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薄膜微萃取技术在分析A549癌细胞中挥发性代谢物的应用

Application of Thin-Film Microextraction to Analyze Volatile Metabolites in A549 Cancer Cells.

作者信息

Filipiak Wojciech, Jaroch Karol, Szeliska Paulina, Żuchowska Karolina, Bojko Barbara

机构信息

Department of Pharmacodynamics and Molecular Pharmacology, Faculty of Pharmacy, Collegium Medicum in Bydgoszcz, Nicolaus Copernicus University in Toruń, Dr. Jurasza 2 Str., 85-089 Bydgoszcz, Poland.

出版信息

Metabolites. 2021 Oct 14;11(10):704. doi: 10.3390/metabo11100704.

Abstract

Volatile organic compounds (VOCs) have been proposed in the last two decades as biomarkers for disease detection and therapeutic monitoring. Model in vitro experiments with established cell lines are fundamental to clarify whether given VOCs originate from normal human cells or pathogens, including transformed cancer cells. Due to the trace concentrations of target metabolites, adsorptive enrichment is needed before gas chromatography-mass spectrometry (GC-MS) analysis, with solid-phase microextraction (SPME) being perfectly suited for this purpose. Here, a modification of SPME, the thin-film microextraction (TFME) technique, is proposed for analysis of cellular VOCs, which utilizes a planar mesh coated with stationary phase to increase the extraction phase volume and active surface area. In this study, four different adsorbents were compared: carboxen, divinylbenzene, hydrophobic-lipophilic balanced and polydimethylsiloxane. Amongst them, HLB sheets using poly(divinylbenzene-co-N-vinyl-pyrrolidone) skeleton structure proved to be the most versatile, enabling the most sensitive analysis of VOCs with a broad polarity and volatility. For HLB, sampling type (internal static headspace, external bi-directional headspace), extraction temperature and extraction time were also examined. An established method was successfully applied to analyze metabolites produced by A549 cells revealing five volatiles at significantly higher (additionally benzaldehyde at lower) levels in cell culture medium compared to the cell-free reference medium headspace.

摘要

在过去二十年中,挥发性有机化合物(VOCs)已被提议作为疾病检测和治疗监测的生物标志物。使用已建立的细胞系进行体外模型实验,对于阐明特定VOCs是源自正常人体细胞还是病原体(包括转化的癌细胞)至关重要。由于目标代谢物的浓度极低,在气相色谱 - 质谱联用(GC-MS)分析之前需要进行吸附富集,而固相微萃取(SPME)非常适合此目的。在此,提出了一种SPME的改进方法——薄膜微萃取(TFME)技术,用于分析细胞VOCs,该技术利用涂有固定相的平面网来增加萃取相体积和活性表面积。在本研究中,比较了四种不同的吸附剂:碳分子筛、二乙烯基苯、疏水性 - 亲脂性平衡型和聚二甲基硅氧烷。其中,使用聚(二乙烯基苯 - 共 - N - 乙烯基吡咯烷酮)骨架结构的HLB片材被证明是用途最广泛的,能够对具有广泛极性和挥发性的VOCs进行最灵敏的分析。对于HLB,还研究了采样类型(内部静态顶空、外部双向顶空)、萃取温度和萃取时间。一种成熟的方法成功应用于分析A549细胞产生的代谢物,结果显示与无细胞参考培养基顶空相比,细胞培养基中五种挥发性物质的含量显著更高(另外苯甲醛含量较低)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0e46/8541397/eeb6c15a950b/metabolites-11-00704-g001.jpg

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