Stephen J Vanderhoeven, John C Lindon, Jeff Troke, Jeremy K Nicholson, Ian D Wilson
Index: J. Pharm. Biomed. Anal. 41(3) , 1002-6, (2006)
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The products arising from the intra-molecular acyl migration reactions of drug ester glucuronides can be reactive towards cellular proteins and have been proposed to cause toxic side effects. The relative reactivity of a range of drug and model glucuronides have previously been determined by measuring the rate of disappearance of a peak characteristic of the 1-beta-O-acyl glucuronide using 1H NMR spectroscopy. Here the degradation rate of ibuprofen 1-beta-O-acyl glucuronide has been investigated using NMR spectroscopy for the first time using material isolated from human urine with solid-phase extraction chromatography (SPEC). The degradation rate was measured by following the disappearance of the 1H NMR signal from the 1-beta-anomeric proton of the glucuronic acid moiety as the reaction progressed in pH 7.4 buffer inside an NMR tube. The measured degradation rate represents a pseudo-first order rate constant, a combination of the transacylation rate (1-beta-isomer to 2-beta-isomer) and the hydrolysis rate, and is presented as a half-life of 3.5 h. This value is compared to those from drug glucuronides where adverse effects have been observed in patients after administration of the drug.
Structure | Name/CAS No. | Molecular Formula | Articles |
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Ibuprofen Acyl-b-D-glucuronide
CAS:115075-59-7 |
C19H26O8 |
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