ROS signaling is required for uncapping activity. (A) Uncapping of actin filaments was measured by the fMLP-induced release of CapZ from partially permeabilized neutrophils. Cells were pretreated with Trolox or mock-treated for 15 minutes before stimulation with 1μM fMLP for 1 minute. Cells and supernatant were separated by centrifugation and analyzed by SDS-PAGE and immunoblotting for CapZ. (B) CapZ in pellets and supernatant were quantified by immunoblotting and subsequent densitometric analysis. Uncapping activity was quantified in 3 independent experiments by determining the ratio between CapZ in supernatant and pellet. The bar diagram depicts the averages ± SEM (n = 3). (C) CapZ-uncapping experiments were performed as described above using neutrophils from Gp91−/− and C57/BL6 control mice. Cells were stimulated with fMLP (1μM) and H2O2 (50μM) and pretreated with Trolox (100μM) where indicated. Bar diagrams depict averages ± SD (n = 3). Asterisks indicate significance, P < .05. (D) Model describing the redox-mediated amplification loop. Activation of Rac induces ROS formation by NOX2, which oxidizes PTEN. The decrease in PTEN activity results in increased PtdIns(3,4,5)P3 levels, facilitating guanine nucleotide exchange factor activity toward Rac. Subsequent Rac activity induces uncapping of actin filaments and local actin polymerization required for directional migration.