Properdin is the only known positive regulator of the alternative pathway of complement activation. Northern blot analysis of cell lines derived from fibroblasts, B-cells, hepatoma cells, and cells of the monocyte-macrophage lineage revealed properdin expression only in the myelomonocytic cell line HL-60, in the monoblastic cell line U-937 and in the monocytic line Mono Mac 6. Culture of Mono Mac 6 cells for 24 h with phorbol 12-myristate 13-acetate, bacterial lipopolysaccharide and the cytokines interleukin-lb and tumour necrosis factor-a enhanced mRNA abundance, with the strongest effect (tenfold) being observed with the lipopolysaccharide. In contrast, recombinant interferon-y consistently halved properdin mRNA abundance. The same pattern was found for the secretion of properdin as detected by ELISA of Mono Mac 6 supernatants. The suppressive effect of interferon-y on properdin mRNA abundance was also demonstrated for primary blood monocytes. The data suggest that the expression and secretion of this complement regulatory protein by monocytes is differentially regulated by cytokines and link the immune response with alternative pathway activation.Properdin is one of the six plasma glycoproteins which constitute the alternative pathway of complement activation [I, 21. Three of these proteins (C3 and factors B and D) form the activation system, whereas the other three (properdin and factors H and I) are regulatory components. Properdin is essential for optimal rates of complement activation by virtue of its ability to bind and stabilize the inherently labile C3 and C5 convertase complexes (C3bBb and C3b,Bb) of the alternative pathway. Stabilization of these complexes by properdin accelerates activation, promotes C3b attachment, and enhances C5 cleavage leading to increased cytolysis and phagocytosis. The importance of this positive regulatory complement component is illustrated by the symptoms experienced by properdin-deficient individuals [3, 41. Approximately 50% of the patients suffer from severe, fulminant, pyrogenic bacterial infections, usually meningococcal with a fatality rate approaching 75%. The deficiency is transmitted as an X-linked, recessive trait consistent with studles mapping the gene to Xp11.23-Xp11.3 [5, 61. In plasma, properdin is present (5-15 pg/rnl) as a polydisperse mixture of cyclic polymers, mainly dimers, trimers, and tetramers, in the ratio 20 : 54:26, formed by the (presumably head-to-tail) interac- Abbreviations. FCS, foetal-calf serum heat-inactivated for 2 h at 56°C; IFN-y, recombinant interferon-y ; IL-1, interleukin-lp; LPS, bacterial lipopolysaccharide; Me,SO, dimethylsulfoxide; NaCW,, 137 mM NaC1,2.6 mM KCl, 4 mM Na2HP04, and 1.8 mM KH,PO, adjusted to pH 7.4; PMA, phorbol 12-myristate 13-acetate; TNF-a, tumour necrosis factor-a.Leicester Royal Infirmary, Leicester LE 1 5WW, England tions of a single, asymmetric monomer of approximately 46kDa [7, 81. cDNA cloning and sequencing provided the complete primary structure of human properdin [9] which is very similar (76% identity)...
