Accelerated development of lupus nephritis in CfH-deficient MRL-lpr mice. (A–D) Representative periodic acid-Schiff–stained kidneys from 12-week-old CfH+/+ MRL-lpr mice (A), showing mild mesangial proliferative GN, and from three individual CfH−/− MRL-lpr mice (B–D), which showed endocapillary and extracapillary proliferative GN. Arrow, wire loop (C); asterisk, cellular crescent (D). (E–I) Merged representative immunofluorescence photomicrographs for IgG (red) and C3 (green), and ultrastructural features of disease in 12-week-old CfH+/+ MRL-lpr mice (E and F), 8-week-old CfH−/− MRL-lpr mice (G), and 12-week-old CfH−/− MRL-lpr mice (H and I). (E and F) Twelve-week-old CfH+/+ MRL-lpr mice had mesangial immune deposits composed of IgG and C3 (arrowheads). (G) Eight-week-old CfH−/− MRL-lpr mice had linear staining for C3 along glomerular capillary walls, with mesangial and moderate peripheral capillary IgG staining that was largely independent from C3. (H) By 12 weeks of age, CfH−/− MRL-lpr mice had extensive IgG deposition in the mesangium and peripheral capillary walls, which colocalized with C3 in some regions of the capillary wall (white underline). (I) By electron microscopy, immune deposits were present in the mesangium, subendothelial (arrows) and subepithelial regions (arrowheads) (underlined region, podocyte effacement). Original magnifications, ×600 (A–E, G, and H), ×10,000 (F and I).