Pre-exposure of human B cells to recombinant IL-1 enhances subsequent proliferation.

Author:

Freedman A S1,Freeman G1,Whitman J1,Segil J1,Daley J1,Nadler L M1

Affiliation:

1. Division of Tumor Immunology, Dana-Farber Cancer Institute, Boston, MA 02115.

Abstract

Abstract The reported effects of the monocyte-derived cytokine IL-1 on human B lymphocytes are both varied and controversial. IL-1 has been reported to augment both proliferation and Ig secretion of previously activated human B cells. In the present study highly purified splenic B cells were cultured with rIL-1 before, simultaneously with, and after the addition of the polyclonal B cell mitogen, anti-Ig. rIL-1 had no significant effect on B cell proliferation when added simultaneously with or after B cell activation with anti-Ig. However, incubation of splenic B cells with rIL-1 for 24 h before stimulation with anti-Ig appeared to enhance mitogenesis. With the observation that rIL-1 exerted effects on resting B cells, the effect of rIL-1 on several events which accompany B cell activation was examined. rIL-1 failed to stimulate RNA synthesis, effect increases in cell size or intracellular Ca2+ levels, or lead to the hyperexpression of MHC class II or B cell activation Ag. These studies suggest that rIL-1 does not activate B cells but primes them to respond to subsequent activation.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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