Abstract
Diabetic patients (n = 23) with chronic renal failure (CRF) accumulate the creatinine (Cr) oxidative metabolites creatol (CTL) and methylguanidine (MG; a uremic toxin) in their sera. Analysis of serum CTL, a key intermediate in mammalian Cr catabolism into MG, is shown to offer some useful diagnostic information on CRF, especially in the determination of an initial stage of pathological renal failure. The sera of all diabetic (n = 23) and nondiabetic (n = 20) patients with CRF (s-Cr > 1.25 mg/dl) contained s-CTL ( > 2 μg/dl), whereas those from normal subjects (n = 18) and diabetic patients (n = 18) without CRF contained no detectable s-CTL. A similar accumulation of s-MG was observed, but only when s-Cr was higher than 2.0 mg/dl. Although each s-CTL (Y: μg/dl, Y’: mol/l) and s-MG level (Z: μg/dl, Z’: mol/l) is highly correlated with s-Cr (X: mg/dl, X’: mol/l) in a normal equation, Y or Z = AX + B, an alternative correlation in a second-order equation, Y or Z = αX2 + βX, could also fit well. Since the quadratic equation can be convertible to Y/X or Z/X = αX + β [Y’/X’ or Z’/X’ = α’X + β’] and active oxygen species, especially hydroxyl radicals, convert Cr into CTL, Y’X, Y’/X’, Z/X and Z’/X’ values which might be a kind of indices for oxygen stress (oxidative stress) increased in proportion to the increased severity of CRF in such patients. Although its meaning and interpretation are still debatable, diabetic CRF patients had a significantly higher α’ value (2.2) than that (0.89) of nondiabetic CRF patients. All serum values for Cr, CTL and MG were measured with HPLC.
