B cell sensitivity to IgE-suppressive activity of IFN-γ Is polymorphic and controlled by a non-H-2-linked gene

Abstract

It has been suggested that at least two distinct genetic factors are involved in developing atopic diseases. One is the major histocompatibity complex which controls antigen-specific polymorphism of IgE antibody responses and the other is an unidentified factor(s) which controls isotype selection, i.e., class switching to IgE. It is conceivable that both expression of and sensitivity to lymphokines that play central roles in controlling IgE biosynthesis may be involved in the latter polymorphism. To explore this possibility, we have examined the sensitivities of several mouse strains to interleukin (IL)-4 and interferon-γ (IFN-γ). The results show that (1) the sensitivity to IgE-suppressive activity of IFN-γ, but not to the IgE-enhancing activity of IL-4, is polymorphic (e.g., C57BL/6 is 8– to 16-fold more sensitive than BALB/c to IFN-γ); (2) F1 of these two strains (CByB6F1) are BALE/ c type and H-2 congenic mice of d haplotype with B6 background are C57BL/6 type, suggesting that low sensitivity is a non-H-2-linked dominant trait; (3) the polymorphism is determined at B cell levels; and (4) sensitivity to IFN-γ is not associated with mRNA expression of IFN-γ receptors (R) by B cells. These data collectively indicate that BALB/c mice have a non-H-2-linked gene which decreases B cell sensitivity to IFN-γ, but the gene effect is not associated with the expression of IFN-γR mRNA on B cells. The possible biological significance of the non-H-2-linked gene is discussed.