[No authors listed]
Cr-EDTA-clearance), 24-hour ambulatory BP, 24-hour urinary albumin/creatinine ratio (UAC) and urinary L-FABP/creatinine ratio (U-L-FABP/C) were determined at baseline and after 18 months of follow-up. For comparison 25 age-matched healthy controls were included. The U-L-FABP/C was elevated in CKD patients when compared to controls (mean U-L-FABP/C 2.3 [95% CI 1.7-2.9] μg/mmol vs 0.6 [0.5-0.7] μg/mmol, pâ<â.001). In CKD patients, log U-L-FABP/C at baseline and at follow-up were positively associated (Pearson correlation coefficient râ=â0.74, pâ<â.001). Baseline log U-L-FABP/C was negatively correlated with baseline GFR (râ=â-0.32, pâ<â.001) and directly correlated with UAC (râ=â0.67, pâ<â.001). The relative change in GFR from baseline to follow-up correlated with baseline UAC (pâ<â.001), 24-hour systolic BP (pâ=â0.05) and log U-L-FABP/C (pâ<â.001). Using multiple regression analysis adjusting for baseline GFR, UAC, BP, age and gender, baseline log U-L-FABP/C was associated with a decline in GFR only in patients with UAC <3âmg/mmol (nâ=â29, pâ=â0.001) and not in patients with UAC â¥3âmg/mmol (nâ=â44, pâ=â0.21). In conclusion urine L-FABP/C is permanently elevated in CKD patients, but only associated with GFR decline in those without albuminuria.
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