Metabolomic profiling of cultured cancer cells

Marie Scoazec, Sylvere Durand, Alexis Chery, Lorenzo Galluzzi, Guido Kroemer

    Research output: Chapter in Book/Report/Conference proceedingChapterpeer-review

    Abstract

    Quantitative proteomics approaches have been developed - and now begin to be implemented on a high-throughput basis - to fill-in the large gap between the genomic/transcriptomic setup of (cancer) cells and their phenotypic/behavioral traits, reflecting a significant degree of posttranscriptional regulation in gene expression as well as a robust posttranslational regulation of protein function. However, proteomic profiling assays not only fail to detect labile posttranslational modifications as well as unstable protein-to-protein interactions but also are intrinsically incapable of assessing the enzymatic activity, as opposed to the mere abundance, of a given protein. Thus, determining the abundance of theoretically all the metabolites contained in a cell/tissue/organ/organism may significantly improve the informational value of proteomic approaches. Several techniques have been developed to this aim, including high-performance liquid chromatography (HPLC) coupled to quadrupole time-of-flight (Q-TOF) high-resolution mass spectrometry (HRMS). This approach is particularly advantageous for metabolomic profiling as it offers elevated accuracy and improved sensitivity. Here, we describe a simple procedure to determine the complete complement of intracellular metabolites in cultured malignant cells by HPLC coupled to Q-TOF HRMS. According to this method, (1) cells are collected and processed to minimize contaminations as well as fluctuations in their metabolic profile; (2) samples are separated by HPLC and analyzed on a Q-TOF spectrometer; and (3) data are extracted, normalized, and deconvoluted according to refined mathematical methods. This protocol constitutes a simple approach to determine the intracellular metabolomic profile of cultured cancer cells. With minimal variations (mostly related to sample collection and processing), this method is expected to provide reliable metabolomic data on a variety of cellular samples.

    Original languageEnglish
    Title of host publicationCell-wide Metabolic Alterations Associated with Malignancy
    PublisherAcademic Press Inc.
    Pages165-178
    Number of pages14
    ISBN (Print)9780128013298
    DOIs
    Publication statusPublished - 1 Jan 2014

    Publication series

    NameMethods in Enzymology
    Volume543
    ISSN (Print)0076-6879
    ISSN (Electronic)1557-7988

    Keywords

    • ATP
    • Cancer
    • Glycolysis
    • HPLC
    • Metabolomic profiling
    • Mitochondrial respiration
    • Q-TOF HRMS

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