The chemokine receptor antagonist AOP-RANTES reduces monocyte infiltrationin experimental glomerulonephritis

Background. This study was designed to evaluate the role of the novel chemo kine receptor antagonist amino-oxypentane RANTES (AOP-RANTES), which blocks the binding of macrophage inflammatory protein-ice (MIP-1 alpha), MIP-1 be ta, and RANTES to the chemokine receptor-5 (CCR-5) on the infiltration of m onocytes in experimental glomerulonephritis. Methods. Rats were treated twice daily with 12.5 mu g AOP-RANTES following an induction of anti-rat-thymocyte antibody-mediated glomerulonephritis. Th e white blood cell count, glomerular monocyte infiltration, chemokine expre ssion, and collagen type IV deposition were assessed. Results. The induction of glomerulonephritis increased glomerular monocyte/ macrophage (M/M) infiltration at 24 hours and at 5 days was still higher th an in controls. AOP-RANTES prevented glomerular MIM infiltration at 24 hour s and at 5 days. This was paralleled by reduced glomerular collagen type IV deposition as a fibrotic marker in nephritic animals. Conclusion. These data show that the CCR-5 chemokine receptor antagonist AO P-RANTES ameliorates MIM infiltration and improves glomerular pathology in experimental glomerulonephritis. The use of chemokine receptor antagonists may offer a new therapeutic option in inflammatory renal injuries.