Despite the risk of kidney damage, lithotripsy is the usual way of treating
calcium oxalate (CaOx) stones, the most common type of nephrolithiasis, because
no effective chemolytic agents are available. However, the search of new calcium
chelators, less toxic than the current ones, continues, and some of them could be
tested in experimental models of nephrolithiasis, after their ability of
dissolving CaOx crystals is verified. In this connection, we developed a simple
assay that requires only inexpensive equipment available in most laboratories for
the screening of substances potentially capable of dissolving CaOx crystals. In
particular, we decided to investigate whether substances previously shown to
inhibit CaOx precipitation were also capable of dissolving this salt. Briefly,
CaOx tablets of highly reproducible weight (4.55 +/- 0.07 mg) were prepared by
spinning, at high speed (16,000 g), microcentrifuge tubes in which 500 microl
aliquots of 0.1 M sodium oxalate and 0.1 M calcium chloride at pH 6 were added.
When these tablets were incubated overnight with solutions at different
concentrations of EDTA, sodium citrate, manganese chloride, sodium sulfate,
sodium chloride, malic acid, succinic acid and gluconic acid, a significant
dissolving activity was observed for EDTA ( approximately 25% at 0.25 M), sodium
citrate ( approximately 30% at 1 M) and manganese chloride ( approximately 20% at
0.5 M). A good linear correlation (r2 = 0.84, p < 0.05) was found between the
affinity for calcium and the activity of EDTA, sodium citrate, sodium sulfate,
malic acid, succinic acid and gluconic acid, indicating that these compounds act
mainly by chelating the calcium ion. Instead, manganese was supposed to act by
interacting with the oxalate ion
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