| First Author | Fontaine M | Year | 2018 |
| Journal | EMBO J | Volume | 37 |
| Issue | 3 | Pages | 398-412 |
| PubMed ID | 29263148 | Mgi Jnum | J:258319 |
| Mgi Id | MGI:6117969 | Doi | 10.15252/embj.201796881 |
| Citation | Fontaine M, et al. (2018) Regulatory T cells constrain the TCR repertoire of antigen-stimulated conventional CD4 T cells. EMBO J 37(3):398-412 |
| abstractText | To analyze the potential role of Tregs in controlling the TCR repertoire breadth to a non-self-antigen, a TCRbeta transgenic mouse model (EF4.1) expressing a limited, yet polyclonal naive T-cell repertoire was used. The response of EF4.1 mice to an I-Ab-associated epitope of the F-MuLV envelope protein is dominated by clones expressing a Valpha2 gene segment, thus allowing a comprehensive analysis of the TCRalpha repertoire in a relatively large cohort of mice. Control and Treg-depleted EF4.1 mice were immunized, and the extent of the Valpha2-bearing, antigen-specific TCR repertoire was characterized by high-throughput sequencing and spectratyping analysis. In addition to increased clonal expansion and acquisition of effector functions, Treg depletion led to the expression of a more diverse TCR repertoire comprising several private clonotypes rarely observed in control mice or in the pre-immune repertoire. Injection of anti-CD86 antibodies in vivo led to a strong reduction in TCR diversity, suggesting that Tregs may influence TCR repertoire diversity by modulating costimulatory molecule availability. Collectively, these studies illustrate an additional mechanism whereby Tregs control the immune response to non-self-antigens. |
