Profiling and identification of (−)-epicatechin metabolites in rats using ultra-high performance liquid chromatography coupled with linear trap-Orbitrap mass spectrometer
| Autor: | Jia-Yu Zhang, Xiaodan Wu, Jian-Qiu Lu, Fei Wang, Zhan-Peng Shang, Shengyun Dai |
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| Rok vydání: | 2017 |
| Předmět: |
0301 basic medicine
Chromatography Chemistry 010401 analytical chemistry Glucuronidation Pharmaceutical Science Methylation Urine Mass spectrometry Orbitrap 01 natural sciences 0104 chemical sciences Analytical Chemistry law.invention 03 medical and health sciences Metabolic pathway 030104 developmental biology In vivo law Toxicity Environmental Chemistry Spectroscopy |
| Zdroj: | Drug Testing and Analysis. 9:1224-1235 |
| ISSN: | 1942-7603 |
| DOI: | 10.1002/dta.2155 |
| Popis: | (-)-Epicatechin (EC), an optical antipode of (+)-catechin (C), possesses many potential significant health benefits. However, the in vivo metabolic pathway of EC has not been clarified yet. In this study, an efficient strategy based on ultra-high performance liquid chromatography coupled with a linear ion trap-Orbitrap mass spectrometer was developed to profile and characterize EC metabolites in rat urine, faeces, plasma, and various tissues. Meanwhile, post-acquisition data-mining methods including high-resolution extracted ion chromatogram (HREIC), multiple mass defect filters (MMDFs), and diagnostic product ions (DPIs) were utilized to screen and identify EC metabolites from HR-ESI-MS1 to ESI-MSn stage. Finally, a total of 67 metabolites (including parent drug) were tentatively identified based on standard substances, chromatographic retention times, accurate mass measurement, and relevant drug biotransformation knowledge. The results demonstrated that EC underwent multiple in vivo metabolic reactions including methylation, dehydration, hydrogenation, glucosylation, sulfonation, glucuronidation, ring-cleavage, and their composite reactions. Among them, methylation, dehydration, glucosylation, and their composite reactions were observed only occurring on EC when compared with C. Meanwhile, the distribution of these detected metabolites in various tissues including heart, liver, spleen, lung, kidney, and brain were respectively studied. The results demonstrated that liver and kidney were the most important organs for EC and its metabolites elimination. In conclusion, the newly discovered EC metabolites significantly expanded the understanding on its pharmacological effects and built the foundation for further toxicity and safety studies. Copyright © 2017 John Wiley & Sons, Ltd. |
| Databáze: | OpenAIRE |
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