(a) Schematic diagram depicts the animal study design. Wild-type (WT)
and MC1R-null (e/e) mice received an intraperitoneal injection of 250μl
rabbit IgG emulsified in complete Freund’s adjuvant (CFA) 6 days before a
tail vein injection of either rabbit NTS or nonimmune IgG, followed by treatment
with repository corticotropin injection (RCI), vehicle gel (Veh gel), the
pan-melanocortin receptor agonist [Nle, DPhe]-α-MSH (NDP-MSH), MC1R
agonist MS05 (custom-made peptide, GL Biochem), or vehicle (Veh) till day 14.
(b) Proteinuria was estimated using the urinary albumin-to-creatinine ratios
(uACR). (c) Kidney function was assessed by measuring blood urea nitrogen (BUN)
levels in sera. (d) Representative micrographs of periodic acid-Schiff staining
of mouse kidneys are shown. Arrowheads indicate glomeruli with crescents (Scale
bar = 50 μm). (e~g) Semi-quantitative morphometric analysis of (e)
glomerulonephritis (GN) score, (f) tubulointerstitial nephritis (TIN) score, and
(g) the percentage of glomeruli with crescents based on periodic acid-Schiff
staining of mouse kidneys. *P<0.05 by analysis of
variance. aP<0.05 versus e/e group treated
with NTS and Veh gel or WT group with NTS and RCI treatment;
bP<0.05 versus e/e mice treated with NTS
and RCI; cP<0.05 versus e/e mice treated with
NTS and Veh or WT mice treated with NTS and NDP-MSH or MS05;
dP<0.05 versus e/e mice treated with NTS
and NDP-MSH; (n=6). q.o.d., every other day; s.c., subcutaneous. To optimize
viewing of this image, please see the online version of this article at
www.kidney-international.org.