FcγRIII targeting by IVIg and 2.4G2 F(ab′)₂ reduces nonimmune inflammatory response in FcγRIIB^−/− mice, but not in FcγRIII^−/− mice. (A) FcγRIIB^−/− or FcγRIII^−/− Balb/c mice were injected intraperitonealy with 2.4G2 F(ab′)₂ (100 μg/20 g; top panel) or IVIg (40 mg/20 g; bottom panels), or their controls rat IgG F(ab′)₂ or BSA, respectively, as indicated. After 24 hours, mice were subjected to surgery for unilateral ureteral obstruction on their left side and 2.4G2 or IVIg or control treatments were continued at 48-hour intervals until day 8 when animals were killed and kidney sections were analyzed. Photographs show immunohistologic staining of CD11b-positive cells in obstructed left kidneys. Corresponding quantitative analysis of infiltrating cells of several animals (n = 6) is shown on the right. (*P < .05,**P < .01; nonparametric Mann-Whitney test). (B) Expression of MCP-1 and TNFα mRNA were analyzed by quantitative real-time PCR in obstructed kidney from mice treated with either IVIg or 2.4G2 F(ab′)₂ (white bar) or with their control treatment BSA or rat IgG F(ab′)₂ (black bar). Data represent relative mRNA expression levels of obstructed versus controlateral kidneys after normalization to GADPH (*P < .05; nonparametric Mann-Whitney test).