In vivo phospholipase activity of the Pseudomonas aeruginosa cytotoxin ExoU and protection of mammalian cells with phospholipase A2 inhibitors

A number of clinical isolates of Pseudomonas aeruginosa are cytotoxic to mammalian cells due to the action of the 74-kDa protein ExoU, which is secreted into host cells by the type III secretion system and whose function is unknown. Here we report that the swift and profound cytotoxicity induced by purified ExoU or by an ExoU-expressing strain of P. aeruginosa is blocked by various inhibitors of cytosolic (cPLA(2)) and Ca2+-independent (iPLA(2)) phospholipase A(2) enzymes. In contrast, no cytoprotection is offered by inhibitors of secreted phospholipase A(2) enzymes or by a number of inhibitors of signal transduction pathways. This suggests that phospholipase A(2) inhibitors may represent a novel mode of treatment for acute P. aeruginosa infections. We find that 300 - 600 molecules of ExoU/cell are required to achieve half-maximal cell killing and that ExoU localizes to the host cell plasma membrane in punctate fashion. We also show that ExoU interacts in vitro with an inhibitor of cPLA(2) and iPLA(2) enzymes and contains a putative serine-aspartate catalytic dyad homologous to those found in cPLA(2) and iPLA(2) enzymes. Mutation of either the serine or the aspartate renders ExoU non-cytotoxic. Although no phospholipase or esterase activity is detected in vitro, significant phospholipase activity is detected in vivo, suggesting that ExoU requires one or more host cell factors for activation as a membrane-lytic and cytotoxic phospholipase.