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采用超高效液相色谱-串联质谱法对人尿液、粪便和血浆中莫沙必利代谢物进行结构鉴定与解析。

Structure identification and elucidation of mosapride metabolites in human urine, feces and plasma by ultra performance liquid chromatography-tandem mass spectrometry method.

作者信息

Sun Xiaohong, Zhao Longshan, Niu Lili, Qin Feng, Lu Xiumei, Xiong Zhili, Li Famei

机构信息

School of Pharmacy, Shenyang Pharmaceutical University , Shenyang , PR China.

出版信息

Xenobiotica. 2014 Aug;44(8):734-42. doi: 10.3109/00498254.2014.880201. Epub 2014 Jan 13.

DOI:10.3109/00498254.2014.880201
PMID:24417754
Abstract

1.  Mosapride citrate (mosapride) is a potent gastroprokinetic agent. The only previous study on mosapride metabolism in human reported one phase I oxidative metabolite, des-p-fluorobenzyl mosapride, in human plasma and urine using HPLC method. Our aim was to identify mosapride phase I and phase II metabolites in human urine, feces and plasma using UPLC-ESI-MS/MS. 2.  A total of 16 metabolites were detected. To the best of our knowledge, 15 metabolites have not been reported previously in human. 3.  Two new metabolites, morpholine ring-opened mosapride (M15) and mosapride N-oxide (M16), alone with one known major metabolite, des-p-fluorobenzyl mosapride (M3), were identified by comparison with the reference standards prepared by our group. The chemical structures of seven phase I and six phase II metabolites of mosapride were elucidated based on UPLC-MS/MS analyses. 4.  There were two major phase I reactions, dealkylation and morpholine ring cleavage. Phase II reactions included glucuronide, glucose and sulfate conjugation. The comprehensive metabolic pathway of mosapride in human was proposed for the first time. 5.  The metabolites in humans were compared with those in rats reported previously. In addition to M10, the other 15 metabolites in humans were also found in rats. This result suggested that there was little qualitative species difference in the metabolism of mosapride between rats and humans. 6.  In all, 16 mosapride metabolites including 15 new metabolites were reported. These results allow a better understanding of mosapride disposition in human.

摘要
  1. 枸橼酸莫沙必利(莫沙必利)是一种强效促胃肠动力药。此前唯一一项关于莫沙必利在人体代谢的研究使用高效液相色谱法在人体血浆和尿液中报告了一种I相氧化代谢物,即去对氟苄基莫沙必利。我们的目的是使用超高效液相色谱-电喷雾串联质谱法鉴定人体尿液、粪便和血浆中的莫沙必利I相和II相代谢物。2. 共检测到16种代谢物。据我们所知,其中15种代谢物此前未在人体中报道过。3. 通过与我们小组制备的参考标准品比较,鉴定出两种新代谢物,即吗啉环开环的莫沙必利(M15)和莫沙必利N-氧化物(M16),以及一种已知的主要代谢物,去对氟苄基莫沙必利(M3)。基于超高效液相色谱-质谱/质谱分析阐明了莫沙必利的7种I相和6种II相代谢物的化学结构。4. 有两种主要的I相反应,即脱烷基化和吗啉环裂解。II相反应包括葡萄糖醛酸、葡萄糖和硫酸盐结合。首次提出了莫沙必利在人体中的综合代谢途径。5. 将人体中的代谢物与此前报道的大鼠中的代谢物进行了比较。除了M10外,人体中的其他15种代谢物在大鼠中也有发现。该结果表明,大鼠和人体在莫沙必利代谢方面几乎没有定性的种属差异。6. 总共报告了16种莫沙必利代谢物,包括15种新代谢物。这些结果有助于更好地了解莫沙必利在人体中的处置情况。

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