Selective suppression of the cytotoxic T cell response to influenza virus in mice

Abstract

Mice injected with inactivated (UV light-irradiated) influenza virus produce specific antibody, become sensitized for a delayed-type hypersensitivity reaction, but do not generate specific cytotoxic T (T_c) cells. If injected 4–5 days later with infectious virus, the formation of T_c cells is suppressed by > 90%. If A strain viruses are used, the suppression observed is cross-reactive within A strain viruses but does not extend to B/LEE or to Sendai virus. Serum from mice injected with UV-irradiated virus contains antibodies which on adoptive transfer can inhibit T_c cell formation when infectious homologous virus is used to challenge the recipients. Spleen cells from the same mice, upon adoptive transfer, also inhibit (50–70%) T_c cell formation if transferred within 24 h of injection of infectious virus, and the specificity pattern observed is cross-reactive within A strains. The activitiy of the cells mediating suppression is destroyed by monospecific anti-Thy-1.2 antibody and complement. The immune cells require I region sharing between donor and recipient mice for their suppressor activity to be effective. (There is also a partial requirement for K. D region sharing, but the possible rejection of transferred cells is not excluded.) Dilution assays in which clonal expansion of T_c precursors is used to estimate their frequency and the presence of T helper (T_h) cells indicate that suppressed mice possess T_c precursors and primed cells which, upon restimulation, act as T_h cells. Furthermore, injection of irradiated T_h cells with inactivated virus does not significantly reduce the ensuing suppression.