We have studied the role of various stromal cells of secondary lymphoid organs in IL-33 driven T cell responses to viral infection. We have used in vivo mouse models to identify the critical cellular sources of IL-33 as well as their contribution in regulating CD8 T cell function. Using IL-33 reporter mice, we identified fibroblastic reticular cells (FRC) and lymphatic endothelial cells (LEC) as the main IL-33 sources in lymph nodes (LN) of naïve and virus-infected mice, both within the T zone and the medulla. During infection with lymphocytic choriomeningitis virus (LCMV) clone 13, these stromal cells lose most IL-33 expression presumably due to release thereby boosting the antiviral T cell response. Using mice lacking IL-33 selectively in FRC versus LEC we identify T zone FRC as the key IL-33 source driving the expansion and function of antiviral CD8+ T cells. Collectively, these findings show that LN FRC not only regulate the homeostasis and priming of T cells but also their expansion and effector cell differentiation.
The research results have been and will be shared with the scientific community by the following means:
• Publications of scientific articles: a manuscript is in preparation (close to being submitted).
• Conferences / Congresses: attendance to national and international scientific meetings, where I have presented the data with poster presentations.
• Seminars / symposiums: I have presented my research in seminars and symposiums, inside and outside my research center.