Novel automated biomarker discovery work flow for urinary peptidomics

Crina I. Balog, Paul J. Hensbergen, Rico Derks, Jaco J. Verweij, Govert J. van Dam, Birgitte J Vennervald, André M. Deelder, Oleg A. Mayboroda

    18 Citations (Scopus)

    Abstract

    Urine is potentially a rich source of peptide biomarkers, but
    reproducible, high-throughput peptidomic analysis is often hampered by the
    inherent variability in factors such as pH and salt concentration. Our goal was
    to develop a generally applicable, rapid, and robust method for screening large
    numbers of urine samples, resulting in a broad spectrum of native peptides, as a
    tool to be used for biomarker discovery. METHODS: Peptide samples were trapped,
    desalted, pH-normalized, and fractionated on a miniaturized automatic
    reverse-phase strong cation exchange (RP-SCX) cartridge system. We analyzed
    eluted peptides using MALDI-TOF, Fourier transform ion cyclotron resonance, and
    liquid chromatography-iontrap mass spectrometry. We determined qualitative and
    quantitative reproducibility of the system and robustness of the method using BSA
    digests and urine samples, and we used a selected set of urine samples from
    Schistosoma haematobium-infected individuals to evaluate clinical applicability.
    RESULTS: The automated RP-SCX sample cleanup and fractionation system exhibits a
    high qualitative and quantitative reproducibility, with both BSA standards and
    urine samples. Because of the relatively high cartridge binding capacity (1-2 mL
    urine), eluted peptides can be measured with high sensitivity using multiple mass
    spectrometric techniques. As proof of principle, hemoglobin-derived peptides were
    identified in urine samples from S. haematobium-infected individuals, even when
    the microhematuria test was negative. CONCLUSIONS: We present a practical,
    step-by-step method for screening and identification of urinary peptides.
    Alongside the analytical method evaluation on standard samples, we demonstrate
    its feasibility with actual clinical material.
    Original languageEnglish
    JournalClinical Chemistry
    Volume55
    Issue number1
    Pages (from-to)117-125
    Number of pages9
    ISSN0009-9147
    DOIs
    Publication statusPublished - 2009

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