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Xanthine urolithiasis: Inhibitors of xanthine crystallization

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Abstract OBJECTIVE To identify in vitro inhibitors of xanthine crystallization that have potential for inhibiting the formation of xanthine crystals in urine and preventing the development of the renal calculi in patients with xanthinuria. METHODS The formation of xanthine crystals in synthetic urine and the effects of 10 potential crystallization inhibitors were assessed using a kinetic turbidimetric system with a photometer. The maximum concentration tested for each compound was: 20 mg/L for 3-methylxanthine (3-MX); 40 mg/L for 7-methylxanthine (7-MX), 1- methylxanthine (1-MX), theobromine (TB), theophylline, paraxanthine, and caffeine; 45 mg/L for 1-methyluric acid; 80 mg/L for 1,3-dimethyluric acid; and 200 mg/L for hypoxanthine. All crystals were examined by scanning electron microscopy. RESULTS Only 7-MX, 3-MX, and 1-MX significantly inhibited xanthine crystallization at the tested concentrations. Mixtures of inhibitors had an additive effect rather than a synergistic effect on crystallization. CONCLUSION Two of the inhibitors identified here —7-MX and 3-MX — are major metabolites of TB. In particular, after TB consumption, 20% is excreted in the urine as TB, 21.5% as 3-MX, and 36 % as 7-MX. Thus, consumption of theobromine could protect patients with xanthinuria from the development of renal xanthine calculi. Clinical trials are necessary to demonstrate these effects in vivo .
Title: Xanthine urolithiasis: Inhibitors of xanthine crystallization
Description:
Abstract OBJECTIVE To identify in vitro inhibitors of xanthine crystallization that have potential for inhibiting the formation of xanthine crystals in urine and preventing the development of the renal calculi in patients with xanthinuria.
METHODS The formation of xanthine crystals in synthetic urine and the effects of 10 potential crystallization inhibitors were assessed using a kinetic turbidimetric system with a photometer.
The maximum concentration tested for each compound was: 20 mg/L for 3-methylxanthine (3-MX); 40 mg/L for 7-methylxanthine (7-MX), 1- methylxanthine (1-MX), theobromine (TB), theophylline, paraxanthine, and caffeine; 45 mg/L for 1-methyluric acid; 80 mg/L for 1,3-dimethyluric acid; and 200 mg/L for hypoxanthine.
All crystals were examined by scanning electron microscopy.
RESULTS Only 7-MX, 3-MX, and 1-MX significantly inhibited xanthine crystallization at the tested concentrations.
Mixtures of inhibitors had an additive effect rather than a synergistic effect on crystallization.
CONCLUSION Two of the inhibitors identified here —7-MX and 3-MX — are major metabolites of TB.
In particular, after TB consumption, 20% is excreted in the urine as TB, 21.
5% as 3-MX, and 36 % as 7-MX.
Thus, consumption of theobromine could protect patients with xanthinuria from the development of renal xanthine calculi.
Clinical trials are necessary to demonstrate these effects in vivo .

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