Oral tolerance to systemic vaccination remains intact without RORt expression in regulatory T cells

Many promising vaccine candidates and licensed vaccines lead to variable immune responses within humans. Studies suggest that environmental exposures in the gastrointestinal tract could contribute to a reduction in vaccine efficacy via immune tolerance at this site; this is partly achieved by a high abundance of regulatory T cells (Tregs). It is unclear if Treg subsets regulate systemic vaccine responses following oral antigen pre-exposure. Here, we implemented a conditional knock-out mouse model of ROR gamma t+ Tregs to examine the role of these cells in mediating this process. Following oral exposure to the model antigen ovalbumin (OVA) prior to immunization, we found similar induction of vaccine-induced antibody responses in mice lacking ROR gamma t expression in Tregs compared to sufficient controls. Use of various adjuvants led to distinct findings. Our data suggest that expression of ROR gamma t+ within Tregs is not required to regulate tolerance to systemic vaccination following oral antigen exposure.