Targeted isolation and identification of bioactive pyrrolidine alkaloids from Codonopsis pilosula using characteristic fragmentation-assisted mass spectral networking

吡咯烷 化学 吡咯里嗪 串联质谱法 银杏内酯 碎片(计算) 吡咯里嗪生物碱 生物碱 质谱法 苄基异喹啉 色谱法 立体化学 传统医学 有机化学 生物 医学 银杏 生态学 生物合成
作者
Xiyang Tang,Cailian Fan,Jiaxing Zeng,Peng-cheng Zhao,Xiaoxing Wang,Wanjun Cai,Ting Li,Yi Dai,Zhihong Yao,Xin‐Sheng Yao
出处
期刊:Chinese Journal of Natural Medicines [Elsevier BV]
卷期号:20 (12): 948-960 被引量:6
标识
DOI:10.1016/s1875-5364(22)60216-4
摘要

Codonopsis pilosula (CP), a well-known food medicine homology plant, is commonly used in many countries. In our preliminary study, a series of pyrrolidine alkaloids with high MS responses were detected as characteristic absorbed constituents in rat plasma after oral administration of CP extract. However, their structures were unclear due to the presence of various isomers and the lack of reference standards. In the present study, an MS-guided targeted isolation of pyrrolidine alkaloids of CP extract was performed by ultra-performance liquid chromatography coupled with quadrupole time-of-flight tandem mass spectrometry (UPLC/Q-TOF MS). For data analysis under fast data directed acquisition mode (Fast-DDA), an effective approach named characteristic fragmentation-assisted mass spectral networking was successfully applied to discover new pyrrolidine alkaloids with high MS response in CP extract. As a result, seven new pyrrolizidine alkaloids [codonopyrrolidiums C-I (3-9)], together with two known ones (1 and 2), were isolated and identified by NMR spectral analysis. Among them, codonopyrrolidium B (1), codonopyrrolidium D (4) and codonopyrrolidium E (5) were evaluated for lipid-lowering activity, and they could improve high fructose-induced lipid accumulation in HepG2 cells. In addition, the characteristic MS/MS fragmentation patterns of these pyrrolizidine alkaloids were investigated, and 17 pyrrolidine alkaloids were identified. This approach could accelerate novel natural products discovery and characterize a class of natural products with MS/MS fragmentation patterns from similar chemical scaffolds. The research also provides a chemical basis for revealingin vivo effective substances in CP.
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