Different Nature of the Proliferation Defects of GLD, LPR and MEV C57BL/6 Mouse Lymphoid Cells

The three non-allelic gld, Ipr and mev mutations in the mouse all lead to profound immunodeficiency besides a splenomegaly and a generalized autoimmunity. Spleen cells from young B6 gld, B6 Ipr and B6 mev mice all display a decreased proliferative response to the T-cell mitogen concanavalin A (ConA), but the nature of the deficiency seems very different. No restoration of proliferation could be obtained by adding exogenous recombinant rIL2 to ConA-treated mev spleen cells, this lack of IL2-responsiveness suggesting a lack of (functional) IL2-receptors. In young mice of both gld and Ipr strains, a B6 wild-type level of proliferation could be reached by rIL2 addition to ConA-treated spleen cells, this normal responsiveness to exogenous IL2 suggesting a normal expression of IL2-receptors. The endogenous IL2 production by ConA-treated spleen cells decreased very much with ageing in both B6 gld and B6 Ipr mice. Yet, IL2 production in young mice revealed an earlier deficiency of the B6 Ipr mice: the young B6 gl...