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A novel strategy for the characterization of glaucocalyxin A metabolites in vivo and in vitro by UHPLC-Q-TOF-MS based on DDA and DIA data acquisitions

机译:基于DDA和DIA数据采集,通过UHPLC-Q-TOF-MS在体内和体外表征Glaucocalyxin的新策略

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摘要

Glaucocalyxin A (GLA) belongs to the natural ent-kauranoid diterpenoids family with antitumor, antifibrotic, anticoagulative, antioxidant, and anti-AD effects. In this study, ultra-high-performance liquid chromatography coupled to quadrupole time-of-flight mass spectrometry (UHPLC-Q-TOF-MS) system was applied to observe probable metabolites of GLA in vitro and in vivo firstly. The mass data were respectively obtained by two typical acquisition methods, 'data-dependent acquisition' (DDA) and 'data-independent acquisition' (DIA) modes. The combinations can not only guarantee sensitivity but also capture more precursor ions and MS/MS spectra. Then, multiple data processing techniques were applied to hunt metabolites rapidly. As a result, 32 phase I metabolites of different structures and 6 phase II metabolites were identified, including 25, 18, 17 and 7 in rat urine, feces, bile, and plasma, respectively. Besides, under the action of rat intestinal flora (RIF), 7 metabolites were detected. In the study, the main bio-transformations were oxidation and demethylation. Conjugation with methylation, sulfate, and glucuronide produced phase II metabolites. This study laid the foundation for the further study of the pharmacological effects of GLA and was conducive to mechanism research.
机译:Glaucocalyxin A(GLA)属于天然Ent-kauranoid DiTitepenoids系列,具有抗肿瘤,抗纤维抗抗菌,抗氧化,抗氧化剂和抗AD效果。在该研究中,偶联与四极杆飞行时间质谱(UHPLC-Q-TOF-MS)系统偶联的超高效液相色谱法首先在体外和体内观察GLA的可能代谢物。群众数据分别通过两个典型的采集方法,“数据相关的采集”(DDA)和“数据无关的采集”(DIA)模式获得。这些组合不仅可以保证敏感性,还可以捕获更多的前体离子和MS / MS光谱。然后,将多种数据处理技术应用于迅速捕获代谢物。结果,鉴定了不同结构和6阶段II代谢物的32级I代谢物,包括在大鼠尿,粪便,胆汁和血浆中25,18,17和7。此外,在大鼠肠菌群(RIF)的作用下,检测到7种代谢物。在研究中,主要的生物转化是氧化和去甲基化。与甲基化,硫酸盐和葡糖醛酸二族代谢物缀合。本研究为进一步研究GLA的药理作用以及有利于机制研究的基础。

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  • 来源
    《RSC Advances》 |2020年第18期|共16页
  • 作者单位

    Hebei Med Univ Sch Pharm Dept Pharmaceut Anal 361 East Zhongshan Rd Shijiazhuang 050017 Hebei Peoples R China;

    Hebei Med Univ Hosp 2 Shijiazhuang 050000 Hebei Peoples R China;

    Hebei Med Univ Hosp 2 Shijiazhuang 050000 Hebei Peoples R China;

    Hebei Med Univ Sch Pharm Dept Pharmaceut Anal 361 East Zhongshan Rd Shijiazhuang 050017 Hebei Peoples R China;

    Hebei Med Univ Sch Pharm Dept Pharmaceut Anal 361 East Zhongshan Rd Shijiazhuang 050017 Hebei Peoples R China;

    Hebei Med Univ Sch Pharm Dept Pharmaceut Anal 361 East Zhongshan Rd Shijiazhuang 050017 Hebei Peoples R China;

    Hebei Med Univ Sch Pharm Dept Pharmaceut Anal 361 East Zhongshan Rd Shijiazhuang 050017 Hebei Peoples R China;

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  • 正文语种 eng
  • 中图分类 化学;
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