Gold compounds alter distribution of protein kinase C activity in human neutrophils.

Slow translocation of protein kinase C was observed by both auranofin and gold sodium thiomalate pretreatment of neutrophils. Both gold compounds failed to influence the activity of this enzyme directly when cell-free studies were performed. In intact neutrophils incubated with 5.1-20.3 microM auranofin, protein kinase C activity decreased in the cytosol in a time- and dose-dependent manner. Concomitantly, the levels of the membrane-associated protein kinase C were significantly elevated, although the amount of activity recovered could not account for that lost from the cytosol. Gold sodium thiomalate (5.0 microM-0.505 mM) demonstrated similar effects but with lesser potency than auranofin. In confirmation of previous results, phorbol myristate acetate (PMA), a cellular stimulus, also induced the translocation of protein kinase C. Key differences were that the reaction was rapid (occurring within minutes after PMA addition) and that relative recovery of kinase activity from the particulate fraction was fourfold greater. The relationship between gold compound-mediated kinase C redistribution and inhibition of neutrophil responses remains to be elucidated.