Interleukin 4 (IL) 4 up‐regulates gene and surface IL 1 receptor type I in murine T helper type 2 cells

Abstract

The T cell-derived cytokine interleukin (IL)4 is known to increase the proliferative response of T cells stimulated with IL1. IL4 is also an autocrine growth factor for type II T helper cells (T_h2) cells. In the present studies, we examined the effect of murine recombinant IL 4 on the expression of the IL 1 receptor type I (IL 1RtI) in murine T_h2 cell lines at the mRNA and surface level. Using a specific anti-murine IL 1RtI monoclonal antibody and flow microfluorometry, we found that IL 4 increased the surface expression of IL 1RtI in a dose-dependent manner. In D10S cells, a subline of the T_h2 cell line D10.G4.1, 50-500 pg/ml IL 4 up-regulated the receptor 1.8- to 3.2-fold (p < 0.05). This up-regulation was also seen at the mRNA level. The effect was not due to increased stability of the mRNA, since IL4 did not modify the half-life of IL 1RtI mRNA. IL4 also up-regulated IL 1RtI on CDC25 cells, another T_h2 cell line. However, we did not observe an effect of IL 4 on gene expression of IL 1RtI in BALB/c 3T3 fibroblasts. IL2 and IL4 showed an additive effect in up-regulating IL 1RtI and D10S cells. These studies indicate that IL4 up-regulates IL 1RtI in murine T_h2 cells by increasing gene expression for IL 1RtI without affecting mRNA stability. Thus, IL 4 production by T_h2 cells may amplify the immune response via up-regulation of IL 1RtI.