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Investigation of urinary volatile organic metabolites as potential cancer biomarkers by solid-phase microextraction in combination with gas chromatography-mass spectrometry

机译:固相微萃取结合气相色谱-质谱法研究尿中挥发性有机代谢物作为潜在的癌症生物标志物

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摘要

BACKGROUND: Non-invasive diagnostic strategies aimed at identifying biomarkers of cancer are of great interest for early cancer detection. Urine is potentially a rich source of volatile organic metabolites (VOMs) that can be used as potential cancer biomarkers. Our aim was to develop a generally reliable, rapid, sensitive, and robust analytical method for screening large numbers of urine samples, resulting in a broad spectrum of native VOMs, as a tool to evaluate the potential of these metabolites in the early diagnosis of cancer. METHODS: To investigate urinary volatile metabolites as potential cancer biomarkers, urine samples from 33 cancer patients (oncological group: 14 leukaemia, 12 colorectal and 7 lymphoma) and 21 healthy (control group, cancer-free) individuals were qualitatively and quantitatively analysed. Dynamic solid-phase microextraction in headspace mode (dHS-SPME) using a carboxenpolydimethylsiloxane (CAR/PDMS) sorbent in combination with GC-qMS-based metabolomics was applied to isolate and identify the volatile metabolites. This method provides a potential non-invasive method for early cancer diagnosis as a first approach. To fulfil this objective, three important dHS-SPME experimental parameters that influence extraction efficiency (fibre coating, extraction time and temperature of sampling) were optimised using a univariate optimisation design. The highest extraction efficiency was obtained when sampling was performed at 501C for 60min using samples with high ionic strengths (17% sodium chloride, wv 1) and under agitation. RESULTS: A total of 82 volatile metabolites belonging to distinct chemical classes were identified in the control and oncological groups. Benzene derivatives, terpenoids and phenols were the most common classes for the oncological group, whereas ketones and sulphur compounds were the main classes that were isolated from the urine headspace of healthy subjects. The results demonstrate that compound concentrations were dramatically different between cancer patients and healthy volunteers. The positive rates of 16 patients among the 82 identified were found to be statistically different (Po0.05). A significant increase in the peak area of 2-methyl3-phenyl-2-propenal, p-cymene, anisole, 4-methyl-phenol and 1,2-dihydro-1,1,6-trimethyl-naphthalene in cancer patients was observed. On average, statistically significant lower abundances of dimethyl disulphide were found in cancer patients. CONCLUSIONS: Gas chromatographic peak areas were submitted to multivariate analysis (principal component analysis and supervised linear discriminant analysis) to visualise clusters within cases and to detect the volatile metabolites that are able to differentiate cancer patients from healthy individuals. Very good discrimination within cancer groups and between cancer and control groups was achieved.
机译:背景:旨在识别癌症生物标志物的非侵入性诊断策略对早期癌症检测非常感兴趣。尿液可能是挥发性有机代谢物(VOM)的丰富来源,可用作潜在的癌症生物标志物。我们的目标是开发一种普遍可靠,快速,灵敏和鲁棒的分析方法来筛查大量尿液样品,从而产生广泛的天然VOM,以此作为评估这些代谢物在癌症早期诊断中的潜力的工具。方法:为了调查尿中挥发性代谢产物作为潜在的癌症生物标志物,定性和定量分析了33例癌症患者(肿瘤组:14例白血病,12例结直肠癌和7例淋巴瘤)和21例健康人(对照组,无癌)的尿液样本。使用羧基聚二甲基硅氧烷(CAR / PDMS)吸附剂与基于GC-qMS的代谢组学相结合的顶空模式动态固相微萃取(dHS-SPME),用于分离和鉴定挥发性代谢物。这种方法提供了一种潜在的早期癌症诊断的非侵入性方法,作为第一种方法。为实现此目标,使用单变量优化设计对影响萃取效率的三个重要dHS-SPME实验参数(纤维涂层,萃取时间和采样温度)进行了优化。当使用高离子强度(17%氯化钠,wv 1)的样品在搅拌下于501℃进行60分钟采样时,可获得最高的提取效率。结果:在对照组和肿瘤学组中共鉴定出82种不同化学类别的挥发性代谢物。苯类衍生物,萜类化合物和苯酚是肿瘤学组中最常见的类别,而酮和硫化合物是从健康受试者尿液顶空分离出的主要类别。结果表明,癌症患者和健康志愿者之间的化合物浓度显着不同。发现在确定的82例患者中有16例患者的阳性率具有统计学差异(Po0.05)。观察到癌症患者的2-甲基3-苯基-2-丙烯,对苯甲基,苯甲醚,4-甲基苯酚和1,2-二氢-1,1,6-三甲基萘的峰面积显着增加。平均而言,在癌症患者中发现统计学上显着较低的二甲基二硫丰度。结论:气相色谱峰面积已提交多变量分析(主成分分析和监督线性判别分析)以可视化病例中的簇,并检测能够区分癌症患者与健康个体的挥发性代谢物。在癌症组内以及癌症和对照组之间实现了很好的区分。

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