Mitogenic activity of anti‐CD28 MoAb CLB‐CD28/1 on peripheral blood mononuclear cells and its cooperation with other anti‐T cells MoAb in the activation of purified T lymphocytes

Abstract

Human T lymphocyte proliferative response induced via CD28 molecule is analyzed. An anti CD28 MoAb, CLB‐CD28/1, induces the proliferation of human peripheral blood mononuclear cells in the absence of other stimuli, indicating that CD28 molecule can directly mediate a mitogenic signal in this system. The mitogenic activity of MoAb CLB‐CD28/1 on PBMC does not require MoAb interaction with monocyte Fc receptors, since F(ab′)₂ fragments from the MoAb are mitogenic to the same extent as whole IgG. Nevertheless, the activity depends on the presence of accessory cells, since purified T lymphocytes require addition of irradiated monocytes and interleukin 2 to proliferate when incubated with MoAb CLB‐CD28/1. On the other hand, MoAb CLB‐CD28/1 induces response to IL‐2 in thymocytes in the absence of accessory cells. Cooperation of MoAb CLB‐CD28/1 with three other MoAbs, recognizing CD3, CD5 and HLA Class I antigens, respectively, induces Tac antigen expression and IL‐2 responsiveness in purified T lymphocytes. This effect is obtained without cross‐linking of the MoAb. It does not rely on a physical association between CD28 and CD3, CD5 or HLA Class I molecules, as demonstrated by co‐modulation experiments. These data indicate that expression of IL‐2 receptor on T lymphocytes can result from interaction of multiple activation pathways and that some of them, such as those mediated by CD5 and HLA Class I antigens, previously reported to serve as modulatory circuits, can instead act as essential elements in the onset of T lymphocyte proliferation.