Second Messenger Function of Arachidonic Acid Lipoxygenation Products in Human Natural Killer Cell Lysis?

Human natural killer (NK) cells were tested in the presence of several fatty acid oxygenase inhibitors such as nordihydroguaiaretic acid (NDGA), 5,8,11,14‐eicosatetraynoic acid, 3‐amino‐l‐ m ‐(trinuoromethyl)‐phenyl‐2‐pyrazoline (BW 755C). and indomcthacin. All drugs inhibited NK lysis at the post‐target cell‐binding level at concentrations that also suppressed lipoxygenation of arachidonic acid, suggesting that such reactivity may be required for effector cell triggering. NDGA gave a 50% NK cell inhibition in the range of 10‐30 μM and also suppressed antibody‐dependent and lectin‐dependenl systems. Further evidence of the involvement of arachidonic acid lipoxygenation was found as NK activity could be reconstituled to NDGA‐suppressed effector cells with several metabolites such as LTB 4 . LTB 4 analogues, and hydroxyeicosatetraenoic acids lipoxygenated at C‐5, C‐12, and C‐15. Cyclic nucleotides such as cGMP and cAMP could also reconstitute activity with optimal effects at approximately 10 −8 M. The combined evidence is compatible with a model for triggering lysis in which lipoxygenation products have a second messenger function. Whether arachidonic acid lipoxygenation is necessary for effector cells at all different activation/differentiation stages and whether the lipoxygenation products activate guanylic cyclase, protein kinase C, or some other target molecule remain to he further investigated.