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环缩酚酸肽的起源与表征:以碱金属阳离子化分子物种的质谱分析为重点的综合结构方法

Origin and characterization of cyclodepsipeptides: Comprehensive structural approaches with focus on mass spectrometry analysis of alkali-cationized molecular species.

作者信息

Liuu Sophie, Damont Annelaure, Perret Alain, Firmesse Olivier, Becher François, Lavison-Bompard Gwenaëlle, Hueber Amandine, Woods Amina S, Darii Ekaterina, Fenaille François, Tabet Jean-Claude

机构信息

Staphylococcus, Bacillus & Clostridium (SBCL) unit, Laboratory for Food Safety, French Agency for Food, Environmental and Occupational Health & Safety (ANSES), Université Paris-Est, Maisons-Alfort, France.

Université Paris-Saclay, CEA-INRAE, Laboratoire Innovations en Spectrométrie de Masse pour la Santé (LI-MS), DRF/Institut Joliot/DMTS/SPI, MetaboHUB, CEA Saclay, Gif sur Yvette, France.

出版信息

Mass Spectrom Rev. 2024 Aug 21. doi: 10.1002/mas.21904.

Abstract

Cyclodepsipeptides (CDPs) represent a huge family of chemically and structurally diverse molecules with a wide ability for molecular interactions. CDPs are cyclic peptide-related natural products made up of both proteinogenic and nonproteinogenic amino acids linked by amide and ester bonds. The combined use of different analytical methods is required to accurately determine their integral structures including stereochemistry, thus allowing deeper insights into their often-intriguing bioactivities and their possible usefulness. Our goal is to present the various methods developed to accurately characterize CDPs. Presently, Marfey's method and NMR (nuclear magnetic resonance) are still considered the best for characterizing CDP configuration. Nevertheless, electrospray-high resolution tandem mass spectrometry (ESI-HRMS/MS) is of great value for efficiently resolving CDP's composition and sequences. For instance, recent data shows that the fragmentation of cationized CDPs (e.g., [M + Li] and [M + Na]) leads to selective cleavage of ester bonds and specific cationized product ions (b series) useful to get unprecedented sequence information. Thus, after a brief presentation of their structure, biological functions, and biosynthesis, we also provide a historic overview of these various analytical approaches as well as their advantages and limitations with a special emphasis on the emergence of methods based on HRMS/MS through recent fundamental works and applications.

摘要

环缩肽(CDPs)是一个化学和结构多样的大家族,具有广泛的分子相互作用能力。CDPs是与环肽相关的天然产物,由通过酰胺键和酯键连接的蛋白质ogenic和非蛋白质ogenic氨基酸组成。需要结合使用不同的分析方法来准确确定其完整结构,包括立体化学,从而更深入地了解其常常引人入胜的生物活性及其可能的用途。我们的目标是介绍为准确表征CDPs而开发的各种方法。目前,马尔费方法和核磁共振(NMR)仍然被认为是表征CDP构型的最佳方法。然而,电喷雾高分辨率串联质谱(ESI-HRMS/MS)对于有效解析CDP的组成和序列具有重要价值。例如,最近的数据表明,阳离子化CDPs(例如,[M + Li]和[M + Na])的碎片化会导致酯键的选择性裂解以及特定的阳离子化产物离子(b系列),这些对于获得前所未有的序列信息很有用。因此,在简要介绍了它们的结构、生物学功能和生物合成之后,我们还提供了这些各种分析方法的历史概述以及它们的优缺点,并特别强调了基于HRMS/MS的方法通过最近的基础研究和应用的出现。

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