The breakdown of pre‐existing advanced glycation end products is associated with reduced renal fibrosis in experimental diabetes

ABSTRACT Renal accumulation of advanced glycation end products (AGEs) has been linked to the progression of diabetic nephropathy. Cleavage of pre‐formed AGEs within the kidney by a crosslink breaker, such as ALT‐711, may confer renoprotection in diabetes. STZ diabetic rats were randomized into a) no treatment (D); b) treatment with the AGE cross‐link breaker, ALT‐711, weeks 16–32 (DALT early); and c) ALT‐711, weeks 24–32 (DALT late). Treatment with ALT‐711 resulted in a significant reduction in diabetes‐induced serum and renal AGE peptide fluorescence, associated with decreases in renal carboxymethyllysine and RAGE immunostaining. Cross‐linking of tail tendon collagen seen in diabetic groups was attenuated only by 16 weeks of ALT‐711 treatment. ALT‐711, independent of treatment duration, retarded albumin excretion rate (AER), reduced blood pressure, and renal hypertrophy. It also reduced diabetes‐induced increases in gene expression of transforming growth factor β1 (TGF‐β1), connective tissue growth factor (CTGF), and collagen IV. However, glomerulosclerotic index, tubulointerstitial area, total renal collagen, nitrotyrosine, protein expression of collagen IV, and TGF‐β1 only showed improvement with early ALT treatment alone. This study demonstrates the utility of a cross‐link breaker as a treatment for diabetic nephropathy and describes effects not only on renal AGEs but on putative mediators of renal injury, such as prosclerotic cytokines and oxidative stress.