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Metabolomics in nutritional epidemiology: identifying metabolites associated with diet and quantifying their potential to uncover diet-disease relations in populations

机译:营养流行病学中的代谢组学:确定与饮食相关的代谢物并量化其发现人群饮食与疾病关系的潜力

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摘要

>Background: Metabolomics is an emerging field with the potential to advance nutritional epidemiology; however, it has not yet been applied to large cohort studies.>Objectives: Our first aim was to identify metabolites that are biomarkers of usual dietary intake. Second, among serum metabolites correlated with diet, we evaluated metabolite reproducibility and required sample sizes to determine the potential for metabolomics in epidemiologic studies.>Design: Baseline serum from 502 participants in the Prostate, Lung, Colorectal, and Ovarian (PLCO) Cancer Screening Trial was analyzed by using ultra-high-performance liquid-phase chromatography with tandem mass spectrometry and gas chromatography–mass spectrometry. Usual intakes of 36 dietary groups were estimated by using a food-frequency questionnaire. Dietary biomarkers were identified by using partial Pearson's correlations with Bonferroni correction for multiple comparisons. Intraclass correlation coefficients (ICCs) between samples collected 1 y apart in a subset of 30 individuals were calculated to evaluate intraindividual metabolite variability.>Results: We detected 412 known metabolites. Citrus, green vegetables, red meat, shellfish, fish, peanuts, rice, butter, coffee, beer, liquor, total alcohol, and multivitamins were each correlated with at least one metabolite (P < 1.093 × 10−6; r = −0.312 to 0.398); in total, 39 dietary biomarkers were identified. Some correlations (citrus intake with stachydrine) replicated previous studies; others, such as peanuts and tryptophan betaine, were novel findings. Other strong associations included coffee (with trigonelline-N-methylnicotinate and quinate) and alcohol (with ethyl glucuronide). Intraindividual variability in metabolite levels (1-y ICCs) ranged from 0.27 to 0.89. Large, but attainable, sample sizes are required to detect associations between metabolites and disease in epidemiologic studies, further emphasizing the usefulness of metabolomics in nutritional epidemiology.>Conclusions: We identified dietary biomarkers by using metabolomics in an epidemiologic data set. Given the strength of the associations observed, we expect that some of these metabolites will be validated in future studies and later used as biomarkers in large cohorts to study diet-disease associations. The PLCO trial was registered at as .
机译:>背景:代谢组学是一个新兴的领域,具有促进营养流行病学发展的潜力; >目标:我们的首要目标是确定代谢物,这些代谢物是日常饮食摄入的生物标志物。其次,在与饮食相关的血清代谢物中,我们评估了代谢物的可重复性和所需的样本量,以确定流行病学研究中代谢组学的潜力。>设计:来自502位前列腺,肺,结肠直肠癌和通过使用超高效液相色谱-串联质谱和气相色谱-质谱联用对卵巢癌(PLCO)癌症筛查试验进行分析。使用食物频率问卷估计了36个饮食组的日常摄入量。通过使用部分皮尔逊相关性和Bonferroni校正进行多重比较,可以识别饮食生物标志物。计算30个个体的子集中间隔1年收集的样本之间的类内相关系数(ICC),以评估个体内代谢物的变异性。>结果:我们检测到412种已知代谢物。柑橘,绿色蔬菜,红肉,贝类,鱼,花生,大米,黄油,咖啡,啤酒,白酒,总酒精和多种维生素均与至少一种代谢产物相关(P <1.093×10 −6 ; r = −0.312至0.398);总共确定了39种饮食生物标志物。一些相关性(柑橘摄入量与水苏氨酸)重复了以前的研究。其他发现,如花生和色氨酸甜菜碱。其他强关联包括咖啡(与三氯萘林-N-甲基烟酸酯和奎宁酸酯)和酒精(与葡糖醛酸乙酯)。代谢物水平(1-y ICC)的个体差异在0.27至0.89之间。在流行病学研究中,需要大量但可达到的样本量来检测代谢物与疾病之间的关联,从而进一步强调代谢组学在营养流行病学中的作用。>结论:我们在流行病学数据中使用代谢组学来鉴定饮食生物标志物组。考虑到所观察到的关联的强度,我们希望其中一些代谢物将在未来的研究中得到验证,并随后在大型人群中用作研究饮食-疾病关联的生物标记。 PLCO试用版的注册网址为。

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