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靶向代谢组学的承诺与陷阱。

Promises and pitfalls of untargeted metabolomics.

机构信息

Biochemical Genetics and Metabolomics Laboratory, Department of Pediatrics, University of California San Diego, 9500 Gilman Dr. La Jolla, CA, 92093-0830, USA.

出版信息

J Inherit Metab Dis. 2018 May;41(3):355-366. doi: 10.1007/s10545-017-0130-7. Epub 2018 Mar 13.

Abstract

Metabolomics is one of the newer omics fields, and has enabled researchers to complement genomic and protein level analysis of disease with both semi-quantitative and quantitative metabolite levels, which are the chemical mediators that constitute a given phenotype. Over more than a decade, methodologies have advanced for both targeted (quantification of specific analytes) as well as untargeted metabolomics (biomarker discovery and global metabolite profiling). Untargeted metabolomics is especially useful when there is no a priori metabolic hypothesis. Liquid chromatography coupled to mass spectrometry (LC-MS) has been the preferred choice for untargeted metabolomics, given the versatility in metabolite coverage and sensitivity of these instruments. Resolving and profiling many hundreds to thousands of metabolites with varying chemical properties in a biological sample presents unique challenges, or pitfalls. In this review, we address the various obstacles and corrective measures available in four major aspects associated with an untargeted metabolomics experiment: (1) experimental design, (2) pre-analytical (sample collection and preparation), (3) analytical (chromatography and detection), and (4) post-analytical (data processing).

摘要

代谢组学是新兴的组学领域之一,使研究人员能够在疾病的基因组和蛋白质水平分析的基础上,补充半定量和定量代谢物水平的分析,这些代谢物是构成特定表型的化学介质。十多年来,针对特定目标(特定分析物的定量)和非靶向代谢组学(生物标志物发现和全局代谢物分析)的方法都得到了发展。当没有先验代谢假设时,非靶向代谢组学尤其有用。鉴于这些仪器在代谢物覆盖范围和灵敏度方面的多功能性,液相色谱-质谱联用 (LC-MS) 已成为非靶向代谢组学的首选方法。在生物样本中解析和分析数以百计到数千种具有不同化学性质的代谢物具有独特的挑战或陷阱。在这篇综述中,我们讨论了与非靶向代谢组学实验相关的四个主要方面的各种障碍和纠正措施:(1)实验设计;(2) 预分析(样本收集和准备);(3)分析(色谱和检测);(4) 后分析(数据处理)。

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