Ferritin is an iron-binding molecule, which comprises 24 subunits, heavy (FeH) and light (FeL) subunits, suggested to have a pathogenic role by the 'hyperferritinemic syndrome'. In this work, we tested (1) FeH and FeL in bone marrow (BM) and sera in patients with macrophage activation syndrome (MAS); (2) pro-inflammatory effects of ferritin, FeL, and FeH on macrophages; (3) ability of FeHstimulated macrophages to stimulate the proliferation of peripheral blood mononuclear cells (PBMCs); (4) production of mature IL-1β and IL-12p70 in extracellular compartments of FeH-stimulated macrophages. Immunofluorescence analysis and liquid chromatography mass spectrometry (LC-MS/ MS) based proteomics were performed to identify FeL and FeH in BM and sera, respectively, in the same patients. Macrophages were stimulated with ferritin, FeH, and FeL to assess pro-inflammatory effects by RT-PCR and western blot. The proliferation of co-cultured PBMCs with FeH-stimulated macrophages was tested. Immunofluorescence showed an increased FeH expression in BMs, whereas LC-MS/MS identified that FeL was mainly represented in sera. FeH induced a significant increase of gene expressions of IL-1β, IL-6, IL-12, and TNF-α, more marked with FeH, which also stimulated NLRP3. FeH-stimulated macrophages enhanced the proliferation of PBMCs. The ELISA assays showed that mature form of IL-1β and IL-12p70 were increased, in extracellular compartments of FeHstimulated macrophages. Our results showed FeH in BM biopsies of MAS patients, whereas, LC-MS/ MS identified FeL in the sera. FeH showed pro-inflammatory effects on macrophages, stimulated NLRP3, and increased PBMCs proliferation. Adult-onset Still's disease (AOSD) is an inflammatory disease characterised by high spiking fevers, arthritis, evanescent skin rash, and a typical increase of serum ferritin levels 1,2. AOSD is considered a multigenic autoinflammatory disease at the "crossroads" of autoinflammatory and autoimmune diseases, considering its complex pathogenesis, which involves both arms of the immune system 3. The aberrant activation of the immune system leads to production and release of pro-inflammatory cytokines including interleukin (IL)-1β, IL-6, IL-18, interferon (IFN)-γ and tumor necrosis factor (TNF-α) 1-3 , which represent common therapeutic targets 4,5. Patients with AOSD may experience several life-threatening complications, mostly macrophage activation syndrome (MAS), a hyperinflammatory syndrome, with high mortality rate 6,7. Considering the frequent association between these two diseases, it has been suggested that MAS and AOSD may be anchored to the same disease spectrum, representing more severe and milder form, respectively 8. Continuous high fever, hepatosplenomegaly, severe peripheral blood cytopenia, high serum ferritin levels, and haemophagocytosis by activated macrophages in bone marrow (BM) are typical features of these patients 9. A multi-layer MAS pathogenic model has been suggested,
