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NMR spectroscopic studies of the transacylation reactivity of ibuprofen 1-beta-O-acyl glucuronide.

机译:核磁共振波谱研究布洛芬1-β-O-酰基葡萄糖醛酸苷的转酰基反应性。

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摘要

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.
机译:药物酯葡糖醛酸苷的分子内酰基迁移反应产生的产物可对细胞蛋白发生反应,并已提出引起毒性副作用的提议。先前已经通过使用1 H NMR光谱测量1-β-O-酰基葡萄糖醛酸苷特征峰消失的速率来确定一系列药物和模型葡萄糖醛酸苷的相对反应性。在这里,使用固相萃取色谱法(SPEC)从人尿液中分离出的物质首次使用核磁共振波谱法研究了布洛芬1-β-O-酰基葡萄糖醛酸苷的降解率。通过在NMR管内的pH 7.4缓冲液中随着反应的进行,通过追踪葡萄糖醛酸部分的1-β-异头质子的1 H NMR信号的消失来测量降解速率。测得的降解速率代表拟一级反应速率常数,是转酰化速率(1-β-异构体到2-β-异构体)和水解速率的组合,半衰期为3.5小时。将该值与来自药物葡糖醛酸苷的那些值进行比较,在药物施用后已在患者中观察到了不良反应。

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