Hessle C, Hanson LA Ê , Wold AE. Interleukin-10 Produced by the Innate Immune System Masks In Vitro Ecidence of Acquired T-Cell Immunity. Scand J Immunol 2000;52:13±20 Bacteria trigger stimulation of antigen-speci®c, as well as innate, immune responses. Cytokines and other products of cells belonging to the innate immune system may interfere with the detection of acquired immunity to whole bacteria in vitro. Proliferation and cytokine production by human blood mononuclear cells in response to a whole UV-killed Escherichia coli was compared with the response to commonly used antigen preparations: puri®ed protein derivative (PPD), Candida albicans and in¯uenza proteins. E. coli induced a weaker proliferative response with later onset than did the other antigens, and production of interferon (IFN)-g comparable with that in response to C. albicans and in¯uenza vaccine, but lower than that induced by PPD. Both proliferation and IFN-g production were abolished by removal of CD4 cells or blocking of HLA-D, but not CD1 antigen-presenting molecules. Puri®ed lipopolysaccharide (LPS) induced neither proliferation nor IFN-g production. None of the antigen preparations stimulated interleukin (IL)-4 production but, in contrast to the other antigens, whole E. coli, as well as puri®ed O6 LPS, induced large quantities of IL-10. IL-10 production was independent of CD4 cells or HLA-D molecules. Blocking of IL-10 by neutralizing antibodies increased both E. coli-induced proliferation and IFN-g production markedly. Conversely, the addition of whole E. coli or LPS to cultures stimulated with other antigens (C. albicans or Staphylococcus aureus) downregulated proliferative and IFN-g responses, an effect which was at least partly IL-10 dependent. The results indicate a substantial T-cell memory to commensal E. coli, but suggest that the evidence of such memory, e.g. proliferation and IFN-g production, is effectively prevented by IL-10 and perhaps other factors produced by monocytes in response to bacteria. Thus, the innate immune responses must be taken into account when acquired immune responses to microbes are measured.
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