Prevention of experimental autoimmune encephalomyelitis by antibodies against interleukin 12.

JP Leonard, KE Waldburger, SJ Goldman - The Journal of experimental …, 1995 - rupress.org
JP Leonard, KE Waldburger, SJ Goldman
The Journal of experimental medicine, 1995rupress.org
Experimental allergic encephalomyelitis (EAE) is an autoimmune disease of the central
nervous system that can be transferred to naive mice via CD4+ T cells isolated from
appropriately immunized mice. We have evaluated the effects of recombinant murine
interleukin 12 (rmIL-12), a potent inducer of interferon gamma (IFN-gamma) and promoter of
Th1 T cell development, on the course of adoptively transferred EAE. The transfer of lymph
node cells (LNC) isolated from proteolipid protein (PLP)-primed animals and stimulated in …
Experimental allergic encephalomyelitis (EAE) is an autoimmune disease of the central nervous system that can be transferred to naive mice via CD4+ T cells isolated from appropriately immunized mice. We have evaluated the effects of recombinant murine interleukin 12 (rmIL-12), a potent inducer of interferon gamma (IFN-gamma) and promoter of Th1 T cell development, on the course of adoptively transferred EAE. The transfer of lymph node cells (LNC) isolated from proteolipid protein (PLP)-primed animals and stimulated in vitro with PLP to naive mice resulted in a progressive paralytic disease culminating in complete hind limb paralysis in the majority of the recipients. When mice were injected with LNC that had been stimulated in vitro with PLP in the presence of rmIL-12, the subsequent course of disease was more severe and prolonged. The addition of rmIL-12 during the in vitro stimulation with PLP resulted in a 10-fold increase in IFN-gamma and a 2-fold increase in tumor necrosis factor (TNF) alpha in the supernatants, relative to LNC stimulated with PLP alone. However, neutralization of IFN-gamma or TNF-alpha in vitro with specific antibodies did not abrogate the ability of rmIL-12 to exacerbate the subsequent disease. Similarly, mice treated with rmIL-12 in vivo after the transfer of antigen-stimulated LNC developed a more severe and prolonged course of disease compared with vehicle-treated control animals. In contrast, treatment of mice with an antibody to murine IL-12 after cell transfer completely prevented paralysis, with only 40% of the mice developing mild disease. These results demonstrate that in vitro stimulation of antigen primed LNC with PLP and rmIL-12 enhances their subsequent encephalitogenicity. Furthermore, inhibition of endogenous IL-12 in vivo after LNC transfer prevented paralysis, suggesting that endogenous IL-12 plays a pivotal role in the pathogenesis of this model of autoimmune disease.
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