| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 3367992 | Journal of Autoimmunity | 2012 | 10 Pages |
Previously we showed that transgenic mice expressing human HLA-DR3 gene are susceptible to PLP91–110 induced experimental autoimmune encephalomyelitis (EAE) and can serve as an animal model of multiple sclerosis (MS). HLA-DR3 mice with EAE showed increased number of CD8 T cells indicating their important role in disease pathogenesis. The role of CD8 T cells in MS, an inflammatory demyelinating disease of CNS, has been enigmatic as it has been assigned both regulatory and pathogenic roles. Therefore, to evaluate the role of CD8 T cells, we generated CD8 deficient HLA-DR3 transgenic mice (DR3.CD8−/−). Immunization with PLP91–110 led to more severe EAE in DR3.CD8−/− mice compared to HLA-DR3 mice indicating a regulatory role for CD8 T cells. Interestingly, DR3.CD8−/− mice with EAE showed decreased CNS pathology compared to DR3 mice thus suggesting a pathogenic role for CD8 T cells. We show that these two subsets of CD8 T cells can be differentiated based on the surface expression of CD122 (IL-2 Rβ chain). CD8 T cells expressing CD122 (CD8+CD122+) play a regulatory role while CD8+CD122− T cells act as a pathogenic subset. CD122 expressing CD8 T cells are the regulatory subset of CD8 T cells and regulate the encephalitogenic CD4 T cells through direct modulation of antigen presenting cells and/or through the release of immunoregulatory cytokines such as IL-10, IFNγ and TGFβ. We also showed that adoptive transfer of CD8CD122− T cells caused increased spinal cord demyelination indicating that these are pathogenic subset of CD8 T cells. Our study suggests that CD8+ T cells play both regulatory as well as pathogenic role in disease pathogenesis of EAE. A better understanding of these subsets could aid in designing novel therapy for MS patients.
► CD4+ T cells are required for development of EAE in HLA-DR3 transgenic mice. ► CD8+ T cells play both regulatory and pathogenic role in PLP91–110 induced EAE. ► CD8+CD122+ T cells are regulatory subset of CD8 T cells. ► CD8+CD122+ cells regulate immune response by modulation of antigen presentation. ► CD8+CD122− T cells are pathogenic subset of CD8 T cells and induce CNS pathology.
