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Improved Mass Spectrometry Assay For Plasma Hepcidin: Detection and Characterization of a Novel Hepcidin Isoform

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  • Coby M M Laarakkers
  • Erwin T Wiegerinck
  • Siem Klaver
  • Maria Kolodziejczyk
  • Hendrik Gille
  • Andreas M Hohlbaum
  • Harold Tjalsma
  • Dorine W Swinkels

Abstract

Mass spectrometry (MS)-based assays for the quantification of the iron regulatory hormone hepcidin are pivotal to discriminate between the bioactive 25-amino acid form that can effectively block the sole iron transporter ferroportin and other naturally occurring smaller isoforms without a known role in iron metabolism. Here we describe the design, validation and use of a novel stable hepcidin-25+40 isotope as internal standard for quantification. Importantly, the relative large mass shift of 40 Da makes this isotope also suitable for easy-to-use medium resolution linear time-of-flight (TOF) platforms. As expected, implementation of hepcidin-25+40 as internal standard in our weak cation exchange (WCX) TOF MS method yielded very low inter/intra run coefficients of variation. Surprisingly, however, in samples from kidney disease patients, we detected a novel peak (m/z 2673.9) with low intensity that could be identified as hepcidin-24 and had previously remained unnoticed due to peak interference with the formerly used internal standard. Using a cell-based bioassay it was shown that synthetic hepcidin-24 was, like the -22 and -20 isoforms, a significantly less potent inducer of ferroportin degradation than hepcidin-25. During prolonged storage of plasma at room temperature, we observed that a decrease in plasma hepcidin-25 was paralleled by an increase in the levels of the hepcidin-24, -22 and -20 isoforms. This provides first evidence that all determinants for the conversion of hepcidin-25 to smaller inactive isoforms are present in the circulation, which may contribute to the functional suppression of hepcidin-25, that is significantly elevated in patients with renal impairment. The present update of our hepcidin TOF MS assay together with improved insights in the source and preparation of the internal standard, and sample stability will further improve our understanding of circulating hepcidin and pave the way towards further optimization and standardization of plasma hepcidin assays.

Suggested Citation

  • Coby M M Laarakkers & Erwin T Wiegerinck & Siem Klaver & Maria Kolodziejczyk & Hendrik Gille & Andreas M Hohlbaum & Harold Tjalsma & Dorine W Swinkels, 2013. "Improved Mass Spectrometry Assay For Plasma Hepcidin: Detection and Characterization of a Novel Hepcidin Isoform," PLOS ONE, Public Library of Science, vol. 8(10), pages 1-12, October.
    • Handle: RePEc:plo:pone00:0075518
    DOI: 10.1371/journal.pone.0075518
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    1. Valeria Santini & Domenico Girelli & Alessandro Sanna & Nicola Martinelli & Lorena Duca & Natascia Campostrini & Agostino Cortelezzi & Michela Corbella & Alberto Bosi & Gianluigi Reda & Oliviero Olivi, 2011. "Hepcidin Levels and Their Determinants in Different Types of Myelodysplastic Syndromes," PLOS ONE, Public Library of Science, vol. 6(8), pages 1-8, August.
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    Cited by:

    1. Ana B. Peinado & Victor M. Alfaro-Magallanes & Nuria Romero-Parra & Laura Barba-Moreno & Beatriz Rael & Cristina Maestre-Cascales & Miguel A. Rojo-Tirado & Eliane A. Castro & Pedro J. Benito & Carmen , 2021. "Methodological Approach of the Iron and Muscular Damage: Female Metabolism and Menstrual Cycle during Exercise Project (IronFEMME Study)," IJERPH, MDPI, vol. 18(2), pages 1-22, January.

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