Functional differences and complementation between dendritic cells and macrophages in T-cell activation.

Functional differences and cell collaboration between murine lymphoid dendritic cells (DC) and macrophages (MØ) in antigen presentation for T-cell activation were analysed with splenic DC and MØ, culture-derived bone-marrow (BM)-MØ, and DC-like and MØ-like cell lines. DC were the best stimulators of allogeneic mixed leucocyte reaction (MLR), but splenic MØ and small activated BM-MØ were almost as effective. In contrast to MLR stimulation, small activated BM-MØ were the most effective antigen-presenting cells (APC) for the presentation of whole Corynebacterium parvum (CP) organisms, possibly by virtue of their phagocytic and lysosomal functions, which could be particularly important for processing particulate antigens. Large activated BM-MØ were ineffective in stimulating MLR and CP-specific T-cell proliferation. The functional differences between BM-MØ subsets could not be explained by failure to express surface la or to take up antigen. Non-phagocytic APC, such as DC and the DC-like line P388AD.4, had low presenting activity for CP and were much less effective at presenting glutaraldehyde-fixed CP than MØ. This suggests that DC are dependent on the shedding of soluble antigen (reduced by glutaraldehyde fixation) from the bacteria, and they may also be less efficient than MØ at processing the fixed bacteria. The la- MØ-like line, P388D1, was devoid of APC activity, but could greatly enhance P388AD.4-induced T-cell proliferation to whole bacterial organisms. Similarly, co-culture of splenic DC and MØ produced very pronounced synergistic effects in proliferative responses to CP and keyhole limpet haemocyanin. The function of MØ in this partnership was sensitive to chloroquine and could not be replaced by MØ culture fluids or recombinant interleukin-1. Thus, MØ may contribute processed antigen in a form more suitable for presentation by DC. These results provide a rationale for the functional dichotomy between DC and MØ. [ABSTRACT FROM AUTHOR]