Lecky, D. A.; Sheriff, L.; Rouvray, S. T.; George, L. S.; Drummond, R. A.; Wraith, D. C.; Bending, D.

Strong T-cell receptor (TCR) and IL-27 signalling influence type-1 regulatory (Tr1) T-cell development but whether other signals determine their differentiation is unclear. Utilising Tg4 TCR transgenic mice we established a model for rapid Tr1 cell induction. A single high dose of [4Y]-MBP peptide drove the differentiation of Il10+ T-cells with bona fide Tr1 cell protein and mRNA signatures. Kinetic transcriptional analysis revealed that the Tr1 cell module was transient and preceded by a burst of Ifng transcription in CD4+ T-cells. Neutralisation of IFN{gamma} reduced Tr1 cell frequency and strong TCR signalling markers, which was correlated with reduced macrophage activation. Antibody depletion experiments inferred that T-cells - but not NK cells - provided the relevant source of IFN{gamma}. Additionally, we show that blocking IL-27 in combination with IFN{gamma} neutralisation additively reduced Tr1 cell frequency in vivo. These findings reveal that during strong tolerogenic TCR signalling IFN-{gamma} has a non-redundant regulatory role in augmenting the differentiation of Tr1 cells in vivo.