Advanced glycation end products (AGEs) activate mast cells

BACKGROUND AND PURPOSEAdvanced glycation endproducts (AGEs) represent one of the many types of chemical modifications that occur with age in long‐lived proteins. AGEs also accumulate in pathologies such as diabetes, cardiovascular diseases, neurodegeneration and cancer. Mast cells are major effectors of acute inflammatory responses that also contribute to the progression of chronic diseases. Here we investigated interactions between AGEs and mast cells.EXPERIMENTAL APPROACHESHistamine secretion from AGEs‐stimulated mast cells was measured. Involvement of a receptor for AGEs, RAGE, was assessed by PCR, immunostaining and use of inhibitors of RAGE. Production of reactive oxygen species (ROS) and cytokines was measured.KEY RESULTSAdvanced glycation endproducts dose‐dependently induced mast cell exocytosis with maximal effects being obtained within 20 s. RAGE mRNA was detected and intact cells were immunostained by a specific anti‐RAGE monoclonal antibody. AGEs‐induced exocytosis was inhibited by an anti‐RAGE antibody and by low molecular weight heparin, a known RAGE antagonist. RAGE expression levels were unaltered after 3 h treatment with AGEs. AGE‐RAGE signalling in mast cells involvesPertussistoxin‐sensitive Gi‐proteins and intracellular Ca2+increases as pretreatment withPertussistoxin, caffeine, 2‐APB and BAPTA‐AM inhibited AGE‐induced exocytosis. AGEs also rapidly stimulated ROS production. After 6 h treatment with AGEs, the pattern of cytokine secretion was unaltered compared with controls.CONCLUSIONS AND IMPLICATIONSAdvanced glycation endproducts activated mast cells and may contribute to a vicious cycle involving generation of ROS, increased formation of AGEs, activation of RAGE and to the increased low‐grade inflammation typical of chronic diseases.