CD38 expression and functional activities are up‐regulated by IFN‐γ on human monocytes and monocytic cell lines

Human CD38, a surface molecule expressed by immature and activated T and B lymphocytes, has been characterized as a molecule transducing activation and proliferation signals, and intervening in adhesion to endothelium via its ligand CD31. CD38 is also a complex ectoenzyme featuring ADP‐ribosyl cyclase/cyclic ADP‐ribose hydrolase activities, leading to the synthesis and degradation of cADPR, a Ca + ‐mobilizing agent. We investigated the effects of monocyte‐activating stimuli (IFN‐γ, IL‐2, LPS, TNF‐α, and GM‐CSF) on the expression and function of CD38, starting from the observation that human monocytes and the derived lines U937, THP‐1, and Mono‐Mac‐6 bear the molecule on their surface. Our results indicate that IFN‐γ is a strong up‐modulator of CD38, and IL‐2 increases its expression only modestly. LPS, TNF‐α, and GM‐CSF had no detectable effects. Treatment with IFN‐γ produced a dose‐ and time‐dependent up‐regulation of CD38 in monocytes and monocytic lines, which was paralleled by increased ADP‐ribosyl cyclase/cyclic ADP‐ribose hydrolase activities. Furthermore, CD38 ligation by specific MoAb reduced the IFN‐γ‐dependent enhancement of monocyte‐dynamic adhesion to endothelial monolayers. These findings identify IFN‐γ as a modulator of monocytic CD38 expression and indicate that CD38 plays a specific role in the activation and adhesion processes performed by monocytes.