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首页> 外文期刊>Chemical research in toxicology >HPLC/1H NMR spectroscopic studies of the reactive alpha-1-O-acyl isomer formed during acyl migration of S-naproxen beta-1-O-acyl glucuronide.
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HPLC/1H NMR spectroscopic studies of the reactive alpha-1-O-acyl isomer formed during acyl migration of S-naproxen beta-1-O-acyl glucuronide.

机译:HPLC / 1H NMR光谱研究在S-萘普生β-1-O-酰基葡糖醛酸苷的酰基迁移过程中形成的反应性α-1-O-酰基异构体。

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A widely held view in drug metabolism and pharmacokinetic studies is that the initial 1-isomer to 2-isomer step in the intramolecular acyl migration of drug ester glucuronides is irreversible, and that alpha-1-O-acyl isomers do not occur under physiological conditions. We investigated this hypothesis using high-performance liquid chromatography directly coupled to proton nuclear magnetic resonance spectroscopy (HPLC/1H NMR) and mass spectrometry (LC/MS) to probe the migration reactions of S-naproxen beta-1-O-acyl glucuronide, in phosphate buffer at pH 7.4, 37 degrees C. We report the first direct observation of the alpha-1-O-acyl isomer of a drug ester glucuronide (S-naproxen) formed in a biosystem via the facile acyl migration of the corresponding pure beta-1-O-acyl glucuronide. The unequivocal identification of the reactive product was achieved using stopped-flow one-dimensional HPLC/1H NMR and two-dimensional 1H-1H total correlation spectroscopy (1H-1H TOCSY). Parallel LC/ion-trap mass spectrometry yielded the confirmatory glucuronide masses. Moreover, "dynamic" stopped-flow HPLC/1H NMR experiments revealed transacylation of the isolated alpha-1-O-acyl isomer to a mixture of alpha/beta-2-O-acyl isomers; the reverse reaction from the isolated alpha/beta-2-O-acyl isomers to the alpha-1-O-acyl isomer was also clearly demonstrated. This application of "dynamic" stopped-flow HPLC/1H NMR allows key kinetic data to be obtained on a reactive metabolite that would otherwise be difficult to follow by conventional HPLC and NMR methods where sample preparation and off-line separations are necessary. These data challenge the widely held view that the alpha-1-O-acyl isomers of drug ester glucuronides do not occur under physiological conditions. Furthermore, the similar formation of alpha-1-O-acyl isomers from zomepirac and diflunisal beta-1-O-acyl glucuronides has recently been confirmed (Corcoran et al., unpublished results). Such reactions are also likely to be widespread for other drugs that form ester glucuronides in biological systems. Ultimately, the presence of significant quantities of the kinetically labile alpha-1-O-acyl glucuronide isomer may also have toxicological implications in terms of reactivity toward cellular proteins.
机译:在药物代谢和药代动力学研究中广泛持有的观点是,药物酯葡糖醛酸苷的分子内酰基迁移中最初的1-异构体到2-异构体步骤是不可逆的,并且在生理条件下不会发生α-1-O-酰基异构体。我们使用高效液相色谱法直接与质子核磁共振波谱(HPLC / 1H NMR)和质谱(LC / MS)耦合,以研究S-萘普生β-1-O-酰基葡萄糖醛酸的迁移反应,在pH 7.4的磷酸盐缓冲液中,温度为37摄氏度。我们报告了在生物系统中通过相应纯净物质的轻松酰基迁移而直接观察到的在生物系统中形成的药物酯葡糖苷酸(S-萘普生)的α-1-O-酰基异构体的方法。 β-1-O-酰基葡糖醛酸。使用停止流一维HPLC / 1H NMR和二维1H-1H总相关光谱法(1H-1H TOCSY)可以明确鉴定反应产物。平行LC /离子阱质谱法得到了证实的葡糖醛酸苷质量。此外,“动态”停止流HPLC / 1H NMR实验表明,分离出的α-1-O-酰基异构体转酰基化为α/β-2-O-酰基异构体的混合物。还清楚地证明了从分离的α/β-2-O-酰基异构体到α-1-O-酰基异构体的逆反应。 “动态”停止流HPLC / 1H NMR的这种应用使您可以在反应性代谢物上获得关键的动力学数据,否则常规的HPLC和NMR方法将难以遵循这些动力学数据,而常规的HPLC和NMR方法则需要样品制备和离线分离。这些数据挑战了普遍持有的观点,即在生理条件下不会发生药物酯葡糖醛酸苷的α-1-O-酰基异构体。此外,近来证实了来自zomipirac和二氟乙醛β-1-O-酰基葡萄糖醛酸苷类似形式的α-1-O-酰基异构体的形成(Corcoran等人,未公开的结果)。对于在生物系统中形成酯葡糖醛酸苷的其他药物,此类反应也很可能会广泛传播。最终,在动力学上不稳定的α-1-O-酰基葡萄糖醛酸苷异构体的存在,就对细胞蛋白的反应性而言,也可能具有毒理学意义。

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