AbstractThe NF-κB family of transcription factors are involved in the regulation of innate and adaptive immune functions associated with resistance to infection. To assess the role of NF-κB2 in the regulation of cell-mediated immunity, mice deficient in the NF-κB2 gene (NF-κB2−/−) were challenged with the intracellular parasite Toxoplasma gondii. Resistance to this opportunistic pathogen is dependent on the production of IL-12, which is required for the development of innate NK cell and adaptive T cell responses dominated by the production of IFN-γ necessary to control replication of this parasite. Although wild-type controls were resistant to T. gondii, NF-κB2−/− mice developed severe toxoplasmic encephalitis and succumbed to disease between 3 and 10 wk following infection. However, NF-κB2 was not required for the ability of macrophages to produce IL-12 or to inhibit parasite replication and during the acute stage of infection, NF-κB2−/− mice had no defect in their ability to produce IL-12 or IFN-γ and infection-induced NK cell responses appeared normal. In contrast, during the chronic phase of the infection, susceptibility of NF-κB2−/− mice to toxoplasmic encephalitis was associated with a reduced capacity of their splenocytes to produce IFN-γ associated with a loss of CD4+ and CD8+ T cells. This loss of T cells correlated with increased levels of apoptosis and with elevated expression of the pro-apoptotic molecule Fas by T cells from infected NF-κB2−/− mice. Together, these results suggest a role for NF-κB2 in the regulation of lymphocyte apoptosis and a unique role for this transcription factor in maintenance of T cell responses required for long-term resistance to T. gondii.