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