Carbon-13-isotopomics and metabolomics of fatty acids from triacylglycerols: overcoming the limitations of GC-C-IRMS for short- and medium-acyl chains

IF 3.8 2区 化学 Q1 BIOCHEMICAL RESEARCH METHODS Analytical and Bioanalytical Chemistry Pub Date : 2024-08-19 DOI:10.1007/s00216-024-05479-3
Tania Mhanna, Mathilde Grand, Anne-Marie Schiphorst, Romain Le Balch, Toufic Rizk, Joseph Bejjani, Gérald S. Remaud, Illa Tea
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Abstract

Carbon-13 isotopomics of triacylglycerol (TAG) fatty acids or free fatty acids in biological matrices holds considerable potential in food authentication, forensic investigations, metabolic studies, and medical research. However, challenges arise in the isotopic analysis of short- and medium-chain (C4 to C10) fatty acid methyl esters (SMCFAMEs) through gas chromatography-combustion-isotope ratio mass spectrometry (GC-C-IRMS). The high volatility of these esters results in losses during their preparation, leading to isotopic fractionation. Moreover, the methoxy group added to acyl chains requires the correction of δ13C values, thereby increasing the uncertainty of the final results. Analyzing free fatty acids (FFAs) addresses both issues encountered with SMCFAMEs. To achieve this objective, we have developed a new protocol enabling the isotopomics of individual fatty acids (FAs) by GC-C-IRMS. The same experiment also provides the FA profile, i.e., the relative percentage of each FA in the TAG hydrolysate or its concentration in the studied matrix. The method exhibited high precision, as evidenced by the repeatability and within-lab reproducibility of results when tested on TAGs from both animal and vegetal origins. Compared to the analysis of FAMEs by GC-C-IRMS, the current procedure also brings several improvements in alignment with the principles of green analytical chemistry and green sample preparation. Thus, we present a two-in-one method for 13C-isotopomic and metabolomic biomarker quantitation within quasi-universal TAG compounds, encompassing the short- and medium-acyl chains.

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三酰甘油脂肪酸的碳-13-同位素组学和代谢组学:克服 GC-C-IRMS 对中短酰链的限制。
生物基质中三酰甘油(TAG)脂肪酸或游离脂肪酸的碳-13 同位素组学在食品鉴定、法医调查、代谢研究和医学研究方面具有相当大的潜力。然而,通过气相色谱-燃烧-同位素比质谱法(GC-C-IRMS)对中短链(C4 至 C10)脂肪酸甲酯(SMCFAMEs)进行同位素分析却面临着挑战。这些酯类的高挥发性会在制备过程中造成损失,从而导致同位素分馏。此外,酰基链上添加的甲氧基需要对 δ13C 值进行校正,从而增加了最终结果的不确定性。分析游离脂肪酸(FFAs)可以解决 SMCFAMEs 所遇到的这两个问题。为实现这一目标,我们开发了一种新的方案,可通过 GC-C-IRMS 对单个脂肪酸 (FA) 进行同位素组学分析。同一实验还提供了 FA 的概况,即每种 FA 在 TAG 水解产物中的相对百分比或其在所研究基质中的浓度。在对动物和植物来源的 TAG 进行测试时,结果的重复性和实验室内的重现性证明该方法具有很高的精确度。与采用气相色谱-电喷雾串联质谱(GC-C-IRMS)分析 FAMEs 相比,本方法在绿色分析化学和绿色样品制备原则方面也有一些改进。因此,我们提出了一种二合一方法,用于对准通用 TAG 化合物(包括短链和中链)进行 13C 同位组学和代谢组学生物标记物定量。
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来源期刊
CiteScore
8.00
自引率
4.70%
发文量
638
审稿时长
2.1 months
期刊介绍: Analytical and Bioanalytical Chemistry’s mission is the rapid publication of excellent and high-impact research articles on fundamental and applied topics of analytical and bioanalytical measurement science. Its scope is broad, and ranges from novel measurement platforms and their characterization to multidisciplinary approaches that effectively address important scientific problems. The Editors encourage submissions presenting innovative analytical research in concept, instrumentation, methods, and/or applications, including: mass spectrometry, spectroscopy, and electroanalysis; advanced separations; analytical strategies in “-omics” and imaging, bioanalysis, and sampling; miniaturized devices, medical diagnostics, sensors; analytical characterization of nano- and biomaterials; chemometrics and advanced data analysis.
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